4.8 Article

A burst of segmental duplications in the genome of the African great ape ancestor

Journal

NATURE
Volume 457, Issue 7231, Pages 877-881

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/nature07744

Keywords

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Funding

  1. NIH [HG002385, U54 HG003079]
  2. Marie Curie fellowship
  3. Departament d'Educacio i Universitats de la Generalitat de Catalunya
  4. ICREA Funding Source: Custom

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It is generally accepted that the extent of phenotypic change between human and great apes is dissonant with the rate of molecular change(1). Between these two groups, proteins are virtually identical(1,2), cytogenetically there are few rearrangements that distinguish ape - human chromosomes(3), and rates of single- base- pair change(4-7) and retrotransposon activity(8-10) have slowed particularly within hominid lineages when compared to rodents or monkeys. Studies of gene family evolution indicate that gene loss and gain are enriched within the primate lineage(11,12). Here, we perform a systematic analysis of duplication content of four primate genomes ( macaque, orang- utan, chimpanzee and human) in an effort to understand the pattern and rates of genomic duplication during hominid evolution. We find that the ancestral branch leading to human and African great apes shows the most significant increase in duplication activity both in terms of base pairs and in terms of events. This duplication acceleration within the ancestral species is significant when compared to lineage- specific rate estimates even after accounting for copy- number polymorphism and homoplasy. We discover striking examples of recurrent and independent gene- containing duplications within the gorilla and chimpanzee that are absent in the human lineage. Our results suggest that the evolutionary properties of copy- number mutation differ significantly from other forms of genetic mutation and, in contrast to the hominid slowdown of single- base- pair mutations, there has been a genomic burst of duplication activity at this period during human evolution.

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