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通过扩展覆盖的下一代测序技术对 HLA-A、-B、-C、-DRB1 和 -DQ 基因座匹配的同胞进行 DPA1 和 DPB1 错配的分析。

Assessment by Extended-Coverage Next-Generation Sequencing Typing of DPA1 and DPB1 Mismatches in Siblings Matching at HLA-A, -B, -C, -DRB1, and -DQ Loci.

机构信息

Service of Hematology, Transfusion and Cell Therapy, Faculty of Medicine, University of Sao Paulo, Sao Paulo, Brazil.

Department of Pathology, Stanford University, School of Medicine, Stanford, California; Histocompatibility, Immunogenetics & Disease Profiling Laboratory, Stanford Blood Center, Palo Alto, California.

出版信息

Biol Blood Marrow Transplant. 2019 Dec;25(12):2507-2509. doi: 10.1016/j.bbmt.2019.07.033. Epub 2019 Aug 2.

DOI:10.1016/j.bbmt.2019.07.033
PMID:31381995
Abstract

Allogeneic hematopoietic stem cell transplant from an HLA matched sibling donor is usually the preferable choice. The use of next-generation sequencing (NGS) for HLA typing in clinical practice provides broader coverage and higher resolution of HLA genes. We evaluated the frequency of DPB1 crossing-over events among patients and potential related donors typed with NGS. From July 2016 to January 2018, 593 patients and 2385 siblings were typed. We evaluated sibling matching status in 546 patients, and 44.8% of these patients had siblings that matched at HLA-A, -B, -C, -DRB1, and -DQB1 loci. In 306 patient-HLA matched sibling pairs, we found 6 pairs (1.96%) with 1 DPB1 mismatch, and 5 of these pairs included an additional mismatch in DPA1. No additional mismatches were observed at the low expression loci. Using the T cell epitope algorithm, 4 of these DP mismatches were classified as permissive, 1 as nonpermissive in the host-versus-graft direction, and 1 as nonpermissive in the graft-versus-host direction. The frequency of DPB1 and DPA1 mismatches is low, and their impact in related donor transplants is not well established. Although DP typing in related transplants goes beyond guidelines, it is especially relevant for sensitized patients. NGS-based HLA typing provides full gene coverage, and its use in clinical practice can enable better donor selection.

摘要

异基因造血干细胞移植来自 HLA 匹配的同胞供者通常是首选。下一代测序 (NGS) 在临床实践中用于 HLA 分型可提供更广泛的 HLA 基因覆盖和更高的分辨率。我们评估了使用 NGS 进行 HLA 分型的患者和潜在相关供者中 DPB1 交叉事件的频率。2016 年 7 月至 2018 年 1 月,对 593 名患者和 2385 名同胞进行了分型。我们评估了 546 名患者的同胞匹配状态,其中 44.8%的患者在 HLA-A、-B、-C、-DRB1 和 -DQB1 位点与同胞匹配。在 306 对患者-HLA 匹配的同胞中,我们发现 6 对(1.96%)存在 1 个 DPB1 错配,其中 5 对在 DPA1 中还存在额外错配。在低表达基因座未观察到其他错配。使用 T 细胞表位算法,其中 4 个 DP 错配被分类为允许,1 个在宿主-移植物方向上为不允许,1 个在移植物-宿主方向上为不允许。DPB1 和 DPA1 错配的频率较低,其在相关供者移植中的影响尚未确定。尽管相关移植中的 DP 分型超出了指南,但对于致敏患者尤其相关。基于 NGS 的 HLA 分型可提供全基因覆盖,其在临床实践中的应用可以实现更好的供者选择。

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