COG6-CDG:一名中国患者的两个新变异和较轻的表型

IF 3.3 2区 医学 Q2 GENETICS & HEREDITY
Xue-Yuan Zhang, Jing Zhang, Yi Lu
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引用次数: 0

摘要

在此,我们介绍了一名高度怀疑患有先天性糖基化障碍 IIL 型(CDG2L;OMIM#614576)的中国汉族女婴。她的临床症状包括转氨酶异常、肝硬化、血象、凝血功能障碍、生长迟缓、智力障碍、频繁感染和牙釉质发育不全。三基因组测序在 COG6 中发现了一个父系变异体 c.1672C>T(p.Gln558Ter)和一个母系变异体 c.153+392A>G(p.?)利用从外周血中分离出的 mRNA 进行的反转录聚合酶链反应(RT-PCR)证实了这两个变异体的致病性。父系变异体导致无义介导的 mRNA 衰减。母本变异体产生了两个异常的 COG6 转录本,有 154 bp 重叠,预计会在同一位置发生框移位,导致产生过早终止密码子。它们可能导致 COG6 合成为截短形式。因此,对该患者进行了基因诊断。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
COG6-CDG: Two Novel Variants and Milder Phenotype in a Chinese Patient

Here, we present a Han Chinese pediatric girl highly suspected of congenial disorder of glycosylation type IIL (CDG2L; OMIM#614576). Her clinical symptoms include transferase abnormal, liver cirrhosis, hemogram, coagulopathy, growth retardation, intellectual disability, frequent infections, and enamel hypoplasia. Trio-genome sequencing identified in COG6 a paternal variant c.1672C>T (p.Gln558Ter) and a maternal variant c.153+392A>G (p.?). Reverse transcription-polymerase chain reaction (RT-PCR) using mRNA isolated from peripheral blood confirmed the pathogenicity of both variants. The paternal variant resulted in nonsense-mediated mRNA decay. The maternal variant generated two aberrant COG6 transcripts with 154 bp overlap and was predicted to result in a frameshift at the same position, leading to generation of a premature termination codon. They might result in synthesis of a truncated form of COG6. Thus, the patient was genetically diagnosed.

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来源期刊
Human Mutation
Human Mutation 医学-遗传学
CiteScore
8.40
自引率
5.10%
发文量
190
审稿时长
2 months
期刊介绍: Human Mutation is a peer-reviewed journal that offers publication of original Research Articles, Methods, Mutation Updates, Reviews, Database Articles, Rapid Communications, and Letters on broad aspects of mutation research in humans. Reports of novel DNA variations and their phenotypic consequences, reports of SNPs demonstrated as valuable for genomic analysis, descriptions of new molecular detection methods, and novel approaches to clinical diagnosis are welcomed. Novel reports of gene organization at the genomic level, reported in the context of mutation investigation, may be considered. The journal provides a unique forum for the exchange of ideas, methods, and applications of interest to molecular, human, and medical geneticists in academic, industrial, and clinical research settings worldwide.
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