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首页> 外文期刊>Biology of blood and marrow transplantation: journal of the American Society for Blood and Marrow Transplantation >Extracorporeal photopheresis attenuates murine graft-versus-host disease via bone marrow-derived interleukin-10 and preserves responses to dendritic cell vaccination.
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Extracorporeal photopheresis attenuates murine graft-versus-host disease via bone marrow-derived interleukin-10 and preserves responses to dendritic cell vaccination.

机译:体外光透疗法可通过骨髓来源的白介素10减轻小鼠移植物抗宿主病,并保留对树突状细胞疫苗接种的反应。

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摘要

Extracorporeal photopheresis (ECP) is emerging as a therapy for graft-versus-host-disease (GVHD), but the full mechanism of action and the impact on immunity have not been fully established. After murine minor histocompatibility antigen-mismatched bone marrow (BM) transplantation (allo-BMT), coinfusion of ECP-treated splenocytes with T cell-replete BM attenuated GVHD irrespective of the donor strain of the ECP-treated splenocytes, and was associated with increased numbers of regulatory T cells. Coculture of myeloid dendritic cells (DCs) with ECP-treated splenocytes resulted in increased interleukin (IL)-10 production after submaximal stimulation with lipopolysaccharide. Furthermore, male myeloid DCs exposed to ECP-treated splenocytes were less potent at inducing CD8(+) HY responses when used as a vaccine in vivo. The efficacy of ECP-treated splenocytes was enhanced when administered just before delayed donor lymphocyte infusion following T cell-depleted allo-BMT, allowing for the administration of sufficient numbers of T cells to respond to myeloid DC vaccination in the absence of a thymus. Finally, the therapeutic effect of ECP-treated splenocytes was lost in recipients of IL-10-deficient BM. We demonstrate that ECP-treated splenocytes attenuate GVHD irrespective of the source of ECP-treated cells via a mechanism that likely involves modulation of DCs and requires IL-10 produced by BM-derived cells. Importantly, the attenuation of GVHD by ECP-treated splenocytes permits donor lymphocyte infusion-dependent responses to DC vaccines after allo-BMT.
机译:体外光穿刺术(ECP)逐渐成为一种抗移植物抗宿主疾病(GVHD)的疗法,但尚未完全建立起完整的作用机制及其对免疫力的影响。小鼠轻微组织相容性抗原失配的骨髓(BM)移植(allo-BMT)后,ECP处理的脾细胞与T细胞充足的BM共融合可减弱GVHD,而与ECP处理的脾细胞的供体无关。调节性T细胞的数量。用脂多糖亚最大刺激后,髓样树突状细胞(DCs)与ECP处理的脾细胞共培养导致白介素(IL)-10产生增加。此外,当用作体内疫苗时,暴露于ECP处理的脾细胞的雄性髓样DC在诱导CD8(+)HY反应中的效力较低。当在T细胞耗尽的all-BMT后延迟供体淋巴细胞输注之前施用时,经ECP处理的脾细胞的功效得到增强,从而允许在没有胸腺的情况下施用足够数量的T细胞对髓样DC疫苗反应。最后,在IL-10缺陷的BM的接受者中,ECP处理的脾细胞的治疗作用丧失了。我们证明,ECP处理的脾细胞通过可能涉及DC调节并需要BM衍生细胞产生的IL-10的机制,不论ECP处理的细胞的来源如何,均会减弱GVHD。重要的是,异体-BMT后,ECP处理的脾细胞对GVHD的减弱允许供体淋巴细胞对DC疫苗的输注依赖于依赖的反应。

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