STOX1 deficiency is associated with renin-mediated gestational hypertension and placental defects
Jacqueline G. Parchem, … , Vincent H. Gattone II, Raghu Kalluri
Jacqueline G. Parchem, … , Vincent H. Gattone II, Raghu Kalluri
Published December 10, 2020
Citation Information: JCI Insight. 2021;6(2):e141588. https://doi.org/10.1172/jci.insight.141588.
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Research Article Cardiology Reproductive biology

STOX1 deficiency is associated with renin-mediated gestational hypertension and placental defects

Abstract

The pathogenesis of preeclampsia and other hypertensive disorders of pregnancy remains poorly defined despite the substantial burden of maternal and neonatal morbidity associated with these conditions. In particular, the role of genetic variants as determinants of disease susceptibility is understudied. Storkhead-box protein 1 (STOX1) was first identified as a preeclampsia risk gene through family-based genetic linkage studies in which loss-of-function variants were proposed to underlie increased preeclampsia susceptibility. We generated a genetic Stox1 loss-of-function mouse model (Stox1 KO) to evaluate whether STOX1 regulates blood pressure in pregnancy. Pregnant Stox1-KO mice developed gestational hypertension evidenced by a significant increase in blood pressure compared with WT by E17.5. While severe renal, placental, or fetal growth abnormalities were not observed, the Stox1-KO phenotype was associated with placental vascular and extracellular matrix abnormalities. Mechanistically, we found that gestational hypertension in Stox1-KO mice resulted from activation of the uteroplacental renin-angiotensin system. This mechanism was supported by showing that treatment of pregnant Stox1-KO mice with an angiotensin II receptor blocker rescued the phenotype. Our study demonstrates the utility of genetic mouse models for uncovering links between genetic variants and effector pathways implicated in the pathogenesis of hypertensive disorders of pregnancy.

Authors

Jacqueline G. Parchem, Keizo Kanasaki, Soo Bong Lee, Megumi Kanasaki, Joyce L. Yang, Yong Xu, Kadeshia M. Earl, Rachel A. Keuls, Vincent H. Gattone II, Raghu Kalluri

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Figure 4

Analysis of scRNA-Seq data from E9.5 mouse placenta shows coexpression of Stox1 with endothelial cell and SpA-TGC markers.

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Analysis of scRNA-Seq data from E9.5 mouse placenta shows coexpression o...
(A) Diagram showing 6 cell clusters defined in data set from Nelson et al. (38). (B) Overview of the number of variable features producing 6 cell populations obtained from the analyzed samples. (C) Scatter plot showing Stox1 expression in profiled single cells. Population of Stox1+ cells analyzed in D and E shown in red. (D) Selected cell population markers expressed in Stox1+ cells. Asterisks mark Kdr and Cd34, which were also markers of the novel Prdm1+ TGC population. (E) Expression of renin-angiotensin pathway members in Stox1+ cells. DEGs, differentially expressed genes; DS, decidual stroma; EC, endothelial cell; NK, natural killer; SpA-TGCs, spiral artery trophoblast giant cell; TGC, trophoblast giant cell. Data are normalized expression values: per cell (C), median ± IQR (D), or mean (E).