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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >PTH expands short-term murine hemopoietic stem cells through T cells
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PTH expands short-term murine hemopoietic stem cells through T cells

机译:PTH通过T细胞扩增短期鼠造血干细胞

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摘要

Intermittent parathyroid hormone (iPTH) treatment expands hemopoietic stem and progenitor cells (HSPCs), but the involved mechanisms and the affected HSPC populations are mostly unknown. Here we show that T cells are required for iPTH to expand short-term HSPCs (STHSPCs) and improve blood cell engraftment and host survival after BM transplantation. Silencing of PTH/PTH-related protein receptor (PPR) in T cells abrogates the effects of iPTH, thus demonstrating a requirement for direct PPR signaling in T cells. Mechanistically, iPTH expands ST-HSPCs by activating Wnt signaling in HSPCs and stromal cells (SCs) through T-cell production of the Wnt ligand Wnt10b. Attesting to the relevance of Wnt10b, iPTH fails to expand STHSPCs in mice with Wnt10b-/- T cells. Moreover, iPTH fails to promote engraftment and survival after BM transplantation in Wnt10b null mice. In summary, direct PPR signaling in T cells and the resulting production of Wnt10b play a pivotal role in the mechanism by which iPTH expands ST-HSPCs. The data suggest that T cells may provide pharmacologic targets for HSPC expansion.
机译:间歇性甲状旁腺激素(iPTH)治疗可扩大造血干细胞和祖细胞(HSPCs),但其中涉及的机制和受影响的HSPC人群大多未知。在这里,我们显示iPTH需要T细胞来扩展短期HSPCs(STHSPCs)并改善BM移植后的血细胞植入和宿主存活。 T细胞中PTH / PTH相关蛋白受体(PPR)的沉默消除了iPTH的作用,因此证明了对T细胞中直接PPR信号传导的需求。从机制上讲,iPTH通过Wnt配体Wnt10b的T细胞产生激活HSPC和基质细胞(SCs)中的Wnt信号,从而扩展ST-HSPC。证明了Wnt10b的相关性,iPTH无法在具有Wnt10b-/-T细胞的小鼠中扩展STHSPCs。此外,iPTH不能促进Wnt10b缺失小鼠BM移植后的移入和存活。总之,T细胞中的直接PPR信号传导和Wnt10b的产生在iPTH扩展ST-HSPC的机制中起着关键作用。数据表明,T细胞可能为HSPC扩展提供药理学靶标。

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