AI Article Synopsis

  • RKIP plays a crucial role in regulating signaling pathways related to placental development and cytotrophoblast differentiation, impacting normal and preeclamptic placentas.
  • RKIP expression is observed in both normal and preeclamptic placentas, with a shift from villous to syncytiotrophoblast in preeclampsia.
  • In vitro studies reveal that inhibiting RKIP disrupts cell motility and alters signaling pathways, indicating its importance in the function of cytotrophoblast cells.

Article Abstract

Raf kinase inhibitor protein (RKIP) regulates growth and differentiation signaling of mitogen-activated protein kinases (MAPK), GRK2 and NF-kappaB pathways each of which regulates cytotrophoblast differentiation and normal placental development. We show here that RKIP is expressed in human normal and preeclampic placentas as detected by immunostaining. RKIP was detected in villous cytotrophoblast in normal placenta and switched to syncytiotrophoblast in pre-eclampsia (PE)-complicated pregnancies. RKIP was also localized in extravillous cytotrophoblast of cell islands and cell columns both in normal and in PE placentas, although staining was less uniform in the latter specimens. In order to test RKIP involvement in cytotrophoblast function, we performed in vitro studies on HTR-8/SVneo cells, a first trimester cytotrophoblast cell line. We show that the RKIP inhibitor locostatin reduces ERK phosphorylation and impairs HTR-8/SV neo cells motility in wound closure experiments. We also document the presence of GRK2 mRNA, the reduction of phosphorylated RKIP expression by locostatin and the induction of PAI mRNA expression in HTR-8/SV neo cells, suggesting the involvement of GRK2 and NF-kappaB pathways in these cells. In conclusion, our work provides evidence that RKIP is a novel factor expressed in cytotrophoblast cells where it likely regulates cell migration.

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Source
http://dx.doi.org/10.1002/jcp.22907DOI Listing

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