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Institute
- Institut für Anatomie und Zellbiologie (254) (remove)
Sonstige beteiligte Institutionen
- Department of Biomedical Imaging, National Cerebral and Cardiovascular Research Center, Suita, Japan (2)
- Division of Medical Technology and Science, Department of Medical Physics and Engineering, Course of Health Science, Osaka University Graduate School of Medicine, Suita Japan (2)
- Institut for Molecular Biology and CMBI, Department of Genomics, Stem Cell Biology and Regenerative Medicine, Leopold-Franzens-University Innsbruck, Innsbruck, Austria (2)
- Johns Hopkins School of Medicine, The Russell H Morgan Department of Radiology and Radiological Science, Baltimore, MD, USA (2)
- Naturalis Biodiversity Centre (2)
- Johns Hopkins School of Medicine (1)
- Johns Hopkins School of Medicine, Baltimore, MD, U.S. (1)
The Best for the Most Important: Maintaining a Pristine Proteome in Stem and Progenitor Cells
(2019)
Pluripotent stem cells give rise to reproductively enabled offsprings by generating progressively lineage-restricted multipotent stem cells that would differentiate into lineage-committed stem and progenitor cells. These lineage-committed stem and progenitor cells give rise to all adult tissues and organs. Adult stem and progenitor cells are generated as part of the developmental program and play critical roles in tissue and organ maintenance and/or regeneration. The ability of pluripotent stem cells to self-renew, maintain pluripotency, and differentiate into a multicellular organism is highly dependent on sensing and integrating extracellular and extraorganismal cues. Proteins perform and integrate almost all cellular functions including signal transduction, regulation of gene expression, metabolism, and cell division and death. Therefore, maintenance of an appropriate mix of correctly folded proteins, a pristine proteome, is essential for proper stem cell function. The stem cells' proteome must be pristine because unfolded, misfolded, or otherwise damaged proteins would interfere with unlimited self-renewal, maintenance of pluripotency, differentiation into downstream lineages, and consequently with the development of properly functioning tissue and organs. Understanding how various stem cells generate and maintain a pristine proteome is therefore essential for exploiting their potential in regenerative medicine and possibly for the discovery of novel approaches for maintaining, propagating, and differentiating pluripotent, multipotent, and adult stem cells as well as induced pluripotent stem cells. In this review, we will summarize cellular networks used by various stem cells for generation and maintenance of a pristine proteome. We will also explore the coordination of these networks with one another and their integration with the gene regulatory and signaling networks.
Taxane (wie Paclitaxel oder Cabazitaxel) sind bewährte Arzneimittel in den systemischen Therapieschemata vieler bösartiger Erkrankungen, einschließlich Brust- und Eierstockkrebs. Sie fördern die Stabilisierung der Mikrotubuli, was zu einem Stillstand des Zellzyklus während der Mitose führt, auf den die Apoptose folgt. Neben dieser antimitotischen Wirkung von Taxanen ist seit einiger Zeit auch eine gefäßverändernde Wirkung von Taxanen bekannt. Kürzlich wurde gezeigt, dass Taxane tatsächlich Störungen in der Gefäßarchitektur verursachen, indem sie den Kalziumeinstrom über TRPC6, einen unselektiven Kationenkanal, auslösen. Der erhöhte intrazelluläre Ca2+-Spiegel bewirkt eine Rundung der Endothelzellen, was zu einer Störung des endothelialen Monolayers, Serumausfluss und Gefäßkollaps führt.
In dieser Arbeit konzentrierten wir uns auf die Gefäßbetten von peripheren Organen wie dem Herzen oder der Niere in Abhängigkeit vom Tumorstadium und der Taxol-Behandlung. Die Organe wurden mit immunhistochemischen Techniken angefärbt, um Veränderungen in der Architektur und Morphologie der Blutgefäße zu untersuchen.
Wir fanden Veränderungen in der Morphologie der Kapillaren des Herzens und darüber hinaus Veränderungen in der Expression endothelialer Antigene in Abhängigkeit vom Tumorstadium, insbesondere eine zunehmende endotheliale Expression von TRPC6 in Abhängigkeit vom Tumorstadium.
Diese Ergebnisse liefern neue Erkenntnisse für das Verständnis der systemischen Auswirkungen maligner Erkrankungen und tragen dazu bei, Folgeerkrankungen bei Patienten mit fortgeschrittenem Krebs zu verhindern.
