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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >The trophic action of IL-7 on pro-T cells: inhibition of apoptosis of pro-T1, -T2, and -T3 cells correlates with Bcl-2 and Bax levels and is independent of Fas and p53 pathways.
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The trophic action of IL-7 on pro-T cells: inhibition of apoptosis of pro-T1, -T2, and -T3 cells correlates with Bcl-2 and Bax levels and is independent of Fas and p53 pathways.

机译:IL-7对pro-T细胞的营养作用:pro-T1,-T2和-T3细胞凋亡的抑制与Bcl-2和Bax水平相关,并且独立于Fas和p53途径。

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Signals from the IL-7R are essential for normal thymocyte development. We isolated thymocytes from early developmental stages and observed that suspensions of pro-T1, -T2, and -T3 cells rapidly died in culture. Addition of IL-7 promoted their survival, but did not induce cell division. Pro-T4 cells did not undergo rapid cell death, and their survival was therefore independent of IL-7. Death in the absence of IL-7 showed the hallmarks of apoptosis, including DNA fragmentation and annexin V binding; however, caspase inhibitors blocked DNA fragmentation, but did not block cell death. The trophic effect of IL-7 was partially inhibited by blocking protein synthesis. The p53 pathway was not involved in this death pathway, since pro-T cells from p53-/- mice also underwent cell death in the absence of IL-7. The Fas/Fas ligand pathway was not involved in cell death, since Fas-deficient pro-T cells died normally in the absence of IL-7, anti-Fas Abs did not protect cells from death in the absence of IL-7, and Fas expression was undetectable on cells at these stages. The IL-7 trophic affect correlated with increased intracellular levels of Bcl-2 and decreased levels of Bax, whereas no Bcl-X(L), Bcl-w, or Bad was detectable. Thus, maintaining a favorable Bcl-2/Bax ratio may account for the trophic action of IL-7.
机译:IL-7R发出的信号对于正常的胸腺细胞发育至关重要。我们从早期发育阶段分离了胸腺细胞,并观察到pro-T1,-T2和-T3细胞的悬浮液在培养中迅速死亡。 IL-7的添加促进了它们的存活,但没有诱导细胞分裂。 Pro-T4细胞没有经历快速的细胞死亡,因此它们的存活独立于IL-7。没有IL-7的死亡显示出凋亡的标志,包括DNA片段化和膜联蛋白V结合。但是,半胱天冬酶抑制剂可以阻止DNA片段化,但不能阻止细胞死亡。 IL-7的营养作用被阻断蛋白合成部分抑制。 p53途径不参与该死亡途径,因为在没有IL-7的情况下,来自p53-/-小鼠的pro-T细胞也经历了细胞死亡。 Fas / Fas配体途径不参与细胞死亡,因为缺乏Fas的pro-T细胞在没有IL-7的情况下可以正常死亡,因此,在没有IL-7的情况下,抗Fas Abs不能保护细胞免于死亡。在这些阶段,无法在细胞上检测到Fas表达。 IL-7的营养影响与细胞内Bcl-2水平升高和Bax水平降低相关,而Bcl-X(L),Bcl-w或Bad均未检出。因此,维持有利的Bcl-2 / Bax比值可以解释IL-7的营养作用。

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