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Proteomic analysis of circulating monocytes in Chinese premenopausal females with extremely discordant bone mineral density
Authors:Deng Fei-Yan  Liu Yao-Zhong  Li Li-Ming  Jiang Chen  Wu Shan  Chen Yuan  Jiang Hui  Yang Fang  Xiong Ji-Xian  Xiao Peng  Xiao Su-Mei  Tan Li-Jun  Sun Xiao  Zhu Xue-Zhen  Liu Man-Yuan  Lei Shu-Feng  Chen Xiang-Ding  Xie Jing-Yun  Xiao Gary G  Liang Song-Ping  Deng Hong-Wen
Affiliation:Laboratory of Molecular and Statistical Genetics, College of Life Sciences, Hunan Normal University, Hunan, P. R. China.
Abstract:Osteoporosis (OP) is a major public health problem, mainly characterized by low bone mineral density (BMD). Circulating monocytes (CMCs) may serve as progenitors of osteoclasts and produce a wide variety of factors important to bone metabolism. However, the specific action mechanism of CMCs in the pathogenesis of OP is far from clear. We performed a comparative protein expression profiling study of CMCs in Chinese premenopausal females with extremely discordant BMD, identified a total of 38 differentially expressed proteins, and confirmed with Western blotting five proteins: ras suppressor protein1 (RSU1), gelsolin (GSN), manganese-containing superoxide dismutase (SOD2), glutathione peroxidase 1(GPX1), and prolyl 4-hydroxylase beta subunit (P4HB). These proteins might affect CMCs' trans-endothelium, differentiation, and/or downstream osteoclast functions, thus contribute to differential osteoclastogenesis and finally lead to BMD variation. The findings promote our understanding of the role of CMCs in BMD determination, and provide an insight into the pathogenesis of human OP.
Keywords:Bone mineral density  Circulating monocyte  Osteoclastogenesis  Protein
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