Refine
Is part of the Bibliography
- yes (201)
Year of publication
Document Type
- Journal article (127)
- Doctoral Thesis (73)
- Report (1)
Keywords
- melanoma (22)
- Melanom (16)
- Merkel cell carcinoma (15)
- Apoptosis (6)
- psoriasis (6)
- therapy (6)
- Allergie (5)
- PD-1 (5)
- Zellmigration (5)
- allergy (5)
- apoptosis (5)
- Invasion (4)
- cell migration (4)
- dermatology (4)
- polyomavirus (4)
- uveal melanoma (4)
- Acne inversa (3)
- Allergy (3)
- Alopecia areata (3)
- Anaphylaxis (3)
- Asthma (3)
- BRAF (3)
- Basaliom (3)
- Immuntherapie (3)
- MAP-Kinase (3)
- Medizin (3)
- Merkel-Zellkarzinom (3)
- T cells (3)
- Therapie (3)
- Tumorzelle (3)
- asthma (3)
- cell staining (3)
- children (3)
- drug adverse reaction (3)
- drug allergy (3)
- drug hypersensitivity (3)
- immune checkpoint blockade (3)
- immunohistochemistry (3)
- immunology (3)
- immunotherapy (3)
- inflammation (3)
- invasion (3)
- migration (3)
- tumor (3)
- Angiogenese (2)
- Apoptose (2)
- Autoantikörper (2)
- Autoimmunität (2)
- B-cell lymphoma (2)
- BP180 (2)
- COVID-19 (2)
- CTLA-4 (2)
- Dendritische Zelle (2)
- Dermatologie (2)
- Dynamik (2)
- Endothel (2)
- Fas-Ligand (2)
- Germany (2)
- Haut (2)
- Hautkrebs (2)
- Hidradenitis suppurativa (2)
- Human papillomavirus (2)
- Hyperhidrose (2)
- Immunologie (2)
- Immunotherapy (2)
- Integrine (2)
- Interferon (2)
- Karzinomzellen (2)
- Klinik (2)
- Krebs <Medizin> (2)
- MAPK (2)
- Melanoma (2)
- Merkel cell polyomavirus (2)
- Migration (2)
- PD-L1 (2)
- Pemphigoid (2)
- T-Lymphozyt (2)
- T-Zelle (2)
- TRAIL (2)
- TRRAP (2)
- Th17 (2)
- Zytokine (2)
- activation (2)
- anaphylaxis (2)
- angiogenesis (2)
- autoantibodies (2)
- basal cell carcinoma (2)
- bee (2)
- biologics (2)
- bullous pemphigoid (2)
- cFLIP (2)
- carcinoma cells (2)
- collective invasion (2)
- dendritic cell (2)
- diagnosis (2)
- extracellular matrix (2)
- extrazelluläre Matrix (2)
- immunosuppression (2)
- large T antigen (2)
- machine learning (2)
- mastocytosis (2)
- melanoma cells (2)
- melanomas (2)
- miRNA (2)
- mouse model (2)
- mucous membrane pemphigoid (2)
- multiple sclerosis (2)
- p53 (2)
- pemphigus (2)
- pemphigus foliaceus (2)
- pemphigus vulgaris (2)
- penicillin allergy (2)
- penicillin hypersensitivity (2)
- peptide vaccination (2)
- polymavirus (2)
- treatment resistance (2)
- trichoblastoma (2)
- urticaria (2)
- 2D (1)
- 3D (1)
- A375 (1)
- ACE inhibitor (1)
- ARCI (1)
- ARCI EM type III (1)
- Actin (1)
- Actin-Filament (1)
- Actin-bindende Proteine (1)
- Akne (1)
- Aktin (1)
- Aktivierung (1)
- Allergiediagnostik (1)
- Aminopenicilline (1)
- Anaphylaxie (1)
- Anaplasma phagocytophilum (1)
- Anaplasma phagozytophilum (1)
- Angiogenesis (1)
- Angiogenin (1)
- Antigen CD147 (1)
- Antigen CD28 (1)
- Antigen CD95 (1)
- Antigenpresentation (1)
- Antigenpräsentation (1)
- Apoptoseresistenz (1)
- Apoptosesensibilisierung (1)
- Assoziationen (1)
- Atopic Dermatitis (1)
- Atopische Dermatitis (1)
- Autoimmunity (1)
- B cells (1)
- B-cells (1)
- B7-H1 Antigen (1)
- BARF-mutated melanoma (1)
- BRAF inhibition (1)
- BRAF mutation (1)
- BRAF mutations (1)
- BRN-3A (1)
- Background Epithelioid haemangioma (1)
- Basalzellkarzinom (1)
- Basophil activation test (1)
- Bcl-2-Proteinfamilie (1)
- Becker naevus (1)
- Becker naevus syndrome (1)
- Beta-blocker (1)
- Bienengiftallergie (1)
- Bildanalyse (1)
- Biomarker (1)
- Biomechanik (1)
- Blasen bildende Autoimmundermatosen (1)
- Blasenbildung (1)
- Blutgefäß (1)
- Blutgefäßdichte (1)
- Bowen’s disease, periungual (1)
- Bronchialasthma (1)
- Bullous (1)
- Bullous pemphigoid (1)
- Bullöse Autoimmundermatosen (1)
- Bullöses Pemphigoid (1)
- CD 10 (1)
- CD10 (1)
- CD105 antigen (1)
- CD274 (1)
- CD30 (1)
- CD34 antigen (1)
- CD8(+) (1)
- COX2 expression (1)
- CRISPR (1)
- CTLA-4 Antigen (1)
- CXCL12 (1)
- CXCR$ (1)
- Ca\(^{2+}\) signalling (1)
- Calcium (1)
- Cancer Cell (1)
- Caspasen (1)
- Chemokine (1)
- Chemoresistenz (1)
- Chemosensitivity (1)
- Chemosensitivität (1)
- Clinical trials (1)
- Clobetasolpropionat (1)
- Clobetasolpropionate (1)
- Collagen VII (1)
- Contact dermatitis (1)
- Covid-19 (1)
- Crohn disease (1)
- Crosstalk (1)
- Cutaneous lymphoma (1)
- Cutaneous metastatic Crohn’s disease (1)
- Cx43 (1)
- Cytostatikum (1)
- DNA (1)
- DNA damage (1)
- DNA repair (1)
- Dapson (1)
- Dapsone (1)
- Dermato (1)
- Desmoplakin (1)
- Desmoplastisches Trichoepitheliom (1)
- Diagnose (1)
- Diagnostik (1)
- Dinitrochlorbenzene (1)
- Dinitrochlorbenzol (1)
- Diphenylcyclopropenon (1)
- Double sensitization (1)
- Drug Therapy, Combination (1)
- Drug allergy (1)
- Drug reaction (1)
- Dynamics (1)
- EBA (1)
- EBER in situ hybridization (1)
- EGR1 (1)
- ERBB receptors (1)
- ERK (1)
- EVER1 (1)
- EVER2 (1)
- Elispot (1)
- Endothelium (1)
- Endothelzellen (1)
- Enoxaparin (1)
- Entzündungsfördernde Mediatoren (1)
- Epigenetic regulation (1)
- Epigenetics (1)
- Epithel (1)
- Epitheliom (1)
- Erbgrind (1)
- Fascin (1)
- Field sting (1)
- Filtrierende Trabekulotomie (FTO) (1)
- Flt3L (1)
- Forkhead Transcription Factors (1)
- Forkhead-Box-Proteine (1)
- FoxO transcription factors (1)
- FoxO3 (1)
- G Protein (1)
- GNA11 (1)
- GNAQ (1)
- GSK3 (1)
- Gemeinschaftseinrichtung (1)
- Glaukom (1)
- Granulozyten (1)
- Grundsubstanz (1)
- HDAC (1)
- HT29 cells (1)
- HaCaT (1)
- Hair follicle (1)
- Hautinfektion (1)
- Hautklinik (1)
- Hautkrankheit (1)
- Hautlymphom (1)
- Hauttumor (1)
- Heparin (1)
- Hiperhidrosis (1)
- Hippo signaling (1)
- Histogenese (1)
- Histogenesis (1)
- Histologie (1)
- Histone deacetylase (1)
- Histopathologie (1)
- Hoden (1)
- Honey bee (1)
- Human Babesiosis (1)
- Human Granulocytic Ehrlichiosis (1)
- Humane Babesiose (1)
- Humane Granulozytäre Ehrlichiose (1)
- Hymenoptera (1)
- Hymenoptera venom (1)
- Hyperhidrosis (1)
- Hypersensitivity (1)
- Hypoxie (1)
- Hämangiom (1)
- IFN (1)
- IL-4/IL-13 inhibitor (1)
- IL‐10 (1)
- Immediate-type (1)
- Immuncytochemie (1)
- Immune Escape (1)
- Immune-related adverse event (1)
- Immunhistochemie (1)
- Immunmodulation (1)
- Immunmonitoring (1)
- Immunoadsorption (1)
- Immunoapheresis (1)
- Immunoblot (1)
- Immunoconjugate (1)
- Immunogenität (1)
- Immunoglobulin E (1)
- Immunologische Synapse (1)
- Immunology (1)
- Immunsuppression (1)
- Immuntherapie ; Hyposensibilisierung (1)
- Integrin (1)
- Interaction (1)
- Interaktion (1)
- Interleukin 13 (1)
- Interleukin 4 (1)
- Interleukin 8 (1)
- Interleukinantagonist QY (1)
- Ipilimumab (1)
- IrAEs (1)
- JAK2 (1)
- JNK (1)
- Juvenile biventricular cardiomyopathy (1)
- Kalzium (1)
- Kaposi sarcoma (1)
- Keimepithel (1)
- Keratinozyten und neutrophile Granulozyten (1)
- Keratoakant (1)
- Kerinokeratosis papulosa (1)
- Kinasen (1)
- Kinder und Jugendliche (1)
- Kollagen (1)
- Kollagen VII (1)
- Kollagenasen (1)
- Kollektive Invasion (1)
- Komorbiditäten (1)
- Konfokalmikroskop (1)
- Kontaktallergie (1)
- Kontaktdermatitis (1)
- Konventionelle Trabekulektomie (TE) (1)
- Krätze (1)
- Krüppel-like factor (1)
- Kutane Sarkome (1)
- Kutane T-Zell-Lymphome (1)
- LEEP-CAM (1)
- LIF (1)
- LRIG1 (1)
- LSD1 (1)
- LTT (1)
- Laminin 5 (1)
- Large T antigen (1)
- Lebensqualität (1)
- Leukozyt (1)
- Leukozyten (1)
- Leukozytoklastische Vaskulitis (1)
- Lipid Rafts (1)
- Lymphozytentransformationstest (1)
- Lysine-specific methylase (1)
- MAPK-Inhibitoren (1)
- MCC (1)
- MCPyV (1)
- MCV-negative (1)
- MEK5/ERK5 (1)
- MEK5/ERK5 cascade (1)
- MELANOM (1)
- MELANOMA (1)
- MHC class I chain-related protein (1)
- MICA (1)
- MICB (1)
- Malignant melanoma (1)
- Mastocytosis (1)
- Matrixmetalloproteinasen (1)
- Matrixmetalloproteinases (1)
- Matrixproteasen (1)
- Matrixumbau (1)
- Maus (1)
- Maus-Modell (1)
- Mausmodell (1)
- Melanin (1)
- Melanomzelle (1)
- Melkersson-Rosenthal-Syndrom (1)
- Merkelzellkarzinom (1)
- Metastase (1)
- Metastasierung (1)
- Metastasis (1)
- Methylprednisolon (1)
- Methylprednisolone (1)
- Minimal change disease (1)
- Molecular imaging (1)
- Morphodynamik (1)
- Mouse model (1)
- Mouse model of allergic airway inflammation (1)
- Multiphotonenmikroskopie (1)
- Mycobacterium marinum (1)
- Mycosis fungoides bullosa (1)
- Mykobakterien (1)
- Mykobakteriose (1)
- NF-kB-Inhibition (1)
- NF-kB-inhibition (1)
- NF-kappa-B (1)
- NIPAL4 (1)
- NRF2 (1)
- Nachweis von Autoantikörpern (1)
- Naevus sebaceus (1)
- Nagelmelanom (1)
- Nail unit (1)
- Narkose (1)
- Nekrose (1)
- Nfatc1 (1)
- Nivolumab (1)
- Non-steroidal anti-inflammatory drug (1)
- Nuklearfaktor (1)
- Nuklearfaktor Kappa B (1)
- Nutlin (1)
- Onkologie (1)
- Operationsverfahren bei Nagelmelanomen (1)
- Orofaziale Granulomatose (1)
- Orofazialer Bereich (1)
- P53 (1)
- PD‐L1 (1)
- PEComa (1)
- PIK3CA mutations (1)
- PRAME (1)
- PVL (1)
- Palmoplantar keratoderma (1)
- Pathologic neovascularization (1)
- Pemphigoid gestationis (1)
- Peripheral eosinophils (1)
- Pfadbildung (1)
- Pinkus-Tumor (1)
- Pityriasis lichenoides (1)
- Plastizität (1)
- Plastizität <Physiologie> (1)
- Plattenepithel (1)
- Plattenepithelcarcinom (1)
- Polyomavirus (1)
- Positron emission tomography (1)
- Priming (1)
- Primär kutanes Lymphom (1)
- Prognose (1)
- Programmed Cell Death 1 Receptor (1)
- Proliferation (1)
- Propranolol (1)
- Propranolol-Therapie (1)
- Proteaseinhibitoren (1)
- Proteasom (1)
- Pruritus (1)
- Pseudo-allergy (1)
- Qinghaosu (1)
- RIP (1)
- RNA modification (1)
- RNA probe (1)
- ROCK (1)
- Rac (1)
- Raman (1)
- Relapse (1)
- Risikofaktoren (1)
- Risk factor (1)
- S2k guidelines (1)
- SARS-CoV-2 (1)
- SERS (1)
- SIT (1)
- STAT3 (1)
- Sarkom (1)
- Schlagwort 1 Melanocyte (1)
- Schlagwort 1 Melanozyten (1)
- Schlagwort 2 MART-1 (1)
- Schlagwort 3 HMB-45 (1)
- Schlagwort 4 epithelialen Tumoren (1)
- Schlagwort 4 skin tumor (1)
- Schlagwort HMB-45 (1)
- Schleimhaut (1)
- Schleimhautpemphigoid (1)
- Schuppenflechte (1)
- Sekundärtumoren (1)
- Senescence (1)
- Sicherheit (1)
- Signaltransduktion (1)
- Skabies (1)
- Skabiesausbruch (1)
- Skin (1)
- Skin Neoplasms (1)
- Somatostatin receptor expression (1)
- Spinaliom (1)
- Staphylococcus aureus (1)
- Stevens-Johnson syndrome (1)
- Stroma (1)
- Sturge-Weber syndrom (1)
- Sunitinib (1)
- T Zell-Aktivierung (1)
- T antigen (1)
- T cell activation (1)
- T lymphocyte (1)
- T-Cells (1)
- T-Zell-Lymphom (1)
- T-Zellaktivierung (1)
- T-Zellhomöostase (1)
- T-antigen (1)
- T-antigens (1)
- T-cell (1)
- T-cell reactivity (1)
- TNF alpha (1)
- TP53 (1)
- TRAIL-Rezeptor (1)
- TRAIL-receptor (1)
- TRP2 (1)
- Targeted therapy (1)
- Therapieresistenz (1)
- Tiermodell (1)
- Tinea capitis (1)
- Tr1 (1)
- Treatment failure (1)
- Tregs (1)
- Trichoblastom (1)
- Trichoepitheliom (1)
- Trichofollikulom (1)
- Tubulin (1)
- Tumor (1)
- Tumor Immunology (1)
- Tumor-Nekrose-Faktor (1)
- Tumor-Nekrose-Faktor <alpha> (1)
- Tumornekrosefaktor (1)
- Tumorstroma (1)
- Typ-IV-Allergie (1)
- Tyrosine kinase inhibition (1)
- Unerwünschte Arzneimittelwirkung (1)
- Unerwünschte immunvermittelte Ereignisse (1)
- United States (1)
- Unterschiede (1)
- V. saphena magna (1)
- VITILIGO (1)
- Vespula (1)
- Waldarbeiter (1)
- Waxy papulosis of childhood (1)
- Werkstatt für Behinderte (1)
- Wespengiftallergie (1)
- Wirksamkeit (1)
- Wundheilung (1)
- XPA (1)
- Y-box binding protein 1 (1)
- YTHDF1 (1)
- Zell-Adhesionsmolekül (1)
- Zellfragmente (1)
- Zielgerichtete Therapie (1)
- Zweitlinientherapie (1)
- acitretin (1)
- actin (1)
- adalimumab (1)
- adhesion molecule (1)
- adjuvant treatment (1)
- advanced cutaneous squamous cell carcinoma (1)
- adverse drug reaction (1)
- adverse event (1)
- age (1)
- agranulocytosis (1)
- akt (1)
- algorithm (1)
- allergies (1)
- allotype (1)
- alopecia areata (1)
- aluminum granuloma (1)
- amoxicillin (1)
- ampicillin (1)
- anergy (1)
- angioedema (1)
- antagomiRs (1)
- anti-tumor Immunantworten (1)
- anti-tumor immune responses (1)
- antibiotic (1)
- antibody–drug conjugates (1)
- antitumor immunity (1)
- artesunate (1)
- aspirin‐exacerbated respiratory disease (1)
- at-home sampling (1)
- atherosclerosis (1)
- autoimmune blistering diseases (1)
- autoimmune bullous skin diseases (1)
- autoimmune disease (1)
- autoimmune diseases (1)
- autoimmune skin blistering disease (1)
- avelumab (1)
- benign trichogenic tumors (1)
- benigne trichogene Tumoren (1)
- biomarker (1)
- biosimilar (1)
- blasenbildende Autoimmunerkrankung (1)
- bleomicina (1)
- bleomycin (1)
- blisters (1)
- blood (1)
- blood vessel density (1)
- bone (1)
- breast cancer (1)
- brown band (1)
- buildup phase (1)
- bullae (1)
- bullöses (1)
- c-flip (1)
- cDC2 subset (1)
- cancer (1)
- cancer microenvironment (1)
- cancer patients (1)
- cancer treatment (1)
- cartilage (1)
- case report (1)
- cell cycle (1)
- cell death (1)
- cell membranes (1)
- cell rich blue nevus (1)
- cell viability testing (1)
- cell-death (1)
- cellfragments (1)
- cemiplimab (1)
- cesioflammea (1)
- checkpoint blocker (1)
- checkpoint inhibitor therapy (1)
- chemokine (1)
- chemokines (1)
- chemoresistence (1)
- children and adolescents (1)
- chromatin regulator (1)
- cicatricial pemphigoid (1)
- classification (1)
- clincal aspects (1)
- collagen (1)
- collagenases (1)
- collodion baby (1)
- combined targeted therapy (1)
- common blue nevus (1)
- communtiy facilities (1)
- comorbid diseases (1)
- comorbidity (1)
- congenital melanocytic nevi (1)
- contact allergy (1)
- conversion (1)
- copy number variations (1)
- coronavirus disease 2019 (1)
- cultured fibroplasts (1)
- cutaneous PEComa (1)
- cutaneous T-cell lymphoma and Merkel cell carcinoma (1)
- cutaneous T-cell lymphomas (1)
- cutaneous T-cell-lymphoma (1)
- cutaneous adverse events (1)
- cutaneous angiosarcoma (1)
- cutaneous lupus erythematosus (1)
- cutaneous lymphomas (1)
- cytokine (1)
- cytokine inhibitor (1)
- cytostatic drugs (1)
- dabrafenib (1)
- dapsone (1)
- dendritic cells (1)
- dendritische Zellen (1)
- dendrtic cells (1)
- dermal melanocytosis (1)
- dermatite flagelada (1)
- desmoplastic trichoepithelioma (1)
- detection of autoantibodies (1)
- differential gene expression (1)
- disease severity (1)
- domain (1)
- drug effectiveness (1)
- drug exanthema (1)
- drug monitoring (1)
- drug therapy (1)
- drug-induced liver injury (DILI) (1)
- eczematous dermatitis (1)
- efgartigimod (1)
- endemic pemphigus foliaceus (1)
- endothelial cells (1)
- endothelium (1)
- environmental factors (1)
- eosinophils (1)
- epidermis (1)
- epigenetic reader (1)
- epigenetic silencing (1)
- epitranscriptome (1)
- exanthem (1)
- experience (1)
- expression (1)
- extracellular-regulated kinase 5 (1)
- extrinsischer Signalweg (1)
- family (1)
- fatty liver disease (1)
- ferroptosis (1)
- fibroepithelio (1)
- fixed drug eruption (1)
- flagellate dermatitis (1)
- flu-like symptoms (1)
- focal adhesion (1)
- forestry workers (1)
- fumaric acid esters (1)
- functional genetics (1)
- fungos shiitake (1)
- gene induction (1)
- genetic association (1)
- germline (1)
- glycogen synthase kinase 3 (1)
- gold nanoparticles (1)
- half-life (1)
- health economics (1)
- health insurance (1)
- health-care costs (1)
- heat shock response (1)
- hemangioma (1)
- hemorrhagic (1)
- henoch-schönlein purpura (1)
- hereditary alpha-tryptasemia (1)
- hidradenitis suppurativa (1)
- high-risk Prostate Cancer (1)
- histologic findings (1)
- histological aspects (1)
- histology (1)
- histone (1)
- histone methyltransferase PRDM8 (1)
- human (1)
- human testis (1)
- hydroxy-dabrafenib (1)
- hymenoptera (1)
- hyperhidrosis (1)
- hypoplasia of fatty tissue (1)
- hypoxia (1)
- ichthyosis (1)
- immune cell infiltration (1)
- immune infiltration (1)
- immune suppression (1)
- immunmonitoring (1)
- immunoblotting analysis (1)
- immunoconjugate (1)
- immunohistochemistry techniques (1)
- immunological synapse (1)
- immunotherapeutics (1)
- improvement (1)
- in vivo (1)
- in-vitro (1)
- in-vivo (1)
- indirect costs (1)
- infantile Hämangiome (1)
- inflammation-induced tissue demage (1)
- inflammatory disease (1)
- inguinal lymph node dissection (1)
- injection site reactions (1)
- inpatients (1)
- integrin (1)
- integrins (1)
- interdisziplinäre Hämangiomsprechstunde (1)
- interferon (1)
- interferon beta (1)
- interferon-\(\beta\) (1)
- interleukin 13 (1)
- interleukin 4 (1)
- interleukin antagonist (1)
- interleukins (1)
- interview (1)
- ipilimumab (1)
- keratinocytes (1)
- keratosis (1)
- kidney cancer (1)
- knockout (1)
- kollektive Invasion (1)
- kutan (1)
- lactate dehydrogenase (1)
- laminin 332 (1)
- laminin 5 (1)
- large cell transformation (1)
- leg cramps (1)
- lesions (1)
- leukocytoclastic vasculitis (1)
- leukozytes (1)
- lichen planus (1)
- life (1)
- lipid rafts (1)
- liver metastasis (1)
- long-term outcome (1)
- lower body (1)
- lumps (1)
- lung cancer (1)
- lymphocytes (1)
- lymphoid hyperplasia (1)
- lymphoma (1)
- mRNA (1)
- mTOR (1)
- m\(^6\)A (1)
- macro-morphology (1)
- malignancy (1)
- malignant melanoma (1)
- management (1)
- matrix proteases (1)
- mechanotransduction (1)
- mediated apoptosis (1)
- medical students (1)
- melanin (1)
- melanocytes (1)
- melanocytic markers (1)
- melanom (1)
- melanoma cell (1)
- melanoma malignancy (1)
- melanoma patients (1)
- membrane proteins (1)
- membrans proteins (1)
- mental health (1)
- mepacrine (1)
- metabolic disease (1)
- metastasis (1)
- metastatic (1)
- methylation (1)
- miR-375 (1)
- micro-morphology (1)
- microRNA-221 (1)
- microvessel density (1)
- migraine (1)
- migration and invasiveness (1)
- mitochondrial DNA (1)
- mitogen-activated protein kinase (1)
- moderate (1)
- morphodynamics (1)
- mtDNA (1)
- multicenter (1)
- multiphoton microscopy (1)
- multiple myeloma (1)
- murine B16 melanoma model (1)
- murines B16 Melanommodel (1)
- mycosis fungoides (1)
- naive T-Zellen (1)
- naive t-cells (1)
- necrotic cell death (1)
- neural crest factors (1)
- neurologic disease (1)
- nivolumab (1)
- nucleotide excision repair (1)
- oesophagogastroduodenoscopy (1)
- oncodermatology (1)
- oncogene-induced senescence (1)
- orale präkanzerosen (1)
- orofacial granulomatosis (1)
- outpatients (1)
- over-the-counter drugs (1)
- oxidative Mitogenese (1)
- oxidative mitogenesis (1)
- p16 immunhistochemie (1)
- p16 immunohistology (1)
- p38 (1)
- pan-RCC (1)
- panel sequencing (1)
- passive transfer of antibodies (1)
- passiver Transfer (1)
- pathways (1)
- patient preferences (1)
- patient survival (1)
- pediatric (1)
- peginterferon bet-1a (1)
- pemphigoid (1)
- pemphigoid gestationis (1)
- perivascular epitheloid cell tumour (1)
- phakomatosis pigmentovascularis (1)
- phosphorylation (1)
- phthalazinone pyrazole (1)
- pityriasis rubra pilaris (1)
- plaque-type psoriasis (1)
- polymerase chain reaction (1)
- population pharmacokinetics (1)
- precancerous lesions (1)
- predictive marker (1)
- primary cutaneous follicular B-cell lymphoma (1)
- primary cutaneous lymphoma (1)
- primary focal hyperhidrosis (1)
- priming (1)
- primäre fokale Hyperhidrose (1)
- programmed cell death receptor-1 (1)
- programmed necrosis (1)
- proliferation (1)
- proliferations (1)
- protease inhibitors (1)
- protein kinase pathway (1)
- protein variant (1)
- pseudolymphoma (1)
- psychische Verfassung (1)
- pustular exanthema (1)
- quality of life (1)
- quinacrine (1)
- quinine (1)
- rare (1)
- re-induction (1)
- real-world data (1)
- regional recurrence (1)
- registry (1)
- regulatory T cell (1)
- renal outcome (1)
- renale Mitbeteiligung (1)
- reporter genes (1)
- resistance (1)
- response durability (1)
- responses (1)
- retinoblastoma protein (1)
- retrospektiv (1)
- review (1)
- rhabdoid differentiation (1)
- rhabdoid melanoma (1)
- risk factor (1)
- safety (1)
- satellitosis (1)
- scabies (1)
- sebaceous nevus (1)
- second-line treatment (1)
- secretion (1)
- senescence (1)
- severe acute respiratory syndrome coronavirus 2 (1)
- sex differences (1)
- sheltered workshop (1)
- shiitake dermatitis (1)
- shiitake mushrooms (1)
- shiitake-dermatite (1)
- signal inhibition (1)
- single nucleotide polymorphism (1)
- skin (1)
- skin cancer (1)
- skin carcinogenesis (1)
- skin neoplasms (1)
- skin reactions (1)
- skin squamous cell carcinoma (1)
- small interfering RNAs (1)
- smoking (1)
- somatic mutations (1)
- squamous cell (1)
- stress signaling (1)
- stroma (1)
- subtypes (1)
- suppression (1)
- suppressor cells (1)
- surgical and invasive medical procedures (1)
- survival (1)
- survivin (1)
- survivin T-cell reactivity (1)
- susceptibility (1)
- switching (1)
- systemic sclerosis (1)
- targeted sequencing (1)
- targeted therapy (1)
- tertiary lymphoid structures (1)
- tertiary lymphoid tissue (1)
- tertiäres lymphatisches Gewebe (1)
- toxic epidermal necrolysis (1)
- toxicity (1)
- trametinib (1)
- transcription factors (1)
- transcriptome (1)
- treatment options (1)
- trichoepithelioma (1)
- trichofolliculoma (1)
- trichogenic tumours (1)
- triptan (1)
- tumor immunity (1)
- tumor microenvironment (1)
- tumor necrosis factor (1)
- tumor suppressor genes (1)
- tumor-draining lymph node (1)
- tumors (1)
- tumour immunology (1)
- tumourigenesis (1)
- typ XVII Collagen (1)
- type XVII collagen (1)
- utaneous adverse events (1)
- vascular endothelial growth (1)
- vasculitis (1)
- venereology (1)
- venom (1)
- vesicles (1)
- vespula (1)
- viral carcinogenesis (1)
- virus (1)
- volumetric absorptive micro-sampling (VAMS) (1)
- wasp (1)
- wound healing (1)
- Ältere Patienten (1)
Institute
- Klinik und Poliklinik für Dermatologie, Venerologie und Allergologie (201) (remove)
Sonstige beteiligte Institutionen
EU-Project number / Contract (GA) number
- 277775 (2)
Auf dem Weg vom Primärtumor zur systemischen Metastasierung, der Haupttodesursache von Krebserkrankungen, ist die Einzelzellmigration von Tumorzellen durch dreidimensionales Bindegewebe ein entscheidender Schritt. Die vorliegende Arbeit zeigt Untersuchungen zur Tumorzellmigration und –plastizität in einem 3D-Migrationsmodell. Kleine G-Proteine kontrollieren Zytoskelettfunktionen, insbesondere Aktinpolymerisation und die Bildung von Zellprotrusionen durch Rac sowie Actomyosinkontraktion durch Rho. Durch pharmakologische Inhibitoren von Rac und dem Rho-Effektor ROCK soll deren Bedeutung für Einzelzellmigration in einem dreidimensionalen Modell und vor allem der Effekt auf Morphologie, Plastizität und Migration von Tumorzellen geklärt werden. Nach Inhibition von ROCK zeigen hochinvasive HT1080 Fibrosarkomzellen einen multipolar-dendritischen und sessilen Phänotyp. Nach Hemmung von Rac wird hingegen ein rundlicher, aber ebenfalls apolarer und sessiler Phänotyp induziert. Bei simultaner Inhibition von Rac und ROCK entstehen rundliche, apolare, sessile Zellen mit abortiven Pseudopodien. Wird das Gleichgewicht von Rac und ROCK durch konstitutive Aktivierung von ROCK gestört, so entsteht eine zweigeteilte Population, bestehend aus rundlichen Zellen, die Blebs bilden, und langgezogenen Zellen. Nach Sortierung nach ihrem ß1-Integrinexpressionsniveau zeigten Zellen mit niedriger Integrin-Expression einen rundlichen Migrationstyp mit blasenartigen dynamischen Protrusionen, während Zellen mit hoher Integrin-Expression langgezogen-mesenchymal migrierten. Somit steuern ROCK und Rac gemeinsam und zeitgleich die mesenchymale Einzelzellmigration. Während Rac Protrusion vermittelt, ist ROCK für Kontraktilität und Retraktion verantwortlich. Erst durch Koordination von Rac und Rho/ROCK entsteht somit Polarität und 3D mesenchymale Migration.
