scholarly journals Improved inference of site-specific positive selection under a generalized parametric codon model when there are multinucleotide mutations and multiple nonsynonymous rates

2019 ◽  
Vol 19 (1) ◽  
Author(s):  
Katherine A. Dunn ◽  
Toby Kenney ◽  
Hong Gu ◽  
Joseph P. Bielawski
2008 ◽  
Vol 82 (10) ◽  
pp. 5099-5103 ◽  
Author(s):  
Errol Strain ◽  
Laura A. Kelley ◽  
Stacey Schultz-Cherry ◽  
Spencer V. Muse ◽  
Matthew D. Koci

ABSTRACT To understand astrovirus biology, it is essential to understand factors associated with its evolution. The current study reports the genomic sequences of nine novel turkey astrovirus (TAstV) type 2-like clinical isolates. This represents, to our knowledge, the largest genomic-length data set available for any one astrovirus type. The comparison of these TAstV sequences suggests that the TAstV species contains multiple subtypes and that recombination events have occurred across the astrovirus genome. In addition, the analysis of the capsid gene demonstrated evidence for both site-specific positive selection and purifying selection.


2021 ◽  
Vol 6 (1) ◽  
Author(s):  
Randi Istrup Juul ◽  
Morten Muhlig Nielsen ◽  
Malene Juul ◽  
Lars Feuerbach ◽  
Jakob Skou Pedersen

AbstractLarge sets of whole cancer genomes make it possible to study mutation hotspots genome-wide. Here we detect, categorize, and characterize site-specific hotspots using 2279 whole cancer genomes from the Pan-Cancer Analysis of Whole Genomes project and provide a resource of annotated hotspots genome-wide. We investigate the excess of hotspots in both protein-coding and gene regulatory regions and develop measures of positive selection and functional impact for individual hotspots. Using cancer allele fractions, expression aberrations, mutational signatures, and a variety of genomic features, such as potential gain or loss of transcription factor binding sites, we annotate and prioritize all highly mutated hotspots. Genome-wide we find more high-frequency SNV and indel hotspots than expected given mutational background models. Protein-coding regions are generally enriched for SNV hotspots compared to other regions. Gene regulatory hotspots show enrichment of potential same-patient second-hit missense mutations, consistent with enrichment of hotspot driver mutations compared to singletons. For protein-coding regions, splice-sites, promoters, and enhancers, we see an excess of hotspots associated with cancer genes. Interestingly, missense hotspot mutations in tumor suppressors are associated with elevated expression, suggesting localized amino-acid changes with functional impact. For individual non-coding hotspots, only a small number show clear signs of positive selection, including known sites in the TERT promoter and the 5’ UTR of TP53. Most of the new candidates have few mutations and limited driver evidence. However, a hotspot in an enhancer of the oncogene POU2AF1, which may create a transcription factor binding site, presents multiple lines of driver-consistent evidence.


2013 ◽  
Vol 781-784 ◽  
pp. 1835-1841
Author(s):  
Yong Xiong ◽  
Chun Yan Zhao ◽  
Qing Song Yang

Rbcl gene of 13 Lilium species were amplified, sequenced and analyzed. By comparing the rbcL sequences with 32 other species retrieved from GenBank, the sequence divergences and the phyletic evolution were analyzed and the phylogenetic tree was constructed. All rbcL sequences across 45 species are 732 bp with an average GC content of 45.1%. Potentially parsimony informative characters (PIC) are 39. From the phylogenetic tree, it can be found that it consists of three branches which are Liliaceae Lilium (I), other Liliaceae genus (II), Trilliaceae and Palmae (III).3D model was structured by homology comparative SWISS-Model online and showed with RasTop sofeware.The evolutionary analyses from the site-specific model, the 142nd and 225th codon sites are found to be under positive selection in rbcL gene.


2016 ◽  
Author(s):  
Jesse D. Bloom

AbstractSites of positive selection are identified by comparing observed evolutionary patterns to those expected under a null model for evolution in the absence of such selection. For protein-coding genes, the most common null model is that nonsynonymous and synonymous mutations fix at equal rates; this unrealistic model has limited power to detect many interesting forms of selection. I describe a new approach that uses a null model based on high-throughput lab measurements of a gene's site-specific amino-acid preferences. This null model makes it possible to identify diversifying selection for amino-acid change and differential selection for mutations to amino acids that are unexpected given the measurements made in the lab. I show that this approach identifies sites of adaptive substitutions in four genes (lactamase, Gal4, influenza nucleoprotein, and influenza hemagglutinin) far better than a comparable method that simply compares the rates of nonsynonymous and synonymous substitutions. As rapid increases in biological data enable increasingly nuanced descriptions of the constraints on individual sites, approaches like the one here can improve our ability to identify many interesting forms of selection.


2012 ◽  
Vol 279 (1746) ◽  
pp. 4433-4440 ◽  
Author(s):  
Shixia Xu ◽  
Yuan Chen ◽  
Yuefeng Cheng ◽  
Dan Yang ◽  
Xuming Zhou ◽  
...  

The enlargement of cetacean brain size represents an enigmatic event in mammalian evolution, yet its genetic basis remains poorly explored. One candidate gene associated with brain size evolution is the abnormal spindle-like microcephaly associated (ASPM), as mutations in this gene cause severe reductions in the cortical size of humans. Here, we investigated the ASPM gene in representative cetacean lineages and previously published sequences from other mammals to test whether the expansion of the cetacean brain matched adaptive ASPM evolution patterns. Our analyses yielded significant evidence of positive selection on the ASPM gene during cetacean evolution, especially for the Odontoceti and Delphinoidea lineages. These molecular patterns were associated with two major events of relative brain size enlargement in odontocetes and delphinoids. It is of particular interest to find that positive selection was restricted to cetaceans and primates, two distant lineages both characterized by a massive expansion of brain size. This result is suggestive of convergent molecular evolution, although no site-specific convergence at the amino acid level was found.


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