| Literature DB >> 31145860 |
Hye In Lee1, Jiae Lee1, Donghyun Hwang2, Gong-Rak Lee1, Narae Kim1, Minjeong Kwon1, Hana Lee2, Donglan Piao3, Hyun Jin Kim1, Nam Young Kim1, Han Sung Kim2, Eun Kyoung Seo3, Dongmin Kang1, Woojin Jeong1.
Abstract
Excessive osteoclast activity can lead to an imbalance between the synthesis and breakdown of bone, with pathologic consequences that include osteoporosis and periodontitis. Thus, controlling osteoclast differentiation and function has significant therapeutic implications. In this study, we investigated the effects of dehydrocostus lactone (DL) on osteoclast differentiation and activation and elucidated the possible mechanisms underlying these processes. DL suppressed osteoclast differentiation by reducing the expression of the nuclear factor of activated T-cells, cytoplasmic 1. When used to challenge differentiated osteoclasts, DL also effectively inhibited their enlargement and resorption activity, and biochemical approaches revealed that DL attenuates osteoclast activation by inhibiting the migration and lysosome biogenesis and secretion via the down-regulation of integrin β3, PKC-β, and autophagy related 5 expression. Furthermore, DL prevented bone destruction in inflammation- and ovariectomy-induced osteolytic mouse models. These results indicate that DL has therapeutic potential to treat bone diseases caused by excessive or hyperactive osteoclasts.-Lee, H. I., Lee, J., Hwang, D., Lee, G.-R., Kim, N., Kwon, M., Lee, H., Piao, D., Kim, H. J., Kim, N. Y., Kim, H. S., Seo, E. K., Kang, D., Jeong, W. Dehydrocostus lactone suppresses osteoclast differentiation by regulating NFATc1 and inhibits osteoclast activation through modulating migration and lysosome function.Entities:
Keywords: Atg5; PKC-β; bone; integrin
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Year: 2019 PMID: 31145860 DOI: 10.1096/fj.201900862R
Source DB: PubMed Journal: FASEB J ISSN: 0892-6638 Impact factor: 5.191