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Isolation of candidate cDNAs for portions of the Duchenne muscular dystrophy gene.
Duchenne muscular dystrophy (DMD) and the less severe Becker muscular dystrophy (BMD) are human X-linked muscle-wasting disorders that have been localized to the band Xp21 by genetic linkage analysis and cytologically detectable abnormalities. A cloned DNA segment, DXS164 (or pERT87), has been shown to detect deletions in the DNA of unrelated DMD and BMD males. Here we present the nucleotide sequence of two highly conserved DNA fragments from the DXS164 locus and their homologous sequences from the mouse X chromosome. One of the human conserved segments hybridized to a large transcript in RNA isolated from human fetal skeletal muscle and was used to isolate cDNA clones which cover approximately 10% of this transcript. The cDNA clones map to Xp21 and hybridize with a minimum of eight small regions that span 130 kilobases (kb) of the DXS164 locus. These expressed sequences are candidates for portions of the gene responsible for both DMD and BMD.
PMID: 3773991 [PubMed - indexed for MEDLINE]
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Cited by over 100 PubMed Central articles
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Applications of metabolomics and proteomics to the mdx mouse model of Duchenne muscular dystrophy: lessons from downstream of the transcriptome.
Griffin JL, Des Rosiers C.
Genome Med. 2009 Mar 25; 1(3):32. Epub 2009 Mar 25.
[Genome Med. 2009]
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Bex1 knock out mice show altered skeletal muscle regeneration.
Koo JH, Smiley MA, Lovering RM, Margolis FL.
Biochem Biophys Res Commun. 2007 Nov 16; 363(2):405-10. Epub 2007 Sep 11.
[Biochem Biophys Res Commun. 2007]
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Zebrafish orthologs of human muscular dystrophy genes.
Steffen LS, Guyon JR, Vogel ED, Beltre R, Pusack TJ, Zhou Y, Zon LI, Kunkel LM.
BMC Genomics. 2007 Mar 20; 8:79. Epub 2007 Mar 20.
[BMC Genomics. 2007]
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