FV Leiden mutation and deep venous thrombosis in Vojvodina: A case-control study

Between September 2007 and February 2010, the occurrence of symptomatic deep venous thrombosis (DVT) was investigated in a cohort of 79 consecutive patients. A case-control study included 71 healthy controls matched with cases for sex and age. The prevalence of factor V G1691A mutation genotype was...

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Main Authors: Salatić Iva, Kiralj Katarina, Mitić Gorana, Veselinović Igor, Vapa Dušan
Format: Article
Language:English
Published: Society of Medical Biochemists of Serbia, Belgrade 2011-01-01
Series:Journal of Medical Biochemistry
Subjects:
Online Access:https://scindeks-clanci.ceon.rs/data/pdf/1452-8258/2011/1452-82581101051S.pdf
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spelling doaj-98b001ea39654deba764b3d301b85fab2020-11-25T03:00:54ZengSociety of Medical Biochemists of Serbia, BelgradeJournal of Medical Biochemistry1452-82581452-82662011-01-0130151541452-82581101051SFV Leiden mutation and deep venous thrombosis in Vojvodina: A case-control studySalatić Iva0Kiralj Katarina1Mitić Gorana2Veselinović Igor3Vapa Dušan4Clinical Center of Vojvodina, Novi SadClinical Center of Vojvodina, Novi SadClinical Center of Vojvodina, Novi SadClinical Center of Vojvodina, Novi SadClinical Center of Vojvodina, Novi SadBetween September 2007 and February 2010, the occurrence of symptomatic deep venous thrombosis (DVT) was investigated in a cohort of 79 consecutive patients. A case-control study included 71 healthy controls matched with cases for sex and age. The prevalence of factor V G1691A mutation genotype was analyzed. Eighteen cases (22.79%; 95% confidence interval (CI) 13.53% to 32.03%) and four controls (5.63%; 95% CI 0.27% to 10.99%) were heterozygous carriers of FV Leiden (p= 0.025). The odds ratio for DVT was 4.94 (95% CI 1.58 to 15.42) and the relative risk 4.04 (95% CI 1.44-11.38) compared with FV 1691G carriers. Four cases were homozygous carriers of FV Leiden, giving a prevalence of 5.06% (95% CI 0.23 to 9.89%) and no controls, therefore OR and RR calculation was based on the prevalence of homozygotes in the general Caucasian population. The OR for DVT was 47.28 (95% CI 0.04 - 52167.3) and the RR 45.57 (95% CI 0.04 to 49540.77; p=0.025) compared with FV 1691 G carriers. Our study confirms that factor V Leiden carriers in Vojvodina, as in similar studies previously carried out in other populations, have an increased risk of developing DVT. The evaluated risk of DVT in heterozygous carriers of the mutation is four to five-fold higher, whereas for homozygous carriers it is 45- to 48-fold higher than in non-carriers. These results confirm that patients with DVT and their relatives should undergo screening for FV Leiden mutation. .https://scindeks-clanci.ceon.rs/data/pdf/1452-8258/2011/1452-82581101051S.pdffactor v leidendeep vein thrombosis
collection DOAJ
language English
format Article
sources DOAJ
author Salatić Iva
Kiralj Katarina
Mitić Gorana
Veselinović Igor
Vapa Dušan
spellingShingle Salatić Iva
Kiralj Katarina
Mitić Gorana
Veselinović Igor
Vapa Dušan
FV Leiden mutation and deep venous thrombosis in Vojvodina: A case-control study
Journal of Medical Biochemistry
factor v leiden
deep vein thrombosis
author_facet Salatić Iva
Kiralj Katarina
Mitić Gorana
Veselinović Igor
Vapa Dušan
author_sort Salatić Iva
title FV Leiden mutation and deep venous thrombosis in Vojvodina: A case-control study
title_short FV Leiden mutation and deep venous thrombosis in Vojvodina: A case-control study
title_full FV Leiden mutation and deep venous thrombosis in Vojvodina: A case-control study
title_fullStr FV Leiden mutation and deep venous thrombosis in Vojvodina: A case-control study
title_full_unstemmed FV Leiden mutation and deep venous thrombosis in Vojvodina: A case-control study
title_sort fv leiden mutation and deep venous thrombosis in vojvodina: a case-control study
publisher Society of Medical Biochemists of Serbia, Belgrade
series Journal of Medical Biochemistry
issn 1452-8258
1452-8266
publishDate 2011-01-01
description Between September 2007 and February 2010, the occurrence of symptomatic deep venous thrombosis (DVT) was investigated in a cohort of 79 consecutive patients. A case-control study included 71 healthy controls matched with cases for sex and age. The prevalence of factor V G1691A mutation genotype was analyzed. Eighteen cases (22.79%; 95% confidence interval (CI) 13.53% to 32.03%) and four controls (5.63%; 95% CI 0.27% to 10.99%) were heterozygous carriers of FV Leiden (p= 0.025). The odds ratio for DVT was 4.94 (95% CI 1.58 to 15.42) and the relative risk 4.04 (95% CI 1.44-11.38) compared with FV 1691G carriers. Four cases were homozygous carriers of FV Leiden, giving a prevalence of 5.06% (95% CI 0.23 to 9.89%) and no controls, therefore OR and RR calculation was based on the prevalence of homozygotes in the general Caucasian population. The OR for DVT was 47.28 (95% CI 0.04 - 52167.3) and the RR 45.57 (95% CI 0.04 to 49540.77; p=0.025) compared with FV 1691 G carriers. Our study confirms that factor V Leiden carriers in Vojvodina, as in similar studies previously carried out in other populations, have an increased risk of developing DVT. The evaluated risk of DVT in heterozygous carriers of the mutation is four to five-fold higher, whereas for homozygous carriers it is 45- to 48-fold higher than in non-carriers. These results confirm that patients with DVT and their relatives should undergo screening for FV Leiden mutation. .
topic factor v leiden
deep vein thrombosis
url https://scindeks-clanci.ceon.rs/data/pdf/1452-8258/2011/1452-82581101051S.pdf
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