Merkel Cell Carcinoma (MCC) is a rare and highly aggressive neuroendocrine skin cancer for which no effective treatment is available. MCC represents a human cancer with the best experimental evidence for a causal role of a polyoma virus. Large T antigens (LTA) encoded by polyoma viruses are oncoproteins, which are thought to require support of cellular heat shock protein 70 (HSP70) to exert their transforming activity. Here we evaluated the capability of MAL3-101, a synthetic HSP70 inhibitor, to limit proliferation and survival of various MCC cell lines. Remarkably, MAL3-101 treatment resulted in considerable apoptosis in 5 out of 7 MCC cell lines. While this effect was not associated with the viral status of the MCC cells, quantitative mRNA expression analysis of the known HSP70 isoforms revealed a significant correlation between MAL3-101 sensitivity and HSC70 expression, the most prominent isoform in all cell lines. Moreover, MAL3-101 also exhibited in vivo antitumor activity in an MCC xenograft model suggesting that this substance or related compounds are potential therapeutics for the treatment of MCC in the future.
5.1 Immuntherapie mit vom Tumorstroma abgeleiteten Peptiden Tumore bestehen nicht nur aus Tumorzellen, sondern auch aus der sie umgebenden extrazellulären Matrix (EZM), und Stromazellen wie Fibroblasten (cancer-associated fibroblast; CAF) und Endothelzellen (tumor endothelial cell; TEC). Diese Stromazellen haben durch die Ausschüttung von Zytokinen, proteolytischen Enzymen, Wachstums- und Angiogenesefaktoren einen entscheidenden Einfluss auf die Tumorprogression. Sie unterscheiden sich von den Stromazellen der normalen Gewebe durch die Expression von sogenannten Tumorstroma-assoziierten Antigenen (TSAA). Damit sollten Therapien, die auf TSAA abzielen, universell einsetzbar und weniger anfällig gegenüber Resistenzentwicklungen (immune escape Mechanismen) sein, da Stromazellen im Gegensatz zu neoplastischen Zellen genetisch relativ stabil sind. Für eine Immuntherapie mit vom Tumorstroma abgeleiteten Peptiden wählten wir die TSAA Endoglin und Fap, welche während der Wundheilung und im Tumorstroma induziert werden. Dabei sollte überprüft werden, ob prophylaktische Vakzinierungen in C57Bl/6j Mäusen Peptid-reaktive T-Zellen induzieren können, und das Wachstum von transplantieren Grm1-transgenen Tumoren reduziert werden kann. In der Tat konnten wir sowohl bei Endoglin- als auch bei Fap Peptid vakzinierten Tieren in vivo Peptid-reaktive Lymphozyten im Blut und zu einem geringeren Anteil auch in der Milz nachweisen, welche Peptid-gepulste syngene Milzzellen lysieren konnten. Allerdings konnte in beiden Fällen keine Reduktion des Tumorwachstums gegenüber der Kontrollgruppe beobachtet werden. Bei der Fap-Peptid-vakzinierten Gruppe war das Tumorwachstum gegenüber der Kontrollgruppe sogar gesteigert. Dies könnte darauf hindeuten, dass die Induktion Fap-Peptid-reaktiver T-Zellen tumorpromovierend wirkt. Möglicherweise könnte aber durch eine Modifikation des Vakzinierungsprotokolls bzw. durch eine Kombination mit anderen Immuntherapeutika ein verbessertes Ansprechen auf eine Endoglin bzw. Fap basierte Immuntherapie erzielt werden. 5.2 Immunsuppressive Mechanismen im Grm1-transgenen Melanom-Modell Grm1-transgene Mäuse entwickeln spontan kutane Melanome. Dieses Modell erlaubte es uns in der vorliegenden Arbeit spontane Immunantworten im Laufe der Melanomentstehung zu untersuchen. Hierfür analysierten wir sowohl ex vivo als auch in vitro aus Milz und Lymphknoten gewonnene Lymphozyten von Mäusen, welche keine Tumorläsionen bzw. eine niedrige oder hohe Tumorlast aufwiesen. Dabei konnten wir ex vivo einen Anstieg der Frequenz aktivierter CD4+ und CD8+ Lymphozyten mit zunehmender Tumorlast zeigen. Bei tumortragenden Tieren exprimierten jedoch hauptsächlich CD4+ T-Zellen Aktivierungsmarker nach in vitro Stimulation. Interessanterweise waren diese Zellen tumortragender Tiere auch funktionell beeinträchtigt, was sich in einer verminderten Proliferationskapazität nach in vitro Stimulation zeigte. Weitere Analysen ergaben, dass die erhöhte Frequenz regulatorischer T Zellen bei tumortragenden Tieren ein frühes Ereignis im Laufe der Tumorentstehung ist. Gleichzeitig konnte auch ein starker Anstieg der immunsupprimierenden Zytokine Tgf-β1 und Il-10 sowohl in den Lymphknoten als auch im Tumorgewebe beobachtet werden. Dabei war die Tgf-β1-Expression sowohl im Tumor als auch im tumor-drainierenden Lymphknoten erhöht, während Il-10 im Tumor nur moderat exprimiert wurde, was eine komplexere Regulation der Il-10-Expression nahe legt. Dies bedeutet, dass in Grm1-transgenen Mäusen ähnlich wie auch bei Melanompatienten zelluläre und zytokinabhängige Mechanismen zur Tumorentstehung beitragen und dieses Modell daher geeignet ist, um präklinisch immunmodulierende Therapieansätze zu testen.
Cellular and cytokine-dependent immunosuppressive mechanisms of grm1-transgenic murine melanoma
(2012)
Grm1-transgenic mice spontaneously develop cutaneous melanoma. This model allowed us to scrutinize the generic immune responses over the course of melanoma development. To this end, lymphocytes obtained from spleens, unrelated lymph nodes and tumor-draining lymph nodes of mice with no evidence of disease, and low or high tumor burden were analyzed ex vivo and in vitro. Thereby, we could demonstrate an increase in the number of activated CD4\(^+\) and CD8+ lymphocytes in the respective organs with increasing tumor burden. However, mainly CD4\(^+\) T cells, which could constitute both T helper as well as immunosuppressive regulatory T cells, but not CD8\(^+\) T cells, expressed activation markers upon in vitro stimulation when obtained from tumor-bearing mice. Interestingly, these cells from tumor-burdened animals were also functionally hampered in their proliferative response even when subjected to strong in vitro stimulation. Further analyses revealed that the increased frequency of regulatory T cells in tumor-bearing mice is an early event present in all lymphoid organs. Additionally, expression of the immunosuppressive cytokines TGF-β1 and IL-10 became more evident with increased tumor burden. Notably, TGF-β1 is strongly expressed in both the tumor and the tumor-draining lymph node, whereas IL-10 expression is more pronounced in the lymph node, suggesting a more complex regulation of IL-10. Thus, similar to the situation in melanoma patients, both cytokines as well as cellular immune escape mechanisms seem to contribute to the observed immunosuppressed state of tumor-bearing grm1-transgenic mice, suggesting that this model is suitable for preclinical testing of immunomodulatory therapeutics.
Pro-migratory signals mediated by the tumor microenvironment contribute to the cancer progression cascade, including invasion, metastasis and resistance to therapy. Derived from in vitro studies, isolated molecular steps of cancer invasion programs have been identified but their integration into the tumor microenvironment and suitability as molecular targets remain elusive. The purpose of the study was to visualize central aspects of tumor progression, including proliferation, survival and invasion by real-time intravital microscopy. The specific aims were to monitor the kinetics, mode, adhesion and chemoattraction mechanisms of tumor cell invasion, the involved guidance structures, and the response of invasion zones to anti-cancer therapy. To reach deeper tumor regions by optical imaging with subcellular resolution, near-infrared and infrared excited multiphoton microscopy was combined with a modified dorsal skinfold chamber model. Implanted HT-1080 fibrosarcoma and B16/F10 and MV3 melanoma tumors developed zones of invasive growth consisting of collective invasion strands that retained cell-cell contacts and high mitotic activity while invading at velocities of up to 200 μm per day. Collective invasion occurred predominantly along preexisting tissue structures, including blood and lymph vessels, collagen fibers and muscle strands of the deep dermis, and was thereby insensitive to RNAi based knockdown and/or antibody-based treatment against β1 and β3 integrins, chemokine (SDF-1/CXCL12) and growth factor (EGF) signaling. Therapeutic hypofractionated irradiation induced partial to complete regression of the tumor main mass, yet failed to eradicate the collective invasion strands, suggesting a microenvironmentally privileged niche. Whereas no radiosensitization was achieved by interference with EGFR or doxorubicin, the simultaneous inhibition of β1 and β3 integrins impaired cell proliferation and survival in spontaneously growing tumors and strongly enhanced the radiation response up to complete eradication of both main tumor and invasion strands. In conclusion, collective invasion in vivo is a robust process which follows preexisting tissue structures and is mainly independent of established adhesion and chemoattractant signaling. Due to its altered biological response to irradiation, collective invasion strands represent a microenvironmentally controlled and clinically relevant resistance niche to therapy. Therefore supportive regimens, such as anoikisinduction by anti-integrin therapy, may serve to enhance radio- and chemoefficacy and complement classical treatment regimens.
Background: There is much evidence that T cells are strongly involved in the pathogenesis of localized and systemic forms of scleroderma (SSc). A dysbalance between FoxP3+ regulatory CD4+ T cells (Tregs) and inflammatory T-helper (Th) 17 cells has been suggested. Methods: The study aimed (1) to investigate the phenotypical and functional characteristics of Th17 and Tregs in SSc patients depending on disease manifestation (limited vs. diffuse cutaneous SSc, dcSSc) and activity, and (2) the transcriptional level and methylation status of Th17- and Treg-specific transcription factors. Results: There was a concurrent accumulation of circulating peripheral IL-17-producing CCR6+ Th cells and FoxP3+ Tregs in patients with dcSSc. At the transcriptional level, Th17- and Treg-associated transcription factors were elevated in SSc. A strong association with high circulating Th17 and Tregs was seen with early, active, and severe disease presentation. However, a diminished suppressive function on autologous lymphocytes was found in SSc-derived Tregs. Significant relative hypermethylation was seen at the gene level for RORC1 and RORC2 in SSc, particularly in patients with high inflammatory activity. Conclusions: Besides the high transcriptional activity of T cells, attributed to Treg or Th17 phenotype, in active SSc disease, Tregs may be insufficient to produce high amounts of IL-10 or to control proliferative activity of effector T cells in SSc. Our results suggest a high plasticity of Tregs strongly associated with the Th17 phenotype. Future directions may focus on enhancing Treg functions and stabilization of the Treg phenotype.
NFATc1 supports imiquimod-induced skin inflammation by suppressing IL-10 synthesis in B cells
(2016)
Epicutaneous application of Aldara cream containing the TLR7 agonist imiquimod (IMQ) to mice induces skin inflammation that exhibits many aspects of psoriasis, an inflammatory human skin disease. Here we show that mice depleted of B cells or bearing interleukin (IL)-10-deficient B cells show a fulminant inflammation upon IMQ exposure, whereas ablation of NFATc1 in B cells results in a suppression of Aldara-induced inflammation. In vitro, IMQ induces the proliferation and IL-10 expression by B cells that is blocked by BCR signals inducing NFATc1. By binding to HDAC1, a transcriptional repressor, and to an intronic site of the Il10 gene, NFATc1 suppresses IL-10 expression that dampens the production of tumour necrosis factor-α and IL-17 by T cells. These data indicate a close link between NFATc1 and IL-10 expression in B cells and suggest NFATc1 and, in particular, its inducible short isoform, NFATc1/αA, as a potential target to treat human psoriasis.
Die vorliegende Arbeit zeigt eine Möglichkeit auf, die bisher meist erfolglose Chemotherapie des malignen Melanoms zu verbessern: Durch Inhibition des Transkriptionsfaktors NF-kB, der für die Regulation vieler tumorrelevanter Gene verantwortlich ist, konnten die Tumorzellen gegenüber der Wirkung von Zytostatika sensibilisiert werden. Zunächst wurden acht verschiedene Melanomzellen in Bezug auf ihre NF-kB-Aktivität und der Expression NF-kB-regulierter Proteine vergleichen. Es konnte gezeigt werden, dass die Mehrzahl der Melanomzellen über konstitutive Aktivität von NF-κB verfügt. Dabei bestand kein eindeutiger Zusammenhang zwischen der Expression NF-kB-regulierter Proteine und der Aktivität dieses Transkriptionsfaktors im Kern, was komplexe Regulationsmechanismen bei der Transkription und Translation vermuten lässt. Anhand einer ausgewählten Melanomzelllinie konnte gezeigt werden, dass zwei verschiedene NF-kB-Inhibitoren, der Proteasom-Inhibitor Bortezomib und der neue IKK-Inhibitor KINK-1 die Aktivität von NF-kB deutlich hemmen. Beim Vergleich beider NF-kB-Inhibitoren ließen sich unerwartet verschiedene molekulare Wirkungsmechanismen nachweisen: Während Bortezomib konzentrationsabhängig eine sehr starke Induktion von NOXA, eine Induktion von p53 sowie eine Abnahme von Cyclin D1 bewirkte, zeigte KINK-1 seine Effekte vor allem in der Reduktion von Chemokinen wie IL-8 und MCP-1. Passend zur Veränderung der Expression zellzyklus-relevanter Proteine hatte Bortezomib einen stärkeren Effekt auf den Zellzyklus als KINK-1. Beide Inhibitoren wurden mit verschiedenen Zytostatika kombiniert und konnten einerseits die Apoptoseinduktion durch Zytostatika verstärken und andererseits die durch Zytostatika reduzierte Invasion weiter reduzieren. Allerdings zeigte sich bei der Untersuchung tumorrelevanter Chemokine, dass KINK-1 im Gegensatz zu Bortezomib synergistische Effekte mit Camptothecin und Doxorubicin aufweist. Trotz molekularer Unterschiede bewirkten beide NF-kB-Inhibitoren vergleichbare funktionelle Effekte auf zellulärer Ebene. Dies galt auch für ein präklinisches in-vivo-Modell, in dem die experimentelle Lungenmetastasierung von B16F10-Melanomzellen in Mäusen ermittelt wurde: Hier wurden die Mäuse mit Camptothecin, KINK-1 und Bortezomib allein im Vergleich zu den jeweiligen Kombinationen aus Zytostatikum und NF-kB-Inhibitor behandelt. Beide Kombinationen zeigten eine signifikante Reduktion des Lungengewichts im Vergleich zu Camptothecin allein. Diese Arbeit konnte also den Nutzen aus NF-kB-Inhibition in Kombination mit Zytostatika für die hier verwendeten Substanzen bekräftigen und dabei einige molekulare Unterschiede aufdecken.
Heparins are one of the most used class of anticoagulants in daily clinical practice. Despite their widespread application immune-mediated hypersensitivity reactions to heparins are rare. Among these, the delayed-type reactions to s.c. injected heparins are well-known usually presenting as circumscribed eczematous plaques at the injection sites. In contrast, potentially life-threatening systemic immediate-type anaphylactic reactions to heparins are extremely rare. Recently, some cases of non-allergic anaphylaxis could be attributed to undesirable heparin contaminants.
A 43-year-old patient developed severe anaphylaxis symptoms within 5–10 minutes after s.c. injection of enoxaparin. Titrated skin prick testing with wheal and flare responses up to an enoxaparin dilution of 1:10.000 indicated a probable allergic mechanism of the enoxaparin-induced anaphylaxis. The basophil activation test as an additional in-vitro test method was negative. Furthermore, skin prick testing showed rather broad cross-reactivity among different heparin preparations tested.
In the presented case, history, symptoms, and results of skin testing strongly suggested an IgE-mediated allergic hypersensitivity against different heparins. Therefore, as safe alternative anticoagulants the patient could receive beneath coumarins the hirudins or direct thrombin inhibitors. Because these compounds have a completely different molecular structure compared with the heparin-polysaccharides.
Autosomal recessive congenital ichthyosis (ARCI) belongs to a heterogeneous group of disorders of keratinization. To date, 10 genes have been identified to be causative for ARCI. NIPAL4 (Nipa‐Like Domain‐Containing 4) is the second most commonly mutated gene in ARCI. In this study, we present a large cohort of 101 families affected with ARCI carrying mutations in NIPAL4. We identified 16 novel mutations and increase the total number of pathogenic mutations in NIPAL4 to 34. Ultrastructural analysis of biopsies from six patients showed morphological abnormalities consistent with an ARCI EM type III. One patient with a homozygous splice site mutation, which leads to a loss of NIPAL4 mRNA, showed additional ultrastructural aberrations together with a more severe clinical phenotype. Our study gives insights into the frequency of mutations, a potential hot spot for mutations, and genotype–phenotype correlations.
Defects in DNA repair pathways have been associated with an improved response to immune checkpoint inhibition (ICI). In particular, patients with the nucleotide excision repair (NER) defect disease Xeroderma pigmentosum (XP) responded impressively well to ICI treatment. Recently, in melanoma patients, pretherapeutic XP gene expression was predictive for anti-programmed cell death-1 (PD-1) ICI response. The underlying mechanisms of this finding are still to be revealed. Therefore, we used CRISPR/Cas9 to disrupt XPA in A375 melanoma cells. The resulting subclonal cell lines were investigated by Sanger sequencing. Based on their genetic sequence, candidates from XPA exon 1 and 2 were selected and further analyzed by immunoblotting, immunofluorescence, HCR and MTT assays. In XPA exon 1, we established a homozygous (c.19delG; p.A7Lfs*8) and a compound heterozygous (c.19delG/c.19_20insG; p.A7Lfs*8/p.A7Gfs*55) cell line. In XPA exon 2, we generated a compound heterozygous mutated cell line (c.206_208delTTG/c.208_209delGA; p.I69_D70delinsN/p.D70Hfs*31). The better performance of the homozygous than the heterozygous mutated exon 1 cells in DNA damage repair (HCR) and post-UV-C cell survival (MTT), was associated with the expression of a novel XPA protein variant. The results of our study serve as the fundamental basis for the investigation of the immunological consequences of XPA disruption in melanoma.
