TY - JOUR
T1 - Myeloid CD11c+ antigen-presenting cells ablation prevents hypertension in response to angiotensin II plus high-salt diet
AU - Hevia, Daniel
AU - Araos, Patricio
AU - Prado, Carolina
AU - Luppichini, Eugenia Fuentes
AU - Rojas, MacArena
AU - Alzamora, Rodrigo
AU - Cifuentes-Araneda, Flavia
AU - Gonzalez, Alexis A.
AU - Amador, Cristian A.
AU - Pacheco, Rodrigo
AU - Michea, Luis
N1 - Funding Information:
This work was supported by FONDECYT-Regular grants 1130550 and 1171869 (L. Michea), 1151423 (R. Alzamora) and 1170093 (R. Pacheco), CONICYT-Basal PFB-16 (R. Pacheco), FONDECYT-Iniciació Amador), FONDECYT-Postdoctorado 3160383 (C. Prado), CONICYT-Doctorado 21130762 (D. Hevia) and 21130482 (P. Araos), and DI-1224-16/R (R. Pacheco) from Universidad Andres Bello. The Millennium Institute on Immunology and Immunotherapy (MIII; P09/016-F ICM) and The Millennium Nucleus of Ion Channels-Associated Diseases (MiNICAD) are supported by the Iniciativa Científica Milenio of the Ministry of Economy, Development and Tourism (Chile).
Publisher Copyright:
© 2017 The Authors.
PY - 2018
Y1 - 2018
N2 - Increasing evidence shows that antigen-presenting cells (APCs) are involved in the development of inflammation associated to hypertension. However, the potential role of APCs in the modulation of renal sodium transport has not been addressed. We hypothesized that APCs participate in renal sodium transport and, thus, development of high blood pressure in response to angiotensin II plus a high-salt diet. Using transgenic mice that allow the ablation of CD11chigh APCs, we studied renal sodium transport, the intrarenal renin-angiotensin system components, blood pressure, and cardiac/renal tissue damage in response to angiotensin II plus a high-salt diet. Strikingly, we found that APCs are required for the development of hypertension and that the ablation/restitution of APCs produces rapid changes in the blood pressure in mice with angiotensin II plus a high-salt diet. Moreover, APCs were necessary for the induction of intrarenal renin-angiotensin system components and affected the modulation of natriuresis and tubular sodium transporters. Consistent with the prevention of hypertension, the ablation of APCs also prevented cardiac hypertrophy and the induction of several indicators of renal and cardiac damage. Thus, our fndings indicate a prominent role of APCs as modulators of blood pressure by mechanisms including renal sodium handling, with kinetics that suggest the involvement of tubular cell functions in addition to the modulation of inflammation and adaptive immune response.
AB - Increasing evidence shows that antigen-presenting cells (APCs) are involved in the development of inflammation associated to hypertension. However, the potential role of APCs in the modulation of renal sodium transport has not been addressed. We hypothesized that APCs participate in renal sodium transport and, thus, development of high blood pressure in response to angiotensin II plus a high-salt diet. Using transgenic mice that allow the ablation of CD11chigh APCs, we studied renal sodium transport, the intrarenal renin-angiotensin system components, blood pressure, and cardiac/renal tissue damage in response to angiotensin II plus a high-salt diet. Strikingly, we found that APCs are required for the development of hypertension and that the ablation/restitution of APCs produces rapid changes in the blood pressure in mice with angiotensin II plus a high-salt diet. Moreover, APCs were necessary for the induction of intrarenal renin-angiotensin system components and affected the modulation of natriuresis and tubular sodium transporters. Consistent with the prevention of hypertension, the ablation of APCs also prevented cardiac hypertrophy and the induction of several indicators of renal and cardiac damage. Thus, our fndings indicate a prominent role of APCs as modulators of blood pressure by mechanisms including renal sodium handling, with kinetics that suggest the involvement of tubular cell functions in addition to the modulation of inflammation and adaptive immune response.
KW - Angiotensin II
KW - Antigen-presenting cells
KW - Epithelial sodium channel
KW - Hypertension
KW - Inflammation
UR - http://www.scopus.com/inward/record.url?scp=85051681622&partnerID=8YFLogxK
U2 - 10.1161/HYPERTENSIONAHA.117.10145
DO - 10.1161/HYPERTENSIONAHA.117.10145
M3 - Article
C2 - 29378857
AN - SCOPUS:85051681622
SN - 0194-911X
VL - 71
SP - 709
EP - 718
JO - Hypertension
JF - Hypertension
IS - 4
ER -