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首页> 外文期刊>Maturitas: International Journal for the Study of the Climacteric >Does the progesterone receptor genetic polymorphism +331G/A hPR influence the risk of venous thromboembolism among postmenopausal women using hormone therapy? The ESTHER Study.
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Does the progesterone receptor genetic polymorphism +331G/A hPR influence the risk of venous thromboembolism among postmenopausal women using hormone therapy? The ESTHER Study.

机译:孕激素受体基因多态性+ 331G / A hPR是否会影响使用激素疗法的绝经后妇女发生静脉血栓栓塞的风险? ESTHER研究。

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摘要

Hormone therapy (HT) increases venous thromboembolism (VTE) risk among postmenopausal women. Data on the influence of steroids receptors polymorphisms on this association remain scarce. Since progesterone receptor (hPR) is expressed in human veins and specific progestogens increase VTE risk, we investigated the impact of the functional +331G/A hPR polymorphism on the association of VTE with HT. Using the data of the ESTHER study, we showed that ORs for VTE in current users of progesterone or progestins were not significantly different by hPR+331G/A genotype status. hPR polymorphism appears not to have a significant effect on VTE risk related to HT.
机译:激素治疗(HT)增加了绝经后妇女的静脉血栓栓塞(VTE)风险。关于类固醇受体多态性对该关联的影响的数据仍然很少。由于孕激素受体(hPR)在人静脉中表达,并且特定的孕激素会增加VTE风险,因此我们研究了+ 331G / A hPR多态性对VTE与HT关联的影响。使用ESTHER研究的数据,我们显示hPR + 331G / A基因型状态对当前孕酮或孕激素使用者中VTE的OR没有显着差异。 hPR多态性似乎对与HT相关的VTE风险没有显着影响。

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