| Literature DB >> 26792721 |
Toshimi Tando1, Yuiko Sato2, Kana Miyamoto1, Mayu Morita3, Tami Kobayashi1, Atsushi Funayama1, Arihiko Kanaji1, Wu Hao1, Ryuichi Watanabe1, Takatsugu Oike1, Masaya Nakamura1, Morio Matsumoto1, Yoshiaki Toyama1, Takeshi Miyamoto4.
Abstract
The number of osteoporosis patients is increasing not only in women but in men. Male osteoporosis occurs due to aging or androgen depletion therapies, leading to fractures. However, molecular mechanisms underlying male osteoporosis remain unidentified. Here, we show that hypoxia inducible factor 1 alpha (Hif1α) is required for development of testosterone deficiency-induced male osteoporosis. We found that in mice Hif1α protein accumulates in osteoclasts following orchidectomy (ORX) in vivo. In vitro, Hif1α protein accumulated in osteoclasts cultured in hypoxic conditions, but Hif1α protein rather than mRNA levels were suppressed by testosterone treatment, even in hypoxia. Administration of a Hif1α inhibitor to ORX mice abrogated testosterone deficiency-induced osteoclast activation and bone loss but did not alter osteoclast activities or bone phenotypes in sham-operated, testosterone-sufficient animals. We conclude that Hif1α protein accumulation due to testosterone-deficiency promotes development of male osteoporosis. Thus Hif1α protein could be targeted to inhibit pathologically-activated osteoclasts under testosterone-deficient conditions to treat male osteoporosis patients.Entities:
Keywords: Bone; Hif1α; Male; Osteoclasts; Osteoporosis; Testosterone
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Year: 2016 PMID: 26792721 DOI: 10.1016/j.bbrc.2016.01.033
Source DB: PubMed Journal: Biochem Biophys Res Commun ISSN: 0006-291X Impact factor: 3.575