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R353Q polymorphism, activated factor VII, and risk of premature myocardial infarction in Japanese men.
Authors:Masakazu Ogawa  Satoshi Abe  Sadatoshi Biro  Masahiko Saigo  Takashi Kihara  Shiro Setoyama  Tatsuru Matsuoka  Hitoshi Toda  Hiroyuki Torii  Yoshihiko Atsuchi  Yoshifumi Toyama  Shigeki Tateishi  Shinichi Minagoe  Ikuro Maruyama  Chuwa Tei
Affiliation:Department of Cardiovascular, Graduate School of Medicine, Kagoshima University, Japan.
Abstract:
BACKGROUND: The association between myocardial infarction (MI) and the R353Q polymorphism of the Factor VII (FVII) gene, which reportedly influences FVII concentrations, activated Factor VII (FVIIa), or FVII antigen (FVIIag), remains controversial. METHODS AND RESULTS: The present case - control study in 127 Japanese men with their first MI at or before 45 years of age and 150 matched healthy controls was designed to clarify this association in premature MI. R353Q polymorphism was determined by polymerase chain reaction, and plasma concentrations of FVIIa and FVIIag were assayed. The distribution of the RR, RQ, and QQ genotypes with respect to R353Q polymorphism was 117, 10, and 0 in the patients, and 131, 17, and 2 in the controls. The Q allele was negatively associated with premature MI (odds ratio =0.41, p=0.038). The plasma concentration of FVIIa was slightly higher in patients (55.1+/-40.9 U/L) than in controls (44.8+/-20.2 U/L), but not significantly (p=0.078); the plasma concentration of FVIIag did not differ between patients (88.7+/-15.7%) and controls (87.0+/-9.0%) (p=0.557). Plasma FVIIa concentrations were influenced by R353Q polymorphism (p<0.001). CONCLUSIONS: The Q allele may be protective against premature MI.
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