Robert Chen, Maria Alejandra Diaz-Miranda, Erfan Aref-Eshghi, Tiffiney R Hartman, Christopher Griffith, Jennifer L Morrison, Patricia G Wheeler, Erin Torti, Gabriele Richard, Margaret Kenna, Elizabeth T Dechene, Nancy B Spinner, Renkui Bai, Laura K Conlin, Ian D Krantz, Sami S Amr, Minjie Luo
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引用次数: 1
摘要
同义变异体已被证明可以改变前mrna的正确剪接并产生致病转录本。这些变异并不是遗传病的罕见病因;然而,在缺乏功能和临床数据的基因检测中,它们经常被忽视。在这里,我们描述了同义变体[NM_005422.4 (TECTA)]的发生:c。[27] c >T, p.(Gly109=)]来自6个无亲缘关系家庭的7例听力损失患者。该变异不位于外显子/内含子边界附近,但预计通过激活TECTA外显子4上的隐剪接供体位点来影响剪接。体外迷你基因分析表明,该变异破坏了规范转录物的阅读框,预计会导致变异下游48个氨基酸的过早终止密码子,导致无义介导的衰变。这种变异存在于人口数据库中,主要存在于非洲血统的拉丁美洲人中,但在其他种族群体中很少见。我们的研究结果表明,这种同义变异体可能是与tecta相关的常染色体隐性听力损失的致病性,并且似乎是在这个特定的拉丁裔亚人群中出现的创始变异体。本研究表明,同义变异体需要仔细的剪接评估和其他测试方法的支持,以确定其临床影响。
Characterization of a possible founder synonymous variant in TECTA in multiple individuals with autosomal recessive hearing loss.
Synonymous variants have been shown to alter the correct splicing of pre-mRNAs and generate disease-causing transcripts. These variants are not an uncommon etiology of genetic disease; however, they are frequently overlooked during genetic testing in the absence of functional and clinical data. Here, we describe the occurrence of a synonymous variant [NM_005422.4 (TECTA):c.327C>T, p.(Gly109=)] in seven individuals with hearing loss from six unrelated families. The variant is not located near exonic/intronic boundaries but is predicted to impact splicing by activating a cryptic splicing donor site in exon 4 of TECTA. In vitro minigene assays show that the variant disrupts the reading frame of the canonical transcript, which is predicted to cause a premature termination codon 48 amino acids downstream of the variant, leading to nonsense-mediated decay. The variant is present in population databases, predominantly in Latinos of African ancestry, but is rare in other ethnic groups. Our findings suggest that this synonymous variant is likely pathogenic for TECTA-associated autosomal recessive hearing loss and seems to have arisen as a founder variant in this specific Latino subpopulation. This study demonstrates that synonymous variants need careful splicing assessment and support from additional testing methodologies to determine their clinical impact.
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.