Active Alu retrotransposons in the human genome
- E. Andrew Bennett1,2,3,
- Heiko Keller4,6,
- Ryan E. Mills2,3,6,
- Steffen Schmidt4,
- John V. Moran5,
- Oliver Weichenrieder4, and
- Scott E. Devine1,2,3,7
- 1 Genetics and Molecular Biology Graduate Program, Emory University School of Medicine, Atlanta, Georgia 30322, USA;
- 2 Department of Biochemistry, Emory University School of Medicine, Atlanta, Georgia 30322, USA;
- 3 Center for Bioinformatics, Emory University School of Medicine, Atlanta, Georgia 30322, USA;
- 4 Department of Biochemistry, Max Planck Institute for Developmental Biology, 72076 Tübingen, Germany;
- 5 Howard Hughes Medical Institute, Department of Human Genetics, University of Michigan Medical School, Ann Arbor, Michigan 48109, USA
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↵6 These authors contributed equally to this work.
Abstract
Alu retrotransposons evolved from 7SL RNA ∼65 million years ago and underwent several rounds of massive expansion in primate genomes. Consequently, the human genome currently harbors 1.1 million Alu copies. Some of these copies remain actively mobile and continue to produce both genetic variation and diseases by “jumping” to new genomic locations. However, it is unclear how many active Alu copies exist in the human genome and which Alu subfamilies harbor such copies. Here, we present a comprehensive functional analysis of Alu copies across the human genome. We cloned Alu copies from a variety of genomic locations and tested these copies in a plasmid-based mobilization assay. We show that functionally intact core Alu elements are highly abundant and far outnumber all other active transposons in humans. A range of Alu lineages were found to harbor such copies, including all modern AluY subfamilies and most AluS subfamilies. We also identified two major determinants of Alu activity: (1) The primary sequence of a given Alu copy, and (2) the ability of the encoded RNA to interact with SRP9/14 to form RNA/protein (RNP) complexes. We conclude that Alu elements pose the largest transposon-based mutagenic threat to the human genome. On the basis of our data, we have begun to identify Alu copies that are likely to produce genetic variation and diseases in humans.
Footnotes
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↵7 Corresponding author.
↵7 E-mail sedevin{at}emory.edu; fax (404) 727-3452.
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[Supplemental material is available online at www.genome.org.]
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Article published online before print. Article and publication date are at http://www.genome.org/cgi/doi/10.1101/gr.081737.108.
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- Received June 3, 2008.
- Accepted September 30, 2008.
- Copyright © 2008, Cold Spring Harbor Laboratory Press