首页> 外文期刊>European Journal of Immunology >Transient decrease in interleukin-7 availability arrests B lymphopoiesis during pregnancy.
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Transient decrease in interleukin-7 availability arrests B lymphopoiesis during pregnancy.

机译:瞬态减少白介素- 7的可用性怀孕期间逮捕B淋巴细胞增殖。

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In mice, B lymphopoiesis is transiently arrested during pregnancy, and this is thought to be due to depletion of a hormone-sensitive bone marrow precursor. In this study, combining in vitro and in vivo approaches with detailed phenotypic and functional analysis of progenitor cells, we have investigated the effects of pregnancy on mouse B cell development. Recently, we characterized a BM progenitor called early progenitor with lymphoid and myeloid potential (EPLM) which, when cultured under B cell conditions, is the immediate precursor of pre-B1 cells. Results obtained show that during late pregnancy, B cell development was blocked at the EPLM-to-pre-B1 transition. This block was associated with a lack of IL-7 due to a down-regulation of IL-7 gene transcription. Moreover, we established that exogenously administered IL-7 could rescue B lymphopoiesis in pregnant mice. We conclude that during pregnancy, rather than directly depleting a hormone-sensitive B cell precursor, hormones dampen BM B cell development by fine-tuning IL-7 availability.
机译:在老鼠中,B淋巴细胞增殖是暂时性的逮捕在怀孕期间,这被认为是由于损耗的荷尔蒙骨髓前体。与详细的表型和体内的方法祖细胞的功能分析,我们调查怀孕小鼠B的影响细胞的发展。祖称为早期与淋巴祖和骨髓潜力(EPLM),当讲究的在B细胞的条件下,是最直接的pre-B1细胞的前体。在怀孕的后期,B细胞的发展被EPLM-to-pre-B1过渡。这一块与IL-7由于缺乏有关IL-7下调的基因转录。此外,我们建立了体内管理IL-7可以挽救B淋巴细胞增殖怀孕的老鼠。而不是直接消耗荷尔蒙B细胞前体,荷尔蒙抑制由微调IL-7 BM B细胞的发展可用性。

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