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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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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Book ChapterDOI
Integrative Modeling and Novel Technologies in Human Genomics
TL;DR: The use of computational tools and methodologies such as single-cell molecular analyses, in addition to model system-derived data, are discussed as a way to gain a more complete understanding of genotype–phenotype relations.
Journal ArticleDOI
Adult-onset very-long-chain acyl-CoA dehydrogenase deficiency (VLCADD).
Farzad Fatehi,Ali Asghar Okhovat,Yalda Nilipour,Magdalena Mroczek,Volker Straub,Ana Töpf,Aleksa Palibrk,Stojan Peric,V. Rakocevic Stojanovic,Hossein Najmabadi,Shahriar Nafissi +10 more
TL;DR: The aim of this study was to describe the clinical and genetic manifestations of six patients with adult‐onset VLCADD.
Journal ArticleDOI
Evaluation of two approaches to lysosomal acid lipase deficiency patient identification: An observational retrospective study.
TL;DR: The measurement of plasma chitotriosidase activity (ChT) and CCL18/PARC concentration in addition to LLP will be a useful approach to identifying LALD patients in retrospective LALD patient studies.
Journal ArticleDOI
A Curriculum for Genomic Education of Molecular Genetic Pathology Fellows: A Report of the Association for Molecular Pathology Training and Education Committee.
Jason N. Rosenbaum,Anna B. Berry,Alanna J. Church,Kristy Crooks,Jeffrey Gagan,Dolores Lopez-Terrada,John D. Pfeifer,Hanna Rennert,Iris Schrijver,Anthony N. Snow,David Wu,Mark D. Ewalt +11 more
TL;DR: The Genomics Task Force of the MGP Program Directors, a working group of the Association for Molecular Pathology Training and Education Committee, has developed a genomics curriculum framework and recommendations specific to the molecular genetic pathology fellowship as mentioned in this paper.
Journal ArticleDOI
Generalized Cytokine Increase in the Setting of a Multisystem Clinical Disorder and Carcinoid Syndrome Associated with a Novel NLRP12 Variant
Noam Jacob,Sonya Dasharathy,Viet L. Bui,Jihane N. Benhammou,Wayne W. Grody,Ram Raj Singh,Joseph R. Pisegna +6 more
TL;DR: A novel variant in the NLRP12 gene is identified in a 63-year-old woman and her daughter, who presented with an unusual clinical syndrome that differs from autoinflammatory disorders previously reported in association with theNLRP subfamily gene mutations.
References
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