1例RHD基因254C>A突变的鉴定及254位点的相关突变分析*

doi:10.3969/j.issn.1671-2587.2026.01.020

临床输血与检验 ›› 2026, Vol. 28 ›› Issue (1): 131-135.DOI: 10.3969/j.issn.1671-2587.2026.01.020

1例RHD基因254C>A突变的鉴定及254位点的相关突变分析^*

朱于莉, 胡彬, 冯智慧, 韩斌, 纪凯伦

青岛市中心血站输血研究所，山东青岛 266071

收稿日期:2025-07-11 发布日期:2026-02-13
作者简介:朱于莉，主要从事免疫血液学及免疫遗传学方面研究，（E-mail）zhuyuli6000@sina.com。
基金资助:
*本课题受2024年度青岛市中心血站站内科研计划项目（No.2024-xz01）资助

Identification of RHD Gene 254C>A Mutation and Analysis of the Related Mutations at Position 254

ZHU Yuli, HU Bin, FENG Zhihui, HAN Bin, JI Kailun

QingDao Blood Center, Qingdao 266071

Received:2025-07-11 Published:2026-02-13

摘要/Abstract

摘要： 目的对1例弱D表型样本进行血清学鉴定和分子机制研究，对发现的突变及该位点其他突变进行综合预测分析。方法采用血清学方法鉴定Rh表型;采用PCR-SSP方法对RHD合子型进行分析，PCR直接测序方法对RHD外显子序列进行分析;采用SOPMA对各种突变前后蛋白二级结构进行分析;采用AlphaFold构建蛋白质的3D模拟结构;采用Mupro进行蛋白稳定性分析;采用PROVEAN和PolyPhen-2分析对蛋白功能的影响。结果不同克隆的抗-D与样本红细胞呈弱反应性，RhCE表型为ccEe;RHD基因测序发现在第2外显子存在c.254C>A (p.Ala85Gly) 新突变;检索发现在254位点还存在其他常见2种碱基T、G突变，通过分析预测提示254位点不同突变所形成的蛋白二级结构未发生明显改变，但c.254C>G和c.254C>A突变影响了蛋白的稳定性且导致功能受损。结论此例标本为1例罕见的c.254C>A导致的弱D表型，虽然254位点位于跨膜区，但是其突变位点是RHD基因的关键位点，存在常见4种碱基形式，该碱基的突变会导致蛋白质稳定性降低，功能受损。

关键词: RHD基因, 弱D, 蛋白结构, 254C＜A位点突变

Abstract: Objective The serological identification of a sample with weak D phenotype were carried out, and the mutation sites were identified. Further the impact of all mutations at this site on protein structure and function as well as molecular mechanism were studied. Methods The Rh phenotype was identified by serological methods. The RHD zygosity analysis was analyzed by PCR-SSP, and the RHD exon sequence was analyzed by direct PCR sequencing. SOPMA was used for prediction of RhD structure. Constructing 3D simulated structures of proteins using AlphaFold. The protein stability was analyzed by Mupro. PROVEAN and PolyPhen-2 analysis were used to investigate the impact on protein function. Results The antibodies from different clones exhibit weak reactivity with sample red blood cells, and the Rh phenotype is ccEe; RHD gene sequencing revealed a novel mutation c.254C>A (p.Ala85Gly) in exon 2; Retrieval revealed the presence of two other base T and G mutations at position 254. Analysis and prediction suggested that the protein secondary structure did not undergo significant changes with different mutations at position 254. However, c.254C>G and c.254C>A mutations affect the stability of the protein and lead to functional impairment. Conclusion This specimen is a rare case of weak D phenotype caused by c.254C>A. Although the 254 site is located in the transmembrane region, it is a key site of the RHD gene and has four common base forms. Mutations can lead to decreased protein stability and impaired function.

Key words: RHD gene, Weak D phenotype, Protein structure, 254C＜A mutation

中图分类号:

R457.1

朱于莉, 胡彬, 冯智慧, 韩斌, 纪凯伦. 1例RHD基因254C>A突变的鉴定及254位点的相关突变分析^*[J]. 临床输血与检验, 2026, 28(1): 131-135.

ZHU Yuli, HU Bin, FENG Zhihui, HAN Bin, JI Kailun. Identification of RHD Gene 254C>A Mutation and Analysis of the Related Mutations at Position 254[J]. JOURNAL OF CLINICAL TRANSFUSION AND LABORATORY MEDICINE, 2026, 28(1): 131-135.

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1例RHD基因254C>A突变的鉴定及254位点的相关突变分析^*

Identification of RHD Gene 254C>A Mutation and Analysis of the Related Mutations at Position 254

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