| Literature DB >> 24833351 |
Jessica Pruessmeyer1, Franz Martin Hess1, Henriette Alert1, Esther Groth1, Tobias Pasqualon1, Nicole Schwarz2, Stella Nyamoya1, Jos Kollert1, Emiel van der Vorst3, Marjo Donners3, Christian Martin1, Stefan Uhlig1, Paul Saftig4, Daniela Dreymueller1, Andreas Ludwig1.
Abstract
Inflammation is a key process in various diseases, characterized by leukocyte recruitment to the inflammatory site. This study investigates the role of a disintegrin and a metalloproteinase (ADAM) 10 and ADAM17 for leukocyte migration in vitro and in a murine model of acute pulmonary inflammation. Inhibition experiments or RNA knockdown indicated that monocytic THP-1 cells and primary human neutrophils require ADAM10 but not ADAM17 for efficient chemokine-induced cell migration. Signaling and adhesion events that are linked to cell migration such as p38 and ρ GTPase-family activation, F-actin polymerization, adhesion to fibronectin, and up-regulation of α5 integrin were also dependent on ADAM10 but not ADAM17. This was confirmed with leukocytes isolated from mice lacking either ADAM10 or ADAM17 in all hematopoietic cells (vav 1 guanine nucleotide exchange factor [Vav]-Adam10(-/-) or Vav-Adam17(-/-) mice). In lipopolysaccharide-induced acute pulmonary inflammation, alveolar recruitment of neutrophils and monocytes was transiently increased in Vav-Adam17(-/-) but steadily reduced in Vav-Adam10(-/-) mice. This deficit in alveolar leukocyte recruitment was also observed in LysM-Adam10(-/-) mice lacking ADAM10 in myeloid cells and correlated with protection against edema formation. Thus, with regard to leukocyte migration, leukocyte-expressed ADAM10 but not ADAM17 displays proinflammatory activities and may therefore serve as a target to limit inflammatory cell recruitment.Entities:
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Year: 2014 PMID: 24833351 DOI: 10.1182/blood-2013-09-511543
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 22.113