INOVASIA Study: A Randomized Open Controlled Trial to Evaluate Pravastatin to Prevent Preeclampsia and its Effects on sFlt1/PLGF Levels.
Muhammad Ilham Aldika AkbarAngelina YosediputraRaditya Eri PratamaNur Lailatul FadhilahSulistyowati SulistyowatiFariska Zata AmaniErnawati ErnawatiErry Gumilar DachlanMuhammad Dikman AngsarGustaaf DekkerPublished in: American journal of perinatology (2021)
Objectives To evaluate the effect of pravastatin to prevent preeclampsia (PE) in pregnant women at a high risk of developing preeclampsia and the maternal and perinatal outcomes and the sFlt1/PLGF ratio. Study Design This is an open labelled RCT part of INOVASIA trial. Pregnant women at a high risk of developing PE were recruited and randomized into an intervention group (40) and a control group (40). The inclusion criteria consisted of pregnant women with positive clinical risk factor and abnormal uterine artery doppler examination at 10-20 weeks gestational age. The control group received low dose aspirin (80 mg/day) and calcium (1 g/day), while the intervention group received additional pravastatin (20 mg twice daily) starting from 14-20 weeks gestation until delivery. Research blood samples were collected before the first dose of pravastatin and before delivery. The main outcome was the rate of maternal preeclampsia, maternal-perinatal outcomes, and sFlt-1, PLGF, sFlt-1/PlGF ratio and sEng levels. Results The rate of preeclampsia was (non-significantly) lower in the pravastatin group compared with the control group (17.5% vs 35%). The pravastatin group also had a (non-significant) lower rate of severe preeclampsia, HELLP syndrome, acute kidney injury and severe hypertension. The rate of (iatrogenic) preterm delivery was significantly (p=0.048) lower in the pravastatin group (n=4) compared with the controls (n=12). Neonates in the pravastatin group had significantly higher birthweights (2931 + 537 vs 2625 + 872 g; p=0.006), lower Apgar scores < 7 (2.5 vs 27.5%, p=0.002), composite neonatal morbidity (0 vs 20%, p=0.005) and NICU admission rates (0 vs 15%, p=0.026). All biomarkers show a significant deterioration in the control group compared with non significant changes in the pravastatin group. Conclusions Pravastatin holds promise in the secondary prevention of preeclampsia and placenta-mediated adverse perinatal outcomes by improving the angiogenic imbalance.
Keyphrases
- pregnant women
- early onset
- pregnancy outcomes
- gestational age
- low dose
- birth weight
- acute kidney injury
- emergency department
- blood pressure
- preterm infants
- physical activity
- type diabetes
- clinical trial
- metabolic syndrome
- open label
- adipose tissue
- double blind
- cardiovascular events
- body mass index
- acute coronary syndrome
- coronary artery disease
- high dose
- minimally invasive
- skeletal muscle
- weight gain
- deep learning
- percutaneous coronary intervention
- antiplatelet therapy
- atrial fibrillation