HLA配型、输血与肾移植

Clinics in Immunology and Allergy Pub Date : 1984-10-01 DOI:10.1016/S0260-4639(22)00198-0

G.G. PERSIJN, G.F.J. HENDRIKS, J.J. VAN ROOD

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引用次数: 10

摘要

欧洲移植数据库的分析表明，HLA-A和-B抗原的匹配不仅对尸体肾移植的存活率有有益影响，而且对患者的存活率也有有益影响。这种有益的效果可以在五年的随访时间后得到最清楚的证明，在各种HLA-a和-B错配类别中有足够数量的供体-受体组合。HLA-DR决定簇的匹配也显著提高了肾移植的存活率。当供体和受体的HLA-DR决定簇以及HLA-A和-B抗原匹配时，可以获得最佳的肾移植存活率。关于移植前输血，从荷兰的前瞻性研究中可以明确地看出，一次白细胞缺乏的输血是一种良好的移植前输血方案。此外，缺乏白细胞的输血，即无白细胞的血液，并不能提高肾移植的存活率。HLA匹配和移植前输血这两个重要因素之间的相互作用表明，HLA-A和-B匹配以及HLA-DR匹配在未输血的受体中最为明显，尽管应该强调的是，当供体和受体的HLA匹配良好并且受体已经输注时，可以获得最佳的肾移植存活率。为了在移植前识别高应答或低应答的患者，可以表明HLA-DRw6抗原的分型在这方面是有帮助的。HLA-DRw6阳性患者是高应答者，应移植HLA-DRw六阳性肾脏。此外，可以证明HLA-DRw6阳性供体肾的移植物存活率高于平均水平，与匹配无关。即使面对一个或两个HLA-DR不匹配，这些供体也能获得良好的肾移植存活率（见表8）。总之，HLA-A、-B和-DR匹配在肾移植存活中的作用过去是，现在仍然是一个非常重要的因素。然而，它们肯定不是唯一起作用的因素。其他方面，如临床管理、免疫抑制治疗、热缺血时间、T细胞亚群比率监测等，也应在进一步分析中予以考虑（van Es等人，1983）。预测移植肾的存活率仍然非常困难，因为它依赖于多种相互作用的因素。

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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HLA Matching, Blood Transfusion and Renal Transplantation

Analysis from the Eurotransplant data base reveals that matching for HLA-A and -B antigens has a beneficial effect not only on cadaveric kidney graft survival but also on patient survival. This beneficial effect can be demonstrated most clearly after five years follow-up time with a sufficient number of donor-recipient combinations in the various HLA-A and -B mismatch categories.

Matching for the HLA-DR determinants also improves kidney graft survival significantly. The best kidney graft survival is obtained when donor and recipient are matched for the HLA-DR determinants as well as for the HLA-A and -B antigens.

Concerning pretransplant blood transfusions, it is unequivocally clear from the prospective study in The Netherlands that one leucocyte-poor blood transfusion is a good pretransplant blood transfusion protocol. Furthermore, transfusions which are depleted of leucocytes, i.e. leucocyte-free blood, do not improve kidney graft survival.

The interaction between the two important factors, HLA-matching and pretransplant blood transfusion, shows that HLA-A and -B matching as well as HLA-DR matching is most apparent in non-transfused recipients, although it should be stressed that the best kidney graft survival is obtained when donor and recipient are well matched for HLA and the recipient has been transfused.

In an attempt to identify patients before transplantation in high or low responders, it can be shown that typing for HLA-DRw6 antigen can be helpful in this respect. HLA-DRw6 positive patients are high responders and should be transplanted with HLA-DRw6 positive kidneys. Furthermore, it can be demonstrated that HLA-DRw6 positive donor kidneys have a better than average graft survival, independent of the match. Good kidney graft survival was obtained with such donors even in the face of one or two HLA-DR mismatches (see Table 8).

In conclusion, the role of HLA-A, -B and -DR matching was, and still is, a very important factor in kidney graft survival. However, they are certainly not the only factors at play. Others, such as clinical management, immunosuppressive treatment, warm ischaemia time, monitoring of T-cell subset ratios, etc., should be considered as well in further analyses (van Es et al, 1983). Predicting renal allograft survival remains extremely difficult, as it is dependent on a multitude of interacting factors.

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Clinics in Immunology and Allergy

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