4.7 Article

Copy number variation and evolution in humans and chimpanzees

期刊

GENOME RESEARCH
卷 18, 期 11, 页码 1698-1710

出版社

COLD SPRING HARBOR LAB PRESS, PUBLICATIONS DEPT
DOI: 10.1101/gr.082016.108

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资金

  1. Coriell Institute for Medical Research
  2. Integrated Primate Biomaterials and Information Resource
  3. New Iberia Research Center
  4. Primate Foundation of Arizona
  5. Leakey Foundation
  6. Wenner-Gren Foundation for Anthropological Research
  7. National Institutes of Health [HG004221]
  8. University of Louisiana at Lafayette-New Iberia Research Center [RR015087, RR014491, RR016483]
  9. Howard Hughes Medical Institute
  10. Wellcome Trust

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Copy number variants (CNVs) underlie many aspects of human phenotypic diversity and provide the raw material for gene duplication and gene family expansion. However, our understanding of their evolutionary significance remains limited. We performed comparative genomic hybridization on a single human microarray platform to identify CNVs among the genomes of 30 humans and 30 chimpanzees as well as fixed copy number differences between species. We found that human and chimpanzee CNVs occur in orthologous genomic regions far more often than expected by chance and are strongly associated with the presence of highly homologous intrachromosomal segmental duplications. By adapting population genetic analyses for use with copy number data, we identified functional categories of genes that have likely evolved under purifying or positive selection for copy number changes. In particular, duplications and deletions of genes with inflammatory response and cell proliferation functions may have been fixed by positive selection and involved in the adaptive phenotypic differentiation of humans and chimpanzees.

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