| Literature DB >> 30054204 |
Hwee Ying Lim1, Sheau Yng Lim1, Chek Kun Tan2, Chung Hwee Thiam1, Chi Ching Goh3, Daniel Carbajo3, Samantha Hui Shang Chew1, Peter See3, Svetoslav Chakarov3, Xiao Nong Wang4, Li Hui Lim1, Louise A Johnson5, Josephine Lum3, Chui Yee Fong6, Ariff Bongso6, Arijit Biswas6, Chern Goh1, Maximilien Evrard3, Kim Pin Yeo1, Ranu Basu7, Jun Kit Wang8, Yingrou Tan3, Rohit Jain9, Shweta Tikoo9, Cleo Choong8, Wolfgang Weninger9, Michael Poidinger3, Richard E Stanley7, Matthew Collin4, Nguan Soon Tan10, Lai Guan Ng3, David G Jackson5, Florent Ginhoux3, Véronique Angeli11.
Abstract
The maintenance of appropriate arterial tone is critically important for normal physiological arterial function. However, the cellular and molecular mechanisms remain poorly defined. Here, we have shown that in the mouse aorta, resident macrophages prevented arterial stiffness and collagen deposition in the steady state. Using phenotyping, transcriptional profiling, and targeted deletion of Csf1r, we have demonstrated that these macrophages-which are a feature of blood vessels invested with smooth muscle cells (SMCs) in both mouse and human tissues-expressed the hyaluronan (HA) receptor LYVE-l. Furthermore, we have shown they possessed the unique ability to modulate collagen expression in SMCs by matrix metalloproteinase MMP-9-dependent proteolysis through engagement of LYVE-1 with the HA pericellular matrix of SMCs. Our study has unveiled a hitherto unknown homeostatic contribution of arterial LYVE-1+ macrophages through the control of collagen production by SMCs and has identified a function of LYVE-1 in leukocytes.Entities:
Keywords: LYVE-1; arterial stiffness; artery; hyaluronan; macrophage; smooth muscle cell
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Year: 2018 PMID: 30054204 DOI: 10.1016/j.immuni.2018.06.008
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745