Abstract

Preeclampsia (PE) is characterized by new onset hypertension and increased uterine artery resistance (UARI), elevated TNF-α, sFlt-1, and decreased of nitric oxide (NO) bioavailability during pregnancy. 17-hydroxyprogesterone caproate (17-OHPC) is approved for cessation of preterm labor in pregnancies not complicated by PE. Therefore, we hypothesized that 17-OHPC administered on day 15 of gestation into RUPP rats could reduce blood pressure (MAP), TNF-α, sFlt-1, UARI, and increase pup weight and NO bioavailability. Carotid catheters were inserted on day 18. MAP, blood and tissues were collected on day 19. MAP in normal pregnant (NP) rats (n=9) was 92 +1.35, 126 +1.98 in RUPP rats (n=17) and 111+1.54 mmHg in RUPP+17-OHPC (n=13), p <0.05. Pup weight was 2.31+0.12 in NP (n=13), 1.88+ 0.05 in RUPP rats (n=24), which improved to 2.01+0.07 grams in RUPP+17-OHPC (n=15), p <0.05. UARI was 0.79+0.03 in RUPP rats (n=4) and 0.59+0.04 in RUPP+17-OHPC (n=5), p<0.05. Plasma levels of TNFα, sFlt1 were 64.0+14.1, 385.9+141 in RUPP rats (n=7), which were blunted to 17.8+9.6, 110.2+11.1 pg/mL in RUPP+17OHPC (n=5), p<0.05. Plasma NOx was 10.82+2.3 in RUPP rats (n=13) but was improved to 25.5+5.2 µM in RUPP+17-OHPC (n=5), p<0.05. In conclusion, early administration of 17-OHPC improves TNF-α, sFtl-1, UARI, hypertension, pup weight and nitric oxide bioavailability in response to placental ischemia and should be considered for addition to the management of severe preterm PE. NIH RO1HD067541, T32HL105324

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