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      PARK7 regulates inflammation-induced pro-labour mediators in myometrial and amnion cells.

      1 , 2 , 1 , 2 , 3 , 2
      Reproduction (Cambridge, England)
      Bioscientifica

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          Abstract

          Preterm birth is a prevalent cause of neonatal deaths worldwide. Inflammation has been implicated in spontaneous preterm birth involved in the processes of uterine contractility and membrane rupture. Parkinson protein 7 (PARK7) has been found to play an inflammatory role in non-gestational tissues. The aims of this study were to determine the expression of PARK7 in myometrium and fetal membranes with respect to term labour onset and to elucidate the effect of PARK7 silencing in primary myometrium and amnion cells on pro-inflammatory and pro-labour mediators. PARK7 mRNA expression was higher in term myometrium and fetal membranes from women in labour compared to non-labouring samples and in amnion from preterm deliveries with chorioamnionitis. In human primary myometrial cells transfected with PARK7 siRNA (siPARK7), there was a significant decrease in IL1B, TNF, fsl-1 and poly(I:C)-induced expression of pro-inflammatory cytokine IL6, chemokines (CXCL8, CCL2), adhesion molecule ICAM1, prostaglandin PGF2α and its receptor PTGFR. Similarly, amnion cells transfected with siPARK7 displayed a decrease in IL1B-induced expression of IL6, CXCL8 and ICAM1. In myometrial cells transfected with siPARK7, there was a significant reduction of NF-κB RELA transcriptional activity when stimulated with fsl-1, flagellin and poly(I:C), but not with IL1B or TNF. Collectively, our novel data describe a role for PARK7 in regulating inflammation-induced pro-inflammatory and pro-labour mediators in human myometrial and amnion cells.

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          Author and article information

          Journal
          Reproduction
          Reproduction (Cambridge, England)
          Bioscientifica
          1741-7899
          1470-1626
          February 2018
          : 155
          : 2
          Affiliations
          [1 ] Obstetrics, Nutrition and Endocrinology Group, Department of Obstetrics and Gynaecology, University of MelbourneMelbourne, Victoria, Australia.
          [2 ] Mercy Perinatal Research CentreMercy Hospital for Women, Heidelberg, Victoria, Australia.
          [3 ] Obstetrics, Nutrition and Endocrinology Group, Department of Obstetrics and Gynaecology, University of MelbourneMelbourne, Victoria, Australia mlappas@unimelb.edu.au.
          Article
          155/2/207
          10.1530/REP-17-0604
          29358306
          ba911b68-5a36-4497-b094-dcb9eaecede3
          © 2018 Society for Reproduction and Fertility.
          History

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