OBJECTIVE:
To demonstrate the role of angiogenesis in the progression of cutaneous squamous cell carcinoma.
INTRODUCTION:
Angiogenesis is a pivotal phenomenon in carcinogenesis. Its time course in cutaneous squamous cell carcinoma has not yet been fully established.
METHODS:
We studied the vascular bed in 29 solar keratoses, 30 superficially invasive squamous cell carcinomas and 30 invasive squamous cell carcinomas. The Chalkley method was used to quantify the microvascular area by comparing panendothelial (CD34) with neoangiogenesis (CD105) immunohistochemical markers. The vascular bed from non-neoplastic adjacent skin was evaluated in 8 solar keratoses, 10 superficially invasive squamous cell carcinomas and 10 invasive squamous cell carcinomas.
RESULTS:
The microvascular area in CD105-stained specimens significantly increased in parallel with cutaneous squamous cell carcinoma progression. However, no differences between groups were found in CD34 sections. Solar keratosis, superficially invasive squamous cell carcinoma and invasive squamous cell carcinoma samples showed significant increases in microvascular area for both CD34- and CD105-stained specimens compared with the respective adjacent skin.
DISCUSSION:
The angiogenic switch occurs early in the development of cutaneous squamous cell carcinoma, and the rate of neovascularization is parallel to tumor progression. In contrast to panendothelial markers, CD105 use allows a dynamic evaluation of tumor angiogenesis.
CONCLUSION:
This study demonstrated the dependence of skin carcinogenesis on angiogenesis.
Background: Kerinokeratosis papulosa (KP) is considered an extremely rare genodermatosis presenting usually as waxy papules on the trunk in childhood.
Objective: To describe and analyze the clinical, histological and potential etiopathological aspects of KP.
Methods: The dermatoscopic features of a new case of KP of childhood are investigated. The presence of human papillomavirus (HPV) DNA in lesional skin was studied by polymerase chain reaction. Furthermore, all cases of KP of childhood reported so far were reviewed.
Results: As a diagnostic tool, we describe for the first time a dermatoscopic feature, namely a cribriform pattern of KP, in an 11-year-old boy. In addition, we detected HPV (type 57) in his KP lesions.
Conclusions: Dermatoscopic examination might be a useful tool to distinguish KP from other skin lesions, e.g. common warts. The detection of HPV type 57 might hint to an etiological role of HPV for KP.
Background:
Inguinal lymph node dissection (LND) is a surgical procedure with a high morbidity rate. Variations in surgical procedure, such as sparing of the saphenous vein, have been proposed to reduce surgical morbidity. While sparing of the saphenous vein has shown promising results in earlier studies, data for this procedure in melanoma patients are rare. In this retrospective study, we report 10-year findings on the effects of saphenous vein-sparing LND on surgical morbidity and oncologic outcomes in melanoma patients.
Methods:
A retrospective analysis of melanoma patients receiving inguinal LND in our facility between 2003 and 2013 was performed. Patients were divided into two groups: the saphenous vein resection group and the vein sparing group. Surgical morbidity, including wound infection, lymphatic fistula, severe bleeding, neurological complications, and chronic lymphedema, as well as regional recurrence-free survival were investigated.
Results:
A total of 106 patients were included in this study; of these, the saphenous vein was spared in 41 patients (38.7%). The rate of lymphatic fistula was 51.6 vs. 48.8%, wound infection occurred in 31.3 vs. 24.4%, and patients suffered from chronic lymphedema in 30.0 vs. 26.5% in V. saphena magna resection vs. sparing group. Differences observed, however, were not significant. No difference in regional recurrence-free survival between the two study groups was detected.
Conclusions:
The results of our retrospective analysis could not confirm the promising results reported in earlier studies. Thus, sparing of the saphenous vein appears to be optional.
Background
Therapeutic vaccination directed to induce an anti-tumoral T-cell response is a field of extensive investigation in the treatment of melanoma. However, many vaccination trials in melanoma failed to demonstrate a correlation between the vaccine-specific immune response and therapy outcome. This has been mainly attributed to immune escape by antigen loss, rendering us in the need of new vaccination targets.
Patients and methods
This phase-II trial investigated a peptide vaccination against survivin, an oncogenic inhibitor-of-apoptosis protein crucial for the survival of tumor cells, in HLA-A1/-A2/-B35-positive patients with treatment-refractory stage-IV metastatic melanoma. The study endpoints were survivin-specific T-cell reactivity (SSTR), safety, response, and survival (OS).
Results
Sixty-one patients (ITT) received vaccination therapy using three different regimens. 55 patients (PP) were evaluable for response and survival, and 41/55 for SSTR. Patients achieving progression arrest (CR + PR + SD) more often showed SSTRs than patients with disease progression (p = 0.0008). Patients presenting SSTRs revealed a prolonged OS (median 19.6 vs. 8.6 months; p = 0.0077); multivariate analysis demonstrated SSTR as an independent predictor of survival (p = 0.013). The induction of SSTRs was associated with gender (female vs. male; p = 0.014) and disease stage (M1a/b vs. M1c; p = 0.010), but not with patient age, HLA type, performance status, or vaccination regimen.
Conclusion
Survivin-specific T-cell reactivities strongly correlate with tumor response and patient survival, indicating that vaccination with survivin-derived peptides is a promising treatment strategy in melanoma.
Background
Therapeutic vaccination directed to induce an anti-tumoral T-cell response is a field of extensive investigation in the treatment of melanoma. However, many vaccination trials in melanoma failed to demonstrate a correlation between the vaccine-specific immune response and therapy outcome. This has been mainly attributed to immune escape by antigen loss, rendering us in the need of new vaccination targets.
Patients and methods
This phase-II trial investigated a peptide vaccination against survivin, an oncogenic inhibitor-of-apoptosis protein crucial for the survival of tumor cells, in HLA-A1/-A2/-B35-positive patients with treatment-refractory stage-IV metastatic melanoma. The study endpoints were survivin-specific T-cell reactivity (SSTR), safety, response, and survival (OS).
Results
Sixty-one patients (ITT) received vaccination therapy using three different regimens. 55 patients (PP) were evaluable for response and survival, and 41/55 for SSTR. Patients achieving progression arrest (CR + PR + SD) more often showed SSTRs than patients with disease progression (p = 0.0008). Patients presenting SSTRs revealed a prolonged OS (median 19.6 vs. 8.6 months; p = 0.0077); multivariate analysis demonstrated SSTR as an independent predictor of survival (p = 0.013). The induction of SSTRs was associated with gender (female vs. male; p = 0.014) and disease stage (M1a/b vs. M1c; p = 0.010), but not with patient age, HLA type, performance status, or vaccination regimen.
Conclusion
Survivin-specific T-cell reactivities strongly correlate with tumor response and patient survival, indicating that vaccination with survivin-derived peptides is a promising treatment strategy in melanoma.
46 Patienten, davon 15 Melanompatienten mit erworbenen Hypopigmentierungen und 31 Patienten mit typischer Vitiligo, wurden klinisch und histologisch untersucht, mit dem Ziel, Gemeinsamkeiten und Unterschiede der beiden Erkrankungen zu erkennen. Untersucht wurden ferner assoziierte Erkrankungen wie Atopie und Autoimmunkrankheiten in Eigen- und Familienanamnese. Daneben erfolgten HLA-Typisierungen und Autoantikörpernachweise. Routinehistologisch und immunhistologisch unterscheiden sich beide Vitiligoformen nicht. Unterschiede fanden sich im Ausbreitungstyp. Während die Vitiligo häufig akral begann und sich zentripetal ausbreitete, fand sich die Melanom-assoziierte-Hypopigmentierung (MAH) primär häufig am Stamm, auch in der Umgebung des Primärmelanoms oder der Metastasen und breitete sich teilweise zentrifugal aus. In der Vitiligogruppe überwogen Frauen (77%), bei den MAH-Patienten war die Geschlechterverteilung etwa ausgeglichen. Die Melanompatienten waren signifikant älter als die Patienten mit klassischer Vitiligo. Bei drei Melanompatienten trat die Hypopigmentierung vor der Melanomdiagnose auf, eine 38-jährige Melanompatientin hatte bereits in der Kindheit eine Vitiligo. Eine positive Familienanamnese bezüglich Vitiligo fand sich bei 13 Vitiligopatienten und bei einer Patientin mit MAH. Die Familienanamnese für Atopie war bei 15 Vitiligopatienten (knapp 50 %), in der MAH-Gruppe nur in zwei Fällen positiv. Eigen- und Familienanamnese für Autoimmunerkrankungen waren in der Vitiligogruppe signifikant häufiger als im MAH-Kollektiv; auch ein positiver Antikörpernachweis war wesentlich häufiger in der Patientengruppe mit klassischer Vitiligo als bei den MAH-Patienten. Bei zehn MAH-Patienten und 30 Vitiligopatienten wurden HLA-Typisierungen durchgeführt. Ein signifikanter Unterschied fand sich bei HLA-A2. Die MAH-Patienten schienen trotz makroskopischer Metastasierung in zehn Fällen eine ungewöhnlich lange Lebensdauer zu haben. (Median neun Jahre) Zusammenfassung: Die Melanom-assoziierte-Hypopigmentierung zeigt klinische Unterschiede zur klassischen Vitiligo. Ob eine klassische Vitiligo einen Schutzfaktor für eine Melanomerkrankung darstellt, muss durch größere Studien geklärt werden.
Merkel cell carcinoma (MCC) is an aggressive, virus-associated, neuroendocrine tumor of the skin mainly affecting immunocompromised patients. Higher intratumoral infiltration with CD3 and CD8 positive T-cells is associated with a better prognosis, highlighting the relevance of the immune system for MCC development and progression. In this study 21 primary MCCs were stained with immune cell markers including CD3, CD4, CD8, CD68, CD20, and S100. Furthermore, tumor-infiltrating neutrophils, tertiary lymphoid structures and PD-L1 expression were analyzed and correlated with overall and recurrence free survival. All MCCs were Merkel Cell Polyomavirus positive. Overall and recurrence-free survival did not correlate with intra-and peritumoral CD3 and CD8 T-cell infiltration. In addition, no significant association regarding prognosis was found for tumor-associated neutrophils, tumor-associated macrophages or PD-L1 positivity in MCCs. Interestingly, the presence of tertiary lymphoid structures (TLS) in the tumor microenvironment significantly correlated with recurrence-free survival (P=0.025). In addition, TLS were significantly associated with a higher CD8/CD4 ratio in the tumor periphery (P=0.032), but not in the center of the tumor (P > 0.999). These results demonstrate for the first time that TLS, easily assessed in paraffin-embedded tissue in the tumor periphery of MCCs, may be a valuable prognostic factor indicating prolonged recurrence free survival.
Treatment of recalcitrant cutaneous lupus erythematosus (CLE) is challenging. In situations where conventional treatment approaches fail mepacrine - an antimalarial/antiinfiammatory drug that has fallen into oblivion in the last decades might still be a promising option. We retrospectively analysed medical records of 10 patients with refractory CLE that were treated with mepacrine (100-200 mg/day) as mono- or combination therapy for various time intervals between 2001 and 2013 at the University Hospital Wurzburg. Mepacrine was generally well tolerated. Side effects were mild and usually resolved after reduction or cessation. Over 50% of the patients experienced amelioration of their symptoms despite a previously recalcitrant clinical course. Altogether, our data demonstrate that mepacrine still remains a useful and effective therapeutic option for otherwise treatment-resistant CLE.
Oesophageal involvement in mucous membrane pemphigoid is considered rare, but it may be underdiagnosed. To assess the incidence of oesophageal involvement in a group of patients with newly diagnosed mucous membrane pemphigoid we retrospectively analysed the medical records of 30 consecutive patients with mucous membrane pemphigoid diagnosed between 2006 and 2016 at the Department of Dermatology, University Hospital Würzburg. Twenty-one patients (70%) reported symptoms indicative of oesophageal mucous membrane pemphigoid. Twelve patients (40%) underwent oesophagogastroduodenoscopy, and oesophageal pathology compatible with mucous membrane pemphigoid was endoscopically found in 9 cases (30%). In all patients indirect and direct immunofluorescence were performed. Patients with and without oesophageal involvement did not differ with regard to the results of indirect immunofluorescence on salt-split human skin and monkey oesophagus. Study results demonstrate the necessity of a standardized diagnostic work-up, including adequate tissue samples for direct immunofluorescence, to prevent underdiagnosis of oesophageal mucous membrane pemphigoid.
Die vorliegende Arbeit analysiert retrospektiv die funktionellen Beeinträchtigungen und Einschränkungen der Lebensqualität von Kindern und Jugendlichen mit primärer fokaler Hyperhidrose.
Grundlage der vorliegenden Untersuchung bildeten ein selbst entworfener Fragebogen sowie die Auswertung der Ambulanzkarten von 35 Kindern und Jugendlichen mit primärer fokaler Hyperhidrose im Alter von unter 18 Jahren, die sich im Zeitraum von Januar 2000 bis Dezember 2009 in der Hyperhidrose-Sprechstunde der Hautklinik des Universitätsklinikums Würzburg vorstellten. Die vorliegende Arbeit spezifiziert die täglichen Einschränkungen, welche die Kinder und Jugendlichen erleben. Für zwei Drittel der Patienten war das Schwitzen nach Maßgabe der Hyperhidrosis Disease Severity Scale kaum zu ertragen oder unerträglich und beeinträchtige häufig oder immer die täglichen Aktivitäten. Zwei Drittel der Patienten gaben an, derart stark unter der Krankheit zu leiden, dass sie ihre Lebensweise der Krankheit anpassten. Weiter konnte gezeigt werden, dass die Einschränkungen ähnlich gravierend sind wie bei Erwachsenen und anderen Dermatosen in der Kindheit. Die psychische und soziale Entwicklung kann bei einigen Betroffenen nachhaltig beeinträchtigt werden, was sich auch auf das spätere Leben auswirken kann. Diese Erkenntnis ist wichtig, um eine frühzeitige Diagnose und adäquate Behandlung voranzutreiben.
Neoplasms of the skin represent the most frequent tumors worldwide; fortunately, most of them are benign or semi-malignant and well treatable. However, the two most aggressive and deadly forms of malignant skin-neoplasms are melanoma and Merkel cell carcinoma (MCC), being responsible for more than 90% of skin-cancer related deaths. The last decade has yielded enormous progress in melanoma therapy with the advent of targeted therapies, like BRAF or MEK inhibitors, and immune-stimulating therapies, using checkpoint antibodies targeting CTLA- 4, PD-1 or PD-L1. Very recent studies suggest that also MCC patients benefit from a treatment with checkpoint antibodies. Nevertheless, in an advanced metastatic stage, a cure for both of these aggressive malignancies is still hard to achieve: while only a subset of patients experience durable benefit from the immune-based therapies, the widely applicable targeted therapies struggle with development of resistances that inevitably occur in most patients, and finally lead to their death. The four articles included in this thesis addressed current questions concerning therapy and carcinogenesis of melanoma and MCC. Moreover, they are discussed in the light of the up-to-date research regarding targeted and immune-based therapies. In article I we demonstrated that besides apoptosis, MAPK pathway inhibition in BRAF-mutated melanoma cells also induces senescence, a permanent cell cycle arrest. These cells may provide a source for relapse, as even permanently arrested cancer cells can contribute to a pro-tumorigenic milieu. To identify molecular factors determining the differential response, we established M14 melanoma cell line derived single cell clones that either undergo cell death or arrest when treated with BRAF/MEK inhibitors. Using these single cell clones, we demonstrated in article IV that downregulation of the pro-apoptotic BH3-only protein BIK via epigenetic silencing is involved in apoptosis deficiency, which can be overcome by HDAC inhibitors. These observations provide a possible explanation for the lack of a complete and durable response to MAPK inhibitor treatment in melanoma patients, and suggest the application of HDAC inhibitors as a complimentary therapy to MAPK pathway inhibition. Concerning MCC, we scrutinized the interactions between the Merkel cell polyomavirus’ (MCV) T antigens (TA) and the tumor suppressors p53 and Rb in article II and III, respectively. In article III, we demonstrated that the cell cycle master regulator Rb is the crucial target of MCV large T (LT), while it - in contrast to other polyomavirus LTs - exhibits much lower affinity to the related proteins p107 and p130. Knockdown of MCV LT led to proliferation arrest in MCC cells, which can be rescued by knockdown of Rb, but not by knockdown of p107 and p130. Contrary to Rb, restriction of p53 in MCC seems to be independent of the MCV TAs, as we demonstrated in article II. In conclusion, the presented thesis has revealed new molecular details, regarding the response of melanoma cells towards an important treatment modality and the mechanisms of viral carcinogenesis in MCC.
Hintergrund:Die Aktivierung naiver T-Zellen ist Folge eines Kontaktes zu Antigen präsentierenden Zellen (APC), die auf ihrer Oberfläche Antigene im MHC-Peptid-Komplex präsentieren. Bisherige Daten zur Kontaktdauer und -dynamik sowie zur nachfolgenden Aktivierung und Proliferation naiver T-Zellen beruhen meist auf Ergebnissen von Experimenten, die in Flüssigkulturmodellen gemacht wurden. Aus diesen resultierte die Beschreibung des sog. statischen Interaktionskonzeptes. Die T-Zell-Aktivierung wird überwiegend als Folge eines einzelnen lang dauernden und statischen Kontaktes zwischen T-Zelle und APC beschrieben (single encounter model), der zu einer kontinuierlichen Stimulation des T-Zell-Rezeptors über mehrere Stunden führt. Dem gegenüber steht das Konzept dynamischer Interaktionen, in dem T-Zell-Aktivierung und -Proliferation als Folge dynamischer, kurz dauernder und sequentieller Kontakte zu einer oder zu verschiedenen DC beschrieben werden (serielles Kontaktmodell). Methode: Da Flüssigkeitskulturen jedoch nicht annähernd das dreidimensionale Netzwerk lymphatischer Organe widerspiegeln, in dem der Kontakt zwischen T-Zellen und APC in vivo stattfindet, sollten in der vorliegenden Arbeit naive T-Zellen und dendritische Zellen (DC) in einer dreidimensionalen (3D) Umgebung kokultiviert und auf Interaktionsdynamik und Mitoseaktivität untersucht werden. Im Verlauf der oxidativen Mitogenese mit autologen DC in einer 3D Kollagenmatrix über 56 Stunden wurden humane naive T-Zellen auf Dauer und Dynamik der Zell-Zell-Interaktionen videomikroskopisch sowie die nachfolgende Aktivierung und Proliferation mittels Durchflusszytometrie untersucht. Ergebnisse: Sowohl während der Oxidativen Mitogenese als auch in nicht stimulierten Kontrollkulturen wurden bei naiven T-Zellen fast ausschließlich kurz dauernde, wenige Minuten anhaltende Kontakte zwischen T-Zellen und DC beobachtet. Die mediane Dauer der Kontakte der Kontroll-T-Zellen zu DC war dagegen während aller Beobachtungsintervalle kürzer als die der naiven T-Zellen unter Oxidative Mitogenese-Bedingungen. Es ergaben sich in der Gesamtpopulation der naiven T-Zellen in allen Beobachtungszeiträumen signifikante Unterschiede bezüglich der medianen Interaktionszeiten unter Oxidative Mitogenese-Bedingungen und Kontrollbedingungen Die mediane Interaktionszeit unter Oxidative Mitogenese-Bedingungen lag in allen Beobachtungszeiträumen bei über fünf bis zehn Minuten, unter Kontrollbedingungen jeweils zwischen drei und sechs Minuten (p jeweils < 0,001). Lediglich in der Gruppe der anfangs DC adhärenten T-Zellen nach 24 – 32 Stunden konnten keine signifikanten Unterschiede bezüglich der Dauer der Kontakte festgestellt werden (p = 0,461). Sowohl die Oxidative Mitogenese - wie auch die Kontrollkulturen zeigten nahezu ausschließlich dynamische und serielle Kontakte zu DC, multizelluläre Aggregate und statische Kontakte traten dagegen nur sehr selten auf. Infolge der Oxidativen Mitogenese, nicht jedoch in Kontrollkulturen, traten 40 %der T-Zellen in den Zellzyklus und durchliefen bis zu sechs Mitosen innerhalb von 96 h. Ausblick: Die Oxidative Mitogenese ist ein suffizientes Modell der vollständigen Aktivierung humaner peripherer naiver T-Lymphozyten in Kokultivierung mit DC. Passend zu in vivo Befunden sowie in vitro Daten muriner TCR-transgener T-Zellen erfolgt die Aktivierung und nachfolgende Proliferation überwiegend durch dynamische und kurzlebige Interaktionen. Die vorliegende Arbeit bestätigt das serielle Kontaktmodell für die Aktivierung naiver humaner T-Zellen.
Systemic treatment of metastatic uveal melanoma: review of literature and future perspectives
(2013)
Up to 50% of patients with uveal melanoma develop metastatic disease with poor prognosis. Regional, mainly liver-directed, therapies may induce limited tumor responses but do not improve overall survival. Response rates of metastatic uveal melanoma (MUM) to systemic chemotherapy are poor. Insights into the molecular biology of MUM recently led to investigation of new drugs. In this study, to compare response rates of systemic treatment for MUM we searched Pubmed/Web of Knowledge databases and ASCO website (1980–2013) for “metastatic/uveal/melanoma” and “melanoma/eye.” Forty studies (one case series, three phase I, five pilot, 22 nonrandomized, and two randomized phase II, one randomized phase III study, data of three expanded access programs, three retrospective studies) with 841 evaluable patients were included in the numeric outcome analysis. Complete or partial remissions were observed in 39/841 patients (overall response rate [ORR] 4.6%; 95% confidence intervals [CI] 3.3–6.3%), no responses were observed in 22/40 studies. Progression-free survival ranged from 1.8 to 7.2, median overall survival from 5.2 to 19.0 months as reported in 21/40 and 26/40 studies, respectively. Best responses were seen for chemoimmunotherapy (ORR 10.3%; 95% CI 4.8–18.7%) though mainly in first-line patients. Immunotherapy with ipilimumab, antiangiogenetic approaches, and kinase inhibitors have not yet proven to be superior to chemotherapy. MEK inhibitors are currently investigated in a phase II trial with promising preliminary data. Despite new insights into genetic and molecular background of MUM, satisfying systemic treatment approaches are currently lacking. Study results of innovative treatment strategies are urgently awaited.
Background
Merkel cell carcinoma (MCC) is a rare cutaneous neoplasm with increasing incidence, aggressive behavior and poor prognosis. Somatostatin receptors (SSTR) are expressed in MCC and represent a potential target for both imaging and treatment.
Methods
To non-invasively assess SSTR expression in MCC using PET and the radiotracers [68Ga]DOTA-D-Phe1-Tyr3-octreotide (DOTATOC) or -octreotate (DOTATATE) as surrogate for tumor burden. In 24 patients with histologically proven MCC SSTR-PET was performed and compared to results of computed tomography (CT).
Results
SSTR-PET detected primary and metastatic MCC lesions. On a patient-based analysis, sensitivity of SSTR-PET was 73% for nodal metastases, 100% for bone, and 67% for soft-tissue metastases, respectively. Notably, brain metastases were initially detected by SSTR-PET in 2 patients, whereas liver and lung metastases were diagnosed exclusively by CT. SSTR-PET showed concordance to CT results in 20 out of 24 patients. Four patients (17%) were up-staged due to SSTR-PET and patient management was changed in 3 patients (13%).
Conclusion
SSTR-PET showed high sensitivity for imaging bone, soft tissue and brain metastases, and particularly in combination with CT had a significant impact on clinical stage and patient management.
