| Literature DB >> 30231995 |
Lilian Schimmel1, Miesje van der Stoel2, Carmela Rianna3, Anne-Marieke van Stalborch1, Aafke de Ligt1, Mark Hoogenboezem4, Simon Tol4, Jos van Rijssel1, Robert Szulcek5, Harm Jan Bogaard5, Patrick Hofmann6, Reinier Boon6, Manfred Radmacher3, Vivian de Waard2, Stephan Huveneers2, Jaap D van Buul7.
Abstract
Leukocytes follow the well-defined steps of rolling, spreading, and crawling prior to diapedesis through endothelial cells (ECs). We found increased expression of DLC-1 in stiffness-associated diseases like atherosclerosis and pulmonary arterial hypertension. Depletion of DLC-1 in ECs cultured on stiff substrates drastically reduced cell stiffness and mimicked leukocyte transmigration kinetics observed for ECs cultured on soft substrates. Mechanistic studies revealed that DLC-1-depleted ECs or ECs cultured on soft substrates failed to recruit the actin-adaptor proteins filamin B, α-actinin-4, and cortactin to clustered ICAM-1, thereby preventing the ICAM-1 adhesome formation and impairing leukocyte spreading. This was rescued by overexpressing DLC-1, resulting in ICAM-1 adhesome stabilization and leukocyte spreading. Our results reveal an essential role for substrate stiffness-regulated endothelial DLC-1, independent of its GAP domain, in locally stabilizing the ICAM-1 adhesome to promote leukocyte spreading, essential for efficient leukocyte transendothelial migration.Entities:
Keywords: DLC-1; ICAM-1; diapedesis; endothelial; leukocyte; mechanosignaling; rolling; spreading; stiffness; transmigration
Year: 2018 PMID: 30231995 DOI: 10.1016/j.celrep.2018.08.045
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423