间充质干细胞
表型
成骨细胞
脂肪生成
骨髓
调节器
细胞生物学
内科学
谱系(遗传)
内分泌学
转基因
转基因小鼠
利基
脂肪因子
化学
负调节器
骨重建
干细胞
生物
基础(医学)
信号转导
祖细胞
祖细胞
癌症研究
造血
细胞分化
骨形成
下调和上调
分泌物
脂肪组织
体外
作者
Yaming Guo,Zeqing Zhang,Junyu He,Peiqiong Luo,Zhihan Wang,Yurong Zhu,Xiaoyu Meng,Limeng Pan,Ranran Kan,Yuxi Xiang,Beibei Mao,Yi He,Siyi Wang,Yan Yang,Fengjing Guo,Hongbo You,Feng Li,Danpei Li,Yong Chen,Xuefeng Yu
出处
期刊:JCI insight
[American Society for Clinical Investigation]
日期:2025-10-21
卷期号:10 (23)
标识
DOI:10.1172/jci.insight.189371
摘要
A distinguishing feature of older mesenchymal stem cells (MSCs) from bone marrow (BM) is the transition in their differentiation capabilities from osteoblasts to adipocytes. However, the mechanisms underlying these cellular events during the aging process remain unclear. We identified angiopoietin-like protein 8 (ANGPTL8), an adipokine implicated in lipid metabolism, that influenced the fate of MSCs in BM during skeletal aging. Our studies revealed that ANGPTL8 steered MSCs toward adipogenic differentiation, overshadowing osteoblastogenesis. Mice with overexpressed ANGPTL8 exhibited reduced bone mass and increased BM adiposity, while those with transgenic depletion of ANGPTL8 showed lowered bone loss and less accumulation of BM fat. ANGPTL8 influenced the BM niche of MSCs by inhibiting the Wnt/β-catenin signaling pathway. Partial inhibition of PPARγ rescued some aspects of the phenotype in MSCs with ANGPTL8 overexpression. Furthermore, treatment with an Angptl8 antisense oligonucleotide improved the phenotype of aging mice. Our research suggests that ANGPTL8 is a crucial regulator of senesence-related changes in the BM niche and the cell-fate switch of MSCs.
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