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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Loss-of-function variants in KCTD19 cause non-obstructive azoospermia in humans
Junyan Liu,Fazal Rahim,Jianteng Zhou,Suixing Fan,Hanwei Jiang,Changping Yu,Jing M. Chen,Jianze Xu,Gang Yang,Wasim Shah,Muhammad Zubair,Asad Ullah Khan,Yang Li,Basit Shah,Daren Zhao,Furhan Iqbal,Xiaohua Jiang,Tonghang Guo,Peng Xu,Bo Xu,Limin Wu,Hui Ma,Yuanwei Zhang,Huan Zhang,Qinghua Shi +24 more
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Prediction of cancer driver genes through integrated analysis of differentially expressed genes at the individual level
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Journal ArticleDOI
Understanding structure-guided variant effect predictions using 3D convolutional neural networks
TL;DR: DeepRank-Mut as mentioned in this paper is a configurable framework designed to extract and learn from physicochemically relevant features of amino acids surrounding missense variants in 3D space, including sequence conservation scores of the surrounding amino acids, and stored in multi-channel 3D voxel grids which are then used to train a 3D convolutional neural network.
Journal ArticleDOI
The genetics of autism spectrum disorder in an East African familial cohort
İslam Oğuz Tuncay,A Gogate,Kiran J Kaur,Ashwani Kumar,Chao Xing,Kimberly Goodspeed,Maria H. Chahrour +6 more
TL;DR: In this paper , the authors investigated the genetics of ASD in an East African cohort (129 individuals) from a population with higher prevalence (5%). Whole-genome sequencing identified 2.13 million private variants in the cohort and potentially pathogenic variants in known ASD genes (including CACNA1C, CHD7, FMR1, and TCF7L2).
Journal ArticleDOI
N6-methyladenosine modification in 18S rRNA promotes tumorigenesis and chemoresistance via HSF4b/HSP90B1/mutant p53 axis.
TL;DR: Zhang et al. as mentioned in this paper revealed that METTL5/TRMT112 and their mediated m6A modification at the 18S rRNA 1832 site (m6A1832) are elevated in nasopharyngeal carcinoma (NPC) and promote oncogenic transformation in vitro and in vivo.
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