首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >Induction of Accommodation by Anti-complement Component 5 Antibody-based Immunosuppression in ABO-incompatible Heart Transplantation
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Induction of Accommodation by Anti-complement Component 5 Antibody-based Immunosuppression in ABO-incompatible Heart Transplantation

机译:通过抗补体组分5抗体的免疫抑制在ABO不相容的心脏移植中诱导

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Background. Plasmapheresis in combination with immunoglobulin and rituximab is often used to induce accommodation in ABO-incompatible (ABOi) living-donor transplantation; however, this regimen cannot be applied to cases of ABOi deceased-donor transplantation. Here, we investigated whether an anti-complement component 5 (C5) antibody-based regimen can induce accommodation in ABOi heart transplantation. Methods. Both IgM and IgG anti-blood type A antibodies were induced in wild-type mice by sensitization using human blood type A antigen. Heterotopic ABOi heart transplantation was performed from human blood type A-transgenic C57BL/6J mice to sensitized wild-type DBA/2 mice. Results. Either anti-C5 antibody or conventional triple immunosuppressants (corticosteroid, tacrolimus, mycophenolate mofetil) alone did not induce accommodation in majority of ABOi heart allografts, whereas their combination induced accommodation in more than 70% of cases despite the presence of anti-A antibodies. The combination therapy markedly suppressed the infiltration of T cells and macrophages into ABOi allografts, despite mild deposition of IgG and C4d. T-cell activation and differentiation into Th1, Th2, and Th17 cells were suppressed along with CD49d(high)CD4(+) T and follicular helper T cells in the combination treatment group. CD24(+) B cells, including both CD24(+)CD23(+) marginal zone B cells and CD24(+)CD23(-) T2-marginal zone B cells, were increased in the accommodation group. Conclusions. C5 inhibitor-based immunosuppression induced accommodation in murine ABOi heart transplantation, presenting a promising strategy for ABOi deceased-donor transplantation.
机译:背景。与免疫球蛋白和Rituximab组合的血浆膜通常用于诱导在Abo-Numpatible(Aboi)的养育助剂移植中的住宿;然而,这种方案不能适应于ABOI死者移植的病例。在这里,我们研究了是否可以在Aboi心脏移植中诱导基于抗补体组分5(C5)基于抗体的方案。方法。通过使用人体血液型抗原致敏,在野生型小鼠中诱导IgM和IgG抗血液抗体。从人血型A-转基因C57BL / 6J小鼠中进行异位ABOI心脏移植,以敏化野生型DBA / 2小鼠。结果。无论是抗C5抗体或已有的三重免疫抑制剂(皮质类固醇,他克莫司,霉酚酸酯)本身并不引起广大ABOi心脏移植的住宿,而他们的组合,尽管抗A抗体的存在而引起的病例中70%以上的住宿。尽管IgG和C4d轻度沉积,但组合疗法显着抑制了T细胞和巨噬细胞的渗透和巨噬细胞进入阿布西同种异体移植物。将T细胞活化和分化为TH1,TH2和TH17细胞以及组合处理组中的CD49D(高)CD4(+)T和滤泡辅助T细胞。 CD24(+)B细胞,包括CD24(+)CD23(+)边缘区B细胞和CD24(+)CD23( - )T2-边缘区B细胞,在容纳组中增加。结论。 C5基于抑制剂的免疫抑制诱导的鼠ABOI心脏移植的住宿,提出了ABOI死者移植的有希望的策略。

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