Mycosis fungoides (MF) is the most common cutaneous T-cell lymphoma (CTCL) (1). Most patients initially respond well to standard therapy, but advanced MF is often treatment refractory. Thus, a combination of the available treatment options is an important strategy. Total skin electron beam radiation (TSEB) is effective in MF, with a complete remission rate of up to 90% in the early stages. However, in patients with more advanced stages, remission rates are considerably lower (2, 3). Denileukin diftitox (DD) (Ontak®) is a recombinant fusion protein of the receptor-binding domain of interleukin (IL)-2 and the enzymatic and translocation domains of diphtheria toxin (4). It targets the alpha-subunit of the IL-2-receptor (CD25). There are no reports on this combination therapy in MF.
COVID‐19, caused by the coronavirus SARS‐CoV‐2, has become pandemic. A further level of complexity opens up as soon as we look at diseases whose pathogenesis and therapy involve different immunological signaling pathways, which are potentially affected by COVID‐19. Medical treatments must often be reassessed and questioned in connection with this infection.
This article summarizes the current knowledge of COVID‐19 in the light of major dermatological and allergological diseases. It identifies medical areas lacking sufficient data and draws conclusions for the management of our patients during the pandemic. We focus on common chronic inflammatory skin diseases with complex immunological pathogenesis: psoriasis, eczema including atopic dermatitis, type I allergies, autoimmune blistering and inflammatory connective tissue diseases, vasculitis, and skin cancers. Since several other inflammatory skin diseases display related or comparable immunological reactions, clustering of the various inflammatory dermatoses into different disease patterns may help with therapeutic decisions. Thus, following these patterns of skin inflammation, our review may supply treatment recommendations and thoughtful considerations for disease management even beyond the most frequent diseases discussed here.
The long search for the environmental trigger of the endemic pemphigus foliaceus (EPF, fogo selvagem) has not yet resulted in any tangible findings. Here, we searched for genetic associations and the differential expression of host genes involved in early viral infections and innate antiviral defense. Genetic variants could alter the structure, expression sites, or levels of the gene products, impacting their functions. By analyzing 3063 variants of 166 candidate genes in 227 EPF patients and 194 controls, we found 12 variants within 11 genes associated with differential susceptibility (p < 0.005) to EPF. The products of genes TRIM5, TPCN2, EIF4E, EIF4E3, NUP37, NUP50, NUP88, TPR, USP15, IRF8, and JAK1 are involved in different mechanisms of viral control, for example, the regulation of viral entry into the host cell or recognition of viral nucleic acids and proteins. Only two of nine variants were also associated in an independent German cohort of sporadic PF (75 patients, 150 controls), aligning with our hypothesis that antiviral host genes play a major role in EPF due to a specific virus–human interaction in the endemic region. Moreover, CCL5, P4HB, and APOBEC3G mRNA levels were increased (p < 0.001) in CD4+ T lymphocytes of EPF patients. Because there is limited or no evidence that these genes are involved in autoimmunity, their crucial role in antiviral responses and the associations that we observed support the hypothesis of a viral trigger for EPF, presumably a still unnoticed flavivirus. This work opens new frontiers in searching for the trigger of EPF, with the potential to advance translational research that aims for disease prevention and treatment.
Infektionen mit der Krätzemilbe Sarcoptes scabiei varietas hominis können in Gemeinschaftseinrichtungen wie Krankenhäusern, Altenpflege- oder Behindertenheimen weit reichende Ausbrüche hervorrufen. In einer großen Werkstatt für behinderte Menschen und den angegliederten Wohnheimen kam es ab August 2003 zu einem weit reichenden Skabiesausbruch, welcher sich über 10 Monate hinzog. Erst nachdem Vertreter der Werkstatt und Wohnheime und Ärzte der Universitäts-Hautklinik gemeinsam ein Behandlungskonzept erstellt hatten, konnte die Skabies erfolgreich eingedämmt werden. Aufgrund der dabei gemachten Erfahrungen sowie in der Fachliteratur publizierter Skabiesausbrüche wurde ein umfangreiches Konzept zum Vorgehen bei Skabiesausbrüchen in Gemeinschaftseinrichtungen erstellt.
The development of two conventional dendritic cells (DC) subsets (cDC1 and cDC2) and the plasmacytoid DC (pDC) in vivo and in cultures of bone marrow (BM) cells is mediated by the growth factor Flt3L. However, little is known about the factors that direct the development of the individual DC subsets. Here, we describe the selective in vitro generation of murine ESAM\(^{low}\) CD103\(^{-}\) XCR1\(^{-}\) CD172a\(^{+}\) CD11b\(^{+}\) cDC2 from BM by treatment with a combination of Flt3L, LIF, and IL‐10 (collectively named as FL10). FL10 promotes common dendritic cell progenitors (CDP) proliferation in the cultures, similar to Flt3L and CDP sorted and cultured in FL10 generate exclusively cDC2. These cDC2 express the transcription factors Irf4, Klf4, and Notch2, and their growth is reduced using BM from Irf4\(^{-/-}\) mice, but the expression of Batf3 and Tcf4 is low. Functionally they respond to TLR3, TLR4, and TLR9 signals by upregulation of the surface maturation markers MHC II, CD80, CD86, and CD40, while they poorly secrete proinflammatory cytokines. Peptide presentation to TCR transgenic OT‐II cells induced proliferation and IFN‐γ production that was similar to GM‐CSF‐generated BM‐DC and higher than Flt3L‐generated DC. Together, our data support that FL10 culture of BM cells selectively promotes CDP‐derived ESAM\(^{low}\) cDC2 (cDC2B) development and survival in vitro.
Die Migration von Tumorzellen im Bindegewebe erfordert adhäsive Zell-Matrix-Interaktionen, die durch Integrine und andere Adhäsionsmoleküle auf der Zelloberfläche vermittelt werden. In 3DKollagenmatrices benötigen hochinvasive MV3-Melanomzellen überwiegend α2β1-Integrine zur Elongation, Adhäsion an den Kollagenfasern und zur Faserbündelung, sowie zur Kraftgenerierung und Migration. Wir haben untersucht, ob die Migration von Tumorzellen in 3D-Kollagenmatrices vollständig durch die Blockade der Integrinfunktion inhibierbar ist, oder ob es kompensatorische Mechanismen gibt, die zur Migration beitragen. Die β1-Integrinfunktion wurde durch verschiedene Methoden reduziert: a) durchflusszytometrische Sortierung der Zellen in Subgruppen mit niedriger und hoher β1-Integrin-Oberflächenexpression; b) Adhäsionsblockade mit monoklonalem anti β1-Antikörper 4B4 oder Rhodocetin, einem selektiven α2β1-Integrininantagonist; und c) Expression von dominant-negativen Peptiden zur Blockade der Funktion der β1-Integrin-zytoplasmatischen Domäne. Alle β1-Integrin-Interferenzstrategien induzierten einen Übergang der konstitutiv vorhandenen mesenchymalen Migration in einen neuen, amöboiden Migrationstyp (Mesenchymal-Amoeboid Transition, MAT), ähnlich der Migrationsweise von Monozyten oder Lymphozyten. Der Übergang zu amöboider Migration ging einher mit dem Verlust der zellvermittelten Kollagenkontraktion und -reorganisation. Subtotale Inhibition der Integrinfunktion (ca. 50%) durch Antikörper 4B4 ergab eine schnelle (0,3-0,4 >m/min) amöboide Migration, während 90-95%ige Absättigung des β1-Integrin- Epitops zu langsamer amöboider Migration (0,03-0,2 >m/min) führte. Induzierte amöboide Migration verursachte eine gleichmäßige Verteilung der β1-Integrine auf der Zelloberfläche, ein diffuses kortikales Aktin-Zytoskelett, und war mit einer ausgeprägten Formanpassung der Zelle an die Matrixstrukturen verbunden, die von kleinen Filopodien oder Oberflächenblebs getragen wurde. Die Befunde wurden für β1-Integrin-defiziente murine embryonale Fibroblasten (MEF) und murine embryonale Stammzellen (GD25) bestätigt. β1-Integrin-defiziente Fibroblasten zeigten eine schnelle, und GD25 ES-Zellen eine langsame amöboide Migration. Somit erfolgte die amöboide Migration ohne β1-Integrin-vermittelte Zell-Matrix-Interaktionen. Weil keine vollständige Immobilisierung der Zellen erzielt wurde, haben wir alternative Mechanismen von Zell-Matrix-Interaktionen untersucht, die zur Restaktivität der amöboiden Migration beitragen. Als potentielle Kandidaten wurden αv-Integrine, die an denaturiertes Kollagen binden, und Oberflächen-Glycokonjugate getestet. Es wurden keine promigratorischen Funktionen RGDabhängiger Integrine (αv oder β3) mittels zyklischer Arginin-Glycin-Asparaginsäure (cRGD)beobachtet. Um herauszufinden, welche Rolle die Oberfächen-Glycokalyx bei der Zellmigration spielen, wurden verschiedene Methoden angewandt: a) Die an die Proteine gebundenen Glycokonjugate wurden mit Hilfe von N- und O-Glycosidasen von der Oberfläche der lebenden Zellen enzymatisch abgespalten; b) um die Sulfatierung der Glycokonjugate zu verhindern, wurden die Zellen in sulfatfreiem Medium kultiviert. Durch beide Methoden wurde die Bindung von Rutheniumrot an die Zelloberfläche(Glycokalyx) um 60% bzw. die von Heparansulfat der Zelloberfläche um 60% bis 100% reduziert. Nicht die Desulfatierung führte zur Ablösung der Zellen vom Kulturflaschenboden, sondern allein dieBehandlung mit N- und O-Glycosidasen. Die gleichzeitige Behandlung von MV3 Melanomzellen mit N-, O- Glycosidase mit Inhibition der β1-, αvβ3-Integrine führten zur Abrundung der Mehrzahl der Zellen, gefolgt von oszillierender Immobilität (‚Running on the spot’) bzw. sehr langsamer Restmigration (<0,1 >m/min). Dagegen war die Migration der MV3-Zellen nach Kultivierung in sulfatfreiem Medium unverändert. Eine ähnliche Hemmung der Migration erfolgte in β1-/- MEFs nach Glycanverdau. Folglich sind β1-Integrine essentiell für fokalisierte Zell-Matrix-Interaktionen, für die mesenchymale Migration und den Matrixumbau, während amöboide Migration ohne Beteiligung von β1-Integrinen erfolgt, aber durch niedrigaffine, diffuse Zell-Matrix-Interaktionen von Oberflächenglycanen vermittelt wird. Somit ist die Glycokalyx ein alternatives Adhäsionssystem für die integrinunabhängige Zellmigration.
ICIs sind inzwischen integrales Therapiemittel vieler Tumoren, selbst in nicht metastasierten Stadien. Das Management von dabei eventuell entstehenden Nebenwirkungen bleibt wichtiger Bestandteil der Therapie vor allem im fortgeschrittenen Alter. Retrospektive Untersuchungen wie unsere tragen dazu bei, das in vielen klinischen Studien unterrepräsentierte Patientenkollektiv älterer Patienten in den klinischen Alltag sowie in Therapieentscheidungen und -planungen zu integrieren.
Der primäre Studienendpunkt unserer Arbeit unterstützt wichtige Erkenntnisse anderer Studien, dass irAEs insgesamt unter älteren Patienten nicht häufiger auftreten. Zwischen allen drei Altersklassen von ~55, ~70 und ~80 Jahren zeigten sich keine signifikanten Unterschiede im Auftreten von irAEs aller Grade, wobei irAEs Grad III/IV etwas häufiger bei ~80-Jährigen auftraten. In unserem Fall stellten wir fest, dass auftretende irAEs im Alter häufiger behandelt wurden, und dass die Immuntherapie häufiger pausiert oder abgebrochen wurde. Zudem war der Anteil an Therapieabbrüchen unter den älteren Patienten wegen bestimmter Ereignisse wie TRAEs und dem Einsatz von Glukokortikoiden höher als bei jüngeren Patienten.
Die Ergebnisse unserer Studie deuten außerdem darauf hin, dass selbst unter Polypharmazie und Multimorbidität irAEs nicht häufiger bei Älteren auftraten. Ebenso können wir die interessante Beobachtung verzeichnen, dass Patienten mit >5 Medikamenten und gleichzeitig >5 Erkrankungen signifikant mehr irAEs Grad III/IV aufwiesen oder mehr Patienten Glukokortikoide verabreicht bekommen haben. Auch der Anteil an Interventionsbedarf oder Therapieabbruch war hier in allen Altersklassen höher. Es stellt sich die Frage, inwiefern hohes Alter, Komorbidität und Polypharmazie Risikofaktoren für Interventionsbedarf oder Therapieabbruch in der Immuntherapie sind, und ob ihnen eher besondere Gewichtung als Risikofaktor zukommt als dem Alter selbst.
Die Expression des p16-Tumorsuppressorgens spielt in der Früherkennung von Gebärmutterhalskrebs eine außerordentlich wichtige Rolle. Hier dient p16INK4a als immunhistochemisch evaluierter Biomarker für präkanzeröse Läsionen der Zervix. In der vorliegenden Arbeit wurde die Expression des p16-Proteins immunhistologisch anhand obligaten Präkanzerosen, potentiell präkanzeröser Entzündungen und Karzinomen der Mundhöhle untersucht. Hierzu wurden 80 Fälle aus dem histologischen Archiv der Klinik und Poliklinik für Dermatologie, Venerologie und Allergologie des Universitäts-Klinikums Würzburg sowie aus dem Institut für Pathologie der Universität Würzburg verwendet. Die Fälle stammen aus dem Zeitraum von 2000 bis 2011. Ziel der vorliegenden Arbeit war zu untersuchen, inwiefern das p16INK4a-Protein als Biomarker für prämaligne und maligne Läsionen fungieren kann. Die untersuchten Präparate beinhalteten orale Leukoplakien mit geringen und hoch dysplastischen Veränderungen sowie orale als auch extraorale Lichen planus und orale Plattenepithelkarzinome. Als Ergebnis lässt sich festhalten, dass die p16-Expression der oralen Leukoplakien nicht mit dem vorliegenden Dysplasiegrad korrelierte und ausgesprochen schwach ausfiel. Die Plattenepithelkarzinome der Mundhöhle zeigten größtenteils (75%) keine p16-Expression im invasiven Anteil des Tumors. Hier geht man davon aus, dass durch homozygote Deletionen, inaktivierende Mutationen sowie durch eine nicht korrekt ausgeführte Promotormethylierung die p16-Expression ausgeschaltet wird. Darüber hinaus wiesen die Fälle des Lichen planus eine zumeist stark positive Expression von p16INK4a auf, da 93,3 % der oralen und 95% der extraoralen Lichen planus positiv ausfielen. Verglichen mit oralen Leukoplakien weisen der orale und kutane Lichen planus ein sehr viel geringeres Risiko der malignen Transformation auf. Zusammenfassend lässt sich sagen, dass die hier demonstrierten Ergebnisse die Hypothese zulassen, dass eine Überexpression des p16-Proteins das Risiko einer malignen Entartung niedrig hält. Ein Herunterfahren des p16-Tumorsuppressorgens kann somit ein erster Schritt der Genese eines malignen Tumors sein. Die Diskussion dieser Hypothesen sollte jedoch durch weiterführende Untersuchungen bestätigt werden.
Antibody–drug conjugates (ADCs) are an emerging class of therapeutics, with twelve FDA- and EMA-approved drugs for hematological and solid cancers. Such drugs consist in a monoclonal antibody linked to a cytotoxic agent, allowing a specific cytotoxicity to tumor cells. In recent years, tremendous progress has been observed in therapeutic approaches for advanced skin cancer patients. In this regard, targeted therapies (e.g., kinase inhibitors) or immune checkpoint-blocking antibodies outperformed conventional chemotherapy, with proven benefit to survival. Nevertheless, primary and acquired resistances as well as adverse events remain limitations of these therapies. Therefore, ADCs appear as an emerging therapeutic option in oncodermatology. After providing an overview of ADC design and development, the goal of this article is to review the potential ADC indications in the field of oncodermatology.
miR-375 is a highly abundant miRNA in Merkel cell carcinoma (MCC). In other cancers, it acts as either a tumor suppressor or oncogene. While free-circulating miR-375 serves as a surrogate marker for tumor burden in patients with advanced MCC, its function within MCC cells has not been established. Nearly complete miR-375 knockdown in MCC cell lines was achieved using antagomiRs via nucleofection. The cell viability, growth characteristics, and morphology were not altered by this knockdown. miR-375 target genes and related signaling pathways were determined using Encyclopedia of RNA Interactomes (ENCORI) revealing Hippo signaling and epithelial to mesenchymal transition (EMT)-related genes likely to be regulated. Therefore, their expression was analyzed by multiplexed qRT-PCR after miR-375 knockdown, demonstrating only a limited change in expression. In summary, highly effective miR-375 knockdown in classical MCC cell lines did not significantly change the cell viability, morphology, or oncogenic signaling pathways. These observations render miR-375 an unlikely intracellular oncogene in MCC cells, thus suggesting that likely functions of miR-375 for the intercellular communication of MCC should be addressed.
Die vorliegende Promotionsarbeit beschäftigte sich mit der Frage, ob der Todesligand TRAIL in Keratinozyten eine Aktivierung verschiedener Mitogen-aktivierter Protein Kinasen (MAPK) induzieren kann und welche physiologische Relevanz diese TRAIL-induzierte MAPK-Aktivität hat. In unseren Analysen konnte nachgewiesen werden, dass TRAIL die MAPKERK1/2, MAPKJNK1/2 und MAPKp38 mit unterschiedlicher Kinetik aktivieren kann. Diese Aktivierung zeigte sich beeinflusst vom verwendeten Zelltyp, der Zeitdauer der Stimulation sowie dem Ausmaß der TRAIL-induzierten Caspase-Aktivität. Die TRAIL-vermittelte Aktivierung der MAPKERK1/2 beginnt sehr rasch und kann über einen längeren Zeitraum detektiert werden, während die MAPKJNK erst spät aktiviert wird. Im Gegensatz dazu zeigt die MAPKp38 eine biphasische Aktivierung. Die TRAIL-induzierte Aktivierung der MAPK ist teilweise von aktiven Caspasen abhängig, denn eine Präinkubation mit dem pharmakologischen Caspase-Inhibitor zVAD-fmk hemmt sowohl die TRAIL-induzierte MAPKJNK- als auch die MAPKp38-Aktivität. Untersuchungen mit ektoper Expression des physiologischen Caspase-8 Inhibitors c-FLIPL konnten zeigen, dass cFLIPL nicht nur die Spaltung von Caspase-8, sondern auch die verzögerte TRAIL-induzierte MAPKp38-Aktivität hemmen kann. In der vorliegenden Arbeit wurde außerdem nachgewiesen, dass TRAIL in Keratinozyten nicht nur Apoptose induziert, sondern auch an der Sekretion des proinflammatorischen Chemokins CXCL-8 beteiligt ist. Dabei war die MAPKp38, aber nicht die MAPKERK1/2 an der TRAIL-induzierten Sekretion von CXCL-8 beteiligt. Zukünftig werden weitere detailliertere Untersuchungen insbesondere zur physiologischen Bedeutung der TRAIL-induzierten MAPKJNK- und MAPKERK1/2-Aktivität erforderlich sein, für die diese Arbeit eine wichtige Grundlage gelegt hat.
Die histologische Differenzialdiagnose zwischen den benignen trichogenen Hauttumoren und dem malignen Basalzellkarzinom stellt aufgrund ihrer Ähnlichkeit eine große Herausforderung dar. Das Ziel der Arbeit war, diese Tumoren auf ihre Expression von CD10, ein Zelloberflächenprotein mit neutraler Endopeptidaseaktivität, zu untersuchen. Anhand dessen sollte der Stellenwert des Antikörpers im Vergleich mit anderen untersucht werden. Auch klinische Daten sollten in Zusammenschau mit der Literatur betrachtet werden. Aus dem Archiv der Universitäts-Hautklinik wurden 119 Präparate sowie die zugehörigen Patientendaten aus dem Zeitraum 2000 bis 2009 entnommen. Darunter befanden sich 28 solide und 15 sklerodermiforme Basalzellkarzinome, 21 Pinkus-Tumoren, 20 Trichoblastome, neun Trichofollikulome, elf Trichoepitheliome, fünf desmoplastische Trichoepitheliome und zehn seborrhoische Keratosen. Es erfolgte eine immunhistochemische Färbung mit dem Antikörper CD10 mit anschließender Begutachtung der Tumor- und peritumoralen Reaktion sowie eine Auswertung der klinischen Daten. Alters- und Geschlechterverteilung sowie die Tumorlokalisation unserer Fallserie entsprach weitestgehend Literaturdaten. Die immunhistochemische Färbung mit CD10 ergab in der gesunden Haut eine Expression in den Strukturen des Haarfollikels sowie in Sebozyten und perivaskulären Fibroblasten. Seborrhoische Keratosen zeigten keine tumorale CD10-Expression. Das solide Basalzellkarzinom war in den randständigen Zellen CD10-positiv, während die Trichoblastome CD10 diffus exprimierten. Eine randständige Expression war darüber hinaus in Pinkus-Tumoren und Trichoepitheliomen zu beobachten. Im desmoplastischen Trichoepitheliom war keine CD10-Expression in den Tumorzellen zu erkennen, während die meisten sklerodermiformen Basalzellkarzinome CD10-positiv waren. Die Trichofollikulome exprimierten CD10 in der Hälfte der Fälle im Tumor. Eine starke peritumorale Reaktion war vor allem in Pinkus-Tumoren und sklerodermiformen Basalzellkarzinomen zu beobachten. Die in dieser Arbeit erhobenen Befunde wurden mit in der Literatur beschriebenen differenzialdiagnostischen Markern verglichen (Androgenrezeptoren, Merkelzellen, PHLDA1 und die Gefäßdichte) und zeigen, dass im Vergleich zu anderen Markern CD10 allenfalls was das epitheliale Expressionsmuster betrifft, differenzialdiagnostische Bedeutung hat, nicht aber, wie in der Literatur postuliert, bezüglich stromaler Reaktivität.
Melanozyten (MZ) sind der zweihäufigste epidermale Zelltyp. Das Wachstum und die metabolische Tätigkeit der MZ wird durch humorale Faktoren sowie den direkten Zell-Zell Kontakt kontrolliert. Der schädigende Einfluss der UV-Strahlung, der mit der Entwicklung von epithelialen Tumoren zusammenhängt, wird durch das Pigmentsystem der Haut vermindert. Im Zeitraum von Juni 2006 bis Juni 2007 wurden Präparate mit vorliegenden histologischen und klinischen Befunden von epithelialen Hauttumoren untersucht und mit Melanin-, Melan-A und HMB-45 gefärbt. Hierzu gehören: 40 Basalzellkarzinome (BCC), 20 Plattenepithelkarzinome (PEC), 20 seborrhoische Keratosen (SK), 9 Morbi Bowen (MB), 7 aktinischen Keratosen (AK), und 5 Kerathoakantome (KA). Ziel der Arbeit war die Identifizierung und Charakterisierung der MZ in verschiedenen epithelialen Hauttumoren. Meist waren die Tumorzellen negativ in der Melaninfärbung. Melan-A wurde am stärksten bei SK, BCC und AK exprimiert. Im Gegensatz dazu zeigten sich bei PEC am wenigsten angefärbten Zellen. Die HMB-45-positiv-MZ färbten sich am stärksten bei AK, MB und BCC an. Obwohl HMB-45 bei allen Tumortypen positiv war, war die Auszählung vom HMB-45-positiven-MZ deutlich geringer als bei Melan-A. Es gibt eine Korrelation zwischen MZ und neoplastischen Keratinozyten, jedoch ist noch nicht nachgewiesen, was die MZ dazu stimuliert, zu proliferieren und darüber hinaus zu kolonisieren. Eine Korrelation zwischen der epithelialen Pigmentierung und der Anzahl an MZ zeigte sich nur in gutartigen epithelialen Hauttumoren (SK), während in allen malignen Tumoren keine Korrelation zwischen der MZ-Zahl und eventueller Pigmentierung bestand. Das weist darauf hin, dass hier die Regulation der Pigmentierung zerstört ist.
