| Literature DB >> 15318213 |
Xinwei She1, Julie E Horvath, Zhaoshi Jiang, Ge Liu, Terrence S Furey, Laurie Christ, Royden Clark, Tina Graves, Cassy L Gulden, Can Alkan, Jeff A Bailey, Cenk Sahinalp, Mariano Rocchi, David Haussler, Richard K Wilson, Webb Miller, Stuart Schwartz, Evan E Eichler.
Abstract
An understanding of how centromeric transition regions are organized is a critical aspect of chromosome structure and function; however, the sequence context of these regions has been difficult to resolve on the basis of the draft genome sequence. We present a detailed analysis of the structure and assembly of all human pericentromeric regions (5 megabases). Most chromosome arms (35 out of 43) show a gradient of dwindling transcriptional diversity accompanied by an increasing number of interchromosomal duplications in proximity to the centromere. At least 30% of the centromeric transition region structure originates from euchromatic gene-containing segments of DNA that were duplicatively transposed towards pericentromeric regions at a rate of six-seven events per million years during primate evolution. This process has led to the formation of a minimum of 28 new transcripts by exon exaptation and exon shuffling, many of which are primarily expressed in the testis. The distribution of these duplicated segments is nonrandom among pericentromeric regions, suggesting that some regions have served as preferential acceptors of euchromatic DNA.Entities:
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Year: 2004 PMID: 15318213 DOI: 10.1038/nature02806
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962