Abstract
Despite significant maternal and fetal morbidity, a treatment for preeclampsia currently remains an unmet need in clinical care. As too does the lifelong cardiovascular risks imparted on preeclampsia sufferers. Endothelial dysfunction and end-organ injury are synonymous with both preeclampsia and cardiovascular disease, including heart failure. We propose that beta-blockers, known to improve endothelial dysfunction in the treatment of cardiovascular disease, and specifically known to reduce mortality in the treatment of heart failure, may be beneficial in the treatment of preeclampsia. Here, we assessed whether the beta-blockers carvedilol, bisoprolol, and metoprolol could quench the release of anti-angiogenic factors, promote production of pro-angiogenic factors, reduce markers of inflammation, and reduce endothelial dysfunction using our in vitro pre-clinical preeclampsia models encompassing primary placental tissue and endothelial cells. Here, we show beta-blockers effected a modest reduction in secretion of anti-angiogenic soluble fms-like tyrosine kinase-1 and soluble endoglin and increased expression of pro-angiogenic placental growth factor, vascular endothelial growth factor and adrenomedullin in endothelial cells. Beta-blocker treatment mitigated inflammatory changes occurring after endothelial dysfunction and promoted cytoprotective antioxidant heme oxygenase-1. The positive effects of the beta-blockers were predominantly seen in endothelial cells, with a less consistent response seen in placental cells/tissue. In conclusion, beta-blockers show potential as a novel therapeutic approach in the treatment of preeclampsia and warrant further investigation.
Highlights
We report that beta-blockers that successfully reduce mortality in heart failure, exert effects consistent with a reduction in endothelial dysfunction in models of preeclampsia
While beta-blockers have exhibited a positive effect on endothelial dysfunction in a cardiovascular disease setting, the actions of beta-blockers in gestational tissues presents novel findings
Most therapeutics being investigated for the treatment of preeclampsia are concerned with lowering excessive placental secretion of anti-angiogenic factors sFlt-1 and soluble endoglin (sENG)
Summary
A medical treatment that is safe in pregnancy, able to restore the angiogenic balance, improve endothelial function, and reduce inflammation, would likely prevent serious, long term damage to the maternal endothelium, and would represent a significant therapeutic advance. While currently labetalol is the only beta-blocker used in the treatment of preeclampsia as an anti-hypertensive agent [51], in general many beta-blockers are considered safe in pregnancy based on their use in pregnant patients with cardiovascular disease [52]. The exception to this is atenolol, which is contraindicated given its association with small-for-gestational-age infants [52,53]. We set out to evaluate the effects of carvedilol, bisoprolol, and metoprolol on the secretion of pro- and anti-angiogenic and inflammatory factors central to preeclampsia pathogenesis from placental and endothelial cells in vitro
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