DNA polymorphisms in ITPA including basis of inosine triphosphatase deficiency

被引：92

作者：

Cao, HN ^{[1
]}

Hegele, RA ^{[1
]}

机构：

[1] John P Robarts Res Inst, Blackburn Cardiovasc Genet Lab, London, ON N6A 5K8, Canada

来源：

JOURNAL OF HUMAN GENETICS | 2002年 / 47卷 / 11期

基金：

加拿大健康研究院;

关键词：

nucleotides; erythrocytes; genomic DNA; sequencing; monogenic disease;

D O I：

10.1007/s100380200095

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

Intracellular concentrations of the nucleotide inosine triphosphate (ITP) are regulated by ITP-ase (EC 3.6.1.19), which is encoded by ITPA on chromosome 20p. Subjects with complete deficiency of ITP-ase activity (MIM 147520) have elevated ITP concentrations in erythrocytes, but no obvious clinical abnormalities. Based on biochemical screening, complete ITP-ase deficiency has been postulated to result from homozygosity for a dysfunctional allele, with an estimated frequency of 0.05 in Caucasians. ITP-ase deficiency has not yet been characterized at the molecular genetic level. Sequencing of the genomic DNA from a Caucasian subject with complete ITP-ase deficiency revealed homozygosity for missense mutation 198C>A, which predicted a threonine for proline substitution at codon 32 (P32T), whereas among 125 normal Caucasians, there were no homozygotes for P32T (P = 0.0079). The P32T allele frequency of 0.07 in Caucasians was similar to the estimates derived from earlier biochemical studies. P32T was found to be present at varying frequency in other ethnic groups. Two common synonymous single-nucleotide polymorphisms were also identified. These ITPA markers, including P32T, provide tools for further study of association with clinical and biochemical phenotypes.

引用

页码：620 / 622

页数：3

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