Alu-Mediated Acquisition of Unstable ATTCT Pentanucleotide Repeats in the Human ATXN10 Gene

doi:10.1093/molbev/msp172

MBE Advance Access originally published online on August 3, 2009
Molecular Biology and Evolution 2009 26(11):2573-2579; doi:10.1093/molbev/msp172

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© The Author 2009. Published by Oxford University Press on behalf of the Society for Molecular Biology and Evolution. All rights reserved. For permissions, please e-mail: journals.permissions@oxfordjournals.org

Research Articles

Alu-Mediated Acquisition of Unstable ATTCT Pentanucleotide Repeats in the Human ATXN10 Gene

Tatsuaki Kurosaki^*^,, Tohru Matsuura, Kinji Ohno and Shintaroh Ueda^*

^* Department of Biological Sciences, Graduate School of Science, The University of Tokyo, Tokyo, Japan
Division of Neurogenetics, Center for Neurological Diseases and Cancer, Nagoya University Graduate School of Medicine, Nagoya, Japan

E-mail: sueda{at}biol.s.u-tokyo.ac.jp.

Accepted for publication July 28, 2009.

Spinocerebellar ataxia type 10 is caused by ATTCT repeat expansionin the ATXN10 gene in humans. We studied the evolutionary historyof the human genome to determine the time and mechanism of theacquisition of unstable ATTCT repeats in the genome. We foundthat long interspersed element-1 (LINE-1) was inserted intoATXN10 intron 9; Alu was then inserted in the middle of LINE-1;and endogenous retrovilcus K was lastly retrotransposed in themiddle of Alu. The ATTCT repeat was located on the boundarybetween the 3'-end of the Alu element and the direct repeatarising from LINE-1. We determined nucleotide sequences of theorthologous region of 50 individuals representing 33 primatespecies and compared them with the human sequence. The analysisrevealed that the ATTCT repeat is present only in human andapes. Old World monkeys also possess pentanucleotide repeats,but their motifs are TGTCT and GGTCT. New World monkeys andprosimians are not informative because they lack the correspondingregion in ATXN10 intron 9. Our studies dictate two parsimoniousscenarios of evolution. First, a TTTCT motif arose from a TTTTTmotif at the junction of Alu and LINE-1, which was followedby introduction of A to make an ATTCT motif in hominoids. Second,an ATTCT motif was directly generated from an ancestral ATTTTmotif in the common ancestor of catarrhines. We also demonstratethat orangutan uniquely introduced G to make a GTTCT motif andlater C to make a GTTCC motif, where newly introduced nucleotidesare underlined. Our studies reveal that nucleotide substitutionsin a poly(A) tail of the Alu element and the following amplificationof pentanucleotides occurred in the lineages of Old World monkeysand hominoids and that unstable ATTCT pentanucleotide repeatsoriginated in the common ancestor of hominoids. These findingsalso highlight a new aspect of the role of retrotransposonsin human disease and evolution, which might be useful in investigatingthe mystery of human uniqueness.

Key Words: spinocerebellar ataxia • SCA10 • pentanucleotide repeat • neurodegenerative disease • Alu

Norihiro Okada, Associate Editor

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