Predicting the impact of Lynch syndrome-causing missense mutations from structural calculations

Sofie V, Nielsen; Amelie Stein; Alexander B. Dinitzen; Elena Papaleo; Michael H. Tatham; Esben Guldahl Poulsen; Maher Mahmoud Kassem; Lene Juel Rasmussen; Kresten Lindorff-Larsen; Rasmus Hartmann-Petersen

doi:10.1371/journal.pgen.1006739

Predicting the impact of Lynch syndrome-causing missense mutations from structural calculations

Sofie V, Nielsen, Amelie Stein, Alexander B. Dinitzen, Elena Papaleo, Michael H. Tatham, Esben Guldahl Poulsen, Maher Mahmoud Kassem, Lene Juel Rasmussen, Kresten Lindorff-Larsen, Rasmus Hartmann-Petersen

42 Citationer (Scopus)

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Abstract

Accurate methods to assess the pathogenicity of mutations are needed to fully leverage the possibilities of genome sequencing in diagnosis. Current data-driven and bioinformatics approaches are, however, limited by the large number of new variations found in each newly sequenced genome, and often do not provide direct mechanistic insight. Here we demonstrate, for the first time, that saturation mutagenesis, biophysical modeling and co-variation analysis, performed in silico, can predict the abundance, metabolic stability, and function of proteins inside living cells. As a model system, we selected the human mismatch repair protein, MSH2, where missense variants are known to cause the hereditary cancer predisposition disease, known as Lynch syndrome. We show that the majority of disease-causing MSH2 mutations give rise to folding defects and proteasome-dependent degradation rather than inherent loss of function, and accordingly our in silico modeling data accurately identifies disease-causing mutations and outperforms the traditionally used genetic disease predictors. Thus, in conclusion, in silico biophysical modeling should be considered for making genotype-phenotype predictions and for diagnosis of Lynch syndrome, and perhaps other hereditary diseases.

Originalsprog	Engelsk
Artikelnummer	e1006739
Tidsskrift	PLoS Genetics
Vol/bind	13
Udgave nummer	4
Antal sider	26
ISSN	1553-7390
DOI	https://doi.org/10.1371/journal.pgen.1006739
Status	Udgivet - 19 apr. 2017

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Citationsformater

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AU - Stein, Amelie

AU - Dinitzen, Alexander B.

AU - Papaleo, Elena

AU - Tatham, Michael H.

AU - Poulsen, Esben Guldahl

AU - Kassem, Maher Mahmoud

AU - Rasmussen, Lene Juel

AU - Lindorff-Larsen, Kresten

AU - Hartmann-Petersen, Rasmus

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AB - Accurate methods to assess the pathogenicity of mutations are needed to fully leverage the possibilities of genome sequencing in diagnosis. Current data-driven and bioinformatics approaches are, however, limited by the large number of new variations found in each newly sequenced genome, and often do not provide direct mechanistic insight. Here we demonstrate, for the first time, that saturation mutagenesis, biophysical modeling and co-variation analysis, performed in silico, can predict the abundance, metabolic stability, and function of proteins inside living cells. As a model system, we selected the human mismatch repair protein, MSH2, where missense variants are known to cause the hereditary cancer predisposition disease, known as Lynch syndrome. We show that the majority of disease-causing MSH2 mutations give rise to folding defects and proteasome-dependent degradation rather than inherent loss of function, and accordingly our in silico modeling data accurately identifies disease-causing mutations and outperforms the traditionally used genetic disease predictors. Thus, in conclusion, in silico biophysical modeling should be considered for making genotype-phenotype predictions and for diagnosis of Lynch syndrome, and perhaps other hereditary diseases.

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Predicting the impact of Lynch syndrome-causing missense mutations from structural calculations

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