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HLA-DPB1 单倍型对 10/10 匹配无关造血干细胞供者移植结局的影响取决于 MHC 连锁微卫星多态性。

Impact of HLA-DPB1 haplotypes on outcome of 10/10 matched unrelated hematopoietic stem cell donor transplants depends on MHC-linked microsatellite polymorphisms.

机构信息

National Reference Laboratory for Histocompatibility, Department of the Medical Specialties, University Hospital Geneva, Geneva, Switzerland.

出版信息

Biol Blood Marrow Transplant. 2012 Apr;18(4):608-16. doi: 10.1016/j.bbmt.2011.09.011. Epub 2011 Oct 1.

DOI:10.1016/j.bbmt.2011.09.011
PMID:21963878
Abstract

Hematopoietic stem cell transplantation (HSCT) with HLA-A, -B, -C, -DRB1, -DQB1 allele matched (10 of 10) unrelated donors is still associated with a significant rate of posttransplantation complications. In order to disclose additional immunogenetic factors, we analyzed the impact of HLA-DPB1 disparities and major histocompatibility complex (MHC)-resident microsatellite polymorphisms in 246 HLA 10 of 10 matched HSCT patients. First we showed that patients with more frequent/conserved HLA haplotypes had a higher 5-year survival (55% ± 18% versus 39% ± 18%, P = .021). In addition, DPB1 incompatibilities and 3 microsatellite alleles were associated with outcome. In a Cox regression model adjusting for European Blood and Marrow Transplant (EBMT) risk score, T cell depletion, and year of treatment, HSCT with a tumor necrosis factor d (TNFd) 4/d5-positive donor was associated with increased mortality (hazard ratio [HR] = 2.03; confidence interval [CI] 1.25-3.31; P = .004), whereas the D6S510-184 allele was protective (HR = 0.44; CI 0.22-0.87; P = .018). The 2 MHC-linked genetic donor factors, DPB1 mismatch (MM), and TNFd4/d5-positivity, acted in synergy with the EBMT risk score with an always lower survival (HR = 2.97; CI 1.27-6.92; P = .012). These data show that multiple MHC-linked genetic donor factors impact on outcome after unrelated donor HSCT. Their additive and potentially divergent effects could explain previous discrepant results, particularly with respect to the role of HLA-DPB1 disparities. We conclude that HLA-DPB1 typing combined with a simple TNFd microsatellite genotyping assay may significantly help in pretransplantation risk assessment for graft-versus-host disease and mortality, particularly for patients with several potential 10 of 10 matched donors.

摘要

造血干细胞移植(HSCT)与 HLA-A、-B、-C、-DRB1、-DQB1 等位基因匹配(10/10)的无关供者仍然与较高的移植后并发症发生率相关。为了揭示其他免疫遗传因素,我们分析了 246 例 HLA 10/10 匹配 HSCT 患者中 HLA-DPB1 差异和主要组织相容性复合体(MHC)驻留微卫星多态性的影响。首先,我们发现具有更频繁/保守 HLA 单体型的患者具有更高的 5 年生存率(55%±18%对 39%±18%,P=0.021)。此外,DPB1 不匹配和 3 个微卫星等位基因与结果相关。在调整欧洲血液和骨髓移植(EBMT)风险评分、T 细胞耗竭和治疗年份的 Cox 回归模型中,携带肿瘤坏死因子 d(TNFd)4/d5 阳性供者的 HSCT 与死亡率增加相关(危险比[HR]为 2.03;置信区间[CI]为 1.25-3.31;P=0.004),而 D6S510-184 等位基因具有保护作用(HR=0.44;CI 为 0.22-0.87;P=0.018)。这两个 MHC 连锁遗传供者因素,DPB1 不匹配(MM)和 TNFd4/d5 阳性,与 EBMT 风险评分协同作用,导致生存率始终较低(HR=2.97;CI 为 1.27-6.92;P=0.012)。这些数据表明,多个 MHC 连锁遗传供者因素影响无关供者 HSCT 后的结果。它们的累加和潜在的发散作用可以解释以前的不一致结果,特别是关于 HLA-DPB1 差异的作用。我们得出结论,HLA-DPB1 分型结合简单的 TNFd 微卫星基因分型检测可能显著有助于移植前移植物抗宿主病和死亡率的风险评估,特别是对于具有多个潜在 10/10 匹配供者的患者。

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