Factor V Leiden and factor II G20210A mutations in patients with recurrent abortion

doi:10.1093/humrep/14.10.2448

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Human Reproduction, Vol. 14, No. 10, 2448-2450, October 1999
© 1999 European Society of Human Reproduction and Embryology

Factor V Leiden and factor II G20210A mutations in patients with recurrent abortion

S.S. Souza¹, R.A. Ferriani¹^,5, A.G. Pontes³, M.A. Zago²^,4 and R.F. Franco²^,4

¹ Sector of Human Reproduction, Department of Gynecology and Obstetrics and ² Department of Clinical Medicine, Faculty of Medicine of Ribeirão Preto, 14049-900 Ribeirão Preto, SP, ³ Department of Gynecology and Obstetrics, Faculty of Medicine of Botucatu, SP, and ⁴ Blood Center of Ribeirão Preto (FUNDHERP), SP, Brazil

Recurrent abortion (RA) represents an intriguing problem inobstetric practice in which genetic and acquired factors mayplay a role. In the present investigation we sought to assessthe possibility that inherited thrombophilia might determinethe risk of RA. We therefore investigated the prevalence oftwo genetic abnormalities frequently associated with venousthrombosis [factor V Leiden (FVL) and factor II G20210A] in56 patients with primary or secondary abortion and in 384 healthycontrol women. Polymerase chain reaction amplification followedby digestion with the restriction enzymes MnlI and HindIII wasused to define the FVL and FII G20210A genotypes respectively.FVL was found in 4/56 patients (7.1%) and in 6/384 controls(1.6%), yielding an odds ratio (OR) for RA related to FVL of4.9 [95% confidence interval (CI): 1.3–17.8]. FII G20210Awas detected in 2/56 (3.6%) patients and in 4/384 (1%) controls(OR for RA: 3.5, CI: 0.6–19.7). In conclusion, FVL andFII G20210A mutations in patients with RA were more prevalentin comparison with controls. These data support a role for bothmutations as determinants of the risk of RA and strengthen thenotion that thrombophilia plays a role in this clinical entity.

Key words: factor V Leiden/factor II G20210A/recurrent abortion/risk factor/thrombophilia

⁵ To whom correspondence should be addressed. E-mail: raferria{at}fmrp.usp.br

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