| Literature DB >> 26456334 |
Jau-Yi Li1, Patrizia D'Amelio2, Jerid Robinson1, Lindsey D Walker1, Chiara Vaccaro1, Tao Luo1, Abdul Malik Tyagi1, Mingcan Yu1, Michael Reott1, Francesca Sassi2, Ilaria Buondonno2, Jonathan Adams1, M Neale Weitzmann3, Giovanni Carlo Isaia2, Roberto Pacifici4.
Abstract
Primary hyperparathyroidism (PHPT) is a common cause of bone loss that is modeled by continuous PTH (cPTH) infusion. Here we show that the inflammatory cytokine IL-17A is upregulated by PHPT in humans and cPTH in mice. In humans, IL-17A is normalized by parathyroidectomy. In mice, treatment with anti-IL-17A antibody and silencing of IL-17A receptor IL-17RA prevent cPTH-induced osteocytic and osteoblastic RANKL production and bone loss. Mechanistically, cPTH stimulates conventional T cell production of TNFα (TNF), which increases the differentiation of IL-17A-producing Th17 cells via TNF receptor 1 (TNFR1) signaling in CD4(+) cells. Moreover, cPTH enhances the sensitivity of naive CD4(+) cells to TNF via GαS/cAMP/Ca(2+) signaling. Accordingly, conditional deletion of GαS in CD4(+) cells and treatment with the calcium channel blocker diltiazem prevents Th17 cell expansion and blocks cPTH-induced bone loss. Neutralization of IL-17A and calcium channel blockers may thus represent novel therapeutic strategies for hyperparathyroidism.Entities:
Keywords: IL-17; IL-17 antibody; IL-17R; PTH; T cells; Th17 cells; bone; hyperparathyroidism
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Year: 2015 PMID: 26456334 PMCID: PMC4635034 DOI: 10.1016/j.cmet.2015.09.012
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 27.287