Basal cell carcinoma (BCC) is the most common neoplasm in the Caucasian population. Only a fraction of BCC exhibits pigmentation. Lack of melanocyte colonization has been suggested to be due to p53-inactivating mutations in the BCC cells interfering with the p53-proopiomelanocortin pathway and the production of alpha melanocyte-stimulating hormone in the tumor. To evaluate this, we determined tumor pigmentation as well as expression of melan-A and of p53 in 49 BCC tissues bymeans of immunohistochemistry. As expected, we observed a positive relation between tumor pigmentation and melan-A positive intratumoral melanocytes.Melanocyte colonization and, to a lesser extent, p53 overexpression showed intraindividual heterogeneity in larger tumors. p53 overexpression, which is indicative of p53 mutations, was not correlated to melanocyte colonization of BCC. Sequencing of exon 5–8 of the p53 gene in selected BCC cases revealed that colonization by melanocytes and BCC pigmentation is neither ablated by p53 mutations nor generally present in BCCs with wild-type p53.
Background
Subcutaneous vaccination or desensitization may induce persistent nodules at the injection sites. Without the knowledge of prior injection, histopathological work-up may be challenging.
Objective
Aim of this study was to contribute to the histopathological work-up of unclear subcutaneous nodules, especially their differentiation from cutaneous lymphoma.
Methods
We retrospectively reviewed clinical data and histopathological slides of four patients with subcutaneous nodules, which were suspected to suffer from cutaneous T- or B-cell lymphoma. Sections of these cases and 12 negative controls were stained with hematoxylin and eosin and a standardized immunohistochemical panel of B- and T-cell markers including EBER in situ hybridization as well as electron microscopy.
Results
In all cases, large histiocytes with granular cytoplasm compatible with intracellular aluminum hydroxide were present. EBER in situ hybridization revealed positive staining of these granular histiocytes while staining was absent in negative controls.
Limitations
Post hoc completion of medical history revealed that vaccination or specific immunotherapy had been applied before at the biopsy site in only three out of four patients; one patient was lost to follow-up.
Conclusion
EBER in situ hybridization is an adjunctive tool to differentiate aluminum-induced granuloma/lymphoid hyperplasia from other forms of pseudolymphoma and cutaneous B- or T-cell lymphomas.
Background
Gap junctions consisting of connexins (Cx) are fundamental in controlling cell proliferation, differentiation, and cell death. Cx43 is the most broadly expressed Cx in humans and is attributed an important role in skin tumor development. Its role in cutaneous vascular neoplasms is yet unknown.
Methods
Fifteen cases each of cutaneous angiosarcoma (cAS), Kaposi sarcoma (KS), and cherry hemangioma (CH) were assessed by immunohistochemistry for expression of Cx43. Expression pattern, intensity, and percentage of positively stained cells were analyzed. Solid basal cell carcinomas served as positive and healthy skin as negative controls.
Results
Most cases of cAS presented with a strong Cx43 staining of almost all tumor cells, whereas endothelia of KS showed medium expression and CH showed mostly weak expression. In comparison with KS or cAS, the staining intensity of CH was significantly lower (P ≤ 0.001). All tissue sections of both cAS and KS were characterized by a mostly diffuse, cytoplasmic staining pattern of the vascular endothelia. None of those showed nuclear staining.
Conclusion
The high-to-intermediate expression of Cx43 observed in all cases of cAS and KS suggests that this Cx may play a role in the development of malignant vascular neoplasms and serve as a helpful diagnostic marker.
Background and objectives
Hidradenitis suppurativa (HS) significantly affects the patient`s quality of life and leads to multiple medical consultations. Aim of this study was to assess the utilization of medical care of HS patients.
Patients and methods
All patients presenting in 2017 for an outpatient, day patient and / or inpatient treatment with leading claim type HS at the Department of Dermatology, University Hospital Würzburg, were included. Primary outcome was the economic burden of HS patients, measured by resource utilization in €.
Results
The largest share of the direct medical costs for HS were the inpatient costs with a leading surgical diagnosis-related group (DRG). Antiseptics were the predominant topical prescription. While doxycycline was the most frequently prescribed systemic therapy, adalimumab was the main cost driver. The difference between in-patient (€ 110.25) and outpatient (€ 26.34) direct non-medical costs was statistically significant (p < 0.001). With regards to indirect medical costs, a statistically significantly higher loss of gross value added (inpatient mean € 1,827.00; outpatient mean € 203.00) and loss of production (inpatient mean € 1,026.00; outpatient mean € 228.00) could be noted (p < 0.001), respectively.
Conclusions
The present study on disease-specific costs of HS confirms that the hospital care of patients with this disease is cost-intensive. However, the primary goal of physicians is not and should not be to save costs regarding their patients`treatment, but rather the premise to utilize the existing resources as efficient as possible. Reducing the use of costly therapeutics and inpatient stays therefore requires more effective therapy options with an improved cost-benefit profile.
Forkhead box O transcription factors are a family of proteins involved in cellular processes downstream of the Insulin-PI3K-PKB pathway. In response to extra- or intracellular stresses, for example starvation or oxidative stress, FoxOs are required to direct cell cycle progression and apoptosis. In endothelial cells, they induce apoptosis, and their deregulation is linked to diseases involving the insulin pathway, such as diabetes. FoxOs also exhibit a complex role in tumour transformation: here their main function is to suppress tumorigenesis. In both physiological and cancer contexts, FoxO activation leads to the transcription of some general targets, such as p27kip1 or IGFBP1. The FoxOs can also induce tissue-specific genes, as ANGPT2 and BIM in the endothelium.
In endothelial cells, another pathway with a pivotal function is the MEK5/ERK5 MAPK signalling way. Its activation promotes cell survival and proliferation in stressful conditions, e.g., when blood vessels are exposed to the shear forces exerted by the blood stream. Furthermore, recent data described ERK5 as a kinase directing tumour resistance upon therapy-induced stress.
Comparing their reported roles in various tumours and in the endothelium, FoxO proteins and the MEK5/ERK5 MAPK cascade appear to exert opposite functions. First non-published data confirmed the hypothesis that FoxO factors are subject to a negative modulation by the MEK5/ERK5 pathway. Hence, one goal of this PhD project was to further characterise this crosstalk at molecular level. The major mechanism of FoxO regulation is the balance among several post translational modifications, such as phosphorylation, acetylation, and ubiquitination. Most importantly, the PKB dependent phosphorylation of FoxOs negatively controls their activity, and it is critical for their subcellular localization. Therefore, the regulation of FoxO localization as mechanism of ERK5 dependent suppression was studied, but the results presented in this thesis argue against this hypothesis. However, additional experiments are required to explore the impact of ERK5 activity on FoxO post-translational modifications.
FoxO activity can also be modulated by the interaction with other proteins, which in turn could explain general- and tissue-specific gene expression. Thus, another objective of this work was to investigate FoxO3-interactome in endothelial cells and the impact of MEK5/ERK5 activation on it. As published in (Fusi et al. 2022) and presented here, this analysis unveiled TRRAP as new FoxO bound protein in several cell types. Moreover, the interaction did not rely on the capacity of the FoxOs to bind their consensus DNA sequences at the promoter of target genes. Functional data demonstrated that TRRAP is required for FoxO-dependent gene transcription in endothelial and osteosarcoma cells. In addition, TRRAP expression in the endothelium is important for FoxO induced apoptosis. In summary, the interaction between FoxO factors and TRRAP revealed a new regulatory mechanism of FoxO-dependent gene transcription. It remains to be analysed whether the MEK5/ERK5 cascade may exert its suppressive effect on FoxO activity by interfering with their binding to TRRAP and whether such a mechanism may be relevant for tumorigenesis.
Forkhead box O (FoxO) transcription factors are conserved proteins involved in the regulation of life span and age-related diseases, such as diabetes and cancer. Stress stimuli or growth factor deprivation promotes nuclear localization and activation of FoxO proteins, which—depending on the cellular context—can lead to cell cycle arrest or apoptosis. In endothelial cells (ECs), they further regulate angiogenesis and may promote inflammation and vessel destabilization implicating a role of FoxOs in vascular diseases. In several cancers, FoxOs exert a tumor-suppressive function by regulating proliferation and survival. We and others have previously shown that FoxOs can regulate these processes via two different mechanisms: by direct binding to forkhead-responsive elements at the promoter of target genes or by a poorly understood alternative process that does not require direct DNA binding and regulates key targets in primary human ECs. Here, we performed an interaction study in ECs to identify new nuclear FoxO3 interaction partners that might contribute to FoxO-dependent gene regulation. Mass spectrometry analysis of FoxO3-interacting proteins revealed transformation/transcription domain–associated protein (TRRAP), a member of multiple histone acetyltransferase complexes, as a novel binding partner of FoxO family proteins. We demonstrate that TRRAP is required to support FoxO3 transactivation and FoxO3-dependent G1 arrest and apoptosis in ECs via transcriptional activation of the cyclin-dependent kinase inhibitor p27\(^{kip1}\) and the proapoptotic B-cell lymphoma 2 family member, BIM. Moreover, FoxO–TRRAP interaction could explain FoxO-induced alternative gene regulation via TRRAP-dependent recruitment to target promoters lacking forkhead-responsive element sequences.
Hintergrund:
Die pathogenetischen Mechanismen der chronisch-entzündlichen Hauterkrankung Acne inversa (AI) beinhalten epidermale Störungen wie psoriasiforme Hyperplasie und Keratinpfröpfe. Bei verschiedenen entzündlichen Hauterkrankungen sind die Keratinozyten eine wichtige Quelle proinflammatorischer Moleküle und können von IL-17+-Zellen stimuliert werden.
Ziele und Methoden:
Um die mögliche Rolle des Epithels in der Pathogenese der AI zu erforschen, führten wir immunhistochemische Färbungen sowie Western Blot-Analysen durch. Mithilfe dieser Untersuchungen wurde die Expression entzündungsassoziierter Moleküle wie Interleukin(IL)-17, der Inflammasom-Komponenten Caspase-1 und NLRP3, und der danger-associated molecular pattern (DAMP)-Moleküle S100A8 und S100A9 (Calprotectin) analysiert. Um eine mögliche Wirkung dieser proinflammatorischen Zytokine auf den entzündlichen Verlauf der AI zu untersuchen, wurde die Zusammensetzung der perifollikulären und tiefen Infiltrate verglichen.
Ergebnisse:
Die Zahl der IL-17+-Zellen ist in läsionaler und periläsionaler AI-Haut erhöht. Die Epidermis produziert proinflammatorische Moleküle und zeigt eine hochregulierte Expression von NLRP3, aktivierter Caspase-1 und S100A8/A9. Zusätzlich zeigt sich im Verlauf des AI-Entzündungsprozesses ein Zustrom von Zellen des angeborenen Immunsystems, insbesondere von IL-17-exprimierenden neutrophilen Granulozyten.
Schlussfolgerungen:
IL-17-produzierende Zellen sind in läsionaler und periläsionaler AI-Haut vermehrt und können die Einleitung des entzündlichen Prozesses beeinflussen. Die Epidermis stellt sich als eine wesentliche Quelle proinflammatorischer Zytokine dar und zeigt eine vermehrte Expression von S100A8/S100A9 sowie eine Aktivierung des Inflammasoms; hierdurch wird möglicherweise die Ausbreitung der Entzündung signifikant beeinflusst. Eine deutliche Zunahme von IL-17-exprimierenden neutrophilen Granulozyten wurde im tiefen Infiltrat beobachtet.
Innerhalb der Gruppe der kutanen T-Zell-Lymphome ist die CD4+ klein-/mittelgroßzellige T-Zell-Lymphoproliferation (SMTCL) eine seltene und bisher als provisorisch erfasste Entität.
Um genauere Kenntnisse zu Klinik und Verlauf, Histologie und Immunphänotyp zu gewinnen, untersuchten wir in dieser Fallserie an 95 Fällen entsprechende Charakteristika. Dabei konnten alle der bisher provisorisch definierten Eigenschaften der SMTCL bestätigt werden. Lediglich die 5-Jahre-Überlebensrate zeigte sich mit 100% weitaus höher als die in der WHO-/EORTC-Klassifikation angegebenen 60–80%. Diese Bestätigung der provisorisch definierten Eigenschaften an einem größeren Kollektiv kann dazu beitragen, dass die SMTCL in die nächste Version der WHO-Klassifikation – durch ausreichende Daten gestützt – als definitive Entität aufgenommen werden kann.
Insgesamt konnten in dieser Studie einige Faktoren, die mit einem weniger indolenten Krankheitsverlauf assoziiert sind, identifiziert werden. So zeigten klinisch ein initial bestehender generalisierter Hautbefall sowie eine extrafaziale Lokalisation der Läsion einen weniger indolenten Verlauf an. Auch Patienten, bei denen ein Verlust von CD2, CD3 oder CD5 bei den Tumorzellen festgestellt wurde, wiesen einen für die CD4+ SMTCL ungewöhnlichen und weniger indolenten Krankheitsverlauf mit häufigeren Rezidiven und seltenerem Erreichen einer kompletten Remission auf. Histopathologisch schien eine oberflächlichere Infiltrattiefe des Präparates sowie das Vorhandensein eines fokalen Epidermotropismus einen negativen prognostischen Wert zu besitzen.
Bezüglich des Gesamtüberlebens hatten allerdings auch Patienten mit einem der identifizierten negativen prognostischen Faktoren eine exzellente Prognose. Bei Vorliegen eines dieser negativen Faktoren sollte jedoch eine engmaschigere klinische Überwachung erfolgen.
Ziel
Ziel dieser Studie war es, die 2‑Jahres-Ergebnisse der filtrierenden Trabekulotomie (FTO) im Vergleich zur konventionellen Trabekulektomie (TE) bei primärem Offenwinkelglaukom, Pseudoexfoliationsglaukom und Pigmentglaukom zu untersuchen.
Patienten und Methoden
Es wurden 30 konsekutive Patienten nach FTO und 87 Patienten nach TE nach intraokularem Druck (IOD) und Alter im Verhältnis 1:3 gematcht. Primärer Endpunkt war das Erreichen des Zieldrucks nach 2 Jahren. Als vollständiger Erfolg wurde ein IOD ohne Medikamente von ≤ 18 mm Hg bei gleichzeitiger IOD-Reduktion um ≥ 30 % definiert, als qualifizierter Erfolg, wenn hierfür zusätzlich Medikamente erforderlich waren. Sekundäre Endpunkte waren mittlere Drucksenkung, resultierende Sehschärfe, Komplikationen und nachfolgende Operationen. Die Operationstechnik der filtrierenden Trabekulotomie ist als Video zu diesem Beitrag abrufbar.
Ergebnisse
Zwei-Jahres-Daten konnten von 27 Patienten aus der FTO-Gruppe und 68 Patienten aus der TE-Gruppe erhoben werden. Die Patienten beider Gruppen wurden vor Beginn der Studie bezüglich Alter und IOD gematcht, waren aber auch bezüglich Sehschärfe, Geschlecht und Medikation nicht unterschiedlich. Der Median des präoperativen IOD unter Therapie betrug in beiden Gruppen 23,0 mm Hg. Nach den oben genannten Kriterien wurde ein qualifizierter 2‑Jahres-Erfolg bei 70,4 % der FTO-Gruppe und bei 77,6 % der TE-Gruppe erzielt (p = 0,60), ein vollständiger 2‑Jahres-Erfolg bei 33,3 % der FTO-Gruppe und bei 56,7 % der TE-Gruppe (p = 0,07). Beide Operationsmethoden senkten den Augeninnendruck nach 24 Monaten signifikant (p < 0,001), und zwar auf 12,8 mm Hg in der FTO-Gruppe und 11,0 mm Hg in der TE-Gruppe. Die Sehschärfe war postoperativ bei beiden Gruppen etwas verringert, unterschied sich jedoch nicht signifikant zwischen beiden Gruppen. Komplikations- und Reoperationsrate waren gering und unterschieden sich nicht zwischen den Gruppen.
Schlussfolgerung
FTO und TE sind nach 2 Jahren weitgehend gleichwertig bezüglich Zieldruck, IOD-Senkung, Sehschärfe und Komplikationen.
The approval of BRAF and MEK inhibitors has signifi-cantly improved treatment outcomes for patients with BRAF-mutated metastatic melanoma. The 3 first-line targeted therapy trials have provided similar results, and thus the identification of predictive biomarkers may generate a more precise basis for clinical deci-sion-making. Elevated baseline lactate dehydrogenase (LDH) has already been determined as a strong prog-nostic factor. Therefore, this indirect analysis compa-red subgroups with elevated baseline LDH across the pivotal targeted therapy trials co-BRIM, COMBI-v and COLUMBUS part 1. The Bucher method was used to compare progression-free survival, objective response rate and overall survival indirectly. The results show a non-significant risk reduction for progression in the subgroup with elevated baseline LDH receiving vemu-rafenib plus cobimetinib compared with dabrafenib plus trametinib and encorafenib plus binimetinib. Al-though an indirect comparison, these data might pro-vide some guidance for treatment recommendations in melanoma patients with elevated LDH.
Background
High response rates of metastatic melanoma have been reported upon immune checkpoint inhibition by PD-1 blockade alone or in combination with CTLA-4 inhibitors. However, the majority of patients with a primary resistance to anti-PD-1 monotherapy is also refractory to a subsequent combined checkpoint inhibition. In BRAF wildtype patients with a primary resistance to PD-1 inhibitors, therapeutic options are therefore limited and immune-related adverse events (irAE) have to be taken into consideration when discussing a subsequent immunotherapy.
Case presentation
We report the case of a 68-year-old male patient with metastatic melanoma who experienced an acute renal failure with nephrotic syndrome due to a minimal change disease developing after a single dose of the anti-PD-1 antibody pembrolizumab. A kidney biopsy revealed a podocytopathy without signs of interstitial nephritis. Renal function recovered to almost normal creatinine and total urine protein levels upon treatment with oral steroids and diuretics. Unfortunately, a disease progression (PD, RECIST 1.1) was observed in a CT scan after resolution of the irAE. In a grand round, re-exposure to a PD-1-containing regime was recommended. Consensually, a combined immunotherapy with ipilimumab and nivolumab was initiated. Nephrotoxicity was tolerable during combined immunotherapy and a CT scan of chest and abdomen showed a deep partial remission (RECIST 1.1) after three doses of ipilimumab (3 mg/kg) and nivolumab (1 mg/kg).
Conclusion
This case illustrates that a fulminant response to combined checkpoint inhibition is possible after progression after anti-PD-1 monotherapy and a severe irAE.
Background
Merkel cell carcinoma (MCC) is a rare and aggressive neuroendocrine cutaneous malignancy with poor prognosis. In Europe, approved systemic therapies are limited to the PD-L1 inhibitor avelumab. For avelumab-refractory patients, efficient and safe treatment options are lacking.
Methods
At three different sites in Germany, clinical and molecular data of patients with metastatic MCC being refractory to the PD-L1 inhibitor avelumab and who were later on treated with combined IPI/NIVO were retrospectively collected and evaluated.
Results
Five patients treated at three different academic sites in Germany were enrolled. Three out of five patients investigated for this report responded to combined IPI/NIVO according to RECIST 1.1. Combined immunotherapy was well tolerated without any grade II or III immune-related adverse events. Two out of three responders to IPI/NIVO received platinum-based chemotherapy in between avelumab and combined immunotherapy.
Conclusion
In this small retrospective study, we observed a high response rate and durable responses to subsequent combined immunotherapy with IPI/NIVO in avelumab-refractory metastatic MCC patients. In conclusion, our data suggest a promising activity of second- or third-line PD-1- plus CTLA-4-blockade in patients with anti-PD-L1-refractory MCC.
Merkel cell carcinoma is a rare, highly aggressive skin cancer with neuroendocrine differentiation. Immune checkpoint inhibition has significantly improved treatment outcomes in metastatic disease with response rates to programmed cell death protein 1/programmed cell death 1 ligand 1 (PD-1/PD-L1) inhibition of up to 62%. However, primary and secondary resistance to PD-1/PD-L1 inhibition remains a so far unsolved clinical challenge since effective and safe treatment options for these patients are lacking.Fourteen patients with advanced (non-resectable stage III or stage IV, Union international contre le cancer 2017) Merkel cell carcinoma with primary resistance to the PD-L1 inhibitor avelumab receiving subsequent therapy (second or later line) with ipilimumab plus nivolumab (IPI/NIVO) were identified in the prospective multicenter skin cancer registry ADOREG. Five of these 14 patients were reported previously and were included in this analysis with additional follow-up. Overall response rate, progression-free survival (PFS), overall survival (OS) and adverse events were analyzed.All 14 patients received avelumab as first-line treatment. Thereof, 12 patients had shown primary resistance with progressive disease in the first tumor assessment, while two patients had initially experienced a short-lived stabilization (stable disease). Six patients had at least one systemic treatment in between avelumab and IPI/NIVO. In total, 7 patients responded to IPI/NIVO (overall response rate 50%), and response was ongoing in 4 responders at last follow-up. After a median follow-up of 18.85 months, median PFS was 5.07 months (95% CI 2.43—not available (NA)), and median OS was not reached. PFS rates at 12 months and 24 months were 42.9% and 26.8 %, respectively. The OS rate at 36 months was 64.3%. Only 3 (21%) patients did not receive all 4 cycles of IPI/NIVO due to immune-related adverse events.In this multicenter evaluation, we observed high response rates, a durable benefit and promising OS rates after treatment with later-line combined IPI/NIVO. In conclusion, our patient cohort supports our prior findings with an encouraging activity of second-line or later-line IPI/NIVO in patients with anti-PD-L1-refractory Merkel cell carcinoma.
Background: Rhabdoid melanoma is a rare variant of malignant melanoma with characteristic cytomorphologic features. Due to the potential loss of conventional melanocytic markers, histopathologic diagnosis is often challenging. We hypothesize that immunostaining for PReferentially expressed Antigen in MElanoma (PRAME) might have the potential to uncover the melanocytic origin of these dedifferentiated tumors. Methods: Four cases of rhabdoid primary melanomas were assessed by immunohistochemistry for expression of PRAME and conventional melanocytic markers. Immunohistochemical expression patterns were analyzed in the rhabdoid primaries and, if available, associated metastases. Results: All four cases of rhabdoid primary melanomas showed a strong nuclear positivity for PRAME, while the expression of conventional melanocytic markers S100, MART-1, SOX-10 and HMB-45 was variable between the analyzed cases. Conclusions: In summary, we report four cases of rhabdoid primary melanoma with high to intermediate expression of PRAME despite the partial and variable loss of other melanocytic markers. Hence, PRAME might facilitate the recognition of this highly aggressive entity to avoid misdiagnosis due to histopathologic pitfalls.
Acne inversa (AI), in der englischen Literatur auch als Hidradenitis suppurativa (HS) bezeichnet, ist eine chronische, entzündliche und schmerzhafte Hautkrankheit, die re- zidivierende Knoten, Fisteln, Abszesse und Vernarbungen vor allem in den Intertrigines verursacht. Es zeigen sich bei Betroffenen neben schwerwiegenden somatischen, auch psychologische Komorbiditäten. Das Ziel der vorliegenden wissenschaftlichen Arbeit war es, an einem an AI erkrankten Patientenkollektiv prospektiv systematisch Komor- biditäten, Lebensqualität und psychische Verfassung zu analysieren und auf Korrelatio- nen zu untersuchen, um daraus Handlungsempfehlungen abzuleiten. Mittels dermatolo- gischer und psychologischer Fragebögen mit Fragebögen zur Lebensqualität wurden pseudonymisierte Daten von 110 Studienteilnehmern gewonnen, statistisch aufbereitet und ausgewertet. Es konnte eine statistisch signifikante Korrelation der Visuellen Ana- logskala Schmerz (VAS-Schmerz) mit dem Hospitality Anxiety Depression Scale (HADS) bzw. dem Skindex-29 aufgezeigt werden. Der Zeitraum zwischen Erstsymp- tomen und Diagnosestellung der AI erfolgte im Median nach 6 Jahren. Weiterhin erfuh- ren AI-Patienten häufig eine nicht leitliniengerechte Therapie und zeigten psychische Belastungen anhand von Schlafstörungen, besonderen Stresssituationen und eine damit einhergehende Verschlechterung der AI. Body Mass Index (BMI), „Waist-to-hip-ratio“ und Bluthochdruck waren oftmals erhöht. Die VAS-Schmerz-Skala könnte ergänzend als Instrument zur ersten Quantifizierung der Krankheitsschwere angewandt werden. Internisten, Chirurgen, Allgemeinmediziner, Gynäkologen und Urologen sollten mit der Dermatose AI besser vertraut gemacht werden, um den Patienten eine schnellere, leitli- niengerechte Therapie zukommen zu lassen. AI-Patienten benötigen neben der dermato- logischen eventuell eine psychologische bzw. psychiatrische Therapie, um das Stressni- veau zu senken, was sich auf die Lebensqualität positiv auswirken könnte.
