Münz Márton, Ruark Elise, Renwick Anthony, Ramsay Emma, Clarke Matthew, Mahamdallie Shazia, Cloke Victoria, Seal Sheila, Strydom Ann, Lunter Gerton, Rahman Nazneen
Wellcome Trust Centre for Human Genetics, Roosevelt Drive, Oxford, OX3 7BN, UK.
Division of Genetics & Epidemiology, The Institute of Cancer Research, 15 Cotswold Road, London, SM2 5NG, UK.
Genome Med. 2015 Jul 28;7(1):76. doi: 10.1186/s13073-015-0195-6.
Next-generation sequencing (NGS) offers unprecedented opportunities to expand clinical genomics. It also presents challenges with respect to integration with data from other sequencing methods and historical data. Provision of consistent, clinically applicable variant annotation of NGS data has proved difficult, particularly of indels, an important variant class in clinical genomics. Annotation in relation to a reference genome sequence, the DNA strand of coding transcripts and potential alternative variant representations has not been well addressed. Here we present tools that address these challenges to provide rapid, standardized, clinically appropriate annotation of NGS data in line with existing clinical standards.
We developed a clinical sequencing nomenclature (CSN), a fixed variant annotation consistent with the principles of the Human Genome Variation Society (HGVS) guidelines, optimized for automated variant annotation of NGS data. To deliver high-throughput CSN annotation we created CAVA (Clinical Annotation of VAriants), a fast, lightweight tool designed for easy incorporation into NGS pipelines. CAVA allows transcript specification, appropriately accommodates the strand of a gene transcript and flags variants with alternative annotations to facilitate clinical interpretation and comparison with other datasets. We evaluated CAVA in exome data and a clinical BRCA1/BRCA2 gene testing pipeline.
CAVA generated CSN calls for 10,313,034 variants in the ExAC database in 13.44 hours, and annotated the ICR1000 exome series in 6.5 hours. Evaluation of 731 different indels from a single individual revealed 92 % had alternative representations in left aligned and right aligned data. Annotation of left aligned data, as performed by many annotation tools, would thus give clinically discrepant annotation for the 339 (46 %) indels in genes transcribed from the forward DNA strand. By contrast, CAVA provides the correct clinical annotation for all indels. CAVA also flagged the 370 indels with alternative representations of a different functional class, which may profoundly influence clinical interpretation. CAVA annotation of 50 BRCA1/BRCA2 gene mutations from a clinical pipeline gave 100 % concordance with Sanger data; only 8/25 BRCA2 mutations were correctly clinically annotated by other tools.
CAVA is a freely available tool that provides rapid, robust, high-throughput clinical annotation of NGS data, using a standardized clinical sequencing nomenclature.
新一代测序(NGS)为扩展临床基因组学提供了前所未有的机遇。它在与其他测序方法的数据及历史数据整合方面也带来了挑战。事实证明,要提供一致的、临床适用的NGS数据变异注释很困难,尤其是对于插入缺失(indels)而言,插入缺失是临床基因组学中的一类重要变异。与参考基因组序列、编码转录本的DNA链以及潜在的替代变异表示相关的注释尚未得到很好的解决。在此,我们展示了一些工具,这些工具应对了这些挑战,以根据现有临床标准对NGS数据进行快速、标准化且临床适用的注释。
我们开发了一种临床测序命名法(CSN),这是一种与人类基因组变异协会(HGVS)指南原则一致的固定变异注释,针对NGS数据的自动变异注释进行了优化。为了实现高通量的CSN注释,我们创建了CAVA(变异的临床注释),这是一个快速、轻量级的工具,设计用于轻松整合到NGS流程中。CAVA允许指定转录本,适当地考虑基因转录本的链,并标记具有替代注释的变异,以促进临床解释以及与其他数据集的比较。我们在全外显子组数据和一个临床BRCA1/BRCA2基因检测流程中对CAVA进行了评估。
CAVA在13.44小时内为ExAC数据库中的10313034个变异生成了CSN调用,并在6.5小时内注释了ICR1000全外显子组系列。对来自一个个体的731个不同插入缺失的评估显示,92%在左对齐和右对齐数据中有替代表示。因此,许多注释工具所执行的左对齐数据注释,对于从正向DNA链转录的基因中的339个(46%)插入缺失会给出临床上不一致的注释。相比之下,CAVA为所有插入缺失提供了正确的临床注释。CAVA还标记了370个具有不同功能类替代表示的插入缺失,这可能会深刻影响临床解释。对临床流程中的50个BRCA1/BRCA2基因突变进行的CAVA注释与桑格测序数据的一致性为100%;其他工具仅对25个BRCA2突变中的8个进行了正确的临床注释。
CAVA是一个免费可用的工具,它使用标准化的临床测序命名法为NGS数据提供快速、可靠、高通量的临床注释。
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