| Literature DB >> 10671058 |
L Flagiello1, V Cirigliano, M Strazzullo, V Cappa, A Ciccodicola, M D'Esposito, I Torrente, R Werner, G Di Iorio, M Rinaldi, A Dallapiccola, A Forabosco, V Ventruto, M D'Urso.
Abstract
Charcot-Marie-Tooth type I demyelinating neuropathies are genetically heterogeneous disorders (chrmosome 17,1,X). There are at least three genes on X chromosome, the more frequently involved being Cx32 in Xq13.1. Cx32 encodes for connexin-32, a gap junction protein of 283 aminoacids. We report the results of molecular studies in a CMTX1 Italian family, in which the mutation, found in the 5'-UTR, resulted in an abnormal mRNA connexin-32 expression. Mutations in PMP22 and P0 genes were also excluded in this family. Cx32 gene analysis carried out by PCR-SSCP on family members genomic DNAs, running a 321 bp fragment spanning the TATA box, the trasciptional start site, and the non coding exon 1b, revealed a shift correlated with a transition from C to T at position 40 of exon 1b of the 12 affected members, while was not found in the controls. Then the RT PCR-SSCP on cDNA from two peripheral nerve biopsies of two heterozygous females of the family were sequenced showing only the wild-type alleles and suggesting that mutated mRNAs were too unstable to be detected. The result also suggests a regulating role of the 5'-UTR of Cx32 mRNA.Entities:
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Year: 1998 PMID: 10671058
Source DB: PubMed Journal: Hum Mutat ISSN: 1059-7794 Impact factor: 4.878