首页> 外文期刊>The journal of clinical investigation >Murine erythroid short-term radioprotection requires a BMP4-dependent, self-renewing population of stress erythroid progenitors
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Murine erythroid short-term radioprotection requires a BMP4-dependent, self-renewing population of stress erythroid progenitors

机译:小鼠红系短期放射防护需要依赖BMP4的,自我更新的应激红系祖细胞群

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Acute anemic stress induces a systemic response designed to increase oxygen delivery to hypoxic tissues. Increased erythropoiesis is a key component of this response. Recovery from acute anemia relies on stress erythropoiesis, which is distinct from steady-state erythropoiesis. In this study we found that the bone morphogenetic protein 4–dependent (BMP4-dependent) stress erythropoiesis pathway was required and specific for erythroid short-term radioprotection following bone marrow transplantation. BMP4 signaling promoted the development of three populations of stress erythroid progenitors, which expanded in the spleen subsequent to bone marrow transplantation in mice. These progenitors did not correspond to previously identified bone marrow steady-state progenitors. The most immature population of stress progenitors was capable of self renewal while maintaining erythropoiesis without contribution to other lineages when serially transplanted into irradiated secondary and tertiary recipients. These data suggest that during the immediate post-transplant period, the microenvironment of the spleen is altered, which allows donor bone marrow cells to adopt a stress erythropoietic fate and promotes the rapid expansion and differentiation of stress erythroid progenitors. Our results also suggest that stress erythropoiesis may be manipulated through targeting the BMP4 signaling pathway to improve survival after injury.
机译:急性贫血引起全身性反应,旨在增加向缺氧组织的氧气输送。促红细胞生成增加是该反应的关键组成部分。急性贫血的恢复依赖于应激性红细胞生成,这与稳态红细胞生成不同。在这项研究中,我们发现,骨髓移植后需要骨形态发生蛋白4依赖性(BMP4依赖性)应激红细胞生成途径,并且该途径对红系短期放射防护具有特异性。 BMP4信号传导促进了三类应激性红系祖细胞的发育,它们在小鼠骨髓移植后在脾脏中扩展。这些祖细胞与先前确定的骨髓稳态祖细胞不对应。当连续移植到受辐照的第二和第三接受者中时,最不成熟的应激祖细胞能够自我更新,同时保持红细胞生成,而对其他谱系无贡献。这些数据表明,在移植后即刻,脾脏的微环境发生了变化,这使得供体骨髓细胞能够适应应激性红细胞生成的命运,并促进应激性红细胞祖细胞的快速扩增和分化。我们的结果还表明,可通过靶向BMP4信号通路来控制应激性红细胞生成,以提高损伤后的生存率。

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