Identification and Functional Characterization of Metabolites for Bone Mass in Peri- and Postmenopausal Chinese Women

代谢物 破骨细胞 内分泌学 内科学 代谢组学 骨重建 骨矿物 成骨细胞 去卵巢大鼠 医学 体内 骨质疏松症 化学 生物 雌激素 生物信息学 生物化学 体外 遗传学 受体
作者
Rui Gong,Hong‐Mei Xiao,Yinhua Zhang,Qi Zhao,Kuan-Jui Su,Xu Lin,Chenglin Mo,Qiang Zhou,Yinan Du,Feng-Ye Lyu,Yuancheng Chen,Cheng Peng,Huimin Liu,Shengqiang Hu,Dao-Yan Pan,Zhi Chen,Zhangfang Li,Ruanbao Zhou,Xia-Fang Wang,Jun‐Min Lu,Zeng‐Xin Ao,Yu-Qian Song,Chanyan Weng,Qing Tian,Martin Schiller,Christopher J. Papasian,Marco Brotto,Hui Shen,Jie Shen,Hong‐Wen Deng
出处
期刊:The Journal of Clinical Endocrinology and Metabolism [The Endocrine Society]
卷期号:106 (8): e3159-e3177 被引量:14
标识
DOI:10.1210/clinem/dgab146
摘要

Although metabolic profiles appear to play an important role in menopausal bone loss, the functional mechanisms by which metabolites influence bone mineral density (BMD) during menopause are largely unknown.We aimed to systematically identify metabolites associated with BMD variation and their potential functional mechanisms in peri- and postmenopausal women.We performed serum metabolomic profiling and whole-genome sequencing for 517 perimenopausal (16%) and early postmenopausal (84%) women aged 41 to 64 years in this cross-sectional study. Partial least squares regression and general linear regression analysis were applied to identify BMD-associated metabolites, and weighted gene co-expression network analysis was performed to construct co-functional metabolite modules. Furthermore, we performed Mendelian randomization analysis to identify causal relationships between BMD-associated metabolites and BMD variation. Finally, we explored the effects of a novel prominent BMD-associated metabolite on bone metabolism through both in vivo/in vitro experiments.Twenty metabolites and a co-functional metabolite module (consisting of fatty acids) were significantly associated with BMD variation. We found dodecanoic acid (DA), within the identified module causally decreased total hip BMD. Subsequently, the in vivo experiments might support that dietary supplementation with DA could promote bone loss, as well as increase the osteoblast and osteoclast numbers in normal/ovariectomized mice. Dodecanoic acid treatment differentially promoted osteoblast and osteoclast differentiation, especially for osteoclast differentiation at higher concentrations in vitro (eg,10, 100 μM).This study sheds light on metabolomic profiles associated with postmenopausal osteoporosis risk, highlighting the potential importance of fatty acids, as exemplified by DA, in regulating BMD.

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