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- W2001664985 abstract "Summary. Nonsense/stop mutations in the ankyrin‐1 gene ( ANK1 ) are a major cause of dominant HS (dHS) (frequency of 23% in German dHS patients). To date, no common mutation has been found and therefore a simple mutation screening is not feasible. The reduced expression of one cDNA allele in the (AC) n microsatellite polymorphism of the ankyrin‐1 gene, as seen in about 20% of Czech patients with dHS, may identify candidates with a possible frameshift/nonsense mutation. In order to verify the efficiency of this screening we screened the ankyrin‐1 gene of 22 Czech dHS patients for both the reduced cDNA allele expression in the frequent (AC) n and the common exonic 26/39 polymorphisms, as well as for polymerase chain reaction (PCR) single‐stranded conformation polymorphisms in any one of the 42 exons of ANK1 . Anomalous PCR products were sequenced. We found seven new ANK1 frameshift/nonsense mutations in nine patients with, but in none of six patients without, a reduced cDNA allele expression (efficiency of 78%). We conclude that screening of dHS patients for such a reduced allele expression in common ANK1 polymorphisms is an efficient procedure for the identification of candidates for frameshift/nonsense mutations in the ankyrin‐1 gene." @default.
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- W2001664985 date "2003-08-01" @default.
- W2001664985 modified "2023-10-16" @default.
- W2001664985 title "Simultaneous (AC)<sub>n</sub> microsatellite polymorphism analysis and single-stranded conformation polymorphism screening is an efficient strategy for detecting ankyrin-1 mutations in dominant hereditary spherocytosis" @default.
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- W2001664985 doi "https://doi.org/10.1046/j.1365-2141.2003.04479.x" @default.
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