4.5 Article

Plasma membrane wound repair is characterized by extensive membrane lipid and protein rearrangements in vascular endothelial cells

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ELSEVIER
DOI: 10.1016/j.bbamcr.2021.118991

Keywords

Actin; Annexin; Calcium; Phospholipid; Plasma membrane repair

Funding

  1. German Research Foundation [DFG GE514/6-3, SFB1009/A06]
  2. graduate school of the Cells-in-Motion Interfaculty Center and the MaxPlanck Institute for Molecular Biomedicine (CIM/IMPRS)

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This study investigated the membrane resealing process in endothelial cells under mechanical stress and found that Ca2+-dependent annexin-phospholipid interactions are crucial for efficient membrane wound repair in endothelial cells.
Vascular endothelial cells are subject to mechanical stress resulting from blood flow and interactions with leukocytes. Stress occurs at the apical, vessel-facing cell surface and leads to membrane ruptures that have to be resealed to ensure cell survival. To mimic this process, we developed a laser ablation protocol selectively inducing wounds in the apical plasma membrane of endothelial cells. We show that Ca2+-dependent membrane resealing is initiated following this wounding protocol and that the process is accompanied by substantial membrane lipid dynamics at the wound site. Specifically, phosphatidylinositol (4,5)-bisphosphate, phosphatidylserine and phosphatidic acid rapidly accumulate at membrane wounds forming potential interaction platforms for Ca2+/phospholipid binding proteins of the annexin (Anx) family that are also recruited within seconds after wounding. Depletion of one annexin, AnxA2, and its putative binding partner S100A11 interferes with membrane resealing suggesting that Ca2+-dependent annexin-phospholipid interactions are required for efficient membrane wound repair in endothelial cells.

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