Evoked Weibel‐Palade Body Exocytosis Modifies the Endothelial Cell Surface by Releasing a Substrate‐Selective Phosphodiesterase

Author:

Naß Johannes1,Terglane Julian1,Zeuschner Dagmar2,Gerke Volker1ORCID

Affiliation:

1. Institute of Medical Biochemistry, Center for Molecular Biology of Inflammation University of Muenster von‐Esmarch‐Str. 56 48149 Muenster Germany

2. Electron Microscopy Facility Max Planck Institute for Molecular Biomedicine Roentgenstr. 20 48149 Muenster Germany

Abstract

AbstractWeibel Palade bodies (WPB) are lysosome‐related secretory organelles of endothelial cells. Commonly known for their main cargo, the platelet and leukocyte receptors von‐Willebrand factor (VWF) and P‐selectin, WPB play a crucial role in hemostasis and inflammation. Here, the authors identify the glycerophosphodiester phosphodiesterase domain‐containing protein 5 (GDPD5) as a WPB cargo protein and show that GDPD5 is transported to WPB following uptake from the plasma membrane via an unique endocytic transport route. GDPD5 cleaves GPI‐anchored, plasma membrane‐resident proteins within their GPI‐motif, thereby regulating their local activity. The authors identify a novel target of GDPD5 , the complement regulator CD59, and show that it is released from the endothelial surface by GDPD5 following WPB exocytosis. This results in increased deposition of complement components and can enhance local inflammatory and thrombogenic responses. Thus, stimulus‐induced WPB exocytosis can modify the endothelial cell surface by GDPD5‐mediated selective release of a subset of GPI‐anchored proteins.

Funder

Deutsche Forschungsgemeinschaft

Publisher

Wiley

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