首次调查中非喀麦隆镰状细胞病患者及相关献血者的 RH 基因多态性。

IF 2.4 3区医学 Q2 HEMATOLOGY

Blood Transfusion Pub Date : 2024-09-01 Epub Date: 2024-01-29 DOI:10.2450/BloodTransfus.660

Jeanne Manga Messina Mbeti, Caroline Bénech, Françoise Ngo Sack, Estelle Wete, Hortense Ngegni Pangetha, Simon Noël Ateba, Jules Tchatchueng, Alexandre Njan Nloga, Yann Fichou

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引用次数: 0

摘要

背景：尽管撒哈拉以南非洲地区 RH 血型系统的遗传多态性已广为人知，但国家/地区的特异性仍有待精确描述。为了更好地描述 RH 表型变异的分子基础，并确定可能导致同种免疫的主要抗原，我们首次在非洲中部的喀麦隆进行了以下研究：1）研究 109 名镰状细胞病患者的 RH 基因；2）在向患者输注红细胞（RBC）的相应供血者（98 名患者中有 108 名供血者）中研究相同的基因；3）根据分子数据预测 RH 表型，并将结果与血清学检测结果进行比较；以及 4）回顾性地识别存在同种异体免疫风险的患者。材料和方法：为了生成一个详尽的数据集，对所有患者和供体样本的 RH 基因进行了系统研究：1）通过短荧光片段定量多重 PCR（QMPSF）分析 RHD 基因的同源性和潜在结构变异（SVs）；2）通过 Sanger 测序鉴定单核苷酸变异（SNVs）。分子分析之后，分别从参考数据库中推断和预测基因型和 RH 表型：结果：在总共 217 名喀麦隆人中，除了参考等位基因外，还在 RHD 和 RHCE 基因中分别发现了多达 24 个和 22 个变异等位基因。有趣的是，65 名 SCD 患者（66.3%）被认为暴露于一种或多种不良 RH 抗原，这些抗原具有不同程度的临床相关性：除了全面报告喀麦隆输血治疗患者RH变异等位基因的性质和分布情况外，这项工作还强调了对当前实践进行广泛审查的必要性，包括常规血清学分型程序，最好是在不久的将来。

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First investigation of RH gene polymorphism in patients with sickle cell disease and associated blood donors in Cameroon, Central Africa.

Background: Although genetic polymorphism of the RH blood group system is well known in sub-Saharan Africa, national/regional specificities still remain to be described precisely. For the first time in Cameroon, Central Africa, and in order to better characterize the molecular basis driving RH phenotype variability, as well as to identify the main antigens that may be potentially responsible for alloimmunization, we sought 1) to study the RH genes in a cohort of 109 patients with sickle cell disease; 2) to study the same genes in the corresponding donors whose red blood cells (RBCs) were transfused to the patients (108 donors in 98 patients); 3) to predict RH phenotype on the basis of the molecular data and compare the results with serologic testing; and 4) to identify retrospectively patients at risk for alloimmunization.

Materials and methods: In order to generate an exhaustive dataset, the RH genes of all patient and donor samples were systematically investigated 1) by quantitative multiplex PCR of short fluorescent fragments (QMPSF) for characterization of RHD gene zygosity and potential structural variants (SVs), and 2) by Sanger sequencing for identification of single nucleotide variants (SNVs). Subsequent to molecular analysis, the genotypes and RH phenotype were deduced and predicted, respectively, from reference databases.

Results: In a total of 217 Cameroonian individuals, as many as 24 and up to 22 variant alleles were identified in the RHD and RHCE genes, respectively, in addition to the reference alleles. Interestingly, 65 patients with SCD (66.3%) were assumed to be exposed to one or more undesirable RH antigen(s) with varying degrees of clinical relevance.

Discussion: Beyond the comprehensive report of the nature and distribution of RH variant alleles in a subset of Cameroonian patients treated by transfusion therapy, this work highlights the need for an extensive review of current practice, including routine serologic typing procedures, preferably in the near future.

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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.