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29 Mammalian Genomes Reveal Novel Exaptations of Mobile Elements for Likely Regulatory Functions in the Human Genome

Overview of attention for article published in PLOS ONE, August 2012
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Title
29 Mammalian Genomes Reveal Novel Exaptations of Mobile Elements for Likely Regulatory Functions in the Human Genome
Published in
PLOS ONE, August 2012
DOI 10.1371/journal.pone.0043128
Pubmed ID
Authors

Craig B. Lowe, David Haussler

Abstract

Recent research supports the view that changes in gene regulation, as opposed to changes in the genes themselves, play a significant role in morphological evolution. Gene regulation is largely dependent on transcription factor binding sites. Researchers are now able to use the available 29 mammalian genomes to measure selective constraint at the level of binding sites. This detailed map of constraint suggests that mammalian genomes co-opt fragments of mobile elements to act as gene regulatory sequence on a large scale. In the human genome we detect over 280,000 putative regulatory elements, totaling approximately 7 Mb of sequence, that originated as mobile element insertions. These putative regulatory regions are conserved non-exonic elements (CNEEs), which show considerable cross-species constraint and signatures of continued negative selection in humans, yet do not appear in a known mature transcript. These putative regulatory elements were co-opted from SINE, LINE, LTR and DNA transposon insertions. We demonstrate that at least 11%, and an estimated 20%, of gene regulatory sequence in the human genome showing cross-species conservation was co-opted from mobile elements. The location in the genome of CNEEs co-opted from mobile elements closely resembles that of CNEEs in general, except in the centers of the largest gene deserts where recognizable co-option events are relatively rare. We find that regions of certain mobile element insertions are more likely to be held under purifying selection than others. In particular, we show 6 examples where paralogous instances of an often co-opted mobile element region define a sequence motif that closely matches a transcription factor's binding profile.

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Geographical breakdown

Country Count As %
Germany 2 2%
Brazil 2 2%
Canada 2 2%
United Kingdom 2 2%
United States 2 2%
Spain 1 <1%
Switzerland 1 <1%
Unknown 97 89%

Demographic breakdown

Readers by professional status Count As %
Student > Ph. D. Student 29 27%
Researcher 25 23%
Student > Bachelor 14 13%
Student > Master 10 9%
Student > Doctoral Student 4 4%
Other 13 12%
Unknown 14 13%
Readers by discipline Count As %
Agricultural and Biological Sciences 60 55%
Biochemistry, Genetics and Molecular Biology 24 22%
Computer Science 3 3%
Medicine and Dentistry 2 2%
Arts and Humanities 1 <1%
Other 3 3%
Unknown 16 15%