| Literature DB >> 30030370 |
Justyna Lisowska1,2,3, Claudia Jasmin Rödel4, Sandra Manet1,2,3, Yekaterina A Miroshnikova1,2,3, Cyril Boyault1,2,3, Emmanuelle Planus1,2,3, Richard De Mets2,5, Hsiao-Hui Lee6, Olivier Destaing1,2,3, Hichem Mertani7, Gwénola Boulday8,9,10, Elisabeth Tournier-Lasserve8,9,10, Martial Balland2,5, Salim Abdelilah-Seyfried4,11, Corinne Albiges-Rizo12,2,3, Eva Faurobert12,2,3.
Abstract
Endothelial integrity relies on a mechanical crosstalk between intercellular and cell-matrix interactions. This crosstalk is compromised in hemorrhagic vascular lesions of patients carrying loss-of-function mutations in cerebral cavernous malformation (CCM) genes. RhoA/ROCK-dependent cytoskeletal remodeling is central to the disease, as it causes unbalanced cell adhesion towards increased cell-extracellular matrix adhesions and destabilized cell-cell junctions. This study reveals that CCM proteins directly orchestrate ROCK1 and ROCK2 complementary roles on the mechanics of the endothelium. CCM proteins act as a scaffold, promoting ROCK2 interactions with VE-cadherin and limiting ROCK1 kinase activity. Loss of CCM1 (also known as KRIT1) produces excessive ROCK1-dependent actin stress fibers and destabilizes intercellular junctions. Silencing of ROCK1 but not ROCK2 restores the adhesive and mechanical homeostasis of CCM1 and CCM2-depleted endothelial monolayers, and rescues the cardiovascular defects of ccm1 mutant zebrafish embryos. Conversely, knocking down Rock2 but not Rock1 in wild-type zebrafish embryos generates defects reminiscent of the ccm1 mutant phenotypes. Our study uncovers the role of the CCM1-CCM2 complex in controlling ROCK1 and ROCK2 to preserve endothelial integrity and drive heart morphogenesis. Moreover, it solely identifies the ROCK1 isoform as a potential therapeutic target for the CCM disease.Entities:
Keywords: CCM; Endothelial integrity; Mechanotransduction; ROCK
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Year: 2018 PMID: 30030370 DOI: 10.1242/jcs.216093
Source DB: PubMed Journal: J Cell Sci ISSN: 0021-9533 Impact factor: 5.285