Inherited thrombophilic disorders in young adults with ischemic stroke and patent foramen ovale

Alessandro Pezzini; Elisabetta Del Zotto; Mauro Magoni; Angelo Costa; Silvana Archetti; Mario Grassi; Nabil Maalikjy Akkawi; Alberto Albertini; Deodato Assanelli; Luigi Amedeo Vignolo; Alessandro Padovani

doi:10.1161/01.str.0000046457.54037.cc

Inherited thrombophilic disorders in young adults with ischemic stroke and patent foramen ovale

Stroke. 2003 Jan;34(1):28-33. doi: 10.1161/01.str.0000046457.54037.cc.

Authors

Alessandro Pezzini¹, Elisabetta Del Zotto, Mauro Magoni, Angelo Costa, Silvana Archetti, Mario Grassi, Nabil Maalikjy Akkawi, Alberto Albertini, Deodato Assanelli, Luigi Amedeo Vignolo, Alessandro Padovani

Affiliation

¹ Clinica Neurologica, Università degli Studi di Brescia, Brescia, Italia. ale_pezzini@hotmail.com

PMID: 12511746
DOI: 10.1161/01.str.0000046457.54037.cc

Abstract

Background and purpose: The pathogenic link between patent foramen ovale (PFO) and stroke remains unknown in most cases. We investigated the association between inherited thrombophilic disorders and PFO-related strokes in a series of young adults in the setting of a case-control study.

Methods: We investigated 125 consecutive subjects (age, 34.7+/-7.3 years) with ischemic stroke and 149 age- and sex-matched control subjects. PFO was assessed in all patients with transcranial Doppler sonography with intravenous injection of agitated saline according to a standardized protocol. Genetic analyses for the factor V (FV)(G1691A) mutation, the prothrombin (PT)(G20210A) variant, and the TT677 genotype of methylenetetrahydrofolate reductase (MTHFR) were performed in all subjects.

Results: A pathogenic role of PFO was presumed in 36 patients (PFO+). Interatrial right-to-left shunt either was not detected or was considered unrelated to stroke occurrence in the remaining 89 patients (PFO-). The PT(G20210A) variant was more frequent in the PFO+ group compared with control subjects and the PFO- group (PFO+ versus control subjects, 11% versus 2%; 95% CI, 0.04 to 0.94; PFO+ versus PFO-, 11% versus 1.1%; 95% CI, 1.09 to 109; P=0.047). A similar distribution was observed for subjects carrying either the PT(G20210A) variant or the FV(G1691A) mutation (PFO+ versus control subjects, 19.4% versus 5.3%; 95% CI, 0.08 to 0.75; PFO+ versus PFO-, 19.4% versus 3.3%; 95% CI, 1.45 to 26.1; P=0.021). Combined thrombophilic defects were observed in 3 subjects of the PFO+ group, in 2 control subjects (8.3% versus 1.3%; 95% CI, 0.01 to 0.66; P=0.015), and in 0 subjects in the PFO- group. A trend toward a difference in the frequency of the FV(G1691A) mutation between PFO+ and control subjects was found after bivariate analysis (11% versus 3.3%; P=0.068) but not after multinomial logistic regression analysis. No significant association was found in the distribution of the TT MTHFR genotype in the 3 groups.

Conclusions: In young adults, the PT(G20210A) variant and, to a lesser extent, the FV(G1691A) mutation may represent risk factors for PFO-related cerebral infarcts. A role of systemic thrombophilic disorders in the pathogenesis of this specific subtype of stroke may be hypothesized.

MeSH terms

Adult
Brain Ischemia / diagnosis
Brain Ischemia / genetics*
Case-Control Studies
Cerebral Infarction / genetics
Factor V / genetics
Female
Genetic Predisposition to Disease
Genetic Variation
Genotype
Heart Septal Defects, Atrial / complications*
Heart Septal Defects, Atrial / diagnosis
Humans
Male
Methylenetetrahydrofolate Reductase (NADPH2)
Oxidoreductases Acting on CH-NH Group Donors / genetics
Prospective Studies
Prothrombin / genetics
Stroke / diagnosis
Stroke / genetics*
Thrombosis / genetics

Substances

Factor V
Prothrombin
Oxidoreductases Acting on CH-NH Group Donors
Methylenetetrahydrofolate Reductase (NADPH2)