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Aged bone matrix-derived extracellular vesicles as a messenger for calcification paradox. 2022
Zhen-Xing Wang, and
Zhong-Wei Luo, and
Fu-Xing-Zi Li, and
Jia Cao, and
Shan-Shan Rao, and
Yi-Wei Liu, and
Yi-Yi Wang, and
Guo-Qiang Zhu, and
Jiang-Shan Gong, and
Jing-Tao Zou, and
Qiang Wang, and
Yi-Juan Tan, and
Yan Zhang, and
Yin Hu, and
You-You Li, and
Hao Yin, and
Xiao-Kai Wang, and
Ze-Hui He, and
Lu Ren, and
Zheng-Zhao Liu, and
Xiong-Ke Hu, and
Ling-Qing Yuan, and
Ran Xu, and
Chun-Yuan Chen, and
Hui Xie
Department of Orthopedics, Xiangya Hospital, Central South University, Changsha, Hunan, China.
Adipocyte differentiation of bone marrow mesenchymal stem/stromal cells (BMSCs) instead of osteoblast formation contributes to age- and menopause-related marrow adiposity and osteoporosis. Vascular calcification often occurs with osteoporosis, a contradictory association called "calcification paradox". Here we show that extracellular vesicles derived from aged bone matrix (AB-EVs) during bone resorption favor BMSC adipogenesis rather than osteogenesis and augment calcification of vascular smooth muscle cells. Intravenous or intramedullary injection of AB-EVs promotes bone-fat imbalance and exacerbates Vitamin D3 (VD3)-induced vascular calcification in young or old mice. Alendronate (ALE), a bone resorption inhibitor, down-regulates AB-EVs release and attenuates aging- and ovariectomy-induced bone-fat imbalance. In the VD3-treated aged mice, ALE suppresses the ovariectomy-induced aggravation of vascular calcification. MiR-483-5p and miR-2861 are enriched in AB-EVs and essential for the AB-EVs-induced bone-fat imbalance and exacerbation of vascular calcification. Our study uncovers the role of AB-EVs as a messenger for calcification paradox by transferring miR-483-5p and miR-2861.
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