Loss of endothelial membrane KIT ligand affects systemic KIT ligand levels but not bone marrow hematopoietic stem cells

干细胞因子 骨髓 造血 配体(生物化学) 生物 造血干细胞 内皮干细胞 干细胞 细胞生物学 原癌基因蛋白质c-kit 免疫学 生物化学 受体 体外
作者
Sahoko Matsuoka,R Facchini,Tiago C. Luís,Joana Carrelha,Petter Woll,Takuo Mizukami,Bishan Wu,Hanane Boukarabila,Mario Buono,Ruggiero Norfo,Fumio Arai,Toshio Suda,Adam J. Mead,Claus Nerlov,Sten Eirik W. Jacobsen
出处
期刊:Blood [American Society of Hematology]
卷期号:142 (19): 1622-1632 被引量:4
标识
DOI:10.1182/blood.2022019018
摘要

Abstract A critical regulatory role of hematopoietic stem cell (HSC) vascular niches in the bone marrow has been implicated to occur through endothelial niche cell expression of KIT ligand. However, endothelial-derived KIT ligand is expressed in both a soluble and membrane-bound form and not unique to bone marrow niches, and it is also systemically distributed through the circulatory system. Here, we confirm that upon deletion of both the soluble and membrane-bound forms of endothelial-derived KIT ligand, HSCs are reduced in mouse bone marrow. However, the deletion of endothelial-derived KIT ligand was also accompanied by reduced soluble KIT ligand levels in the blood, precluding any conclusion as to whether the reduction in HSC numbers reflects reduced endothelial expression of KIT ligand within HSC niches, elsewhere in the bone marrow, and/or systemic soluble KIT ligand produced by endothelial cells outside of the bone marrow. Notably, endothelial deletion, specifically of the membrane-bound form of KIT ligand, also reduced systemic levels of soluble KIT ligand, although with no effect on stem cell numbers, implicating an HSC regulatory role primarily of soluble rather than membrane KIT ligand expression in endothelial cells. In support of a role of systemic rather than local niche expression of soluble KIT ligand, HSCs were unaffected in KIT ligand deleted bones implanted into mice with normal systemic levels of soluble KIT ligand. Our findings highlight the need for more specific tools to unravel niche-specific roles of regulatory cues expressed in hematopoietic niche cells in the bone marrow.
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