Serological screening and genetic analysis of RhCE variants in the Chinese Southern Han donors

• Published in: Transfusion medicine (Oxford, England) Vol. 31; no. 4; pp. 271 - 276
• Main Authors: Jia, Shuangshuang, Chen, Jingwang, Wen, Jizhi, Wang, Zhen, Wei, Ling, Fu, Yongshui, Luo, Guangping, Ji, Yanli
• Format: Journal Article
• Language: English
• Published: Oxford, UK Blackwell Publishing Ltd 01.08.2021
• Subjects: Alleles; Blood Donors; China; Genotype; Humans; Rh-Hr Blood-Group System - genetics; RhCE variants; RHCECe375G; RHCECe667T; China; RHCECe667T; RhCE variants; RHCECe375G
• ISSN: 0958-7578; 1365-3148; 1365-3148
• DOI: 10.1111/tme.12788

Objectives To screen RhCE variants in the Chinese Southern Han donors for molecular genetic analysis. Background More than hundreds of RhCE variant alleles have been described to resulting in weak and/or partial expression of RhCE antigens, generation of low‐prevalence antigens and/or absence of a high‐prevalence antigen of Rh system, which mainly reported in the people of African origin. In this study, the serological screening and molecular genetic analysis of RhCE variants were performed in the Chinese Southern Han donors. Methods The blood samples of E(+) donors were preliminarily collected. Then, RhCE antigens of the E(+) samples were further typed by using two sets of monoclonal anti‐C, anti‐c, anti‐e and another anti‐E. When weak expression of RhCE antigens was found, direct sequencing for 10 exons of RHCE gene, RH genotyping analysis by using multiplex ligation–dependent probe amplification, flow cytometric analysis and even cDNA sequencing were performed. Results A total of 4487 E(+) samples were collected and four samples with weak expression of antigens were detected. RHCE*Ce375G and RHCE*Ce667T variant alleles were identified in two samples with weak expression of e antigen, respectively. But no variant alleles were found in another two samples with weak expression of C antigen. Conclusion The variant RHCE*Ce375G validated by mRNA sequencing and the deduced RHCE*Ce667T alleles were firstly identified in the Chinese population. The DCE haplotype might account for the weak expression of C antigen in two donors.