普伐他汀改善早期严重胎儿生长受限妊娠期血管生成因子和胎胎盘多普勒:一例报告

M. Mendoza
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引用次数: 0

摘要

早期胎儿生长受限(FGR)是围产期发病率和死亡率的主要原因。对于生长受限的胎儿或任何胎盘相关疾病(如先兆子痫),没有任何治疗策略被证明对改善胎儿和新生儿结局有效。送出胎儿和胎盘是唯一有效的治疗方法。然而,最近的研究表明,普伐他汀在妊娠期似乎是安全的,可以改善胎盘灌注和胎儿生长,防止血管生成失衡。血管生成(PlGF)和抗血管生成(sFlt-1)因子和胎母多普勒评价与胎儿生长受限预后和严重程度密切相关。因此,普伐他汀被认为是一种很有前途的治疗胎儿生长限制的药物。我们报告一例早发性FGR患者每日服用普伐他汀40mg直至分娩。在此期间,记录胎母多普勒和血管生成谱演变。普伐他汀应用后,胎儿和胎盘血流灌注及血管生成失衡均有所改善。sFlt-1的下调比PlGF的上调更明显。患者在妊娠27+6周时出现严重的先兆子痫(PE),由于高血压难以充分治疗,需要立即取出胎儿。本报告支持进一步研究使用普伐他汀改善FGR胎儿血管生成特征和胎母循环。
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Pravastatin Improves Angiogenic Factors and Feto- Placental Doppler in Pregnancy with Early Severe Fetal Growth Restriction: A Case Report
Early fetal growth restriction (FGR) is a leading cause of perinatal morbidity and mortality. No therapeutic strategies have proved to be effective in improving fetal and neonatal outcomes either in growth restricted fetuses or any placenta-related disorder such as preeclampsia. Delivery of the fetus and placenta is the only definitive cure. However, recent studies suggest that pravastatin appears to be safe in pregnancy, improves placental perfusion and fetal growth and prevents angiogenic imbalance. Angiogenic (PlGF) and antiangiogenic (sFlt-1) factors and feto-maternal Doppler evaluation are strongly associated with fetal growth restriction prognosis and severity. Thus, pravastatin has been proposed as a promising therapeutic drug for fetal growth restriction. We report the findings of a case of early-onset FGR treated with pravastatin 40mg daily until delivery. During this time, feto-maternal Doppler and angiogenic profile evolution were recorded. Fetal and placental perfusion observed on Doppler and angiogenic imbalance improved after pravastatin was started. sFlt-1 down-regulation was more marked than PlGF up-regulation. The patient developed severe preeclampsia (PE) at 27+6 weeks of gestation, necessitating immediate fetal extraction owing to hypertension refractory to adequate treatment. This report supports further investigation on the use of pravastatin to improve angiogenic profile and feto-maternal circulation in FGR fetuses.
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