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bias of selection on human copy-number variants偏见的选择对人类人类基因组变异
Bias of Selection on Human Copy-Number
Variants
*
Duc-Quang Nguyen, Caleb Webber, Chris P. Ponting
MRC Functional Genetics Unit, Department of Human Anatomy and Genetics, University of Oxford, Oxford, United Kingdom
Although large-scale copy-number variation is an important contributor to conspecific genomic diversity, whether
these variants frequently contribute to human phenotype differences remains unknown. If they have few functional
consequences, then copy-number variants (CNVs) might be expected both to be distributed uniformly throughout the
human genome and to encode genes that are characteristic of the genome as a whole. We find that human CNVs are
significantly overrepresented close to telomeres and centromeres and in simple tandem repeat sequences.
Additionally, human CNVs were observed to be unusually enriched in those protein-coding genes that have
experienced significantly elevated synonymous and nonsynonymous nucleotide substitution rates, estimated between
single human and mouse orthologues. CNV genes encode disproportionately large numbers of secreted, olfactory, and
immunity proteins, although they contain fewer than expected genes associated with Mendelian disease. Despite
mouse CNVs also exhibiting a significant elevation in synonymous substitution rates, in most other respects they do
not differ significantly from the genomic background. Nevertheless, they encode proteins that are depleted in
olfactory function, and they exhibit significantly decreased amino acid sequence divergence. Natural selection appears
to have acted discriminately among human CNV genes. The significant overabundance, within human CNVs, of genes
associated with olfaction, immunity, protein secretion, and elevated coding se
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