Chun Li, Zelan Gu, Yijun Hou, Qi Gao, Guping Xu, Hua Lu
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引用次数: 0
摘要
H 抗原缺失通常是由 FUT1 基因突变引起的,这是一种非常罕见的血型。在本病例中,研究人员对一名 26 岁的患者(原告)及其三名家庭成员进行了 H 抗原表型、FUT1、FUT2 序列和家族遗传学调查。结果显示,该患者及其小弟弟均为 H 抗原缺乏表型,他们的 ABO 基因型均为 A/O1 型,父亲为 A/B 型,母亲为 O1/O1 型。她和弟弟的 FUT1 表型均为 h3|h3,FUT1 基因中的 658C > T 为同源突变,而他们父母的 FUT1 表型为 H|h3,FUT1 基因中的 658C > T 为杂合突变。全基因测序结果显示,该患者的父亲在 FUT1 基因中缺失了 CHR19.49,255,178-49,257,177(以 hg19 为参照)。家系调查结果显示,子代与父母之间的 FUT1 基因 658 位点突变符合孟德尔遗传规律。
A Pedigree Investigation of H-antigen Deletion Caused by Mutation of 658 C to T in the FUT1 Gene.
H-antigen deletion is often caused by FUT1 gene mutation, which is a very rare blood group. In this case, the H-antigen phenotype, FUT1, FUT2 sequences, and family genetic investigation of a 26-year-old patient (proband) and her three family members were studied. The results showed that the proband and little her brother were H-deficient phenotype, their ABO genotype of both was A/O1, her father was A/B, and her mother was O1/O1. The proband and her little brother's FUT1 phenotype were both h3|h3, with a homozygous mutation 658C > T in their FUT1 gene, and the FUT1 phenotype of their parents' were H|h3, with a heterozygous mutation (658C > T) in their FUT1 gene. The result of whole gene sequencing showed that the father of the proband had a deletion of CHR19.49,255,178-49,257,177 in the FUT1 gene (hg19 was used as the reference). The results of the family investigation showed that the mutation of site 658 in the FUT1 gene between offspring and parents was consistent with Mendelian inheritance law.
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