Classifying<i>MLH1</i>and<i>MSH2</i>variants using bioinformatic prediction, splicing assays, segregation, and tumor characteristics

Arnold, Sven; Buchanan, Daniel D.; Barker, Melissa; Jaskowski, L.; Walsh, Michael D.; Birney, Genevieve; Woods, Michael O.; Hopper, John L.; Jenkins, Mark A.; Brown, Melissa A.; Tavtigian, Sean V.; Goldgar, David E.; Young, Joanne; Spurdle, Amanda B.

doi:10.1002/humu.20936

Cited by 61 publications

(70 citation statements)

References 49 publications

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“…Instead, for MMR genes, there are not well-established models or well-characterized features 42 so that, at the time of writing, a very few groups have attempted to classify MMR UVs with the Bayesian likelihood method. The study by Arnold et al 24 investigated several variants, three of which are in common with our data (MLH1 c.307-29CϾA, c.1039-8 TϾA and MSH2 p.Gly322Asp): only c.307-29CϾA was analyzed by a similar comprehensive approach and assigned to class 3, as it is in our study.…”

Section: Discussionsupporting

confidence: 65%

“…Moreover, three of the class 1 or 2 UVs (MSH2 p.Gly322Asp, MLH1 p.Ser406Asn and p.Val716Met) were classified as benign in a structured assessment study on MMR ambiguous mutations by Barnetson et al 34 MSH2 p.Gly322Asp and MLH1 c.1039-8TϾA were also considered by Arnold et al, 24 but not studied further, because they were found at polymorphic frequency in unaffected controls. This points to the potential value of our classification scheme.…”

Section: Discussionmentioning

confidence: 99%

“…16 -23 Statistical evaluation UVs were classified using likelihood of pathogenicity for both quantitative and qualitative data. For individual variants, we used a Bayesian approach to incorporate direct and indirect evidence of pathogenicity in a single model, 4,13 starting from a prior probability of 0.5 24 and assuming statistical independence of the sources of information. Posterior probability of pathogenicity was obtained from the likelihood ratio and categorized in five classes.…”

Section: In Silico Analysismentioning

confidence: 99%

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Integrated analysis of unclassified variants in mismatch repair genes

Pastrello

Marroni

et al. 2011

Genetics in Medicine

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Purpose: Lynch syndrome is a genetic disease that predisposes to colorectal tumors, caused by mutation in mismatch repair genes. The use of genetic tests to identify mutation carriers does not always give perfectly clear results, as happens when an unclassified variant is found. This study aimed to define the pathogenic role of 35 variants present in MSH2, MLH1, MSH6, and PMS2 genes identified in our 15-year case study. Methods: We collected clinical and molecular data of all carriers, and then we analyzed the variants pathogenic role with web tools and molecular analyses. Using a Bayesian approach, we derived a posterior probability of pathogenicity and classified each variant according to a standardized five-class system. Results: The MSH2 p.Pro349Arg, p.Met688Arg, the MLH1 p.Gly67Arg, p.Thr82Ala, p.Lys618Ala, the MSH6 p.Ala1236Pro, and the PMS2 p.Arg20Gln were classified as pathogenic, and the MSH2 p.Cys697Arg and the PMS2 p.Ser46Ile were classified as likely pathogenic. Seven variants were likely nonpathogenic, 3 were nonpathogenic, and 16 remained uncertain. Conclusion: Quantitative assessment of several parameters and their integration in a multifactorial likelihood model is the method of choice for classifying the variants. As such classifications can be associated with surveillance and testing recommendations, the results and the method developed in our study can be useful for helping laboratory geneticists in evaluation of genetic tests and clinicians in the management of carriers. Genet Med 2011:13(2):115-124.

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Section: Discussionsupporting

confidence: 65%

Section: Discussionmentioning

confidence: 99%

Section: In Silico Analysismentioning

confidence: 99%

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Integrated analysis of unclassified variants in mismatch repair genes

Pastrello

Marroni

et al. 2011

Genetics in Medicine

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“…An intronic variant, c.1668-1 G > A, found in a heterozygous individual in 2KJPN, may cause exon skipping and is considered to be pathogenic [40]. Another missense variant, p.Arg687Trp, found in a heterozygous individual, was previously reported in two Japanese families with LS [41].…”

Section: Lynch Syndrome Genesmentioning

confidence: 94%

Evaluation of reported pathogenic variants and their frequencies in a Japanese population based on a whole-genome reference panel of 2049 individuals

et al. 2017

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Clarifying allele frequencies of disease-related genetic variants in a population is important in genomic medicine; however, such data is not yet available for the Japanese population. To estimate frequencies of actionable pathogenic variants in the Japanese population, we examined the reported pathological variants in genes recommended by the American College of Medical Genetics and Genomics (ACMG) in our reference panel of genomic variations, 2KJPN, which was created by whole-genome sequencing of 2049 individuals of the resident cohort of the Tohoku Medical Megabank Project. We searched for pathogenic variants in 2KJPN for 57 autosomal ACMG-recommended genes responsible for 26 diseases and then examined their frequencies. By referring to public databases of pathogenic variations, we identified 143 reported pathogenic variants in 2KJPN for the 57 ACMG recommended genes based on a classification system. At the individual level, 21% of the individuals were found to have at least one reported pathogenic allele. We then conducted a literature survey to review the variants and to check for evidence of pathogenicity. Our results suggest that a substantial number of people have reported pathogenic alleles for the ACMG genes, and reviewing variants is indispensable for constructing the information infrastructure of genomic medicine for the Japanese population.

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“…For genes with a large diagnostic interest, for example, breast and colon cancer, a committee of experts can be established that regularly meets to discuss the topic and give their expert opinion on the associated functional consequences and list this in the database. This committee can use software tools specifically built for the gene of interest to evaluate the potential consequences of each variant [Arnold et al, 2009;Jordan et al, 2011;Tavtigian et al, 2008].…”

Section: Answering Questionsmentioning

confidence: 99%

Curating gene variant databases (LSDBs): Toward a universal standard

et al. 2011

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Gene variant databases or Locus-Specific DataBases (LSDBs) are used to collect and display information on sequence variants on a gene-by-gene basis. Their most frequent use is in relation to DNA-based diagnostics, giving clinicians and scientists easy access to an up-to-date overview of all gene variants identified worldwide and whether they influence the function of the gene ("pathogenic or not"). While literature on gene variant databases is extensive, little has been published on the process of database curation itself. Based on our extensive experience as LSDB curators and our contributions to database curation courses, we discuss the subject of database curation. We describe the tasks involved, the steps to take, and the issues that might occur. Our overview is a first step toward establishing overall guidelines for database curation and ultimately covers one aspect of establishing quality-assured gene variant databases.

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ClassifyingMLH1andMSH2variants using bioinformatic prediction, splicing assays, segregation, and tumor characteristics

Cited by 61 publications

References 49 publications

Integrated analysis of unclassified variants in mismatch repair genes

Integrated analysis of unclassified variants in mismatch repair genes

Evaluation of reported pathogenic variants and their frequencies in a Japanese population based on a whole-genome reference panel of 2049 individuals

Curating gene variant databases (LSDBs): Toward a universal standard

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