Different profiles of alloantibody responses are observed in the clinic, with those that persist, often despite targeted treatment, associated with poorer long-term transplant outcomes. Although such responses would suggest an underlying germinal center (GC) response, the relationship to cellular events within the allospecific B cell population is unclear. Here we examine the contribution of germinal center (GC) humoral alloimmunity to chronic antibody mediated rejection (AMR). A murine model of chronic AMR was developed in which T cell deficient (Tcrbd−/−) C57BL/6 recipients were challenged with MHC-mismatched BALB/c heart allografts and T cell help provided by reconstituting with 103 “TCR75” CD4 T cells that recognize self-restricted allopeptide derived from the H-2Kd MHC class I alloantigen. Reconstituted recipients developed Ig-switched anti-Kd alloantibody responses that were slow to develop, but long-lived, with confocal immunofluorescence and flow cytometric characterization of responding H-2Kd-allospecific B cells confirming persistent splenic GC activity. This was associated with T follicular helper (TFH) cell differentiation of the transferred TCR75 CD4 T cells. Heart grafts developed progressive allograft vasculopathy, and were rejected chronically (MST 50 days), with explanted allografts displaying features of humoral vascular rejection. Critically, late alloantibody responses were abolished, and heart grafts survived indefinitely, in recipients reconstituted with Sh2d1a−/− TCR75 CD4 T cells that were genetically incapable of providing TFH cell function. The GC response was associated with affinity maturation of the anti-Kd alloantibody response, and its contribution to progression of allograft vasculopathy related principally to secretion of alloantibody, rather than to enhanced alloreactive T cell priming, because grafts survived long-term when B cells could present alloantigen, but not secrete alloantibody. Similarly, sera sampled at late time points from chronically-rejecting recipients induced more vigorous donor endothelial responses in vitro than sera sampled earlier after transplantation. In summary, our results suggest that chronic AMR and progression of allograft vasculopathy is dependent upon allospecific GC activity, with critical help provided by TFH cells. Clinical strategies that target the TFH cell subset may hold therapeutic potential.This work is composed of two parts, of which this is Part II. Please read also Part I: Alsughayyir et al., 2019.
展开▼
机译:在临床上观察到同种抗体反应的不同情况,尽管经过靶向治疗,但持续存在的情况与长期移植效果较差有关。尽管这种反应表明潜在的生发中心(GC)反应,但与同种异体B细胞群体内的细胞事件的关系尚不清楚。在这里,我们检查了生发中心(GC)体液同种免疫对慢性抗体介导排斥(AMR)的贡献。建立了一种慢性AMR小鼠模型,其中MHC不匹配的BALB / c心脏同种异体移植物挑战了T细胞缺陷(Tcrbd -/-)C57BL / 6受体,并通过重组10来提供T细胞帮助识别源自H-2K d MHC I类同种抗原的自我限制的异肽的 3 “ TCR75” CD4 T细胞。重组受体产生了Ig转换的抗K d 异源抗体反应,该反应缓慢发展,但寿命长,具有共聚焦免疫荧光和响应H-2K d 的流式细胞仪表征-allospecific B细胞证实持续的脾脏GC活性。这与转移的TCR75 CD4 T细胞的T卵泡辅助细胞(TFH)分化有关。心脏移植物发展为进行性同种异体血管病变,并被慢性排斥(MST 50天),同种异体移植后表现出体液性排斥。至关重要的是,在用基因无法提供TFH细胞功能的Sh2d1a -/- TCR75 CD4 T细胞重组的受体中,晚期异体抗体反应被取消,心脏移植物无限期存活。 GC反应与抗K d 同种抗体反应的亲和力成熟有关,其对同种异体血管病进展的贡献主要与同种抗体的分泌有关,而不是与增强的同种反应性T细胞启动有关,因为移植当B细胞可以表达同种抗原但不能分泌同种抗体时,它可以长期存活。类似地,在晚期时间点从长期拒绝接受者那里采集的血清比在移植后早期采集的血清在体外诱导出更强烈的供体内皮反应。总而言之,我们的结果表明,慢性AMR和同种异体血管病变的进展取决于同种异体GC活性,而TFH细胞提供了关键的帮助。针对TFH细胞亚群的临床策略可能具有治疗潜力。这项工作包括两个部分,其中第二部分。另请阅读第一部分:Alsughayyir等人,2019年。
展开▼
