TY - JOUR A1 - Rommel, Marcel G. E. A1 - Milde, Christian A1 - Eberle, Regina A1 - Schulze, Harald A1 - Modlich, Ute T1 - Endothelial–platelet interactions in influenza‐induced pneumonia: A potential therapeutic target JF - Anatomia, Histologia, Embryologia N2 - Every year, influenza viruses spread around the world, infecting the respiratory systems of countless humans and animals, causing illness and even death. Severe influenza infection is associated with pulmonary epithelial damage and endothelial dysfunction leading to acute lung injury (ALI). There is evidence that an aggressive cytokine storm and cell damage in lung capillaries as well as endothelial/platelet interactions contribute to vascular leakage, pro‐thrombotic milieu and infiltration of immune effector cells. To date, treatments for ALI caused by influenza are limited to antiviral drugs, active ventilation or further symptomatic treatments. In this review, we summarize the mechanisms of influenza‐mediated pathogenesis, permissive animal models and histopathological changes of lung tissue in both mice and men and compare it with histological and electron microscopic data from our own group. We highlight the molecular and cellular interactions between pulmonary endothelium and platelets in homeostasis and influenza‐induced pathogenesis. Finally, we discuss novel therapeutic targets on platelets/endothelial interaction to reduce or resolve ALI. KW - endothelial cell KW - influenza KW - interaction KW - laboratory animals KW - lung injury KW - platelet KW - pneumonia KW - therapy Y1 - 2020 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-213610 VL - 49 IS - 5 SP - 606 EP - 619 ER - TY - JOUR A1 - Pollitt, Alice Y. A1 - Poulter, Natalie S. A1 - Gitz, Eelo A1 - Navarro-Nuñez, Leyre A1 - Wang, Ying-Jie A1 - Hughes, Craig E. A1 - Thomas, Steven G. A1 - Nieswandt, Bernhard A1 - Douglas, Michael R. A1 - Owen, Dylan M. A1 - Jackson, David G. A1 - Dustin, Michael L. A1 - Watson, Steve P. T1 - Syk and Src Family Kinases Regulate C-type Lectin Receptor 2 (CLEC-2)-mediated Clustering of Podoplanin and Platelet Adhesion to Lymphatic Endothelial Cells* JF - The Journal of Biological Chemistry N2 - The interaction of CLEC-2 on platelets with Podoplanin on lymphatic endothelial cells initiates platelet signalling events that are necessary for prevention of blood-lymph mixing during development. In the present study, we show that CLEC-2 signalling via Src family and Syk tyrosine kinases promotes platelet adhesion to primary mouse lymphatic endothelial cells at low shear. Using supported lipid bilayers containing mobile Podoplanin, we further show that activation of Src and Syk in platelets promotes clustering of CLEC-2 and Podoplanin. Clusters of CLEC-2-bound Podoplanin migrate rapidly to the centre of the platelet to form a single structure. Fluorescence life-time imaging demonstrates that molecules within these clusters are within 10 nm of one another and that the clusters are disrupted by inhibition of Src and Syk family kinases. CLEC-2 clusters are also seen in platelets adhered to immobilised Podoplanin using direct stochastic optical reconstruction microscopy (dSTORM). These findings provide mechanistic insight by which CLEC-2 signalling promotes adhesion to Podoplanin and regulation of Podoplanin signalling thereby contributing to lymphatic vasculature development. KW - endothelial cell KW - lipid bilayer KW - platelet receptor KW - tyrosine-protein kinase KW - CLEC-2 ITAM KW - podoplanin KW - Src family KW - kinase Syk Y1 - 2014 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-120770 VL - 289 IS - 52 ER - TY - THES A1 - Müller, Verena T1 - Candida albicans-induzierte Genexpression in primären humanen Endothelzellen - Mechanismen der Signaltransduktion und Möglichkeiten der Intervention T1 - Candida albicans-induced gene expression in primary human endothelial cells - mechanisms of signal transduction and possibilities of intervention N2 - Endothelzellen sind ein aktiver Bestandteil der angeborenen Immunabwehr des Menschen gegen mikrobielle Pathogene. Unter ungünstigen Bedingungen kann die Abwehrreaktion sogar zu einer lebensbedrohlichen Sepsis führen. Hier wurde die bislang wenig bekannte Endothelantwort auf den fakultativ humanpathogenen Hefepilz Candida albicans, einem der häufigsten Verursacher von letaler