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Evolution of Human-Specific Neural SRGAP2 Genes by Incomplete Segmental Duplication
Author(s) -
Megan Y. Dennis,
Xander Nuttle,
Peter H. Sudmant,
Francesca Antonacci,
Tina Graves,
Mikhail Nefedov,
Jill A. Rosenfeld,
Saba Sajjadian,
Maika Malig,
Holland Kotkiewicz,
Cynthia J. Curry,
Susan Shafer,
Lisa G. Shaffer,
Pieter J. de Jong,
Richard K. Wilson,
Evan E. Eichler
Publication year - 2012
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2012.03.033
Subject(s) - biology , gene duplication , gene , genetics , evolutionary biology , adaptive evolution , computational biology
Gene duplication is an important source of phenotypic change and adaptive evolution. We leverage a haploid hydatidiform mole to identify highly identical sequences missing from the reference genome, confirming that the cortical development gene Slit-Robo Rho GTPase-activating protein 2 (SRGAP2) duplicated three times exclusively in humans. We show that the promoter and first nine exons of SRGAP2 duplicated from 1q32.1 (SRGAP2A) to 1q21.1 (SRGAP2B) ∼3.4 million years ago (mya). Two larger duplications later copied SRGAP2B to chromosome 1p12 (SRGAP2C) and to proximal 1q21.1 (SRGAP2D) ∼2.4 and ∼1 mya, respectively. Sequence and expression analyses show that SRGAP2C is the most likely duplicate to encode a functional protein and is among the most fixed human-specific duplicate genes. Our data suggest a mechanism where incomplete duplication created a novel gene function-antagonizing parental SRGAP2 function-immediately "at birth" 2-3 mya, which is a time corresponding to the transition from Australopithecus to Homo and the beginning of neocortex expansion.

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