Department of Human Genetics, Leiden University Medical Center, Leiden, the Netherlands.
Princess Maxima Center for Child Oncology, Utrecht, the Netherlands.
Hum Mutat. 2022 Sep;43(9):1249-1258. doi: 10.1002/humu.24387. Epub 2022 Apr 28.
The large majority of germline alterations identified in the DNA mismatch repair (MMR) gene PMS2, a low-penetrance gene for the cancer predisposition Lynch syndrome, represent variants of uncertain significance (VUS). The inability to classify most VUS interferes with personalized healthcare. The complete in vitro MMR activity (CIMRA) assay, that only requires sequence information on the VUS, provides a functional analysis-based quantitative tool to improve the classification of VUS in MMR proteins. To derive a formula that translates CIMRA assay results into the odds of pathogenicity (OddsPath) for VUS in PMS2 we used a set of clinically classified PMS2 variants supplemented by inactivating variants that were generated by an in cellulo genetic screen, as proxies for cancer-predisposing variants. Validation of this OddsPath revealed high predictive values for benign and predisposing PMS2 VUS. We conclude that the OddsPath provides an integral metric that, following the other, higher penetrance, MMR proteins MSH2, MSH6 and MLH1 can be incorporated as strong evidence type into the upcoming criteria for MMR gene VUS classification of the American College of Medical Genetics and Genomics and the Association for Molecular Pathology (ACMG/AMP).
大多数在 DNA 错配修复 (MMR) 基因 PMS2 中发现的种系改变,PMS2 是癌症易感性林奇综合征的低外显率基因,代表意义不明的变异 (VUS)。大多数 VUS 无法分类会干扰个性化医疗保健。完全体外 MMR 活性 (CIMRA) 测定法仅需要 VUS 的序列信息,提供了一种基于功能分析的定量工具,可改善 MMR 蛋白中 VUS 的分类。为了从 CIMRA 测定结果得出 PMS2 中 VUS 致病性的可能性 (OddsPath),我们使用了一组临床分类的 PMS2 变体,这些变体由细胞内遗传筛选产生的失活变体补充,作为致癌易感性变体的代表。对这种 OddsPath 的验证显示了良性和易感性 PMS2 VUS 的高预测值。我们得出的结论是,OddsPath 提供了一个整体指标,在其他更高外显率的 MMR 蛋白 MSH2、MSH6 和 MLH1 之后,可以作为强有力的证据类型纳入即将出台的美国医学遗传学与基因组学学院和分子病理学协会 (ACMG/AMP) 的 MMR 基因 VUS 分类标准。
