Maternal Thrombophilic and Hypofibrinolytic Genetic Variants in Idiopathic Recurrent Pregnancy Loss: a Continuing Mystery

被引:0
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作者
Mahmoud Younis
Mohamed A. M. Ali
Doaa A. Ghareeb
Rehab Youssef
Shadia A. Fathy
机构
[1] Department of Molecular Genetics,Department of Biology, College of Science
[2] Al Borg Diagnostics,Department of Biochemistry, Faculty of Science
[3] Imam Mohammad Ibn Saud Islamic University,Bio
[4] Ain Shams University,Screening and Preclinical Trial Lab, Department of Biochemistry, Faculty of Science
[5] Alexandria University,Fetomaternal Ultrasound Unit, Department of Obstetrics and Gynecology, Faculty of Medicine
[6] Alexandria University,undefined
来源
Reproductive Sciences | 2023年 / 30卷
关键词
Gene polymorphisms; Inherited thrombophilias; Fibrinolytic pathway disorders; Recurrent miscarriage; Genetic association study;
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摘要
Despite the fact that multiple recurrent pregnancy loss (RPL) etiologies have been identified, 50–70% of RPL cases remain enigmatic, and idiopathic RPL is still a serious medical challenge. A plethora of studies have investigated the correlation of RPL with variations in coagulation and/or fibrinolytic factors-encoding genes. Notwithstanding, evidence for a link between these variations and RPL remains discordant. We aimed to explore the association of thrombophilic and hypofibrinolytic gene variations with RPL development. Two hundred Saudi women were recruited in this study, comprising 150 women experiencing RPL and 50 healthy women. Thirteen genetic variants, including FV G1691A, FV A4070G, F2 G20210A, F13A1 G103T, FGB − 455G > A, PAI-1 − 675 4G/5G, ITGB3 T1565C, MTHFR C677T, MTHFR A1298C, ACE I/D, APOB G10708A, APOE T388C, and APOE C526T were genotyped using ViennaLab StripAssay. Women experiencing RPL harbor significantly higher frequencies of the F13A1 103 T, FGB − 455A, and ITGB3 1565C alleles than control women (p < 0.001). No differences in the prevalence of other investigated variants were identified between control women and those with RPL. No considerable link of F5 1691G > A/4070A > G, MTHFR 677C > T/1298A > C, and APOE 388 T > C/526C > T haplotypes with RPL risk was demonstrated. F13A1 G103T, FGB − 455G > A, and ITGB3 T1565C variants are connected to a higher likelihood of developing RPL and, hence, may have the potential to identify those women at risk of RPL, thereby, improving RPL susceptibility prediction. Incorporating molecular testing of thrombophilic and hypofibrinolytic genetic variants into routine workup could confer a promising approach for refined RPL risk assessment.
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页码:656 / 666
页数:10
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