Sepsis beim Menschen, näher untersucht. Mittels Oligonukleotid-Mikroarray-Analyse von HUVEC nach Exposition mit C. albicans konnten 56 hochregulierte Gene identifiziert werden, während 69 Gene herunterreguliert wurden. Ein bedeutender Anteil der regulierten Gene ist an Prozessen der angeborenen Immunantwort beteiligt und dient hauptsächlich der Rekrutierung von Neutrophilen. Weitere Untersuchungen ergaben eine zentrale Rolle des proinflammatorischen NF-kappaB-Weges bei der Regulation des Candida-induzierten Transkriptoms von Endothelzellen. Es konnte gezeigt werden, dass C. albicans diesen Signalweg sequenziell aktiviert. Zusätzlich konnte durch die Expression einer dominant-negativen Mutante einer Signalkomponente des NF-kappaB-Signalwegs die Candida-vermittelte Induktion von kappaB-abhängigen Genen gehemmt werden. Mit einem pharmakologischen Ansatz wurde der p38 MAP Kinase-Signalweg als weiterer bedeutsamer Signalweg identifiziert, der die Expression einzelner Candida-Zielgene wie CXCL8/IL-8 moduliert. Schließlich wurde gezeigt, dass die Candida-induzierte NF-kappaB-Aktivierung im untersuchten endothelialen Zellsystem unabhängig von den Toll-like Rezeptoren TLR2 und TLR4 geschieht, die üblicherweise an der Erkennung mikrobieller Pathogene beteiligt sind. Durch RNA-Interferenz-Experimente konnte jedoch dargelegt werden, dass das Adaptermolekül MyD88 und die Kinase IRAK1, die beide entscheidend an der TLR-vermittelten Signaltransduktion beteiligt sind, essentiell für die Weiterleitung des Signals in Endothelzellen sind. Nachfolgend konnte mit TLR3 zumindest einer der signaltransduzierenden Rezeptoren identifiziert werden. Als erste umfassende Untersuchung der endothelialen Antwort auf Candida albicans erlaubt die vorliegende Arbeit neue Einblicke in die komplexen Signalmuster von Endothelzellen, die dieser klinisch bedeutende Krankheitserreger auslöst. N2 - Endothelial cells (ECs) actively participate in the innate defence against microbial pathogens. Under unfavourable conditions defence reactions can even turn into life-threatening responses resulting in sepsis. Here the so far largely unknown EC reaction patterns to Candida albicans were studied. C. albicans is a facultative human pathogenic fungus and a major cause of lethality in septic patients. Oligonucleotide microarray analysis revealed 56 genes that were transcriptionally up-regulated and 69 that were suppressed upon exposure of ECs to C. albicans. A major portion of these genes is involved in defence mechanisms of the innate immune system with a high representation of genes serving the recruitment of neutrophils to sites of infection. Further examination of candidate signalling cascades established a central role of the proinflammatory NF-kappaB pathway in the regulation of the Candida-modulated transcriptome of ECs. It was shown that the NF-kappaB signalling pathway becomes activated at various levels. In addition, expression of a dominant negative mutant of a NF-kappaB signalling pathway compound blocked the Candida-induced kappaB-dependent gene expression. Using a pharmacological approach the stress-activated p38 mitogen-activated protein (MAP) kinase pathway was identified as a second major regulatory pathway which critically contributes to the regulation of selected Candida target genes such as CXCL8/IL-8. Candida-induced NF-kappaB activation is mediated independently of Toll-like receptors (TLR) 2 and 4 that commonly have been implicated with microbial pattern recognition. Nevertheless, knock-down of the adapter molecule MyD88 and the essential downstream kinase of TLR-, IL-1R- and IL-18R-signalling, IRAK1, suggested that recognition and signalling via a TLR apart from TLR2/TLR4 is crucial for Candida-induced gene expression in primary ECs. Finally, RNAi experiments indicate that most likely TLR3 represents this receptor. These data provide the first comprehensive analysis of endothelial gene responses to Candida albicans and present novel insights into the complex signalling patterns triggered by this important pathogen. KW - Angeborene Immunität KW - Endothelzelle KW - Toll-like-Rezeptoren KW - Candida albicans KW - Entzündung KW - innate immunity KW - endothelial cell KW - toll-like receptors KW - Candida albicans KW - inflammation Y1 - 2007 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-26224 ER -