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Cell Death and Disease, volume 13, issue 5, publication number 494

miR-188-3p targets skeletal endothelium coupling of angiogenesis and osteogenesis during ageing

Wen Zhen He 1
Mi Yang 1
YangZi Jiang 2
Chen He 1
Yu-Chen Sun 1
Ling Liu 1
Mei Huang 1
Yu Rui Jiao 1
KAI XUAN CHEN 1
Jing Hou 1
Min Huang 1
Yi Li Xu 1
Xu Feng 1
Ya Liu 1
Qi Guo 1
Hui Peng 1
Yan Huang 1
Tian Su 1
Ye Xiao 1
Yusheng Li 3, 4, 5
Chao Zeng 3, 4, 5
Guanghua Lei 3, 4, 5
Xiang-Hang Luo 1, 5, 6
Chang Jun Li 1, 5, 6
Show full list: 24 authors
Publication typeJournal Article
Publication date2022-05-25
scimago Q1
SJR2.447
CiteScore15.1
Impact factor8.1
ISSN20414889
Cancer Research
Cell Biology
Cellular and Molecular Neuroscience
Immunology
Abstract
A specific bone capillary subtype, namely type H vessels, with high expression of CD31 and endomucin, was shown to couple angiogenesis and osteogenesis recently. The number of type H vessels in bone tissue declines with age, and the underlying mechanism for this reduction is unclear. Here, we report that microRNA-188-3p (miR-188-3p) involves this process. miRNA-188-3p expression is upregulated in skeletal endothelium and negatively regulates the formation of type H vessels during ageing. Mice with depletion of miR-188 showed an alleviated age-related decline in type H vessels. In contrast, endothelial-specific overexpression of miR-188-3p reduced the number of type H vessels, leading to decreased bone mass and delayed bone regeneration. Mechanistically, we found that miR-188 inhibits type H vessel formation by directly targeting integrin β3 in endothelial cells. Our findings indicate that miR-188-3p is a key regulator of type H vessel formation and may be a potential therapeutic target for preventing bone loss and accelerating bone regeneration.
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