HLA typing—A case-based approach to donor selection

Neema P. Mayor, Bronwen E. Shaw
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Abstract

In the early years of hematopoietic cell transplantation (HCT), matching of patients and donors was poorly understood and complications related to genetic (especially HLA) mismatching were profound, resulting in a very high incidence of fatal graft-versus-host disease (GVHD). This essentially limited the choice of a donor to a sibling, and as the understanding of HLA improved, defined the donor as an HLA-identical sibling. As patient outcomes improved, the use of an unrelated donor (URD) became more common. Later, with the advent of URD registries and improved HLA typing techniques, the use of an URD overtook that of an HLA-identical sibling in frequency both in Europe and in the United States (US). Increasing confidence in our ability to manage and prevent the immune complications of HCT led to the use of HLA-mismatched donors being expanded, in the setting of umbilical cord blood (UCB) and haploidentical transplantation. In 2018, it is unusual for a patient not to go to transplant due to the lack of a suitable donor option. In this manuscript, we describe the impact of genetic factors, in particular HLA, and the technologies for typing these, on the outcomes of HCT. We highlight both well-accepted donor selection practices and newer or more controversial advances in donor selection.

HLA分型-基于病例的供体选择方法
在造血细胞移植(HCT)的早期,人们对患者和供体的匹配知之甚少,与遗传(尤其是HLA)错配相关的并发症也很严重,导致致命性移植物抗宿主病(GVHD)的发生率非常高。这从本质上限制了对供体的选择,而随着对HLA的理解的提高,供体被定义为与HLA相同的兄弟姐妹。随着患者预后的改善,使用非亲属供体(URD)变得越来越普遍。后来,随着URD登记的出现和HLA分型技术的改进,在欧洲和美国,URD的使用频率超过了HLA相同的兄弟姐妹。对我们管理和预防HCT免疫并发症能力的信心日益增强,导致在脐带血(UCB)和单倍体移植的情况下,hla错配供体的使用得到扩大。在2018年,由于缺乏合适的供体选择,患者不去移植是很不寻常的。在这篇文章中,我们描述了遗传因素,特别是HLA,以及分型技术对HCT结果的影响。我们强调了被广泛接受的供体选择实践和更新或更具争议的供体选择进展。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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