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人类白细胞抗原分子错配可对肾移植受者进行风险分层。

Human leukocyte antigen molecular mismatch to risk stratify kidney transplant recipients.

机构信息

Department of Medicine, University of Manitoba.

Shared Health Services Manitoba.

出版信息

Curr Opin Organ Transplant. 2020 Feb;25(1):8-14. doi: 10.1097/MOT.0000000000000714.

Abstract

PURPOSE OF REVIEW

Stalled drug development and the lack of improvement in long-term graft survival reflect the unmet need for prognostic and predictive biomarkers in transplantation. Although conventional human leukocyte antigen (HLA) mismatch is too imprecise to fulfill this need, HLA molecular mismatch increases the precision in alloimmune risk assessment by quantifying the difference between donors and recipients at the molecular level.

RECENT FINDINGS

Within each conventional HLA mismatch, recipients exhibit a wide range of HLA molecular mismatches with their donors. Quantifying HLA molecular mismatch improves the precision of alloimmune risk assessment for de novo donor-specific antibody development (dnDSA). Alloimmune risk categories developed analyzing dnDSA development were also found to correlate with T-cell-mediated rejection, antibody-mediated rejection, and all cause graft loss in adjusted and unadjusted models.

SUMMARY

All alloimmunity is driven by differences between donors and recipients at the molecular level. HLA molecular mismatch may represent a fast, reproducible, cost-effective, way to improve alloimmune risk assessment at the time of transplantation to move the field towards precision medicine.

摘要

目的综述

药物研发停滞不前,移植物长期存活率未见改善,这反映出在移植领域中,人们对预后和预测生物标志物的需求尚未得到满足。尽管传统的人类白细胞抗原(HLA)错配不够精确,无法满足这一需求,但 HLA 分子错配通过定量比较供者和受者之间的分子差异,提高了同种异体免疫风险评估的精确性。

最新发现

在每个传统的 HLA 错配中,受者与供者之间存在广泛的 HLA 分子错配。量化 HLA 分子错配可提高新产生的供者特异性抗体(dnDSA)发展的同种异体免疫风险评估的精确性。在调整和未调整模型中,分析 dnDSA 发展而制定的同种异体免疫风险类别也与 T 细胞介导的排斥、抗体介导的排斥和所有原因的移植物丢失相关。

总结

所有同种异体免疫都是由供者和受者之间的分子差异驱动的。HLA 分子错配可能代表一种快速、可重复、具有成本效益的方法,可在移植时改善同种异体免疫风险评估,使该领域朝着精准医学的方向发展。

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