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Long-term tolerance of islet allografts in nonhuman primates induced by apoptotic donor leukocytes

机译:凋亡供体白细胞诱导的非人灵长类动物的胰岛同种异体移植的长期耐受性

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摘要

Immune tolerance to allografts has been pursued for decades as an important goal in transplantation. Administration of apoptotic donor splenocytes effectively induces antigen-specific tolerance to allografts in murine studies. Here we show that two peritransplant infusions of apoptotic donor leukocytes under short-term immunotherapy with antagonistic anti-CD40 antibody 2C10R4, rapamycin, soluble tumor necrosis factor receptor and anti-interleukin 6 receptor antibody induce long-term (≥1 year) tolerance to islet allografts in 5 of 5 nonsensitized, MHC class I-disparate, and one MHC class II DRB allele-matched rhesus macaques. Tolerance in our preclinical model is associated with a regulatory network, involving antigen-specific Tr1 cells exhibiting a distinct transcriptome and indirect specificity for matched MHC class II and mismatched class I peptides. Apoptotic donor leukocyte infusions warrant continued investigation as a cellular, nonchimeric and translatable method for inducing antigen-specific tolerance in transplantation.
机译:对同种异体移植物的免疫耐受已经作为移植的重要目标追求了数十年。在鼠类研究中,给予凋亡的供体脾细胞可有效诱导对同种异体移植的抗原特异性耐受。在这里,我们显示了在短期免疫疗法下,以拮抗性抗CD40抗体2C10R4,雷帕霉素,可溶性肿瘤坏死因子受体和抗白介素6受体抗体进行的两次移植治疗中注入的凋亡供体白细胞诱导了对胰岛的长期耐受(≥1年)在5个非敏化,I类MHC不同和1个MHC II类DRB等位基因匹配的恒河猴中进行了5个同种异体移植。在我们的临床前模型中,耐受性与调控网络有关,涉及抗原特异性的Tr1细胞,它们对匹配的II类MHC和错配的I类肽表现出独特的转录组和间接特异性。凋亡供体白细胞输注作为用于诱导移植中抗原特异性耐受的细胞,非嵌合和可翻译方法值得继续研究。

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