In this study, the impact of reconstruction sharpness on the visualization of the appendicular skeleton in ultrahigh-resolution (UHR) photon-counting detector (PCD) CT was investigated. Sixteen cadaveric extremities (eight fractured) were examined with a standardized 120 kVp scan protocol (CTDI\(_{vol}\) 10 mGy). Images were reconstructed with the sharpest non-UHR kernel (Br76) and all available UHR kernels (Br80 to Br96). Seven radiologists evaluated image quality and fracture assessability. Interrater agreement was assessed with the intraclass correlation coefficient. For quantitative comparisons, signal-to-noise-ratios (SNRs) were calculated. Subjective image quality was best for Br84 (median 1, interquartile range 1–3; p ≤ 0.003). Regarding fracture assessability, no significant difference was ascertained between Br76, Br80 and Br84 (p > 0.999), with inferior ratings for all sharper kernels (p < 0.001). Interrater agreement for image quality (0.795, 0.732–0.848; p < 0.001) and fracture assessability (0.880; 0.842–0.911; p < 0.001) was good. SNR was highest for Br76 (3.4, 3.0–3.9) with no significant difference to Br80 and Br84 (p > 0.999). Br76 and Br80 produced higher SNRs than all kernels sharper than Br84 (p ≤ 0.026). In conclusion, PCD-CT reconstructions with a moderate UHR kernel offer superior image quality for visualizing the appendicular skeleton. Fracture assessability benefits from sharp non-UHR and moderate UHR kernels, while ultra-sharp reconstructions incur augmented image noise.
Objectives: This study investigated the feasibility and image quality of ultra-low-dose unenhanced abdominal CT using photon-counting detector technology and tin prefiltration. Materials and Methods: Employing a first-generation photon-counting CT scanner, eight cadaveric specimens were examined both with tin prefiltration (Sn 100 kVp) and polychromatic (120 kVp) scan protocols matched for radiation dose at three different levels: standard-dose (3 mGy), low-dose (1 mGy) and ultra-low-dose (0.5 mGy). Image quality was evaluated quantitatively by means of contrast-to-noise-ratios (CNR) with regions of interest placed in the renal cortex and subcutaneous fat. Additionally, three independent radiologists performed subjective evaluation of image quality. The intraclass correlation coefficient was calculated as a measure of interrater reliability. Results: Irrespective of scan mode, CNR in the renal cortex decreased with lower radiation dose. Despite similar mean energy of the applied x-ray spectrum, CNR was superior for Sn 100 kVp over 120 kVp at standard-dose (17.75 ± 3.51 vs. 14.13 ± 4.02), low-dose (13.99 ± 2.6 vs. 10.68 ± 2.17) and ultra-low-dose levels (8.88 ± 2.01 vs. 11.06 ± 1.74) (all p ≤ 0.05). Subjective image quality was highest for both standard-dose protocols (score 5; interquartile range 5–5). While no difference was ascertained between Sn 100 kVp and 120 kVp examinations at standard and low-dose levels, the subjective image quality of tin-filtered scans was superior to 120 kVp with ultra-low radiation dose (p < 0.05). An intraclass correlation coefficient of 0.844 (95% confidence interval 0.763–0.906; p < 0.001) indicated good interrater reliability. Conclusions: Photon-counting detector CT permits excellent image quality in unenhanced abdominal CT with very low radiation dose. Employment of tin prefiltration at 100 kVp instead of polychromatic imaging at 120 kVp increases the image quality even further in the ultra-low-dose range of 0.5 mGy.
Combined pulmonary fibrosis and emphysema (CPFE) is a recently recognized syndrome that, as its name indicates, involves the existence of both interstitial lung fibrosis and emphysema in one individual, and is often accompanied by pulmonary hypertension. This debilitating, progressive condition is most often encountered in males with an extensive smoking history, and is presented by dyspnea, preserved lung volumes, and contrastingly impaired gas exchange capacity. The diagnosis of the disease is based on computed tomography imaging, demonstrating the coexistence of emphysema and interstitial fibrosis in the lungs, which might be of various types and extents, in different areas of the lung and several relative positions to each other. CPFE bears high mortality and to date, specific and efficient treatment options do not exist. In this review, we will summarize current knowledge about the clinical attributes and manifestations of CPFE. Moreover, we will focus on pathophysiological and pathohistological lung phenomena and suspected etiological factors of this disease. Finally, since there is a paucity of preclinical research performed for this particular lung pathology, we will review existing animal studies and provide suggestions for the development of additional in vivo models of CPFE syndrome.
