Immunoglobulin G subclass analysis of HLA donor specific antibodies in heart and renal transplant recipients.

Clinical transplants Pub Date : 2013-01-01
James C Cicciarelli, Noriyuki Kasahara, Nathan A Lemp, Robert Adamson, Walter Dembitsky, Barry Browne, Steven Steinberg
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Abstract

Immunoglobulin G (IgG) subclasses IgG1 (G1) and lgG3 (G3) can induce complement dependent cytotoxicity (CDC) and bind to Fc receptors (FcR), which induces phagocytosis and antibody dependent cellular cytotoxicity. In contrast, IgG2 has low CDC activity, lgG4 (G4) has no CDC activity, and neither binds high affinity FcR. Seven transplant recipients were analyzed for G1- G4 human leukocyte antigen (HLA) donor-specific antibodies (DSAs); six had active rejection and one had stable function. Patients with rejection had equal numbers of DSAs, which were G1 and G3, but no G4. The predominant DSAs were directed against HLA Class II proteins. Even with successful anti-rejection therapy, DSA persisted, albeit in several instances with lowered levels. Our findings are consistent with the presence of CDC-inducing G1 and G3 subclass DSAs during rejection. One heart transplant recipient followed for over 42 months had consistent, continuous G4 HLA DSA and stable function. We hypothesize that the presence of G4 DSA in the heart transplant recipient is akin to the allergen specific G4 that has been found in allergic desensitization tolerance, controlled by regulatory T-cells, and that manipulating G4 class switching through HLA antigen desensitzation could produce a tolerant state.

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心脏和肾脏移植受者HLA供者特异性抗体的免疫球蛋白G亚类分析。
免疫球蛋白G (IgG)亚类IgG1 (G1)和lgG3 (G3)可诱导补体依赖性细胞毒性(CDC),并与Fc受体(FcR)结合,诱导吞噬和抗体依赖性细胞毒性。相比之下,IgG2具有较低的CDC活性,lgG4 (G4)没有CDC活性,两者都不结合高亲和力的FcR。对7例移植受者进行G1- G4人白细胞抗原(HLA)供者特异性抗体(dsa)检测;6例有积极排斥反应,1例功能稳定。排斥反应患者的dsa数目相同,均为G1和G3,但没有G4。主要的dsa针对HLA II类蛋白。即使有成功的抗排斥治疗,DSA仍然存在,尽管在一些情况下水平降低。我们的发现与排斥反应中存在诱导cdc的G1和G3亚类dsa一致。一名心脏移植受者随访超过42个月,G4 HLA DSA一致,功能稳定。我们假设心脏移植受体中G4 DSA的存在类似于在过敏性脱敏耐受中发现的过敏原特异性G4,由调节性t细胞控制,并且通过HLA抗原脱敏操纵G4类转换可以产生耐受状态。
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HLA Matching The Lazarus phenomenon. HLA Epitopes and Shared Molecular Eplet Characterization and Their Implication on Transplant Outcome: The Experience of One Center. Acute Rejection, Kidney Allograft Function, and Graft Survival in Patients with Circulating Pre-Transplant IgG Antibodies Directed Against Donor HLA-A, -B, or -C Locus Determined Antigens. Pre-empting Antibody-Mediated Rejection: A Program of DSA Monitoring and Treatment Can Effectively Prevent Antibody Mediated Rejection.
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