Concepedia

Publication | Open Access

Angiotensin II synergizes with BAFF to promote atheroprotective regulatory B cells

34

Citations

44

References

2017

Year

Abstract

Angiotensin II (AngII) promotes hypertension, atherogenesis, vascular aneurysm and impairs post-ischemic cardiac remodeling through concerted roles on vascular cells, monocytes and T lymphocytes. However, the role of AngII in B lymphocyte responses is largely unexplored. Here, we show that chronic B cell depletion (Baffr deficiency) significantly reduces atherosclerosis in Apoe <sup>-/-</sup> mice infused with AngII. While adoptive transfer of B cells in Apoe <sup>-/-</sup> /Baffr <sup>-/-</sup> mice reversed atheroprotection in the absence of AngII, infusion of AngII in B cell replenished Apoe <sup>-/-</sup> /Baffr <sup>-/-</sup> mice unexpectedly prevented the progression of atherosclerosis. Atheroprotection observed in these mice was associated with a significant increase in regulatory CD1d<sup>hi</sup>CD5<sup>+</sup> B cells, which produced high levels of interleukin (IL)-10 (B10 cells). Replenishment of Apoe <sup>-/-</sup> /Baffr <sup>-/-</sup> mice with Il10 <sup>-/-</sup> B cells reversed AngII-induced B cell-dependent atheroprotection, thus highlighting a protective role of IL-10<sup>+</sup> regulatory B cells in this setting. Transfer of AngII type 1A receptor deficient (Agtr1a <sup>-/-</sup>) B cells into Apoe <sup>-/-</sup> /Baffr <sup>-/-</sup> mice substantially reduced the production of IL-10 by B cells and prevented the AngII-dependent atheroprotective B cell phenotype. Consistent with the in vivo data, AngII synergized with BAFF to induce IL-10 production by B cells in vitro via AngII type 1A receptor. Our data demonstrate a previously unknown synergy between AngII and BAFF in inducing IL-10 production by B cells, resulting in atheroprotection.

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