变体解释不一致的原因和解决办法

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2023-05-22 DOI:10.1155/2023/4955235
Liling Lin, H. Pan, Y. Qi, Yinan Ma, L. Qiu
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引用次数: 0

摘要

在后基因组时代,变异解释对于单基因疾病的诊断至关重要,是精准医学的前提。遗传病诊断的瓶颈和困难已经从检测技术的难以获得转向测序结果的解释。多项研究表明,实验室间变异解释的不一致性约为10~40%。然而,目前许多临床医生对这方面的重视程度还不够。在这篇综述中,我们总结了不一致的原因,包括分类方法、翻译人员获得的信息、证据应用和专家判断。对于临床医生、遗传咨询师和分子病理学家来说,在临床实践中有必要重新评估遗传报告,特别是那些有旧文献和数据库支持的报告。对于无法解决的病例,需要进行谱系分析,与研究实验室合作进行功能实验,并进行长期随访,将先进的临床表现与最新的数据和文献结合起来。
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Reasons and Resolutions for Inconsistent Variant Interpretation
In the postgenomic era, variant interpretation is crucial for diagnosing monogenic diseases, which is the premise of precision medicine. The bottleneck and difficulty of genetic disease diagnosis have switched from the inaccessibility of detection technology to the interpretation of sequencing results. Multiple studies have suggested that the inconsistency rate of interlaboratory variant interpretation is approximately 10~40%. However, many clinicians have not paid enough attention to this area at present. In this review, we summarized the reasons for inconsistency, including classification methodology, information obtained by the interpreter, evidence application, and expert judgement. For clinicians, genetic counsellors, and molecular pathologists, it is necessary to reevaluate genetic reports, especially those supported by old literature and databases in clinical practice. For unresolvable cases, pedigree analysis, collaboration with research labs for functional experiments, and long-term follow-up to combine advanced clinical presentations with updated data and literature are needed.
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来源期刊
CiteScore
7.20
自引率
4.30%
发文量
567
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