MSH2
林奇综合征
错义突变
MLH1
DNA错配修复
生物
遗传学
微卫星不稳定性
突变
结直肠癌
基因
癌症
等位基因
微卫星
作者
Elizabeth Chao,Jonathan L. Velasquez,Mavee Witherspoon,Laura S. Rozek,David Peel,Pauline C. Ng,Stephen B. Gruber,Patrice Watson,Gad Rennert,Hoda Anton‐Culver,Henry T. Lynch,Steven M. Lipkin
出处
期刊:Human Mutation
[Wiley]
日期:2008-06-01
卷期号:29 (6): 852-860
被引量:104
摘要
Lynch syndrome, also known as hereditary nonpolyposis colon cancer (HNPCC), is the most common known genetic syndrome for colorectal cancer (CRC). MLH1/MSH2 mutations underlie approximately 90% of Lynch syndrome families. A total of 24% of these mutations are missense. Interpreting missense variation is extremely challenging. We have therefore developed multivariate analysis of protein polymorphisms-mismatch repair (MAPP-MMR), a bioinformatic algorithm that effectively classifies MLH1/MSH2 deleterious and neutral missense variants. We compiled a large database (n>300) of MLH1/MSH2 missense variants with associated clinical and molecular characteristics. We divided this database into nonoverlapping training and validation sets and tested MAPP-MMR. MAPP-MMR significantly outperformed other missense variant classification algorithms (sensitivity, 94%; specificity, 96%; positive predictive value [PPV] 98%; negative predictive value [NPV], 89%), such as SIFT and PolyPhen. MAPP-MMR is an effective bioinformatic tool for missense variant interpretation that accurately distinguishes MLH1/MSH2 deleterious variants from neutral variants.
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