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RUFY4 deletion prevents pathological bone loss by blocking endo-lysosomal trafficking of osteoclasts

摘要Mature osteoclasts degrade bone matrix by exocytosis of active proteases from secretory lysosomes through a ruffled border.However,the molecular mechanisms underlying lysosomal trafficking and secretion in osteoclasts remain largely unknown.Here,we show with GeneChip analysis that RUN and FYVE domain-containing protein 4(RUFY4)is strongly upregulated during osteoclastogenesis.Mice lacking Rufy4 exhibited a high trabecular bone mass phenotype with abnormalities in osteoclast function in vivo.Furthermore,deleting Rufy4 did not affect osteoclast differentiation,but inhibited bone-resorbing activity due to disruption in the acidic maturation of secondary lysosomes,their trafficking to the membrane,and their secretion of cathepsin K into the extracellular space.Mechanistically,RUFY4 promotes late endosome-lysosome fusion by acting as an adaptor protein between Rab7 on late endosomes and LAMP2 on primary lysosomes.Consequently,Rufy4-deficient mice were highly protected from lipopolysaccharide-and ovariectomy-induced bone loss.Thus,RUFY4 plays as a new regulator in osteoclast activity by mediating endo-lysosomal trafficking and have a potential to be specific target for therapies against bone-loss diseases such as osteoporosis.

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作者 Minhee Kim [1] Jin Hee Park [2] Miyeon Go [1] Nawon Lee [1] Jeongin Seo [1] Hana Lee [3] Doyong Kim [3] Hyunil Ha [4] Taesoo Kim [7] Myeong Seon Jeong [5] Suree Kim [6] Han Sung Kim [3] Dongmin Kang [8] Hyunbo Shim [1] Soo Young Lee [7] 学术成果认领
作者单位 Department of Life Science,Ewha Womans University,Seoul 03760,South Korea [1] Department of Life Science,Ewha Womans University,Seoul 03760,South Korea;The Research Center for Cellular Homeostasis,Ewha Womans University,Seoul 03760,South Korea [2] Department of Biomedical Engineering,Yonsei University,Wonju 26493,South Korea [3] KM Convergence Research Division,Korea Institute of Oriental Medicine,Daejeon 34054,South Korea [4] Chuncheon Center,Korea Basic Science Institute,Chuncheon 24341,South Korea [5] Fluorescence Core Imaging Center and Bioimaging Data Curation Center,Ewha Womans University,Seoul 03760,South Korea [6] Department of Life Science,Ewha Womans University,Seoul 03760,South Korea;The Research Center for Cellular Homeostasis,Ewha Womans University,Seoul 03760,South Korea;Multitasking Macrophage Research Center,Ewha Womans University,Seoul 03760,South Korea [7] Department of Life Science,Ewha Womans University,Seoul 03760,South Korea;Fluorescence Core Imaging Center and Bioimaging Data Curation Center,Ewha Womans University,Seoul 03760,South Korea [8]
栏目名称 ORIGINAL ARTICLES
DOI 10.1038/s41413-024-00326-8
发布时间 2024-08-19
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骨研究(英文版)

骨研究(英文版)

2024年12卷2期

407-420页

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