Background
Pemphigus vulgaris and pemphigus foliaceus are potentially life-threatening autoimmune disorders triggered by IgG autoantibodies against mucosal and epidermal desmogleins. There is an unmet need for fast-acting drugs that enable patients to achieve early sustained remission with reduced corticosteroid reliance.
Objectives
To investigate efgartigimod, an engineered Fc fragment that inhibits the activity of the neonatal Fc receptor, thereby reducing serum IgG levels, for treating pemphigus.
Methods
Thirty-four patients with mild-to-moderate pemphigus vulgaris or foliaceus were enrolled in an open-label phase II adaptive trial. In sequential cohorts, efgartigimod was dosed at 10 or 25 mg kg\(^{-1}\) intravenously with various dosing frequencies, as monotherapy or as add-on therapy to low-dose oral prednisone. Safety endpoints comprised the primary outcome. The study is registered at ClinicalTrials.gov (identifier NCT03334058).
Results
Adverse events were mostly mild and were reported by 16 of 19 (84%) patients receiving efgartigimod 10 mg kg\(^{-1}\) and 13 of 15 (87%) patients receiving 25 mg kg−1, with similar adverse event profiles between dose groups. A major decrease in serum total IgG and anti-desmoglein autoantibodies was observed and correlated with improved Pemphigus Disease Area Index scores. Efgartigimod, as monotherapy or combined with prednisone, demonstrated early disease control in 28 of 31 (90%) patients after a median of 17 days. Optimized, prolonged treatment with efgartigimod in combination with a median dose of prednisone 0·26 mg \(^{-1}\) per day (range 0·06–0·48) led to complete clinical remission in 14 of 22 (64%) patients within 2–41 weeks.
Conclusions
Efgartigimod was well tolerated and exhibited an early effect on disease activity and outcome parameters, providing support for further evaluation as a therapy for pemphigus.
Allergic disease are inflammatory disorders in which aberrant immune regulation occurs, and susceptible individuals mount allergen specific T helper 2 (Th2) responses, which drives disease pathology. Recent studies indicate that Th2 responses that are characteristic of allergic manifestations can be regulated by both naturally occurring CD4+CD25+ regulatory (Treg) cells and antigen-driven IL-10-secreting CD4+ regulatory T cells. Evidence is also emerging that successful Allergen specific immunotherapy (SIT) might work through the induction of IL-10-secreting regulatory T cells. In the first part of this work, I demonstrated the efficiency of allergen specific immunotherapy in the mouse model for allergic airway inflammation. Here I could show that intranasal administration of SIT abrogates allergic symptoms more efficiently, than the subcutaneous treatment. Furthermore, an IL-4/IL-13 (QY) inhibitor was used as an adjuvant for SIT, which has been demonstrated to have an anti-allergic potential, when administered prophylactically during allergic sensitization. However, the combination therapy with SIT and the inhibitory molecule QY did not show any significant enhancement in regards to all measured allergic parameters, when compared to monotherapy with SIT. These results provide the evidence, that shift from Th2 to Th1 cytokine profile might not be a key event in successful SIT. Subsequently, the investigation of immune mechanisms under successful SIT demonstrate that the increase of IL-10 secreting CD4+ T regulatory cells is associated with the suppression of airway inflammation in our mouse system, suggesting that these T cell subsets might be involved in the regulatory mechanisms of allergic disorders. In agreement with these findings is the second part of this work, where superagonistic a-CD28 mAb´s were used for the expansion of T regulatory cell subsets in our murine model for allergic airway inflammation. Here I could show, that the application of a-CD28 mAb during allergic sensitization, resulted in the establishment of a Th2 state, rather than a stimulation of a Treg cell population, supporting the Th2 promoting role of a-CD28 mAb together with TCR engagement. However, interesting findings were obtained by application of the superagonistic a-CD28 mAb in the challenge phase in established allergy. Conversely to the previous experiment, therapeutic administration of a-CD28 mAb lead to the generation of IL-10 secreting CD4+CD25+ T cell population in line with the induction of anti-allergic effects. Taking together the results of this study argue for the anti-inflammatory properties of T regulatory cells in allergic disease and highlights importance of these T cell subsets in the suppression of Th2 cell-driven response to allergen. Moreover, these observations suggest that the induction of IL-10 in vivo by T regulatory cells may represent a novel treatment strategy for allergic disorders.
Approximately half of all melanoma patients harbour activating mutations in the serine/threonine kinase BRAF. This is the basis for one of the main treatment strategies for this tumor type, the targeted therapy with BRAF and MEK inhibitors. While the initial responsiveness to these drugs is high, resistance develops after several months, frequently at sites of the previously responding tumor. This indicates that tumor response is incomplete and that a certain tumor fraction survives even in drug-sensitive patients, e.g., in a therapy-induced senescence-like state. Here, we show in several melanoma cell lines that BRAF inhibition induces a secretome with stimulating effect on fibroblasts and naive melanoma cells. Several senescence-associated factors were found to be transcribed and secreted in response to BRAF or MEK inhibition, among them members of the fibroblast growth factor family. We identified the growth factor FGF1 as mediator of resilience towards BRAF inhibition, which limits the pro-apoptotic effects of the drug and activates fibroblasts to secrete HGF. FGF1 regulation was mediated by the PI3K pathway and by FRA1, a direct target gene of the MAPK pathway. When FGFR inhibitors were applied in parallel to BRAF inhibitors, resilience was broken, thus providing a rationale for combined therapeutical application.
Background: Bowen’s disease (BD) of the nail unit is associated with human papillomavirus (HPV) infection. Objective: This study aimed to investigate the frequency of high-risk HPV infection, gender, age and digital distribution in this condition.
Methods: Biopsy specimens of 3 consecutive cases with periungual BD were investigated for the presence of HPV DNA by in situ hybridization and by polymerase chain reaction (PCR). Furthermore, 74 cases of ungual BD conducted with HPV genotyping as reported in the literature were reviewed.
Results: PCR of biopsy specimens revealed in 2 cases infection with HPV-16 and in 1 case with HPV-73. Additionally, in 1 HPV-16-positive case HPV-31/33 was detected by in situ hybridization. In line, review of the literature demonstrated a clear association of HPV-positive BD with high-risk HPV types. Interestingly, age at diagnosis was significantly lower in women. Whereas in both genders the second to fourth fingers on both hands were commonly diseased, only in men the thumbs were also prominently affected.
Conclusions: Infection with high-risk HPV types is common in BD of the nail unit suggesting the aetiological cause. Therefore, patients and partners should be closely followed up for digital and genital HPV-associated lesions.
Immune checkpoint blockade therapy is beneficial and even curative for some cancer patients. However, the majority don’t respond to immune therapy. Across different tumor types, pre-existing T cell infiltrates predict response to checkpoint-based immunotherapy. Based on in vitro pharmacological studies, mouse models and analyses of human melanoma patients, we show that the cytokine GDF-15 impairs LFA-1/β2-integrin-mediated adhesion of T cells to activated endothelial cells, which is a pre-requisite of T cell extravasation. In melanoma patients, GDF-15 serum levels strongly correlate with failure of PD-1-based immune checkpoint blockade therapy. Neutralization of GDF-15 improves both T cell trafficking and therapy efficiency in murine tumor models. Thus GDF-15, beside its known role in cancer-related anorexia and cachexia, emerges as a regulator of T cell extravasation into the tumor microenvironment, which provides an even stronger rationale for therapeutic anti-GDF-15 antibody development.
p53 is a central tumor suppressor protein and its inhibition is believed to be a prerequisite for cancer development. In approximately 50% of all malignancies this is achieved by inactivating mutations in the p53 gene. However, in several cancer entities, including melanoma, p53 mutations are rare. It has been recently proposed that tyrosinase related protein 2 (TRP2), a protein involved in melanin synthesis, may act as suppressor of the p53 pathway in melanoma. To scrutinize this notion we analyzed p53 and TRP2 expression by immunohistochemistry in 172 melanoma tissues and did not find any correlation. Furthermore, we applied three different TRP2 shRNAs to five melanoma cell lines and could not observe a target specific effect of the TRP2 knockdown on either p53 expression nor p53 reporter gene activity. Likewise, ectopic expression of TRP2 in a TRP2 negative melanoma cell line had no impact on p53 expression. In conclusion our data suggest that p53 repression critically controlled by TRP2 is not a general event in melanoma.
Merkel cell carcinoma (MCC) is a highly aggressive skin cancer with an increasing incidence. The understanding of the molecular carcinogenesis of MCC is limited. Here, we scrutinized the PI3K/AKT pathway, one of the major pathways activated in human cancer, in MCC. Immunohistochemical analysis of 41 tumor tissues and 9 MCC cell lines revealed high levels of AKT phosphorylation at threonine 308 in 88% of samples. Notably, the AKT phosphorylation was not correlated with the presence or absence of the Merkel cell polyoma virus (MCV). Accordingly, knock-down of the large and small T antigen by shRNA in MCV positive MCC cells did not affect phosphorylation of AKT. We also analyzed 46 MCC samples for activating PIK3CA and AKT1 mutations. Oncogenic PIK3CA mutations were found in 2/46 (4%) MCCs whereas mutations in exon 4 of AKT1 were absent. MCC cell lines demonstrated a high sensitivity towards the PI3K inhibitor LY-294002. This finding together with our observation that the PI3K/AKT pathway is activated in the majority of human MCCs identifies PI3K/AKT as a potential new therapeutic target for MCC patients.
IL-4 und IL-13 sind wichtige Faktoren bei der Entwicklung allergischer Erkrankungen. In dieser Arbeit wird die Rolle von IL-4 und IL-13 in einem Maus-Modell für allergisches Asthma während der allergischen Sensibilisierung und in einer etablierten asthmatischen Erkrankung untersucht. Weiterhin wird die Rolle von IL-4 und IL-13 in frühen Stadien der atopischen Dermatitis in einem Maus-Modell betrachtet. In einem Maus-Modell für allergisches Asthma mit anhaltender IgE-Synthese und einer persistierenden allergischen Atemwegspathologie konnte gezeigt werden, dass die Inhibition des IL-4/IL-13 Systems während der allergischen Sensibilisierung zu einer dosisabhängigen Reduktion der allergen-spezifischen IgE-Titer, zur Inhibition der Atemwegseosinophilie, zur Reduktion der IL-5-Spiegel in der BAL und zu einer gesenkten Anzahl von IL-4 sezernierenden CD4+ T-Zellen. Weiterhin konnte durch die Inhibition des IL-4/IL-13 Systems die Becherzellmetaplasie signifikant gesenkt werden. Die Inhibition des IL-4/IL-13 Systems nach der Entwicklung der allergischen Atemwegspathologie führte hingegen nicht zu einer signifikanten Reduktion der gemessenen Allergie-Parameter. Daraus lässt sich schließen, dass IL-4 und IL-13 nur eine untergeordnete Rolle in einer etablierten Allergie spielt. Diese Ergebnisse sind insbesondere wichtig, wenn man über das Verwendungspotential eines IL-4/IL-13-Inhibitors in der Allergie-Therapie bei asthmatischen Patienten spekuliert. Weiterhin konnte in dieser Arbeit gezeigt werden, dass die NC/Nga-Maus ein Modell für die humane atopische Dermatitis darstellt. NC/Nga Mäuse, die unter konventionellen Bedingungen gehalten wurden, entwickeln makroskopische und histologische Hautpathologien, die der humanen atopischen Dermatitis sehr ähneln. Weiterhin entwickeln unter konventionellen Bedingungen gehaltenen NC/Nga Mäuse hohe IgE-Titer im Serum, die mit einer erhöhten Produktion an Th2-Zytokinen verbunden war. Die Inhibition des IL-4/IL-13-Systems führte in diesem Modell jedoch nicht zu einer Reduktion von Symptomen und Pathologien der humanen atopischen Dermatitis. Deswegen kann man spekulieren, dass die Inhibition des IL-4/IL-13-Systems zu einem zu späten Zeitpunkt erfolgte. Des Weiteren kann eine nicht-standardisierte Sensibilisierung bei Mäusen, die in einer konventionellen Tierhaltung gehalten werden, zu einem sehr unterschiedlichen Ausbruch der Dermatitis führen. Deshalb werden weitere Tierversuche mit einer höheren Anzahl von Tieren, die zwischen den Würfen randomisiert werden, nötig sein, um die Rolle von IL-4 und IL-13 in der atopischen Dermatitis zu klären.
Cutaneous squamous cell carcinoma (cSCC) is a common malignancy of the skin and has an overall favorable outcome, except for patients with an advanced stage of the disease. The efficacy of checkpoint inhibitors (CPI) for advanced cSCC has been demonstrated in recent clinical studies, but data from real-world cohorts and trial-ineligible cSCC patients are limited. We retrospectively investigated patients with advanced cSCC who have been treated with CPI in a first-line setting at eight German skin cancer centers registered within the multicenter registry ADOReg. Clinical outcome parameters including response, progression-free (PFS) and overall survival (OS), time-to-next-treatment (TTNT), and toxicity were analyzed and have been stratified by the individual immune status. Among 39 evaluable patients, the tumor response rate (rwTRR) was 48.6%, the median PFS was 29.0 months, and the median OS was not reached. In addition, 9 patients showed an impaired immune status due to immunosuppressive medication or hematological diseases. Our data demonstrated that CPI also evoked tumor responses among immunocompromised patients (rwTRR: 48.1 vs. 50.0%), although these responses less often resulted in durable remissions. In line with this, the median PFS (11 vs. 40 months, p = 0.059), TTNT (12 months vs. NR, p = 0.016), and OS (29 months vs. NR, p < 0.001) were significantly shorter for this patient cohort. CPI therapy was well tolerated in both subcohorts with 15% discontinuing therapy due to toxicity. Our real-world data show that first-line CPI therapy produced strong and durable responses among patients with advanced cSCC. Immunocompromised patients were less likely to achieve long-term benefit from anti-PD1 treatment, despite similar tumor response rates.
Background
Healthcare workers and medical students faced new challenges during the COVID-19 pandemic. Processes within many hospitals were completely disrupted. In addition, the face to face teaching of medical students was drastically reduced. Those at risk of developing mental health problems appear to be younger health care workers and women.
Objective
To investigate potential COVID-19 pandemic-related gender differences in psychological distress among medical students and physicians in their first years of practice.
Design and setting
An anonymous survey was carried out online between December 1, 2021, and March 31, 2022, at the Mannheim Medical Faculty and the Würzburg Medical Faculty, Germany, after obtaining informed consent. Primary outcome measures were changes in anxiety and depression symptoms using the Hospital Anxiety and Depression Scale (HADS), and changes in participants' current quality of life using the WHO Quality of Life BREF.
Results
The results show wave-like courses for perceived anxiety and burden overlapping with the course of the COVID-19 incidence. In comparison to men, women showed a significant higher increase in HADS (p = 0.005) and a reduced life quality (p = 0.007) after COVID-19. Both sexes showed different frequencies of the factors influencing quality of life, with the presence of a previous mental illness and mean anxiety having a significant higher negative impact in women.
Conclusion
Future and young female physicians reported a disproportionate higher burden during COVID-19 compared to their male colleges. These observations suggest an increased need for support and prevention efforts especially in this vulnerable population.
Background
Apart from biologics, no systemic drugs are approved in Europe for children with moderate-to-severe psoriasis. Retrospective observational studies have shown promising results for fumaric acid esters (FAE) in this setting.
Objectives
To show superiority of FAE over placebo in terms of treatment response after 20 weeks in children and adolescents aged 10–17 years.
Methods
In a multicentre, randomized, double-blind, placebo-controlled phase IIIb study, patients aged 10–17 years with moderate-to-severe plaque psoriasis requiring systemic therapy were randomized 2 : 1 to receive FAE (n = 91) or placebo (n = 43) over 20 weeks, followed by an open-label FAE treatment phase. The coprimary endpoints were ≥ 75% improvement in Psoriasis Area and Severity Index (PASI 75) and Physician’s Global Assessment (PGA) score of 0 or 1 (clear or almost clear) at week 20. The study was registered with EudraCT number 2012-000035-82.
Results
At week 20, 55% [95% confidence interval (CI) 0·44–0·65] of FAE-treated patients achieved a PASI 75 response vs. 19% (95% CI 0·08–0·33) in the placebo group (absolute difference 36%, 95% CI 0·20–0·53; P < 0·001). In total, 42% (95% CI 0·32–0·53) in the FAE group vs. 7% (95% CI 0·01–0·19) in the placebo group achieved a PGA score of 0 or 1 at week 20 (absolute difference 35%, 95% CI 0·21–0·49; P < 0·001). During the double-blind period, drug-related adverse events occurred more frequently in patients receiving FAE compared with placebo (76% vs. 47%). Gastrointestinal disorders were the most common adverse events.
Conclusions
FAE administered over a period of 20 weeks demonstrated a better response than placebo; the difference was statistically significant and clinically meaningful. Application up to 40 weeks was generally well tolerated. However, further studies are required.
Skin Tumors in Childhood
(2011)
Background:
Dermatologists, paediatricians, and general practitioners are often consulted by worried parents for the evaluation of a cutaneous tumor.
Methods:
Selective literature review.
Results:
Only 1-2% of skin tumors excised in children turn out to be malignant when examined histologically. Warning signs of malignancy include rapid growth, firm consistency, diameter exceeding 3 cm, ulceration, a non-movable mass, and presence in the neonatal period. The more common malignant skin tumors in adults-basal cell carcinoma, cutaneous squamous cell carcinoma, and melanoma-are very rare in childhood. Congenital melanocytic nevi and sebaceous nevi bear a lower malignant potential than previously believed; nevertheless, their excision is often indicated. A Spitz nevus can mimic a melanoma both clinically and histologically. Some benign skin tumors of childhood tend to regress spontaneously within a few years but may cause complications at particular locations and when multiple. For infantile hemangiomas requiring systemic treatment because of imminent obstruction or ulceration, propranolol seems to have a far more favorable risk-benefit ratio than corticosteroids.
Conclusion:
Physicians need specialized knowledge in order to decide whether a skin tumor in a child should be excised, non-surgically treated, or further evaluated, or whether it can be safely left untreated because of the likelihood of spontaneous remission.
Die Todesrezeptoren der TNF-Familie sind neben der Vermittlung von Apoptosesignalen auch in der Lage, nicht-apoptotische intrazelluläre Signalwege zu beeinflussen. Der Caspase-8-Inhibitor cFLIPlong inhibiert dosisabhängig die Prozessierung der Initiator-Caspase-8 am TRAIL-DISC (death inducing signalling complex) und hemmt die Aktivierung des NF-kappa-B-Signalweges über die Modulation der Rekrutierung und Spaltung des für die NF-kappa-B-Aktivierung notwendigen RIP (receptor interactin protein)am DISC.
Obwohl die Behandlung mit Penicillinen zu den effektivsten und sichersten Antibiotika-Therapien zählt, treten bei dieser Stoffklasse, verglichen mit anderen Antibiotika-Gruppen, häufiger Allergien auf. Zurzeit gilt in der Diagnostik von ß-Lactam-Antibiotika-Allergien eine Kombination aus Hauttests und einer anschließenden oralen Exposition – bei negativem Hauttestbefund – als Goldstandard. Daneben wurden auch nicht-invasive in-vitro Methoden als weitere Bausteine der Allergiediagnostik von Arzneimittelreaktionen entwickelt. Zu ihnen zählt unter anderem der Lymphozytentransformationstest (LTT).
In der vorliegenden Arbeit sollte untersucht werden, wie sich eine zusätzliche Stimulation der Zellen mit dem Antikörper gegen CD3/CD28 auf die Ergebnisse des LTT aus-wirkt. Als Kenngrößen wurden die Sensitivität und Spezifität des konventionellen und des modifizierten LTT verglichen. Damit soll analysiert werden, ob ein modifizierter LTT im klinischen Alltag zur erweiterten Diagnostik angewandt werden kann.
In dieser prospektiven Studie wurden 37 Patienten mit dem Verdacht auf eine Aminopenicillin-Allergie zusätzlich zur standardisierten allergologischen Diagnostik mit dem Lymphozytentransformationstest (LTT) untersucht. Mit den Haut- und Expositionstestungen konnte bei 11 der 37 Patienten eine Spättypallergie gegen Aminopenicilline / Pencillin G/V diagnostiziert werden.
Die Sensitivität des konventionellen LTT für die Allergiediagnose betrug 63,6 %. Im kostimulierten LTT wurde die Sensitivität durch die Testmodifikation auf 81,8 % gesteigert. Bei 26 Patienten wurde eine Aminopenicillin-Allergie durch negative Hauttests und anschließende negative Expositionstests definitiv ausgeschlossen. Die errechnete Spezifität liegt bei 92,3 %. Der Anteil fasch-positiver LTT-Ergebnisse stieg durch den Zusatz von Antikörpern gegen CD3/CD28 an, die Spezifität betrug somit nur noch 76,9 %.
Prinzipiell ist der LTT eine geeignete Methode zur Diagnose von Typ IV-Sensibilisierungen gegen Aminopenicilline. Die Testergebnisse sollten aber immer im Kontext mit anderen etablierten allergologischen Testverfahren interpretiert werden. Die Frage, ob der modifizierte LTT dem konventionellen LTT überlegen ist, lässt sich anhand der erhobenen Daten nicht eindeutig beantworten. Während die beobachtete Steigerung der Sensitivität für die Variante mit den Antikörpern CD3/CD28 spricht, erweist sich die geringere Spezifität dieser Testmodifikation als nachteilig. Insgesamt ist aufgrund der hohen Spezifität der konventionelle LTT dem modifizierten LTT als Testmethode überlegen. Der LTT könnte bei Patienten, bei denen Expositionstests kontraindiziert sind, als Alternativmethode dienen. Zum sicheren Ausschluss einer Penicillin-Allergie bleibt aber auch in Zukunft die kontrollierte Expositionstestung unverzichtbar.
Zellmigration ist essentiell für die Invasion und Metastasierung maligner Tumore. Neben der Bewegung von Einzelzellen zeigen Tumore sowohl epithe¬lialen als auch mesenchymalen Ursprungs auch kollektive Migration und Invasion multizellulärer Zellverbände, die sich unter Beibehaltung von Zell-Zell-Adhäsionen koordiniert als Gruppe bewegen. Ziel der Arbeit war, primäre humane Melanomexplantate mittels organotypischer Kultur in 3D Kollagenmatrices einzusetzen, um mittels Zeit-raffermikroskopie und experimentellen Blockadestrategien die zellulären und molekularen Grundlagen kollektiver Migration darzustellen, insbesondere die Bedeutung von Zell-Matrix-Interaktionen und Integrinen. In 3D Explantatkulturen bildeten primäre Melanomexplantate reproduzierbar Invasionszonen und sich ablösende und kollektiv wandernde Zellcluster aus. Diese zeichneten sich durch eine ausgeprägte Polarität mit motiler Vorderfront mit zugartig reorientierten Kollagenfasern und nachgezogenem hinteren Teil der Gruppen aus, vergleichbar der Asymmetrie haptokinetisch migrierender Fibroblasten. β1 Integrine zeigten ein heterogenes Verteilungsmuster mit Fokalisierung an Zell-Matrix-Interaktionen vor allem an der Vorderfront und linearer Anordnung entlang der Zell-Zell-Grenzen. Adhäsionsblockierende anti- β1 Integrin-Antikörper bewirkten nahezu vollständige Hemmung der kollektiven Migration, mit Verlust der Zellgruppenpolarität und Migrationspersistenz. Nach Integrinblockade zerfielen Zellverbände infolge Loslösung von Einzelzellen, die sich mittels β1 Integrin-unabhängiger, amöboider Migration durch die Kollagenmatrix bewegten. Der Übergang von β1 Integrin-abhängiger, kollektiver Migration zu amöboider Einzelzellwanderung (kollektiv-amöboide Transition) ist ein Beispiel für die Plastizität von Tumorzellwanderung, die in Anpassung an das Milieu einen Wechsel der Migrationsstrategie erlaubt. Die Plastizität der Tumorzellmigration muss bei der Entwicklung therapeutischer Konzepte, die auf Hemmung von Tumorinvasion und -metastasierung abzielen, berücksichtigt werden.
