An integrated multi-omics analysis reveals osteokines involved in global regulation

计算生物学 串扰 衰老 细胞生物学 骨髓 平衡 成骨细胞 生物 骨重建 分泌物 生物信息学 免疫学 内分泌学 生物化学 体外 物理 光学
作者
Wenquan Liang,Tiantian Wei,Le Hu,Meijun Chen,Liping Tong,Zhou Wu,Xingwei Duan,Xiaoyang Zhao,Weijie Zhou,Qing Jiang,Guozhi Xiao,Weiguo Zou,Di Chen,Zhipeng Zou,Xiaochun Bai
出处
期刊:Cell Metabolism [Cell Press]
卷期号:36 (5): 1144-1163.e7 被引量:29
标识
DOI:10.1016/j.cmet.2024.03.006
摘要

Highlights•Multi-omic analysis reveals previously unknown osteokines and their cellular sources•Osteokines change in response to aging and mechanical dynamics•Osteokines establish intercellular crosstalk between bone and extraskeletal organs•FABP3, an aging-related osteokine, promotes VSMC senescence related to atherogenesisSummaryBone secretory proteins, termed osteokines, regulate bone metabolism and whole-body homeostasis. However, fundamental questions as to what the bona fide osteokines and their cellular sources are and how they are regulated remain unclear. In this study, we analyzed bone and extraskeletal tissues, osteoblast (OB) conditioned media, bone marrow supernatant (BMS), and serum, for basal osteokines and those responsive to aging and mechanical loading/unloading. We identified 375 candidate osteokines and their changes in response to aging and mechanical dynamics by integrating data from RNA-seq, scRNA-seq, and proteomic approaches. Furthermore, we analyzed their cellular sources in the bone and inter-organ communication facilitated by them (bone-brain, liver, and aorta). Notably, we discovered that senescent OBs secrete fatty-acid-binding protein 3 to propagate senescence toward vascular smooth muscle cells (VSMCs). Taken together, we identified previously unknown candidate osteokines and established a dynamic regulatory network among them, thus providing valuable resources to further investigate their systemic roles.Graphical abstract
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