AI Article Synopsis

  • Short contiguous peptide minimotifs can impact human variation and are influenced by selection, often showing a high level of conservation with 94% invariance.
  • Analysis of approximately 300,000 minimotifs in nearly 1,100 human genomes revealed that most minimotifs are under negative selection, with some experiencing neutral drift or positive selection similar to coding regions.
  • The study suggests minimotifs contribute to genetic variation, potentially affect DNA packaging due to variations in histone tails, and indicate adaptive evolution across different human populations.

Article Abstract

Since the function of a short contiguous peptide minimotif can be introduced or eliminated by a single point mutation, these functional elements may be a source of human variation and a target of selection. We analyzed the variability of ∼300 000 minimotifs in 1092 human genomes from the 1000 Genomes Project. Most minimotifs have been purified by selection, with a 94% invariance, which supports important functional roles for minimotifs. Minimotifs are generally under negative selection, possessing high genomic evolutionary rate profiling (GERP) and sitewise likelihood-ratio (SLR) scores. Some are subject to neutral drift or positive selection, similar to coding regions. Most SNPs in minimotif were common variants, but with minor allele frequencies generally <10%. This was supported by low substation rates and few newly derived minimotifs. Several minimotif alleles showed different intercontinental and regional geographic distributions, strongly suggesting a role for minimotifs in adaptive evolution. We also note that 4% of PTM minimotif sites in histone tails were common variants, which has the potential to differentially affect DNA packaging among individuals. In conclusion, minimotifs are a source of functional genetic variation in the human population; thus, they are likely to be an important target of selection and evolution.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4513861PMC
http://dx.doi.org/10.1093/nar/gkv580DOI Listing

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