The parotid gland is one of the major salivary glands producing a serous secretion, and it plays an essential role in the digestive and immune systems. Knowledge of peroxisomes in the human parotid gland is minimal; furthermore, the peroxisomal compartment and its enzyme composition in the different cell types of the human parotid gland have never been subjected to a detailed investigation. Therefore, we performed a comprehensive analysis of peroxisomes in the human parotid gland’s striated duct and acinar cells. We combined biochemical techniques with various light and electron microscopy techniques to determine the localization of parotid secretory proteins and different peroxisomal marker proteins in parotid gland tissue. Moreover, we analyzed the mRNA of numerous gene encoding proteins localized in peroxisomes using real-time quantitative PCR. The results confirm the presence of peroxisomes in all striated duct and acinar cells of the human parotid gland. Immunofluorescence analyses for various peroxisomal proteins showed a higher abundance and more intense staining in striated duct cells compared to acinar cells. Moreover, human parotid glands comprise high quantities of catalase and other antioxidative enzymes in discrete subcellular regions, suggesting their role in protection against oxidative stress. This study provides the first thorough description of parotid peroxisomes in different parotid cell types of healthy human tissue.
Eine pentaploide Sippe aus der Pilosella macranthela-Verwandtschaft wurde in Unterfranken/Bayern entdeckt, die hier als P. macranthela subsp. sylvae-pici neu beschrieben wird. Sie wächst hauptsächlich im bayerischen Buntsandstein-Spessart und kommt mit drei kleinen, isolierten Wuchsorten auch in den Kalkgebieten des Maintals und Tauberbereichs vor. Die Wuchsform steht zwischen dem Furcata- und Laxicephala-Typus von Pilosellinen mit ober- und teils unterirdischen Ausläufern und zeigt Neigung, Horste zu bilden. Die Ober- und Unterseiten der Rosettenblätter besitzen Sternhaare. Die Korbstiele und Hüllblätter sind dicht mit dunkel gestielten Drüsenhaaren mit gelblichen Drüsenköpfen besetzt. Die seitlichen Zähne der Blütenzungen sind oft durch Einschnitte abgetrennt. Tetra- und pentaploide Zwischenarten zwischen P. macranthela subsp. sylvae-pici und P. officinarum werden als P. ottonis neu beschrieben. P. ottonis ist tetra- und pentaploid mit bis zu 7 Körben, ist an den Hüllblättern mit dunklen Stieldrüsen besetzt und ähnelt vom Habitus Formen von P. acutlifolia. Die Hüllen von P. ottonis besitzen wie die von P. macranthela subsp. sylvae-pici und P. glomerata zahlreiche, ca. 10–20 μm dicke Epidermispapillen, die stets bei P. officinarum fehlen. Heterogene P. marcanthela-Sippen (tetra- und heptaploid) kommen als Spontanhybride zwischen P. glomerata und P. officinarum auch außerhalb des Spessartgebiets vor und wurden auch ohne benachbarte P. glomerata gefunden.
Recombinant beta interferons-1 (IFNβ-1) are used as first line therapies in patients with relapsing multiple sclerosis (MS), a chronic inflammatory and neurodegenerative disease of the CNS. IFNβ-1a/b has moderate effects on the prevention of relapses and slowing of disease progression. Fibroblast growth factors (FGFs) and FGF receptors (FGFRs) are known to play a key role in the pathology of MS and its model EAE. To investigate the effects of short-term treatment with s.c. IFNβ-1a versus the combined application of s.c. IFNβ-1a and oligodendrocyte-specific deletion of FGFR1 (Fgfr1\(^{ind−/−}\) mice) in MOG\(_{35-55}\)-induced EAE. IFNβ-1a (30 mg/kg) was applied s.c. from days 0–7 p.i. of EAE in controls and Fgfr1\(^{ind−/−}\) mice. FGFR signaling proteins associated with inflammation/degeneration in MS/EAE were analyzed by western blot in the spinal cord. Further, FGFR1 in Oli-neu oligodendrocytes were inhibited by PD166866 and treated with IFNβ-1a (400 ng/mL). Application of IFNβ-1a over 8 days resulted in less symptoms only at the peak of disease (days 9–11) compared to controls. Application of IFNβ-1a in Fgfr1\(^{ind−/−}\) mice resulted in less symptoms primarily in the chronic phase of EAE. Fgfr1\(^{ind−/−}\) mice treated with IFNβ-1a showed increased expression of pERK and BDNF. In Oli-neu oligodendrocytes, treatment with PD166866 and IFNβ-1a also showed an increased expression of pERK and BDNF/TrkB. These data suggest that the beneficial effects in the chronic phase of EAE and on signaling molecules associated with ERK and BDNF expression are caused by the modulation of FGFR1 and not by interferon beta-1a. FGFR may be a potential target for therapy in MS.