Psoriasis is an immune-mediated systemic inflammatory disease that is not limited to the skin but may be associated with arthritis, cardiovascular diseases, metabolic syndrome including diabetes and obesity and, as identified more recently, non-alcoholic fatty liver disease (NAFLD) that occurs in approximately 50 % of all patients with psoriasis. NAFLD is characterized by accumulation of fat in hepatocytes in the absence of excessive alcohol consumption. Over the last two decades, NAFLD has developed to the most common chronic liver disease with an estimated prevalence of 25 % in the Western population. NAFLD ranges from non-inflammatory or bland hepatic steatosis to inflammation of hepatic tissue (non-alcoholic steatohepatitis, NASH) and consecutive liver fibrosis. It is controversial whether the underlying systemic inflammation of psoriasis is contributing to development of NAFLD or if comorbid diseases such as obesity enhance NAFLD development. Recent findings indicate that cytokine-mediated inflammation through TNFα, interleukin (IL)-6 and IL-17 might be the common link between psoriasis and NAFLD. Considering the shared inflammatory pathways, IL-17 pharmacological blockade, which is already well-established for psoriasis, may be a promising strategy to treat both psoriasis and NAFLD. Therefore, early detection of NAFLD and a better understanding of its pathophysiology in the context of the systemic inflammation in psoriasis is important with regard to individualized treatment approaches.
Pathogenic relevance of autoantibodies to type XVII collagen from pemphigoid gestationis patients
(2007)
Pemphigoid gestationis (PG) and bullous pemphigoid (BP) are subepidermal autoimmune blistering diseases characterized by self-reactive T and B cells specific for the transmembrane hemidesmosomal protein type XVII collagen/BP180. Major T and B cell epitopes are located within the immunodominant 16th non-collagenous domain A (NC16A) of type XVII collagen. It has been suggested that pathogenically relevant autoantibodies also bind to this immunodominant region. The aim of this study was to map the epitopes targeted by blister-inducing human autoantibodies. For this purpose, we used an in vitro model of autoantibody-induced leucocyte-dependent dermal-epidermal separation. In contrast to the majority of patients with BP (7 of 10), preadsorption against a recombinant form of the NC16A region abolished the blister-inducing potential of autoantibodies from all PG patients tested (n=5). Using overlapping synthetic peptides, we demonstrate that PG autoantibodies bind to 2 defined epitopes within the NC16A region (aa 500-514 and aa 511-523). Preadsorption using an affinity matrix containing these two epitopes completely abolished dermal-epidermal separation induced by PG autoantibodies (in 8 of 9 patients). These findings provide new insights into the pathogenesis of pemphigoid diseases and should prove helpful for the development of an antigen-specific immunoadsorption therapy in PG.
The pocket protein (PP) family consists of the three members RB1, p107 and p130 all possessing tumor suppressive properties. Indeed, the PPs jointly control the G1/S transition mainly by inhibiting E2F transcription factors. Notably, several viral oncoproteins are capable of binding and inhibiting PPs. Merkel cell polyomavirus (MCPyV) is considered as etiological factor for Merkel cell carcinoma (MCC) with expression of the viral Large T antigen (LT) harboring an intact PP binding domain being required for proliferation of most MCC cells. Therefore, we analyzed the interaction of MCPyV-LT with the PPs. Co-IP experiments indicate that MCPyV-LT binds potently only to RB1. Moreover, MCPyV-LT knockdown-induced growth arrest in MCC cells can be rescued by knockdown of RB1, but not by p107 or p130 knockdown. Accordingly, cell cycle arrest and E2F target gene repression mediated by the single PPs can only in the case of RB1 be significantly reverted by MCPyV-LT expression. Moreover, data from an MCC patient indicate that loss of RB1 rendered the MCPyV-positive MCC cells LT independent. Thus, our results suggest that RB1 is the dominant tumor suppressor PP in MCC, and that inactivation of RB1 by MCPyV-LT is largely sufficient for its growth supporting function in established MCPyV-positive MCC cells.
The incidence of melanoma and nonmelanoma skin cancer has increased tremendously in recent years. Although novel treatment options have significantly improved patient outcomes, the prognosis for most patients with an advanced disease remains dismal. It is, thus, imperative to understand the molecular mechanisms involved in skin carcinogenesis in order to develop new targeted treatment strategies. Receptor tyrosine kinases (RTK) like the ERBB receptor family, including EGFR/ERBB1, ERBB2/NEU, ERBB3, and ERBB4, are important regulators of skin homeostasis and their dysregulation often results in cancer, which makes them attractive therapeutic targets. Members of the leucine‐rich repeats and immunoglobulin‐like domains protein family (LRIG1‐3) are ERBB regulators and thus potential therapeutic targets to manipulate ERBB receptors. Here, we analyzed the function of LRIG1 during chemically induced skin carcinogenesis in transgenic mice expressing LRIG1 in the skin under the control of the keratin 5 promoter (LRIG1‐TG mice). We observed a significant induction of melanocytic tumor formation in LRIG1‐TG mice and no difference in papilloma incidence between LRIG1‐TG and control mice. Our findings also revealed that LRIG1 affects ERBB signaling via decreased phosphorylation of EGFR and increased activation of the oncoprotein ERBB2 during skin carcinogenesis. The epidermal proliferation rate was significantly decreased during epidermal tumorigenesis under LRIG1 overexpression, and the apoptosis marker cleaved caspase 3 was significantly activated in the epidermis of transgenic LRIG1 mice. Additionally, we detected LRIG1 expression in human cutaneous squamous cell carcinoma and melanoma samples. Therefore, we depleted LRIG1 in human melanoma cells (A375) by CRISPR/Cas9 technology and found that this caused EGFR and ERBB3 downregulation in A375 LRIG1 knockout cells 6 h following stimulation with EGF. In conclusion, our study demonstrated that LRIG1‐TG mice develop melanocytic skin tumors during chemical skin carcinogenesis and a deletion of LRIG1 in human melanoma cells reduces EGFR and ERBB3 expression after EGF stimulation.
Die Bienen-/Wespengiftallergie ist auf der einen Seite eine potentiell lebensbedrohliche IgE-vermittelte Allergiekrankheit, in Deutschland neben den Nahrungsmittelallergien die häufigste Ursache für eine tödlich verlaufende Anaphylaxie. Auf der anderen Seite steht mit der Bienen-/Wespengift-spezifischen Immuntherapie (SIT) gerade für diese Allergie seit Jahrzehnten eine hochwirksame kausale Therapie zur Verfügung. Placebokontrollierte Studien mit unbehandelten Patienten sind daher aus ethischen Gründen nicht vertretbar. Neue Erkenntnisse zur Sicherheit dieser Therapieform können nur aus der Verlaufsbeobachtung standardisiert behandelter Patientenkollektive gewonnen werden. Der besondere Wert der hier analysierten großen Patientenserie liegt vor allem darin, dass alle Patienten in einer Allergieambulanz (der Klinik und Poliklinik für Dermatologie, Venerologie und Allergologie) betreut wurden. Im gesamten Behandlungszeitraum aller 679 Patienten wurde die Diagnostik und Therapie der Bienen-/Wespengiftallergie hoch standardisiert durchgeführt und nicht verändert. Die dadurch gleichbleibende Betreuung garantierten Qualität, Umfang und Homogenität der Dokumentation und damit die Vergleichbarkeit der retrospektiv erfassten Daten über den gesamten Zeitraum 1988 bis 2008. Für die besonders wichtige Verlaufsbeobachtung nach Ende der spezifischen Immuntherapie (SIT) wurden zusätzlich 616 der 679 Patienten aus Unterfranken und Umgebung direkt telefonisch befragt. Die bekannten charakteristischen Merkmale von Patienten mit Bienen-/Wespengiftallergie zeigten sich auch in dem untersuchten Kollektiv. Imkertätigkeit ist die wahrscheinlichste Erklärung warum Bienengiftallergiker jünger und häufiger männlich sind. Die prognostisch bedeutsamen Schweregrade der allergischen Indikatorstichreaktion (das Stichereignis mit der schwersten anaphylaktischen Reaktion vor SIT) unterscheiden sich zwischen Bienen- und Wespengiftallergikern dagegen nicht. In den diagnostischen Untersuchungen vor und auch am Ende der SIT waren die Schwellenwertkonzentrationen des Intrakutan- und Pricktests bei Bienengiftallergikern im Vergleich zu den Wespengiftallergikern signifikant niedriger, die spezifischen IgE-Serumspiegel höher. Die Wirksamkeit der SIT mit Bienengift betrug 89,0 %. Nur 11,0 % der Patienten (8 von 73 Patienten mit erneutem Bienenstich) hatten nach Beginn der SIT erneut eine
Asthma bronchiale ist eine chronische, entzündliche Erkrankung der Atemwege, charakterisiert durch bronchiale Hyperreaktivität und variable Atemwegs-obstruktion. Die Interleukine 4 und 13 sind entscheidend an den pathophysiologischen Vor-gängen beim allergischen Asthma bronchiale beteiligt. IL-4 gilt als spezifisches Zytokin für die Differenzierung von nativen T-Helferzellen zu TH2-Zellen. Gemeinsam mit IL-13 führt es zum Immunglobulinklassenswitch der B-Zellen. Ziel dieser Arbeit war es, in einem etablierten Mausmodell für allergisches Asthma verschiedene Applikationsformen des IL-4/IL-13-Antagonisten QY in ihrer Wirkung während der allergischen Sensibilisierung zu vergleichen. Dazu wurden Balb/c-Mäuse über einen Zeitraum von 6 Wochen wöchentlich mit 50µg OVA sensibilisiert. In zwei Therapiegruppen wurden zu jeder Sensibilisierung jeweils 10µg QY intranasal bzw. intraperitoneal verabreicht. Wöchentlich wurde das Serum der Versuchstiere auf allergenspezifische Antikörper untersucht. Nach sechs Wochen wurde eine bronchoalveoläre Lavage durchgeführt, um den Zytokingehalt und die allergeninduzierte Eosinophilie zu bestimmen. Sowohl die intranasale als auch die intraperitoneale Gabe von QY resultierte in einer signifikanten Abnahme allergenspezifischer IgE-Antikörper im Serum der Versuchstiere. Ebenso konnten die Zahl der inflammativen eosinophilen Granu-lozyten und der IL-5-Spiegel in der BAL signifikant gesenkt werden. Zusammenfassend wurde gezeigt, dass die prophylaktische Behandlung mit dem IL-4/IL-13-Antagonisten QY zuverlässig eine allergische Sensibilisierung der Versuchstiere verhindert. Die intranasale und intraperitoneale Applikation unterscheiden sich hierbei praktisch nicht in ihrer Wirksamkeit.
Pigment cells and neuronal cells both are derived from the neural crest. Here, we describe the Pit-Oct-Unc (POU) domain transcription factor Brn3a, normally involved in neuronal development, to be frequently expressed in melanoma, but not in melanocytes and nevi. RNAi-mediated silencing of Brn3a strongly reduced the viability of melanoma cell lines and decreased tumour growth in vivo. In melanoma cell lines, inhibition of Brn3a caused DNA double-strand breaks as evidenced by Mre11/Rad50-containing nuclear foci. Activated DNA damage signalling caused stabilization of the tumour suppressor p53, which resulted in cell cycle arrest and apoptosis. When Brn3a was ectopically expressed in primary melanocytes and fibroblasts, anchorage-independent growth was increased. In tumourigenic melanocytes and fibroblasts, Brn3a accelerated tumour growth in vivo. Furthermore, Brn3a cooperated with proliferation pathways such as oncogenic BRAF, by reducing oncogene-induced senescence in non-malignant melanocytes. Together, these results identify Brn3a as a new factor in melanoma that is essential for melanoma cell survival and that promotes melanocytic transformation and tumourigenesis.
Background
Severe acute respiratory syndrome coronavirus 2 is a virus affecting different organs and causing a wide variety and severity of symptoms. Headache as well as loss of smell and taste are the most frequently reported neurological manifestations of coronavirus disease 2019 induced by severe acute respiratory syndrome coronavirus 2. Here we report on a patient with chronic migraine and medication overuse headache, who experienced remarkable mitigation of migraine following coronavirus disease 2019.
Case presentation
For many years prior to the severe acute respiratory syndrome coronavirus 2 infection, a 57-year-old Caucasian male suffered from very frequent migraine attacks and for control of headaches he had been taking triptans almost daily. In the 16-month period before the outbreak of coronavirus disease 2019, triptan was taken 98% of the days with only a 21-day prednisolone-supported triptan holiday, which, however, had no longer-lasting consequences on migraine frequency. Upon severe acute respiratory syndrome coronavirus 2 infection, the patient developed only mild symptoms including fever, fatigue, and headache. Directly following recovery from coronavirus disease 2019, the patient surprisingly experienced a period with largely reduced frequency and severity of migraine attacks. Indeed, during 80 days following coronavirus disease 2019, migraine as well as triptan usage were restricted to only 25% of the days, no longer fulfilling criteria of a chronic migraine and medication overuse headache.
Conclusion
Severe acute respiratory syndrome coronavirus 2 infection might be capable of triggering mitigation of migraine.
Merkel cell carcinoma (MCC) is frequently caused by the Merkel cell polyomavirus (MCPyV), and MCPyV-positive tumor cells depend on expression of the virus-encoded T antigens (TA). Here, we identify 4-[(5-methyl-1H-pyrazol-3-yl)amino]-2H-phenyl-1-phthalazinone (PHT) — a reported inhibitor of Aurora kinase A — as a compound inhibiting growth of MCC cells by repressing noncoding control region (NCCR)-controlled TA transcription. Surprisingly, we find that TA repression is not caused by inhibition of Aurora kinase A. However, we demonstrate that β-catenin — a transcription factor repressed by active glycogen synthase kinase 3 (GSK3) — is activated by PHT, suggesting that PHT bears a hitherto unreported inhibitory activity against GSK3, a kinase known to function in promoting TA transcription. Indeed, applying an in vitro kinase assay, we demonstrate that PHT directly targets GSK3. Finally, we demonstrate that PHT exhibits in vivo antitumor activity in an MCC xenograft mouse model, suggesting a potential use in future therapeutic settings for MCC.
The best characterized polyomavirus family member, i.e., simian virus 40 (SV40), can cause different tumors in hamsters and can transform murine and human cells in vitro. Hence, the SV40 contamination of millions of polio vaccine doses administered from 1955–1963 raised fears that this may cause increased tumor incidence in the vaccinated population. This is, however, not the case. Indeed, up to now, the only polyomavirus family member known to be the most important cause of a specific human tumor entity is Merkel cell polyomavirus (MCPyV) in Merkel cell carcinoma (MCC). MCC is a highly deadly form of skin cancer for which the cellular origin is still uncertain, and which appears as two clinically very similar but molecularly highly different variants. While approximately 80% of cases are found to be associated with MCPyV the remaining MCCs carry a high mutational load. Here, we present an overview of the multitude of molecular functions described for the MCPyV encoded oncoproteins and non-coding RNAs, present the available MCC mouse models and discuss the increasing evidence that both, virus-negative and -positive MCC constitute epithelial tumors.
Merkel cell carcinoma (MCC) is an aggressive skin cancer frequently caused by the Merkel cell polyomavirus (MCPyV), and proliferation of MCPyV-positive MCC tumor cells depends on the expression of a virus-encoded truncated Large T antigen (LT) oncoprotein. Here, we asked in which phases of the cell cycle LT activity is required for MCC cell proliferation. Hence, we generated fusion-proteins of MCPyV-LT and parts of geminin (GMMN) or chromatin licensing and DNA replication factor1 (CDT1). This allowed us to ectopically express an LT, which is degraded either in the G1 or G2 phase of the cell cycle, respectively, in MCC cells with inducible T antigen knockdown. We demonstrate that LT expressed only in G1 is capable of rescuing LT knockdown-induced growth suppression while LT expressed in S and G2/M phases fails to support proliferation of MCC cells. These results suggest that the crucial function of LT, which has been demonstrated to be inactivation of the cellular Retinoblastoma protein 1 (RB1) is only required to initiate S phase entry.
Background: Inactivation of the p53 pathway that controls cell cycle progression, apoptosis and senescence, has been proposed to occur in virtually all human tumors and p53 is the protein most frequently mutated in human cancer. However, the mutational status of p53 in melanoma is still controversial; to clarify this notion we analysed the largest series of melanoma samples reported to date. Methodology/Principal Findings: Immunohistochemical analysis of more than 180 melanoma specimens demonstrated that high levels of p53 are expressed in the vast majority of cases. Subsequent sequencing of the p53 exons 5–8, however, revealed only in one case the presence of a mutation. Nevertheless, by means of two different p53 reporter constructs we demonstrate transcriptional inactivity of wild type p53 in 6 out of 10 melanoma cell lines; the 4 other p53 wild type melanoma cell lines exhibit p53 reporter gene activity, which can be blocked by shRNA knock down of p53. Conclusions/Significance: In melanomas expressing high levels of wild type p53 this tumor suppressor is frequently inactivated at transcriptional level.
Bullous pemphigoid is the most common autoimmune blistering disease in industrialized countries and particularly affects the elderly. In this patient population, comorbid diseases are frequent and may complicate management and treatment of bullous pemphigoid. A better understanding why distinct diseases are more frequent in bullous pemphigoid patients may lead to new pathophysiological insights and - as a consequence - result in better patient care. The association of bullous pemphigoid with neurological and psychiatric diseases is well known and confirmed by several case-control studies. Association with further diseases such as malignancy and metabolic diseases are still discussed controversially. In recent years new relationships between bullous pemphigoid and autoimmune as well as inflammatory skin diseases have been reported. This review provides a systematic overview on studies addressing comorbidity in bullous pemphigoid patients. Increasing the awareness of both, common and rare comorbid diseases, may enable clinicians to optimize patient support and individualized treatment of bullous pemphigoid.
Im Rahmen der vorliegenden Arbeit wurden sämtliche histologischen Schnittpräparate mit Naevus sebaceus der Universitäts-Hautklinik Würzburg des Zeitraums 1996 bis 2005 auf die Ausprägung histologischer Merkmale sowie die Entstehung von Sekundärproloferationen untersucht. Klinische Daten wurden den Patientenakten entnommen. In der Einleitung wird eine genaue Beschreibung der Entität Naevus sebaceus sowie eine historische Abhandlung gegeben. Im Folgenden werden Material und Methoden des Vorgehens sowie die Ergebnisse beschrieben. Von klinischer Seite werden Lokalisation, Manifestationsalter, klinische Veränderung, Farbe, Größe, Linearität, etc. sowie von histologischer Seite die Ausprägung der Merkmale des Naevus sebaceus in Abhängigkeit vom Alter des Patienten und v.a. die genauen Daten zu Sekundärtumoren beleuchtet. Diese Ergebnisse werden in der Diskussion mit denen früherer Arbeiten verglichen. Eine Zusammenfassung sowie ein ausführlicher Bildanhang schließen sich an.
Cutaneous metastatic Crohn’s disease (MCD) is a rare but challenging dermatologic manifestation of Crohn’s disease. It is histologically defined as the presence of non-caseating granulomas at skin sites separated from and non-contiguous to the gastrointestinal tract. Cutaneous metastatic Crohn’s disease should be distinguished from the much more frequent contiguous cutaneous manifestations of Crohn’s disease that present at perianal or, less common, peristomal sites with direct extension from the intestine to the adjacent skin. Versatile clinical presentation and the fact that occurrence can predate the initial diagnosis of Crohn’s disease may lead to misdiagnosis, delayed treatment and underreporting. As case numbers are small and randomized controlled studies on management are lacking, the therapeutic approach remains challenging and is often unsatisfactory. We here performed a systematic literature search identifying 264 published pediatric and adult cases of MCD and additionally report three of our own cases. Our review summarizes clinical characteristics, putative etiopathology, histologic findings, differential diagnoses and treatment options for MCD.
Simple Summary
In melanoma patients treated with dabrafenib and trametinib, dose reductions and treatment discontinuations related to adverse events (AE) occur frequently. However, the associations between patient characteristics, AE, and exposure are unclear. Our prospective study analyzed serum (hydroxy-)dabrafenib and trametinib exposure and investigated its association with toxicity and patient characteristics. Additionally, the feasibility of at-home sampling of capillary blood was assessed, and a model to convert capillary blood concentrations to serum concentrations was developed. (Hydroxy-)dabrafenib or trametinib exposure was not associated with age, sex, body mass index, or AE. Co-medication with P-glycoprotein inducers was associated with lower trough concentrations of trametinib but not (hydroxy-)dabrafenib. The applicability of the self-sampling of capillary blood was demonstrated. Our conversion model was adequate for estimating serum exposure from micro-samples. The monitoring of dabrafenib and trametinib may be useful for dose modification and can be optimized by at-home sampling and our new conversion model.
Abstract
Patients treated with dabrafenib and trametinib for BRAF\(^{V600}\)-mutant melanoma often experience dose reductions and treatment discontinuations. Current knowledge about the associations between patient characteristics, adverse events (AE), and exposure is inconclusive. Our study included 27 patients (including 18 patients for micro-sampling). Dabrafenib and trametinib exposure was prospectively analyzed, and the relevant patient characteristics and AE were reported. Their association with the observed concentrations and Bayesian estimates of the pharmacokinetic (PK) parameters of (hydroxy-)dabrafenib and trametinib were investigated. Further, the feasibility of at-home sampling of capillary blood was assessed. A population pharmacokinetic (popPK) model-informed conversion model was developed to derive serum PK parameters from self-sampled capillary blood. Results showed that (hydroxy-)dabrafenib or trametinib exposure was not associated with age, sex, body mass index, or toxicity. Co-medication with P-glycoprotein inducers was associated with significantly lower trough concentrations of trametinib (p = 0.027) but not (hydroxy-)dabrafenib. Self-sampling of capillary blood was feasible for use in routine care. Our conversion model was adequate for estimating serum PK parameters from micro-samples. Findings do not support a general recommendation for monitoring dabrafenib and trametinib but suggest that monitoring can facilitate making decisions about dosage adjustments. To this end, micro-sampling and the newly developed conversion model may be useful for estimating precise PK parameters.
The transcription factor NRF2 is the major mediator of oxidative stress responses and is closely connected to therapy resistance in tumors harboring activating mutations in the NRF2 pathway. In melanoma, such mutations are rare, and it is unclear to what extent melanomas rely on NRF2. Here we show that NRF2 suppresses the activity of the melanocyte lineage marker MITF in melanoma, thereby reducing the expression of pigmentation markers. Intriguingly, we furthermore identified NRF2 as key regulator of immune-modulating genes, linking oxidative stress with the induction of cyclooxygenase 2 (COX2) in an ATF4-dependent manner. COX2 is critical for the secretion of prostaglandin E2 and was strongly induced by H\(_2\)O\(_2\) or TNFα only in presence of NRF2. Induction of MITF and depletion of COX2 and PGE2 were also observed in NRF2-deleted melanoma cells in vivo. Furthermore, genes corresponding to the innate immune response such as RSAD2 and IFIH1 were strongly elevated in absence of NRF2 and coincided with immune evasion parameters in human melanoma datasets. Even in vitro, NRF2 activation or prostaglandin E2 supplementation blunted the induction of the innate immune response in melanoma cells. Transcriptome analyses from lung adenocarcinomas indicate that the observed link between NRF2 and the innate immune response is not restricted to melanoma.
Die Einführung von zielgerichteter Therapie und Immuntherapie hat die Behandlungsmöglichkeiten des Melanoms revolutioniert. Jedoch profitieren viele Patienten nicht langfristig von diesen Therapien. Derzeit werden klinische Studien durchgeführt, die zielgerichtete Therapie und Immuntherapie miteinander kombinieren.
In dieser Arbeit wurden in vitro Untersuchungen an den drei BRAF-V600E-mutieren Melanomzelllinien UACC 257, Malme 3M und Sk-Mel 5 unter kombinierter MAPK-Inhibitortherapie durchgeführt. Es wurden die aus der klinischen Routine bekannten Kombinationen aus BRAF- und MEK-Inhibitor – Vemurafenib und Cobimetinib, Dabrafenib und Trametinib sowie Encorafenib und Binimetinib – verwendet. Es wurde untersucht, ob obige zielgerichtete Therapeutika einen Effekt auf immunologische Marker im Melanom haben und ob sich eine der Kombinationen in ihrer Wirkung signifikant von den übrigen unterscheidet.
