Author: Ferraro, Francesco; Patella, Francesca; Costa, Joana R.; Ketteler, Robin; Kristonâ€Vizi, Janos; Cutler, Daniel F.
Title: Modulation of endothelial organelle size as an antithrombotic strategy Cord-id: n5ilem3q Document date: 2020_10_16
ID: n5ilem3q
Snippet: BACKGROUND: It is long established that von Willebrand factor (VWF) is central to hemostasis and thrombosis. Endothelial VWF is stored in cellâ€specific secretory granules, Weibelâ€Palade bodies (WPBs), organelles generated in a wide range of lengths (0.5â€5.0 µm). WPB size responds to physiological cues and pharmacological treatment, and VWF secretion from shortened WPBs dramatically reduces platelet and plasma VWF adhesion to an endothelial surface. OBJECTIVE: We hypothesized that WPBâ€sh
Document: BACKGROUND: It is long established that von Willebrand factor (VWF) is central to hemostasis and thrombosis. Endothelial VWF is stored in cellâ€specific secretory granules, Weibelâ€Palade bodies (WPBs), organelles generated in a wide range of lengths (0.5â€5.0 µm). WPB size responds to physiological cues and pharmacological treatment, and VWF secretion from shortened WPBs dramatically reduces platelet and plasma VWF adhesion to an endothelial surface. OBJECTIVE: We hypothesized that WPBâ€shortening represented a novel target for antithrombotic therapy. Our objective was to determine whether compounds exhibiting this activity do exist. METHODS: Using a microscopy approach coupled to automated image analysis, we measured the size of WPB bodies in primary human endothelial cells treated with licensed compounds for 24 hours. RESULTS AND CONCLUSIONS: A novel approach to identification of antithrombotic compounds generated a significant number of candidates with the ability to shorten WPBs. In vitro assays of two selected compounds confirm that they inhibit the proâ€hemostatic activity of secreted VWF. This set of compounds acting at a very early stage of the hemostatic process could well prove to be a useful adjunct to current antithrombotic therapeutics. Further, in the current SARSâ€CoVâ€2 pandemic, with a considerable fraction of critically ill COVIDâ€19 patients affected by hypercoagulability, these WPB sizeâ€reducing drugs might also provide welcome therapeutic leads for frontline clinicians and researchers.
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