HLA class I expression on human platelets is highly variable and correlates with distinct allele group frequencies.

IF 2.4 3区医学 Q2 HEMATOLOGY

Blood Transfusion Pub Date : 2024-09-01 Epub Date: 2024-01-11 DOI:10.2450/BloodTransfus.571

Rocco Cantisani, Valeria Del Re, Francesca Toraldo, Silvia Cantara, Simone Pozzessere, Giuseppe Marotta, Adriano Spreafico

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Abstract

Background: Human leukocyte antigen (HLA) class I molecules are expressed on platelets and can represent a source of alloimmunization in recipients of platelet transfusions. HLA mismatch between donors and recipients may be associated with the induction of anti-HLA antibodies, which can culminate in refractoriness to platelet transfusions. In the present study we analyzed HLA allele group frequencies and HLA expression levels on human platelets from blood donors.

Materials and methods: Platelet-rich plasma was collected from 139 donors to monitor platelet HLA class I expression by flow cytometry. DNA from donors with high and low platelet HLA expression was used in the genotype studies. Frequencies of large and normal-sized platelet subpopulations were determined and HLA class I expression was studied. Mean platelet volume (MPV) and platelet large-cell ratio (P-LCR) were analyzed in both groups of donors.

Results: The analysis showed variable platelet HLA class I expression with significant differences among donors. HLA class I allele group frequencies in donors with high and low platelet HLA expression showed distinctive genotypic features strictly related to expression level. The main allele groups found in samples with high platelet HLA class I expression were HLA-A*02, -A*68, -B*15, -B*49, and -C*03. Platelet HLA class I expression did not change over time or during freezing-thawing cycles. The analysis of platelet subpopulations showed a statistically significant higher expression of HLA class I molecules on large platelets than on normal-sized platelets. Moreover, donors with high HLA class I expression showed a higher frequency of large platelets (p<0.0001). The analysis of P-LCR in both groups of donors showed a statistically significant difference (p<0.05) within high HLA-expressing donors.

Discussion: Our data suggest an allele-dependent expression of HLA class I molecules on human platelets with distinct HLA allele group frequencies and different platelet subpopulation frequencies among blood donors.

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人体血小板上的 HLA I 类表达变化很大，并与不同的等位基因群频率相关。

背景：人类白细胞抗原（HLA）Ⅰ类分子在血小板上表达，可成为血小板输注受体的异体免疫源。献血者和受血者之间的 HLA 不匹配可能与诱导抗 HLA 抗体有关，最终导致对血小板输注的耐受性。在本研究中，我们分析了献血者血小板上的 HLA 等位基因组频率和 HLA 表达水平：从 139 名献血者身上采集富含血小板的血浆，通过流式细胞术监测血小板 HLA I 类表达。血小板 HLA 高表达和低表达献血者的 DNA 被用于基因型研究。确定了大血小板亚群和正常大小血小板亚群的频率，并对 HLA I 类表达进行了研究。分析了两组供体的平均血小板体积（MPV）和血小板大细胞比率（P-LCR）：结果：分析表明，血小板 HLA I 类表达各不相同，不同供体之间存在显著差异。血小板 HLA 高表达和低表达供体的 HLA I 类等位基因组频率显示出与表达水平密切相关的独特基因型特征。在血小板 HLA I 类高表达样本中发现的主要等位基因组为 HLA-A*02、-A*68、-B*15、-B*49 和 -C*03。血小板 HLA I 类表达不随时间或冻融循环而变化。对血小板亚群的分析表明，大血小板的 HLA I 类分子表达明显高于正常大小的血小板。此外，HLA I 类高水平表达的供体中出现大血小板的频率更高（讨论：我们的数据表明，HLA I 类分子在人体血小板上的表达依赖于等位基因，献血者的 HLA 等位基因组频率不同，血小板亚群频率也不同。

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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来源期刊

Blood Transfusion HEMATOLOGY-

CiteScore

6.10

自引率

2.70%

发文量

审稿时长

2 months

期刊介绍： Blood Transfusion welcomes international submissions of Original Articles, Review Articles, Case Reports and Letters on all the fields related to Transfusion Medicine.