DNA sequence and analysis of human chromosome 9

S. J. Humphray,K. Oliver,A. R. Hunt,R. W. Plumb,J. E. Loveland,K. L. Howe,T. D. Andrews,S. Searle,S. E. Hunt,C. E. Scott,M. C. Jones,R. Ainscough,J. P. Almeida,K. D. Ambrose,R. I. S. Ashwell,A. K. Babbage, S. Babbage,C. L. Bagguley,J. Bailey,R. Banerjee,D. J. Barker,K. F. Barlow,K. Bates,H. Beasley,O. Beasley,C. P. Bird,S. Bray-Allen,A. J. Brown,J. Y. Brown,D. Burford,W. Burrill,J. Burton,C. Carder,N. P. Carter,J. C. Chapman,Y. Chen, G. Clarke,S. Y. Clark,C. M. Clee,S. Clegg,R. E. Collier,N. Corby, M. Crosier, A. T. Cummings,J. Davies,P. Dhami,M. Dunn, I. Dutta, L. W. Dyer,M. E. Earthrowl,L. Faulkner,C. J. Fleming,A. Frankish,J. A. Frankland,L. French, D. G. Fricker,P. Garner,J. Garnett,J. Ghori,J. G. R. Gilbert, C. Glison,D. V. Grafham,S. Gribble,C. Griffiths, S. Griffiths-Jones, R. Grocock, J. Guy,R. E. Hall,S. Hammond,J. L. Harley, E. S. I. Harrison,E. A. Hart,P. D. Heath, C. D. Henderson, B. L. Hopkins, P. J. Howard,P. J. Howden,E. Huckle,C. Johnson,D. Johnson, A. A. Joy,M. Kay, S. Keenan, J. K. Kershaw,A. M. Kimberley,A. King, A. Knights,G. K. Laird,C. Langford,S. Lawlor,D. A. Leongamornlert,M. Leversha,C. Lloyd,D. M. Lloyd,J. Lovell,S. Martin,M. Mashreghi-Mohammadi,L. Matthews,S. McLaren,K. E. McLay,A. McMurray,S. Milne,T. Nickerson, J. Nisbett, G. Nordsiek,A. V. Pearce,A. I. Peck,K. M. Porter, R. Pandian, S. Pelan,B. Phillimore, S. Povey,Y. Ramsey,V. Rand, M. Scharfe,H. K. Sehra, R. Shownkeen,S. K. Sims,C. D. Skuce,M. Smith,C. A. Steward,D. Swarbreck,N. Sycamore,J. Tester,A. Thorpe,A. Tracey,A. Tromans,D. W. Thomas,M. Wall,J. M. Wallis,A. P. West,S. L. Whitehead,D. L. Willey, S. A. Williams,L. Wilming,P. W. Wray,L. Young,J. L. Ashurst,A. Coulson, H. Blöcker,R. Durbin,J. E. Sulston,T. Hubbard, M. J. Jackson,D. R. Bentley,S. Beck,J. Rogers,I. Dunham

Nature（2004）

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摘要

Chromosome 9 is highly structurally polymorphic. It contains the largest autosomal block of heterochromatin, which is heteromorphic in 6–8% of humans, whereas pericentric inversions occur in more than 1% of the population. The finished euchromatic sequence of chromosome 9 comprises 109,044,351 base pairs and represents >99.6% of the region. Analysis of the sequence reveals many intra- and interchromosomal duplications, including segmental duplications adjacent to both the centromere and the large heterochromatic block. We have annotated 1,149 genes, including genes implicated in male-to-female sex reversal, cancer and neurodegenerative disease, and 426 pseudogenes. The chromosome contains the largest interferon gene cluster in the human genome. There is also a region of exceptionally high gene and G + C content including genes paralogous to those in the major histocompatibility complex. We have also detected recently duplicated genes that exhibit different rates of sequence divergence, presumably reflecting natural selection.

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human chromosome,dna sequence

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