Mittels MTS-Assay und Zellzyklusanalysen konnte eine konzentrationsabhängige Wirkung der Inhibitoren gezeigt und in ihrer Wirkung vergleichbare Inhibitorkonzentrationen eingestellt werden. Unter kombinierter MAPK-Inhibitortherapie zeigte sich ein begrenzter Effekt auf die theoretische Immunogenität des Melanoms. So konnte eine erhöhte MHC-I-Expression (+14 %) und eine verminderte PD-L1-Expression (-24 %) gezeigt werden. Die gewählten Dosen an Inhibitoren induzierten keinen ER-Stress. Ebenso konnte keine Ekto-Calreticulin-Expression auf lebenden Zellen nachgewiesen werden. Zwischen den drei Inhibitorkombinationen zeigten sich keine signifikanten Unterschiede.
Die in dieser Arbeit gezeigten begrenzten immunologischen Effekte unter kombinierter MAPK-Inhibitortherapie legen nahe, dass eine Kombination mit Immuntherapie in Teilen synergistisch wirken könnte. Hier sind die Ergebnisse weiterer Studien abzuwarten, die zielgerichtete und Immuntherapie miteinander kombinieren, um ein tiefgreifenderes Verständnis bzgl. etwaiger Synergien zu generieren. Da zwischen den Inhibitorkombinationen keine signifikanten Unterschiede hinsichtlich ihrer Wirkung auf die Immunogenität des Melanoms gefunden wurden, ist anzunehmen, dass sie sich grundsätzlich alle gleichermaßen für eine Kombination mit einer Immuntherapie eignen. Die gezeigte MHC-I-Erhöhung trat bereits bei geringen Inhibitorkonzentrationen auf. Möglicherweise genügt bei einer Kombination mit Immuntherapie bereits eine niedrige Dosis der zielgerichteten Therapie, um die Immuntherapie zu boostern. Um die Frage nach einer möglichen Kombinationstherapie fortwährend zu analysieren, sollten zusätzliche Aspekte der Immunogenität unter kombinierter MAPK-Inhibitortherapie untersucht und die Inhibitortitration zum Vergleich der zielgerichteten Therapeutika weiter präzisiert werden.
Pruritus tritt verstärkt bei älteren Menschen auf und ist mit vielen verschiedenen Dermatosen unterschiedlichen Ursprungs vergesellschaftet. Pruritus und ein fortgeschrittenes Lebensalter sind auch charakteristisch für die häufigste blasenbildende Autoimmundermatose, das bullöse Pemphigoid. Im prämonitorischen Stadium treten häufig nur Juckreiz und unspezifische Hautveränderungen auf. Das Prodromalstadium eines bullösen Pemphigoids dauert wenige Wochen bis zu mehreren Jahren.
Ziel dieser Arbeit war es, die pruriginösen Erkrankungen Prurigo simplex subacuta [L28.2], Prurigo nodularis [L28.1], eosinophilenreiche Dermatitis [L30.8] und Prurigoform eines atopischen Ekzems [L20.0] im Hinblick auf das klinische, laborchemische und histologische Bild bei der Erstdiagnose der Erkrankungen auszuwerten. Insbesondere sollte überprüft werden, ob bei der Erstdiagnose typische Autoantikörper einer subepidermalen blasenbildenden Autoimmundermatose (BP180, BP230) nachgewiesen werden konnten und trotz des letzendlich ungewöhnlichen Erscheinungsbildes letztlich ein bullöses Pemphigoid vorgelegen haben könnte.
Es erfolgte eine retrospektive Auswertung der oben genannten pruriginösen Erkrankungen, die über einen Zeitraum von über 10 Jahren in der Klinik für Dermatologie, Venerologie und Allergologie des Universitätsklinikums Würzburg behandelt wurden. Die Patienten wurden gemäß ICD-Kodierung in die vier oben genannten Gruppen unterteilt. Nebst Patientencharakteristika wurden die Parameter direkte Immunfluoreszenz (DIF), indirekte Immunfluoreszenz (IIF), ELISA-Testverfahren, Immunoblot, eosinophile Granulozyten, Gesamt-IgE, histologische Untersuchung, Dermographismus und Blasenbildung ausgewertet.
Es konnten insgesamt 325 Patienten in die Studie eingeschlossen werden, bei denen bei der Erstdiagnose einer pruriginösen Erkankung eine IIF auf der humanen Spalthaut und/oder auf dem Affenösophagus als Substrat veranlasst wurde.
Es konnten bei insgesamt 54 (16,7%) Patienten Autoantikörper gegen IgG oder IgA mittels IIF nachgewiesen werden. Bei 42 (76,4%) Patienten wurde eine weiterführende Diagnostik mittels DIF durchgeführt, die bei 37 (88,1%) Personen als negativ befundet wurde. Bei fünf (11,9%) Patienten konnten Autoantikörper gegen IgG, IgA und IgM nachgewiesen werden. Alle stammten aus der Gruppe mit einer Prurigo simplex subacuta [L28.2]. Bei diesen fünf Patienten wurde zusätzlich noch ein ELISA-Test durchgeführt. Nur bei einem Patienten konnten Autoantikörper gegen BP180 und Desmoglein 1 nachgewiesen werden.
66
Mit dieser Studie konnte aufgezeigt werden, dass bei Patienten mit den Erkrankungen Prurigo simplex subacuta [L28.2], Prurigo nodularis [L28.1], eosinophilenreiche Dermatitis [L30.8] und Prurigoform eines atopischen Ekzems [L20.0] keine erhöhte Bildung von Autoantikörpern gegen die dermoepidermale Junktionszone stattfindet. Dennoch sollte bei Patienten mit pruriginösen Erkrankungen eine serologische Untersuchung mittels IIF – und im Falle einer Positivität mittels ELISA und ggf. DIF durchgeführt werden, vor allem bei älteren Patienten, bei welchen der Pruritus als führendes Symptom beschrieben wird, um die Diagnose einer bullösen Autoimmundermatose sicher ausschließen zu können. Zudem sollte eine Verlaufskontrolle über mehrere Jahre erfolgen, um die Auswirkung des Pruritus als Trigger auf die Bildung von Autoantikörpern einer bullösen Autoimmundermatose zu verfolgen.
The relevance of the adaptor protein TNF receptor-associated factor 2 (TRAF2) for signal transduction of the death receptor tumour necrosis factor receptor1 (TNFR1) is well-established. The role of TRAF2 for signalling by CD95 and the TNF-related apoptosis inducing ligand (TRAIL) DRs, however, is only poorly understood. Here, we observed that knockdown (KD) of TRAF2 sensitised keratinocytes for TRAIL- and CD95L-induced apoptosis. Interestingly, while cell death was fully blocked by the pan-caspase inhibitor benzyloxycarbonyl-Val-Ala-Asp(OMe)-fluoromethylketone (zVAD-fmk) in control cells, TRAF2-depleted keratinocytes were only partly rescued from TRAIL- and CD95L-induced cell death. In line with the idea that the only partially protective effect of zVAD-fmk on TRAIL- and CD95L-treated TRAF2-depleted keratinocytes is due to the induction of necroptosis, combined treatment with zVAD-fmk and the receptor interacting protein 1 (RIP1) inhibitor necrostatin-1 fully rescued these cells. To better understand the impact of TRAF2 levels on RIP1- and RIP3-dependent necroptosis and RIP3-independent apoptosis, we performed experiments in HeLa cells that lack endogenous RIP3 and HeLa cells stably transfected with RIP3. HeLa cells, in which necroptosis has no role, were markedly sensitised to TRAIL-induced caspase-dependent apoptosis by TRAF2 KD. In RIP3-expressing HeLa transfectants, however, KD of TRAF2 also strongly sensitised for TRAIL-induced necroptosis. Noteworthy, priming of keratinocytes with soluble TWEAK, which depletes the cytosolic pool of TRAF2-containing protein complexes, resulted in strong sensitisation for TRAIL-induced necroptosis but had only a very limited effect on TRAIL-induced apoptosis. The necroptotic TRAIL response was not dependent on endogenously produced TNF and TNFR signalling, since blocking TNF by TNFR2-Fc or anti-TNFα had no effect on necroptosis induction. Taken together, we identified TRAF2 not only as a negative regulator of DR-induced apoptosis but in particular also as an antagonist of TRAIL- and CD95L-induced necroptosis.
In der vorgelegten Promotionsarbeit wurden die typischen bakteriellen MSSA bzw. MRSA Hautinfektionen einer dermatologischen Klinik mit dem Einzugsgebiet Nordbayern auf krankheitsrelevante Faktoren von PVL untersucht.
Interessanterweise fand sich bei der Präsenz von PVL keine Korrelation mit Methicillinresistenz oder Krankheitsschwere. Weder atopische Diathese noch Rauchen oder Körpergewicht scheinen das Auftreten des Pathogenitätsfaktors zu begünstigen. Allerdings traten die PVL positiven S. aureus Hautinfektionen bevorzugt bei jüngeren und weiblichen Patienten auf. Bei den untersuchten Hauterkrankungen zeigten S. aureus Stämme eine ausgeprägte Vielfalt. Es konnte kein spezieller epidemiologischer Stamm identifiziert werden.
Die Ergebnisse dieser Studie sind jedoch nur eingeschränkt auf ein großes Kollektiv projizierbar, da der Untersuchungszeitraum insgesamt nur 7 Jahre betrug und sich das Patientenkollektiv auf das Einzugsgebiet des Klinikums beschränkte.
HINTERGRUND: Verschiedene Therapieoptionen für die orofaziale Granulomatose (OFG) wurden in Fallberichten und kleinen Fallserien beschrieben, randomisierte Studien mit Berücksichtigung von Langzeitverläufen sowie standardisierte Therapieempfehlungen fehlen jedoch.
ZIELSETZUNG: Ziele der aktuellen Auswertung waren 1.) die Charakterisierung klinischer Basisparameter bei einer großen Anzahl von Patientinnen/-en mit OFG; 2.) eine Untersuchung der krankheitsbedingten psychischen Belastung; 3.) die Bewertung aktueller Behandlungsstrategien in Hinblick auf den langfristigen Verlauf; und 4.) die Entwicklung eines Therapiealgorithmus zur Verwendung in einer Standard operating procedure (SOP)
METHODE: Wir werteten retrospektiv 61 Patientinnen/-en mit OFG aus, die zwischen 2004 und 2019 in der Klinik für Dermatologie, Venerologie und Allergologie in Würzburg behandelt worden waren. Die Datenerhebung beinhaltete Geschlecht, Alter bei Erkrankungsbeginn, klinische Manifestationen der OFG, Histologie, Begleiterkrankungen und die jeweils eingesetzte Therapie. Dreiundvierzig Patientinnen/-en, bei denen nach der Erstvorstellung mindestens zwei weitere Kontrolltermine dokumentiert waren, wurden gebeten, anhand eines standardisierten Fragenbogens Auskünfte zu ihrer krankheitsbedingten psychischen Belastung und zum langfristigen Verlauf der OFG zu geben.
ERGEBNISSE: Das mediane Alter bei Erkrankungsbeginn lag bei 45 (Gesamtspanne 7-
77) Jahren. Die Mehrzahl der Patientinnen/-en litt an einer Cheilitis granulomatosa (n=58; 95,1 %); nur 6 (9,8 %) wiesen die komplette Trias eines Melkersson-Rosenthal- Syndroms, bestehend aus Cheilitis granulomatosa, Fazialisparese und Lingua plicata auf. Ein Morbus Crohn war in 9 (14,8 %) Fällen nachzuweisen. Von 23 Patientinnen/- en, die auf den Fragenbogen antworteten, berichteten 16 (69,6 %) über eine relevante (mäßige bis schwere) psychische Beeinträchtigung durch die kosmetischen Auswirkungen der OFG. Deutlich weniger fühlten sich durch Schwierigkeiten beim Essen (n=5, 21,7 %) oder beim Sprechen (n=1; 4,3 %) relevant beeinträchtigt. Fünfundzwanzig (41,0 %) Patientinnen/-en wurden mit Prednisolon behandelt. Die
Mehrheit zeigte unter steroidaler Therapie eine Verbesserung (68,0 %) oder sogar eine vollständige Remission (12,0 %), Rückfälle mit dem Ausschleichen des Steroids waren jedoch häufig. Der am häufigsten steroidsparend eingesetzte Wirkstoff war Sulfasalazin (18 Fälle); das therapeutische Ansprechen war uneinheitlich. Nur 2 Patienten mit assoziiertem Morbus Crohn wurden mit Infliximab behandelt, beide zeigten ein ausgezeichnetes Ansprechen. Das mediane Zeitintervall zwischen der letzten ambulanten Vorstellung bis zur Beantwortung des Fragenbogens betrug 49,5 (0-129) Monate. Zum Zeitpunkt der Datenerfassung befanden sich 12 (52,2 %) von 23 Patientinnen/-en in vollständiger Remission und weitere 10 (43,5 %) berichteten über eine leichte, persistierende Schwellung. Nur 5 (21,7 %) Patientinnen/-en berichteten über Episoden eines aktiven Anschwellens innerhalb der letzten 12 Monate vor der Datenerhebung.
SCHLUSSFOLGERUNGEN: Die OFG betrifft alle Altersgruppen und ist nicht auf Kinder bzw. junge Erwachsene beschränkt. Sie geht mit einer erheblichen psychischen Belastung einher, selbst wenn die objektivierbaren funktionellen Einschränkungen nur gering ausfallen. Systemische Steroide erlauben keine langfristige Krankheitskontrolle. Aufgrund seines relativ günstigen Nebenwirkungsprofils kann Sulfasalazin bei Patientinnen/-en steroidsparend eingesetzt werden, die für eine Behandlung mit TNF- alpha-Inhibitoren nicht in Betracht kommen. Angesichts der insgesamt guten Langzeitergebnisse auch bei unbehandelten Patientinnen/-en kommt in milden bis moderat ausgeprägten Fällen auch eine „Wait-and-Watch“-Strategie in Betracht.
Merkel cell carcinoma (MCC) is a rare and aggressive skin cancer. In approximately 80% of cases, genomic integration of the Merkel cell polyomavirus (MCPyV) is observed and overexpression of the two MCPyV T antigens (TAgs) is regarded as the main oncogenic determinant of MCPyV-positive MCC cases. However, the nature of the cells from which MCC arises is unknown. Therefore, the goal of the present work was to determine the cell of origin of MCC.
First, we characterized MCC patients’ tumors and demonstrated a high similarity of MCPyV- negative MCC with extracutaneous neuroendocrine carcinoma while MCPyV-positive MCC differs from these two groups with respect to morphology, immunohistochemical profile, genetics, origin and behavior. Based on the analysis of a trichoblastoma/MCC combined tumor, we demonstrated that a MCPyV-positive MCC can arise following MCPyV integration in an epithelial cell. In addition, the high similarity between trichoblastoma cells and Merkel cell (MC) progenitors of the hair follicle suggests that these hair follicle cells may represent a general start point for the development of MCPyV-positive MCC. A contribution of the viral TAgs to the development of the characteristic Merkel cell-like MCC phenotype is suggested by experiments demonstrating induction of Merkel cell markers upon TAg expression in human primary keratinocytes or hair follicle cells. As potential mechanisms mediating these phenotypic changes, we identified the capability of MCPyV LT to repress degradation of master regulator of MC development, i.e. the transcription factor ATOH1.
To conclude, our work suggests that MCPyV integration in epithelial cells of the hair follicle may represent an important path for MCC development.
Since 2021, adalimumab biosimilar ABP 501 can be used alternatively to adalimumab originator (ADAO) in the treatment of hidradenitis suppurativa (HS). Effectiveness and safety data remain scarce. We investigated the impact of switching from ADAO to ABP 501 on disease severity and the occurrence of adverse events (AEs) in patients with HS. We analyzed clinical data on patients enrolled in the German HSBest registry. Evaluation outcomes were assessed at three time points (baseline of originator (t0), prior to switching to biosimilar (t1) and 12 to 14 weeks after switching (t2)) and included patient-reported AEs and disease severity using the International Hidradenitis Suppurativa Severity Score System (IHS4) score. In total, 94 patients were switched from ADAO to ABP 501. Overall, 33.3% (n = 31/94) of the patients developed AEs and/or loss of response (LoR) within 12 to 14 weeks after switching. Of these, 61.3% (n = 19/31) experienced LoR but no AEs, 22.6% (n = 7/31) LoR combined with AEs and 16.1% (n = 5/31) AEs only. Our study showed that switching HS patients from ADAO to ABP 501 does significantly affect treatment effectiveness. Switching patients who are on remission maintenance therapy should be viewed critically.
Introduction: Mycosis fungoides, the most common type of cutaneous T-cell lymphoma, can manifest in a variety of clinical and histological forms. Bulla formation is an uncommon finding in mycosis fungoides and only approximately 20 cases have been reported in the literature. Case presentation: We present a case of rapidly progressive mycosis fungoides in a 68-year-old Caucasian man who initially presented with erythematous plaques characterised by blister formation. Conclusion: Although mycosis fungoides bullosa is extremely rare, it has to be regarded as an important clinical subtype of cutaneous T-cell lymphoma. Mycosis fungoides bullosa represents a particularly aggressive form of mycosis fungoides and is associated with a poor prognosis. The rapid disease progression in our patient confirms bulla formation as an adverse prognostic sign in cutaneous T-cell lymphoma.
Blue nevus is a benign melanocytic lesion, typically asymptomatic and of unknown etiology. Several histologic and clinical variants have been distinguished, the most frequent being common blue nevus, cellular blue nevus, and combined blue nevus. Although melanocytic nevi with a satellite lesion are usually suggestive of locally advanced malignant melanoma, very few cases of blue nevi with satellite lesions have been reported. The diagnosis of common or cellular blue nevi is generally straightforward; however, the presence of structures such as irregular edges or satellitosis are highly suggestive for malignancy, and differential diagnoses such as locally advanced malignant melanoma and malignant blue nevus should be considered. Recurrent blue nevi can display atypical features not seen in the primary lesion, such as pleomorphism and mitotic activity. They usually tend to follow a benign course; however, in some cases, recurrence may indicate malignant transformation. We here report the unique case of a 64-year-old woman with a recurrent cellular blue nevus accompanied by satellite lesions. Such a biological behavior resulting in a clinical presentation as a melanoma-like lesion is a rarity in blue nevus and has not been described before.
Background: Since there is no standardized and effective treatment for advanced uveal melanoma (UM), the prognosis is dismal once metastases develop. Due to the availability of immune checkpoint blockade (ICB) in the real-world setting, the prognosis of metastatic UM has improved. However, it is unclear how the presence of hepatic and extrahepatic metastasis impacts the response and survival after ICB. Methods: A total of 178 patients with metastatic UM treated with ICB were included in this analysis. Patients were recruited from German skin cancer centers and the German national skin cancer registry (ADOReg). To investigate the impact of hepatic metastasis, two cohorts were compared: patients with liver metastasis only (cohort A, n = 55) versus those with both liver and extra-hepatic metastasis (cohort B, n = 123). Data were analyzed in both cohorts for response to treatment, progression-free survival (PFS), and overall survival (OS). The survival and progression probabilities were calculated with the Kaplan–Meier method. Log-rank tests, χ\(^2\) tests, and t-tests were performed to detect significant differences between both cohorts. Results: The median OS of the overall population was 16 months (95% CI 13.4–23.7) and the median PFS, 2.8 months (95% CI 2.5–3.0). The median OS was longer in cohort B than in cohort A (18.2 vs. 6.1 months; p = 0.071). The best objective response rate to dual ICB was 13.8% and to anti-PD-1 monotherapy 8.9% in the entire population. Patients with liver metastases only had a lower response to dual ICB, yet without significance (cohort A 8.7% vs. cohort B 16.7%; p = 0.45). Adverse events (AE) occurred in 41.6%. Severe AE were observed in 26.3% and evenly distributed between both cohorts. Conclusion: The survival of this large cohort of patients with advanced UM was more favorable than reported in previous benchmark studies. Patients with both hepatic and extrahepatic metastasis showed more favorable survival and higher response to dual ICB than those with hepatic metastasis only.
Re-induction with immune checkpoint blockade (ICB) needs to be considered in many patients with uveal melanoma (UM) due to limited systemic treatment options. Here, we provide hitherto the first analysis of ICB re-induction in UM. A total of 177 patients with metastatic UM treated with ICB were included from German skin cancer centers and the German national skin cancer registry (ADOReg). To investigate the impact of ICB re-induction, two cohorts were compared: patients who received at least one ICB re-induction (cohort A, n = 52) versus those who received only one treatment line of ICB (cohort B, n = 125). In cohort A, a transient benefit of overall survival (OS) was observed at 6 and 12 months after the treatment start of ICB. There was no significant difference in OS between both groups (p = 0.1) with a median OS of 16.2 months (cohort A, 95% CI: 11.1–23.8) versus 9.4 months (cohort B, 95% CI: 6.1–14.9). Patients receiving re-induction of ICB (cohort A) had similar response rates compared to those receiving ICB once. Re-induction of ICB may yield a clinical benefit for a small subgroup of patients even after resistance or development of toxicities.
Cutaneous adverse events associated with interferon-\(\beta\) treatment of multiple sclerosis
(2015)
Interferons are widely used platform therapies as disease-modifying treatment of patients with multiple sclerosis. Although interferons are usually safe and well tolerated, they frequently cause dermatological side effects. Here, we present a multiple sclerosis (MS) patient treated with interferon-\(\beta\) who developed new-onset psoriasis. Both her MS as well as her psoriasis finally responded to treatment with fumarates. This case illustrates that interferons not only cause local but also systemic adverse events of the skin. These systemic side effects might indicate that the Th17/IL-17 axis plays a prominent role in the immunopathogenesis of this individual case and that the autoimmune process might be deteriorated by further administration of interferons. In conclusion, we think that neurologists should be aware of systemic cutaneous side effects and have a closer look on interferon-associated skin lesions. Detection of psoriasiform lesions might indicate that interferons are probably not beneficial in the individual situation. We suggest that skin lesions may serve as biomarkers to allocate MS patients to adequate disease-modifying drugs.
Background:
Interferon (IFN) beta drugs have been approved for the treatment of relapsing forms of multiple sclerosis (RMS) for more than 20years and are considered to offer a favourable benefit-risk profile. In July 2014, subcutaneous (SC) peginterferon beta-1a 125g dosed every 2weeks, a pegylated form of interferon beta-1a, was approved by the EMA for the treatment of adult patients with RRMS and in August 2014 by the FDA for RMS. Peginterferon beta-1a shows a prolonged half-life and increased systemic drug exposure resulting in a reduced dosing frequency compared to other available interferon-based products in MS. In the Phase 3 ADVANCE trial peginterferon beta-1a demonstrated significant positive effects on clinical and MRI outcome measures versus placebo after one year. Furthermore, in the ATTAIN extension study, sustained efficacy with long-term treatment for nearly 6years was shown.
Main text
In July 2016, an interdisciplinary panel of German and Austrian experts convened to discuss the management of side effects associated with peginterferon beta-1a and other interferon beta-based treatments in MS in daily practice. The panel was composed of experts from university hospitals and private clinics comprised of neurologists, dermatologists, and an MS nurse. In this paper we report recommendations regarding best practices for adverse event management, focussing on peginterferon beta-1a. Injection site reactions (ISRs) and influenza-like illness are the most common adverse effects of interferon beta therapies and can present a burden for MS patients leading to non-adherence and discontinuation of therapy. Peginterferon beta-1a shows improved pharmacological properties. In clinical trials, the adverse event (AE) profile of peginterferon beta-1a was similar to other interferon beta formulations. The most common AEs were mild to moderate ISRs, influenza-like illness, pyrexia, and headache. Current information on the underlying cause of skin reactions associated with SC interferon treatment, and the management strategies for these AEs are limited. In pivotal trials, ISRs were mainly characterized and classified by neurologists, while dermatologists were only rarely consulted.
Conclusions
This report addresses expert recommendations on the management of most relevant adverse effects related to peginterferon beta-1a and other interferon betas, based on literature and interdisciplinary experience.