Haplotype structure,LD blocks,and uneven recombination within the LRP5 gene |
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| Authors: | Twells Rebecca C J Mein Charles A Phillips Michael S Hess J Fred Veijola Riitta Gilbey Matthew Bright Matthew Metzker Michael Lie Benedicte A Kingsnorth Amanda Gregory Edward Nakagawa Yusuke Snook Hywel Wang William Y S Masters Jennifer Johnson Gillian Eaves Iain Howson Joanna M M Clayton David Cordell Heather J Nutland Sarah Rance Helen Carr Philippa Todd John A |
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| Affiliation: | JDRF/WT Diabetes and Inflammation Laboratory, Cambridge Institute for Medical Research, University of Cambridge, Cambridge CB2 2XY, UK. rebecca.twells@cimr.cam.ac.uk |
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| Abstract: | Patterns of linkage disequilibrium (LD) in the human genome are beginning to be characterized, with a paucity of haplotype diversity in "LD blocks," interspersed by apparent "hot spots" of recombination. Previously, we cloned and physically characterized the low-density lipoprotein-receptor-related protein 5 (LRP5) gene. Here, we have extensively analysed both LRP5 and its flanking three genes, spanning 269 kb, for single nucleotide polymorphisms (SNPs), and we present a comprehensive SNP map comprising 95 polymorphisms. Analysis revealed high levels of recombination across LRP5, including a hot-spot region from intron 1 to intron 7 of LRP5, where there are 109 recombinants/Mb (4882 meioses), in contrast to flanking regions of 14.6 recombinants/Mb. This region of high recombination could be delineated into three to four hot spots, one within a 601-bp interval. For LRP5, three haplotype blocks were identified, flanked by the hot spots. Each LD block comprised over 80% common haplotypes, concurring with a previous study of 14 genes that showed that common haplotypes account for at least 80% of all haplotypes. The identification of hot spots in between these LD blocks provides additional evidence that LD blocks are separated by areas of higher recombination. |
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