Herzkreislauferkrankungen sind weit verbreitet und nicht nur eine große Belastung für die Betroffenen, sondern auch für das Gesundheitssystem. Die Folgen von Herzkreislauferkrankungen wie z.B. Myokardinfarkt und koronare Herzkrankheit stellen weltweit die häufigste Todesursache dar. Prävention, frühzeitige Erkennung und konsequente Behandlung sind daher von großer Bedeutung.
Um das Verständnis für die Pathophysiologie zu fördern und ferner Therapieansätze ausfindig zu machen, ist es notwendig, nicht nur die Herzmuskelzellen im Blick zu haben, sondern auch die Komponenten des Herzmuskelstromas, die deren Funktion beeinflussen können.
Das Verständnis und die Rekonstruktion des kardialen Gewebes auf ultrastruktureller Ebene, sowie die Charakterisierung und Wechselwirkungen der verschiedenen Zellen des Herzens haben deshalb das Interesse vieler Forschergruppen geweckt.
Das Ziel dieser Arbeit war die detaillierte ultrastrukturelle Analyse kardialer Perizyten, Endothelzellen sowie Kapillarwand-assoziierter Zellen und deren Kontakte im Arbeitsmyokard der Maus mittels verschiedener elektronenmikroskopischer Methoden.
Zu Beginn der Arbeit wurde die transmissionselektronenmikroskopische Probenaufbereitung optimiert und ein modifiziertes Protokoll zur hervorragenden Kontrastierung der biologischen Membranen und zum bestmöglichen Erhalt der Ultrastruktur etabliert. Die optimierte Probenaufbereitung bot dann die ideale Grundlage für die Generierung elektronenmikroskopischer Datensätze mittels serieller Block-Face Rasterelektronenmikroskopie (SBF-SEM) und anschließender Erzeugung dreidimensionaler Modelle der Mikrovaskulatur des Arbeitsmyokards der Maus.
Die detaillierte ultrastrukturelle Analyse in drei Dimensionen offenbart neue morphologische Merkmale der kardialen Mikrovaskulatur und zeigt, dass die kardialen Perizyten vereinzelt Fortsätze abgeben, die mit den Endothelzellen assoziiert sind. Dadurch entsteht nicht nur eine perizytäre-endotheliale Einheit, die von derselben Basallamina umschlossen wird. Die Rekonstruktion zeigt ebenfalls, dass die Kapillarwand-assoziierten Zellen sehr groß und weit verzweigt sind und nicht von der die Perizyten und Endothelzellen umgebenden Basallamina umschlossen werden. Sie stehen an vereinzelten Stellen in direktem Kontakt mit den Endothelzellen.
Immunelektronenmikroskopische Analysen zeigen, dass die Kapillarwand-assoziierten Zellen sowohl CD34-positiv als auch CD44-positiv sind.
Größer angelegte Studien zur weiteren dreidimensionalen Analyse z.B. in der Intima einer Arteriole könnten zur weiteren Charakterisierung der Perizyten und der Kapillarwand-assoziierten Zellen beitragen und sogar eine Einteilung möglich machen.
Eine Beteiligung von Perizyten im Rahmen des kardialen Remodeling nach einem Myokardinfarkt wurde bereits nachgewiesen. Außerdem spielen die Membranproteine CD34 und CD44 eine wichtige Rolle in der Hämatopoese und auch der Angiogenese.
In Zukunft könnten sich auch daraus interessante neue Ansätze für gezielte Therapien nach einem Myokardinfarkt ergeben.