The COL4A5 gene in Japanese Alport syndrome patients: Spectrum of mutations of all exons

The COL4A5 gene in Japanese Alport syndrome patients: Spectrum of mutations of all exons. To determine the spectrum of mutations of the COL4A5 gene encoding type IV collagen among Japanese Alport syndrome (AS) patients, 60 unrelated patients (47 males and 13 females) from all over the country were r...

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Veröffentlicht in:Kidney international 1996-03, Vol.49 (3), p.814-822
Hauptverfasser: Kawai, Shinichiro, Nomura, Shinsuke, Harano, Teruo, Harano, Keiko, Fukushima, Tatsuo, Osawa, Gengo, Japanese Alport Network
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Sprache:eng
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Zusammenfassung:The COL4A5 gene in Japanese Alport syndrome patients: Spectrum of mutations of all exons. To determine the spectrum of mutations of the COL4A5 gene encoding type IV collagen among Japanese Alport syndrome (AS) patients, 60 unrelated patients (47 males and 13 females) from all over the country were recruited. Screening for mutations in all the exons (1 to 51) of the COL4A5 gene was carried out by PCR-SSCP analysis. A mobility shift was observed in 22 of 60 patients, and their genomic DNA were analyzed by the direct sequence method and using cloned ssDNA. Nine of these had missense mutations in the collagenous domain (in exons 39, 37, 31, 29, 28, 27, 21, 20,19). Eight of these mutations were observed in a codon of glycine residue. Two were altered to arginine, two to valine, two to glutamic acid and two to aspartic acid. The other missense mutation was a change from isoleucine to serine in a interruption region. Five patients had small size base deletions and one had a 4bp insertion resulting in frameshift (in exons 49, 41, 19, 14, 13). Three had a splice site mutation (in exons 49,47,27). One had a nonsense mutation (in exon 17). These mutations seemed to be pathogenic, but the phenotype, which includes extrarenal manifestations, can vary with respect to both expression and severity. The remaining mutations were three silent ones (in exons 19, 39, 46). In addition, major gene rearrangement seemed to be rare in Japanese AS patients.
ISSN:0085-2538
1523-1755
DOI:10.1038/ki.1996.113