Predicting the functional, molecular, and phenotypic consequences of amino acid substitutions using hidden Markov models.
Hashem A. Shihab,Julian Gough,David Neil Cooper,Peter D. Stenson,Gary L A Barker,Keith J. Edwards,Ian N. M. Day,Tom R. Gaunt +7 more
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TLDR
The Functional Analysis Through Hidden Markov Models (FATHMM) software and server is described: a species‐independent method with optional species‐specific weightings for the prediction of the functional effects of protein missense variants, demonstrating that FATHMM can be efficiently applied to high‐throughput/large‐scale human and nonhuman genome sequencing projects with the added benefit of phenotypic outcome associations.Abstract:
The rate at which nonsynonymous single nucleotide polymorphisms (nsSNPs) are being identified in the human genome is increasing dramatically owing to advances in whole-genome/whole-exome sequencing technologies. Automated methods capable of accurately and reliably distinguishing between pathogenic and functionally neutral nsSNPs are therefore assuming ever-increasing importance. Here, we describe the Functional Analysis Through Hidden Markov Models (FATHMM) software and server: a species-independent method with optional species-specific weightings for the prediction of the functional effects of protein missense variants. Using a model weighted for human mutations, we obtained performance accuracies that outperformed traditional prediction methods (i.e., SIFT, PolyPhen, and PANTHER) on two separate benchmarks. Furthermore, in one benchmark, we achieve performance accuracies that outperform current state-of-the-art prediction methods (i.e., SNPs&GO and MutPred). We demonstrate that FATHMM can be efficiently applied to high-throughput/large-scale human and nonhuman genome sequencing projects with the added benefit of phenotypic outcome associations. To illustrate this, we evaluated nsSNPs in wheat (Triticum spp.) to identify some of the important genetic variants responsible for the phenotypic differences introduced by intense selection during domestication. A Web-based implementation of FATHMM, including a high-throughput batch facility and a downloadable standalone package, is available at http://fathmm.biocompute.org.uk.read more
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FH4=STAP1. Another gene for familial hypercholesterolemia? Relevance to cascade testing and drug development?
TL;DR: The apparent identification of a further FH gene (dubbed FH4 by Fouchier et al4) should be of significant interest to geneticists, lipid clinics, general doctors, and cardiologists with an interest in tracing or treating familial hypercholesterolemics, and to pharmaceutical companies engaged with the development of new approaches to treating hyperCholesterolemia.
Journal ArticleDOI
Systematic alanine scanning of PAX8 paired domain reveals functional importance of the N-subdomain.
Megumi Iwahashi,Satoshi Narumi +1 more
TL;DR: This is the first alanine scanning mutagenesis study, in which 132Alanine variants located in the paired domain of PAX8 were created and systematically evaluated in vitro and tested the accuracy of seven computational algorithms for pathogenicity prediction.
Posted ContentDOI
KCNQ gene family members act as both tumor suppressors and oncogenes in gastrointestinal cancers
David Shorthouse,Eric P. Rahrmann,Cassandra Kosmidou,Benedict Greenwood,Michael W. J. Hall,Ginny Devonshire,Richard J. Gilbertson,Rebecca C. Fitzgerald,Benjamin A. Hall +8 more
TL;DR: It is proposed that mutation/copy number alteration of KCNQ genes can significantly alter patient prognosis in GI cancers, and potentially as prognostic markers or therapeutic targets, and implicate KCNZ genes in control/mediation of the WNT pathway in cancer.
DissertationDOI
Comprehensive genomic characterization of matched primary-metastatic lung adenocarcinomas using a multiparameter nuclei flow-sorting approach
TL;DR: The observation that established metastases spread to other sites in a cascading manner argues in favor of aggressive local treatment of all metastatic sites in patients with oligometastatic disease.
Journal ArticleDOI
Phenotypic screening models for rapid diagnosis of genetic variants and discovery of personalized therapeutics.
TL;DR: In this article , the utility of animal models, with a focus mainly on C. elegans, was discussed, as a contrast to tissue culture and in silico approaches, with emphasis on how these systems are used in determining pathogenicity of variants with uncertain significance and then used to screen for novel therapeutics.
References
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Marco Punta,Penny Coggill,Ruth Y. Eberhardt,Jaina Mistry,John Tate,Chris Boursnell,Ningze Pang,Kristoffer Forslund,Goran Ceric,Jody Clements,Andreas Heger,Liisa Holm,Erik L. L. Sonnhammer,Sean R. Eddy,Alex Bateman,Robert D. Finn +15 more
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