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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Predominace of NK1.1~+TCR#alpha##beta#~+ or DX5~+TCR#alpha##beta#~+ T cells in mice conditioned with fractionated lymphoid irradiation protects against graft-versus-host disease:'Natural suppressor'cells
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Predominace of NK1.1~+TCR#alpha##beta#~+ or DX5~+TCR#alpha##beta#~+ T cells in mice conditioned with fractionated lymphoid irradiation protects against graft-versus-host disease:'Natural suppressor'cells

机译:在分次淋巴样照射条件下的小鼠中,主要的NK1.1〜+ TCR#alpha ## beta#〜+或DX5〜+ TCR#alpha ## beta#〜+ T细胞可预防移植物抗宿主病:“天然抑制剂“细胞

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摘要

We developed a nonmyeloablative host conditioning regimen in a mouse model of MHC-mismatched bone marrow transplantationthat not only reduces radiation toxicity,but also protects against graft-vs-host disease. The regimen of fractionated irradiation directed to the lymphoid tissues and depietive anti-T cell Abs results in a marked change in the residual host T cells, such that NK1.1~+ or DX5~+ asialo-GM1~+ T cells become the predominant T cell subset in the lymphoid tissues of C57BL/6 and BALB/c mice,respectively.The latter “natural suppressor” T cells protect hosts from graft-vs-host disease after the infusion of allogeneic bone marrow and peripheral blood cells that ordinarily kill hosts conditioned with sublethal or lethal total body irradiation. Protected hosts become stable mixed chimeras, but fail to show the early expansion and infiltration of donor T cells in the gut, liver, and blood associated with host tissue injury. Cytokine secretion and adoptive transfer studies using wild-type and IL-4~(-1-) mice showed that protection afforded by NK1.1~+ and DX5~+ asialo-GM1~+ T cells derived from either donors or hosts conditioned with lymphoid irradiation is dependent on their secretion of high levels of IL-4.
机译:我们在MHC不匹配的骨髓移植小鼠模型中开发了一种非清髓性宿主调节方案,该方案不仅可以降低放射毒性,而且还可以预防移植物抗宿主病。针对淋巴组织和侵袭性抗T细胞Abs的分级照射方案导致残留的宿主T细胞发生显着变化,从而使NK1.1〜+或DX5〜+无唾液酸GM1〜+ T细胞成为主要的分别在C57BL / 6和BALB / c小鼠的淋巴组织中的T细胞亚群。在注入同种异体骨髓和通常会杀死小鼠的外周血细胞后,后者的“天然抑制” T细胞使宿主免受移植物抗宿主病的侵害接受亚致死或致死性全身照射的宿主。受保护的宿主变成稳定的混合嵌合体,但无法显示出与宿主组织损伤相关的肠道,肝脏和血液中供体T细胞的早期扩增和浸润。使用野生型和IL-4〜(-1-)小鼠进行的细胞因子分泌和过继转移研究表明,NK1.1〜+和DX5〜+去唾液酸GM1〜+ T细胞可从受到供体或宿主条件调节的宿主中获得保护淋巴样照射取决于它们分泌高水平的IL-4。

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