Contribution of factor VII genotype to activated FVII levels - Differences in genotype frequencies between northern and southern European populations

被引:92
|
作者
Bernardi, F
Arcieri, P
Bertina, RM
Chiarotti, F
Corral, J
Pinotti, M
Prydz, H
Samama, M
Sandset, PM
Strom, R
Garcia, VV
Mariani, G
机构
[1] UNIV ROMA LA SAPIENZA, DIPARTIMENTO BIOTECNOL CELLULARI & EMATOL, ROME, ITALY
[2] UNIV LEIDEN HOSP, HAEMOSTASIS & THROMBOSIS RES CTR, NL-2300 RC LEIDEN, NETHERLANDS
[3] IST SUPER SANITA, I-00161 ROME, ITALY
[4] UNIV MURCIA, GEN HOSP, HAEMATOL UNIT, MURCIA, SPAIN
[5] UNIV OSLO, CTR BIOTECHNOL, OSLO, NORWAY
[6] HOP HOTEL DIEU, LAB THROMBOSE EXPT, FAC BROISSAIS, PARIS, FRANCE
[7] UNIV OSLO, ULLEVAAL HOSP, HAEMATOL LAB, MED CLIN, N-0407 OSLO, NORWAY
[8] UNIV PALERMO, CATTEDRA EMATOL, PALERMO, ITALY
关键词
factor VIIa; factor VII genotype; multicenter study;
D O I
10.1161/01.ATV.17.11.2548
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
The relationship between coagulation factor VII (FVII) levels in plasma and FVII genotypes, determined by three polymorphisms (5'F7, IVS7, and 353R/Q), were studied in 500 control subjects enrolled in a European multicenter study. The selection of particular FVII genotypes and the analysis of variance clearly indicated the independent contribution of a single 5'F7 insertion (A2) or 353Q (M2) allele to lowering plasma levels of activated FVII (FVIIa) (by a mean 25%). The M2 allele alone was found to make a major contribution to the genetically determined component of the FVIIa levels. Genotypes associated with low FVII levels were significantly rarer in the northern part of Europe (Oslo) than in the southern part (Rome, Murcia). The contribution made by the FVII genotype to the total variance of FVIIa levels was higher (30%) than that made to either FVII activity (25%) or FVII antigen (12%). Subjects with different FVII genotypes showed up to fivefold differences in mean FVIIa values, thus allowing attribution of a substantial part of the considerable interindividual variation to genetic variation, which may be of assistance in the interpretation of FVIIa levels on an individual basis. When FVII levels were adjusted by age and by triglyceride levels, the contribution of FVII genotypes to the FVII phenotypic variance was virtually unchanged. Taken together, these data indicate that in healthy control subjects the FVII genotype is a major predictor of plasma FVIIa levels and would support further study on the role of FVII genetic components in the development of cardiovascular disease.
引用
收藏
页码:2548 / 2553
页数:6
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