A mechanosensitive peri-arteriolar niche for osteogenesis and lymphopoiesis

干细胞 细胞生物学 祖细胞 造血 压电1 骨髓 淋巴细胞生成 生物 机械敏感通道 间质细胞 间充质干细胞 免疫学 癌症研究 受体 离子通道 生物化学
作者
Bo Shen,Alpaslan Tasdogan,Jessalyn M. Ubellacker,Jingzhu Zhang,E. D. Nosyreva,Liming Du,Malea M. Murphy,Shuiqing Hu,Yating Yi,Nergis Kara,Xin Liu,Shay Guela,Yuemeng Jia,Vijayashree Ramesh,Claire Embree,Evann C. Mitchell,Yunduo Charles Zhao,Lining Arnold Ju,Hu Zhao,Genevieve M. Crane,Zhiyu Zhao,Ruhma Syeda,Sean J. Morrison
出处
期刊:Nature [Springer Nature]
卷期号:591 (7850): 438-444 被引量:195
标识
DOI:10.1038/s41586-021-03298-5
摘要

Stromal cells in adult bone marrow that express leptin receptor (LEPR) are a critical source of growth factors, including stem cell factor (SCF), for the maintenance of haematopoietic stem cells and early restricted progenitors1–6. LEPR+ cells are heterogeneous, including skeletal stem cells and osteogenic and adipogenic progenitors7–12, although few markers have been available to distinguish these subsets or to compare their functions. Here we show that expression of an osteogenic growth factor, osteolectin13,14, distinguishes peri-arteriolar LEPR+ cells poised to undergo osteogenesis from peri-sinusoidal LEPR+ cells poised to undergo adipogenesis (but retaining osteogenic potential). Peri-arteriolar LEPR+osteolectin+ cells are rapidly dividing, short-lived osteogenic progenitors that increase in number after fracture and are depleted during ageing. Deletion of Scf from adult osteolectin+ cells did not affect the maintenance of haematopoietic stem cells or most restricted progenitors but depleted common lymphoid progenitors, impairing lymphopoiesis, bacterial clearance, and survival after acute bacterial infection. Peri-arteriolar osteolectin+ cell maintenance required mechanical stimulation. Voluntary running increased, whereas hindlimb unloading decreased, the frequencies of peri-arteriolar osteolectin+ cells and common lymphoid progenitors. Deletion of the mechanosensitive ion channel PIEZO1 from osteolectin+ cells depleted osteolectin+ cells and common lymphoid progenitors. These results show that a peri-arteriolar niche for osteogenesis and lymphopoiesis in bone marrow is maintained by mechanical stimulation and depleted during ageing. A peri-arteriolar niche in the bone marrow for osteogenesis and lymphopoiesis is maintained by mechanical stimulation and is depleted during ageing.
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