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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Constitutively active Stat5b in CD4+ T cells inhibits graft-versus-host disease lethality associated with increased regulatory T-cell potency and decreased T effector cell responses.
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Constitutively active Stat5b in CD4+ T cells inhibits graft-versus-host disease lethality associated with increased regulatory T-cell potency and decreased T effector cell responses.

机译:CD4 + T细胞中的组成型活性STAT5B抑制与增加的调节性T细胞效力和降低T效应细胞反应相关的移植物与宿主疾病致死。

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摘要

Overexpression of a constitutively active form of Stat5b (Stat5b-CA) increases regulatory T cells (Tregs). We show that Stat5b-CA transgenic (TG) CD4(+) T cells had a markedly reduced graft-versus-host disease (GVHD) capacity versus wild-type (WT) T cells. Stat5b-CA TG versus WT CD4(+) T cells had a higher proportion of Tregs, which were superior in suppressing alloresponses mediated by CD4(+)CD25(-) effector T cells (Teffs). By day 5 after transplantation, Stat5b-CA TG Tregs had expanded approximately 3-fold more than WT Tregs. Purified Stat5b-CA TG Tregs added to WT CD4(+)CD25(-) Teffs were superior on a per-cell basis for inhibiting GVHD versus WT Tregs. Surprisingly, rigorously Treg-depleted Stat5b-CA TG versus WT CD4(+)CD25(-) Teffs caused less GVHD lethality associated with diminished Teff proinflammatory and increased Th2 anti-inflammatory cytokine responses. Reduced GVHD by Stat5b-CA TG versus WT Teffs could not be explained by conversion into Tregs in day 10 posttransplantation spleen or small intestine. In addition, Stat5b-CA TG Teffs retained a graft-versus-leukemia response. These results indicate a major role for Stat5 in Treg expansion and potency along with a lesser but significant role in Teff activation and suggest a strategy of pharmacologic Stat5b up-regulation as a means of decreasing GVHD while retaining a graft-versus-leukemia effect.
机译:组成型活性形式的STAT5B(Stat5B-CA)的过表达增加了调节性T细胞(Tregs)。我们表明Stat5B-Ca转基因(Tg)CD4(+)T细胞具有显着降低的移植物与宿主疾病(GVHD)能力与野生型(WT)T细胞。 STAT5B-CA TG与WT CD4(+)T细胞具有较高比例的Tregs,其在抑制由CD4(+)CD25( - )效应器T细胞(Teffs)介导的反应中的抑制反应。在移植后第5天,Stat5B-CA TG Tregs的扩展比WT Tregs大约3倍。加入到WT CD4(+)CD25( - )Teff的纯化的Stat5b-Ca Tg Trefms在抑制GVHD与WT Tregs的每个细胞基础上优异。令人惊讶的是,严格的Treg耗尽的Stat5B-Ca Tg与WT CD4(+)CD25( - )Teff引起的GVHD致死性较少,与Teff促炎和增加的抗炎细胞因子反应增加。通过STAT5B-CA TG减少GVHD与WT Teffs不能通过转化为第10天后持续的脾脏或小肠的Tregs来解释。此外,Stat5B-CA TG Teffs保留了移植物与白血病的反应。这些结果表明TREG扩张和效力中的STAT5的主要作用以及TEFF激活中的表现较小,并表明药理学Stat5B上调的策略作为降低GVHD的方法,同时保留接枝 - 与白血病效应。

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