| Literature DB >> 18064309 |
Afshin Ameri1, Deepa K Machiah, Thuy T Tran, Cynthia Channell, Valerie Crenshaw, Karl Fernstrom, Manana Khachidze, Alexander Duncan, Sebastien Fuchs, Tom E Howard.
Abstract
We identified a previously unknown mutation by sequencing the factor (F)X gene in a severely haemorrhagic 14-year-old male African-American individual with undetectable plasma FX-activity and -antigen levels. This mutation, called F10-Augusta, was homozygote and is a combination of an 8bp insertion in flanking 3'-genomic-DNA and a 5bp terminal exon-8 deletion involving codons 437 and 438. Sequencing of RT-PCR and 3'-RACE products showed that the F10-Augusta transcript is normally processed but lacks an in-frame stop codon. An allele specific 3'-RACE-based RFLP assay demonstrated that the steady-state concentration of the mutant transcript was markedly lower than that of the wild-type message in total-RNA samples from the patient's unaffected heterozygous parents. The recently discovered nonstop decay mechanism, a component pathway of the mRNA surveillance system, is a possible explanation for the reduced concentration of the mutant FX transcript. This is the first report implying such a mechanism in the pathogenesis of inherited bleeding disorders.Entities:
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Year: 2007 PMID: 18064309 DOI: 10.1160/th07-02-0125
Source DB: PubMed Journal: Thromb Haemost ISSN: 0340-6245 Impact factor: 5.249