| Literature DB >> 28679951 |
Allison E Norlander1, Mohamed A Saleh2,3, Arvind K Pandey4, Hana A Itani2, Jing Wu1, Liang Xiao2, Jooeun Kang1, Bethany L Dale1, Slavina B Goleva1, Fanny Laroumanie2, Liping Du5, David G Harrison1,2, Meena S Madhur1,2,3.
Abstract
We previously showed that angiotensin II (Ang II) increases T cell production of IL-17A, and that mice deficient in IL-17A have blunted hypertension and attenuated renal and vascular dysfunction. It was recently shown that salt enhances IL-17A production from CD4+ T cells via a serum- and glucocorticoid-regulated kinase 1-dependent (SGK1-dependent) pathway. Thus, we tested the hypothesis that SGK1 signaling in T cells promotes hypertension and contributes to end-organ damage. We show that loss of T cell SGK1 results in a blunted hypertensive response to Ang II infusion by 25 mmHg. Importantly, renal and vascular inflammation is abrogated in these mice compared with control mice. Furthermore, mice lacking T cell SGK1 are protected from Ang II-induced endothelial dysfunction and renal injury. Loss of T cell SGK1 also blunts blood pressure and vascular inflammation in response to deoxycorticosterone acetate-salt (DOCA-salt) hypertension. Finally, we demonstrate that the Na+-K+-2Cl- cotransporter 1 (NKCC1) is upregulated in Th17 cells and is necessary for the salt-induced increase in SGK1 and the IL-23 receptor. These studies demonstrate that T cell SGK1 and NKCC1 may be novel therapeutic targets for the treatment of hypertension and identify a potentially new mechanism by which salt contributes to hypertension.Entities:
Keywords: Adaptive immunity; Cardiology; Cardiovascular disease; Hypertension; Inflammation
Year: 2017 PMID: 28679951 PMCID: PMC5499362 DOI: 10.1172/jci.insight.92801
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708