| Literature DB >> 33200983 |
LouJin Song1, Xian Chen2,3, Terri A Swanson4, Brianna LaViolette2, Jincheng Pang1, Teresa Cunio1,5, Michael W Nagle1,6, Shoh Asano1, Katherine Hales1, Arun Shipstone7, Hanna Sobon7, Sabra D Al-Harthy2,3, Youngwook Ahn8, Steven Kreuser2, Andrew Robertson3, Casey Ritenour3, Frank Voigt3, Magalie Boucher3, Furong Sun4, William C Sessa9, Rachel J Roth Flach1.
Abstract
The lymphatic vasculature is involved in the pathogenesis of acute cardiac injuries, but little is known about its role in chronic cardiac dysfunction. Here, we demonstrate that angiotensin II infusion induced cardiac inflammation and fibrosis at 1 week and caused cardiac dysfunction and impaired lymphatic transport at 6 weeks in mice, while co-administration of VEGFCc156s improved these parameters. To identify novel mechanisms underlying this protection, RNA sequencing analysis in distinct cell populations revealed that VEGFCc156s specifically modulated angiotensin II-induced inflammatory responses in cardiac and peripheral lymphatic endothelial cells. Furthermore, telemetry studies showed that while angiotensin II increased blood pressure acutely in all animals, VEGFCc156s-treated animals displayed a delayed systemic reduction in blood pressure independent of alterations in angiotensin II-mediated aortic stiffness. Overall, these results demonstrate that VEGFCc156s had a multifaceted therapeutic effect to prevent angiotensin II-induced cardiac dysfunction by improving cardiac lymphatic function, alleviating fibrosis and inflammation, and ameliorating hypertension.Entities:
Keywords: cardiac dysfunction; cell biology; endothelial; fibrosis; human; hypertension; inflammation; lymphatic; medicine; mouse
Mesh:
Substances:
Year: 2020 PMID: 33200983 PMCID: PMC7695461 DOI: 10.7554/eLife.58376
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140