• Title of article

    Polymorphisms in the thrombopoietin gene are associated with risk of myocardial infarction at a young age

  • Author/Authors

    Karen E. Webb، نويسنده , , John F. Martin، نويسنده , , Anders Hamsten، نويسنده , , Per Eriksson، نويسنده , , Licia Iacoviello، نويسنده , , Marinella Gattone، نويسنده , , Maria Benedetta Donati، نويسنده , , Augusto Di Castelnuovo، نويسنده , , Jorge Erusalimsky، نويسنده , , Steve E. Humphries، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2001
  • Pages
    9
  • From page
    703
  • To page
    711
  • Abstract
    Five polymorphisms in the thrombopoietin (TPO) gene were identified, one in the 5′ untranslated region (UTR) (C1796T), two within intron 5 (C4830A and A4877C), and two in the 3′ UTR (A5713G and A6160T). The allele frequencies were determined in a group of 450 healthy middle aged men from the UK and found to be 0.46 for 1796T, 0.38 for 4830A, 0.004 for 4877C, 0.47 for 5713G and 0.07 for 6160T. Genotypes for the three common polymorphisms were determined in a group of 176 young male Swedish survivors of a myocardial infarction (MI) and 186 age-matched controls and a group of 156 young Italian survivors of an MI and 147 age and sex matched controls. In both the Swedish and the Italian studies polymorphisms were found to be associated with increased risk of MI. In the Swedish sample the frequency of 4830A was significantly higher in controls (0.40) compared with patients (0.29) (P=0.003), with an odds ratio for AA homozygotes of 0.48 (0.25–0.92; P=0.03) compared with CC homozygotes. In the Italian sample the frequency of 5713G was significantly lower in controls (0.31) compared with cases (0.40) (P=0.03), with an odds ratio for GG homozygotes of 2.29 (1.08–4.89; P=0.03) compared with AA homozygotes. These risk associations are consistent since 4830A and 5713A show strong allelic association. After adjusting for other measured risk factors the effect on risk was still significant in the Italian sample 2.39 (1.02–5.58), but not in the Swedish sample 0.46 (0.16–1.32). The observation of frequency differences between cases and controls in two independent samples strongly suggests that the TPO gene is involved as a risk factor for developing MI at a young age, but the identified polymorphisms are probably acting as markers for an unidentified functional mutation elsewhere in the gene locus.
  • Keywords
    platelet , Thrombopoietin , myocardial infarction , polymorphism
  • Journal title
    Atherosclerosis
  • Serial Year
    2001
  • Journal title
    Atherosclerosis
  • Record number

    630267