News Release

Mouse model provides new insight in to preeclampsia

Peer-Reviewed Publication

JCI Journals

Worldwide, preeclampsia is a leading cause of maternal deaths and preterm births. This serious pregnancy complication results in extremely high blood pressure and organ damage. The onset of preeclampsia is associated with elevated levels of a secreted protein, sFLT1, in maternal blood. However, the factors that regulate sFLT1 production are poorly understood. A new study in the Journal of Clinical Investigation suggests that placental cells produce sFLT1 in response to maternal increases in VEGF, which binds sFLT1 and affects blood vessel formation and function. Nihar Nayak and colleagues at Wayne State University evaluated tissue samples from women with preeclampsia and determined that VEGF is increased in maternal cells and sFLT1 is increased in placental cells. In a mouse model, enhanced VEGF expression in maternal cells induced expression of placental sFLT1. Moreover, maternal VEGF expression induced preeclampsia-like symptoms and pregnancy loss in these mice. The results from this study suggest that alterations in VEGF and sFLT1 levels during pregnancy could have serious consequences and that caution should be used for use of therapies targeting these proteins for treating preeclampsia.



Endometrial VEGF induces placental sFLT1 and leads to pregnancy complications


Nihar Nayak
Wayne State University School of Medicine, Detroit, MI, USA
Phone: 313-577-8910; E-mail:

View this article at:


sFLT1 in preeclampsia: trophoblast defense against a decidual VEGFA barrage?


S Lee Adamson
Samuel Lunenfeld Research Institute, Toronto, ON, CAN
Phone 1: 416-586-8377

View this article at:

Disclaimer: AAAS and EurekAlert! are not responsible for the accuracy of news releases posted to EurekAlert! by contributing institutions or for the use of any information through the EurekAlert system.