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Analysis of the tandem repeat locus D4Z4 associated with facioscapulohumeral muscular dystropothhy
Authors:Hewitt, Jane E.   Lyle, Robert   Clark, Lorraine N.   Valleley, Elizabeth M.   Wright, Tracy J.   Wijmenga, Cisca   van Deutekom, Judith C.T.   Francis, Fiona   Sharpe, Paul T.   Hofker, Marten   Frants, Rune R.   Williamson, Robert
Affiliation:1School of Biological Sciences, 3.239 Stopford Building. University of Manchester Oxford Road, Manchester M13 9PT 2Department of Biochemistry and Molecula Genetics, St Mary's Hospital Medical School, Imperial College of Science, Technonology and Medicine London W2 1PG, UK 3MGC-Department of Human Genetics, Leiden University 2333 AL Leiden, the Netherlands 4Genome Analysis, ICRF, 44 Lincoln's Inn Fields London WC2 3PX 5Department of Craniofacial Development, UMDS, Guy's Hospital London Bridge, London SE1 9RT, UK
Abstract:The sequence of the tandem repeat sequence (D4Z4) associatedwith facioscapulohumeral muscular dystrophy (FSHD) has beendetermined: each copy of the 3.3 kb repeat contains two homeoboxesand two previously described repetitive sequences, LSau anda GC-rich low copy repeat designated hhspm3. By Southern blotting,FISH and isolation of cDNA and genomic clones we show that thereare repeat sequences similar to D4Z4 at other locations in thehuman genome. Southern blot analysis of primate genomic DNAindicates that the copy number of D4Z4-like repeats has increasedmarkedly within the last 25 million years. Two cDNA clones wereisolated and found to contain stop codons and frameshifts withinthe homeodomains. An STS was produced to the cDNAs and analysisof a somatic cell hybrid panel suggests they map to chromosome14. No cDNA clones mapping to the chromosome 4q35 D4Z4 repeatshave been Identified, although the possiblilty that they encodea protein cannot be ruled out. Although D4Z4 may not encodea protein, there is an association between deletions withinthis locus and FSHD. The D4Z4 repeats contain LSau repeats andare adjacent to 68 bp Sau3A repeats. Both of these sequencesare associated with heterochromatic regions of DNA, regionsknown to be involved in the phenomenon of position effect variegation.We postulate that deletion of D4Z4 sequences could produce aposition effect.
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