Author:
Soma Tomoya,Iwasaki Ryotaro,Sato Yuiko,Kobayashi Tami,Ito Eri,Matsumoto Tatsuaki,Kimura Atsushi,Miyamoto Kana,Matsumoto Morio,Nakamura Masaya,Morita Mayu,Asoda Seiji,Kawana Hiromasa,Nakagawa Taneaki,Miyamoto Takeshi
Abstract
AbstractInvasive dental treatment such as tooth extraction following treatment with strong anti-bone resorptive agents, including bisphosphonates and denosumab, reportedly promotes osteonecrosis of the jaw (ONJ) at the extraction site, but strategies to prevent ONJ remain unclear. Here we show that in mice, administration of either active vitamin D analogues, antibiotics or anti-inflammatory agents can prevent ONJ development induced by tooth extraction during treatment with the bisphosphonate zoledronate. Specifically, tooth extraction during treatment with zoledronate induced osteonecrosis in mice, but administration of either 1,25(OH)2D3 or ED71, both active vitamin D analogues, significantly antagonized osteonecrosis development, even under continuous zoledronate treatment. 1,25(OH)2D3 or ED71 administration also significantly inhibited osteocyte apoptosis induced by tooth extraction and bisphosphonate treatment. Administration of either active vitamin D analogue significantly inhibited elevation of serum inflammatory cytokine levels in mice in response to injection of lipopolysaccharide, an infection mimetic. Furthermore, administration of either anti-inflammatory or antibiotic reagents significantly blocked ONJ development following tooth extraction and zoledronate treatment. These findings suggest that administration of active vitamin D, anti-inflammatory agents or antibiotics could prevent ONJ development induced by tooth extraction in patients treated with zoledronate.
Funder
grant-in-aid for Scientific Research in Japan
Japan Agency for Medical Research and Development
Publisher
Springer Science and Business Media LLC
Cited by
14 articles.
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