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[中国人群中罕见顺式AB变异体的分子遗传学分析。]

[Molecular genetic analysis of rare cisAB variants in Chinese population.].

作者信息

Xu Xian-Guo, Liu Ying, Hong Xiao-Zhen, Ma Kai-Rong, Zhu Fa-Ming, Lv Hang-Jun, Yan Li-Xing

机构信息

Key Laboratory of Blood Safety Research, Ministry of Health, Institute of Transfusion Medicine, Blood Center of Zhejiang Province, Hangzhou 310006, China E-mail:

出版信息

Yi Chuan. 2008 Oct;30(10):1295-300. doi: 10.3724/sp.j.1005.2008.01295.

Abstract

We investigated the molecular genetic basis of rare cisAB variants at the ABO locus in Chinese population. Serological techniques were performed to characterize erythrocyte phenotype of 12 discrepant samples and 116 randomly selected samples. Mutations of complete exon 6 and 7 including flanking intron in the ABO genes were screened by PCR and directly sequencing. The haplotypes of diverse genotypes were also analyzed by cloning sequencing. Twelve samples were identified as AweakB or ABweak phenotype by serological technology, and were also identified as cisAB variants including four genotypes by directly sequencing. Two cisAB alleles were found by haplotype sequencing. One allele was cisAB01, in which four nucleotide acid alterations were observed (467C>T and 803G>C in exon 7, 163T>C and 179C>T in intron 6); the other allele maintained a nucleotide acid of A101 allele (803G) compared with B101 allele, which resulted in a polypep-tide containing 176G, 235S, 266M, and 268G four amino acids. This is a novel allele, which has been named cisAB05 by Blood Group Antigen Gene Mutation Database. According to systematically investigation of the molecular genetic basis of the cisAB variants in Chinese population, we found a novel cisAB05 allele and presumed that the cisAB01 allele is derived from homologues exchange of A101-B101 combination.

摘要

我们研究了中国人群中ABO血型位点罕见顺式AB变异体的分子遗传基础。采用血清学技术对12例血型不符样本和116例随机选取样本的红细胞表型进行鉴定。通过聚合酶链反应(PCR)和直接测序筛选ABO基因第6和第7外显子及其侧翼内含子的突变。通过克隆测序分析不同基因型的单倍型。血清学技术鉴定出12例样本为弱A弱B或弱AB表型,直接测序鉴定其为顺式AB变异体,包括4种基因型。单倍型测序发现2个顺式AB等位基因。一个等位基因为顺式AB01,外显子7有4个核苷酸改变(467C>T和803G>C),内含子6有2个核苷酸改变(163T>C和179C>T);另一个等位基因与B101等位基因相比保留了A101等位基因的一个核苷酸(803G),导致多肽含有176G、235S、266M和268G这4个氨基酸。这是一个新的等位基因,已被血型抗原基因突变数据库命名为顺式AB05。通过对中国人群顺式AB变异体分子遗传基础的系统研究,我们发现了一个新的顺式AB05等位基因,并推测顺式AB01等位基因来源于A101-B101组合的同源交换。

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