Cx43 regulates mechanotransduction mechanisms in human preterm amniotic membrane defects

Author:

Costa Eleni1,Thrasivoulou Christopher2,Becker David L.3,Deprest Jan A.45ORCID,David Anna L.45ORCID,Chowdhury Tina T.1ORCID

Affiliation:

1. Centre for Bioengineering School of Engineering and Materials Science Queen Mary University of London London UK

2. Department of Cell and Developmental Biology University College London London UK

3. Lee Kong Chian School of Medicine Nanyang Technological University Singapore Singapore

4. Department of Obstetrics and Gynaecology University Hospitals Leuven Leuven Belgium

5. Elizabeth Garrett Anderson Institute for Women's Health University College London Medical School Building London UK

Abstract

AbstractObjectiveThe effects of mechanical stimulation in preterm amniotic membrane (AM) defects were explored.MethodsPreterm AM was collected from women undergoing planned preterm caesarean section (CS) due to fetal growth restriction or emergency CS after spontaneous preterm prelabour rupture of the membranes (sPPROM). AM explants near the cervix or placenta were subjected to trauma and/or mechanical stimulation with the Cx43 antisense. Markers for nuclear morphology (DAPI), myofibroblasts (αSMA), migration (Cx43), inflammation (PGE2) and repair (collagen, elastin and transforming growth factor β [TGFβ1]) were examined by confocal microscopy, second harmonic generation, qPCR and biochemical assays.ResultsIn preterm AM defects, myofibroblast nuclei were highly deformed and contractile and expressed αSMA and Cx43. Mechanical stimulation increased collagen fibre polarisation and the effects on matrix markers were dependent on tissue region, disease state, gestational age and the number of fetuses. PGE2 levels were broadly similar but reduced after co‐treatment with Cx43 antisense in late sPPROM AM defects. TGFβ1 and Cx43 gene expression were significantly increased after trauma and mechanical stimulation but this response dependent on gestational age.ConclusionMechanical stimulation affects Cx43 signalling and cell/collagen mechanics in preterm AM defects. Establishing how Cx43 regulates mechanosignalling could be an approach to repair tissue integrity after trauma.

Funder

Great Ormond Street Hospital for Children

Rosetrees Trust

Publisher

Wiley

Subject

Genetics (clinical),Obstetrics and Gynecology

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