Recurrent pregnancy loss is associated with a pro-senescent decidual response during the peri-implantation window.
Emma S LucasPavle VrljicakJoanne MuterMaria M Diniz-da-CostaPaul J BrightonChow-Seng KongJulia LipeckiKatherine J FishwickJoshua OdendaalLauren Jade EwingtonSiobhan QuenbySascha OttJan Joris BrosensPublished in: Communications biology (2020)
During the implantation window, the endometrium becomes poised to transition to a pregnant state, a process driven by differentiation of stromal cells into decidual cells (DC). Perturbations in this process, termed decidualization, leads to breakdown of the feto-maternal interface and miscarriage, but the underlying mechanisms are poorly understood. Here, we reconstructed the decidual pathway at single-cell level in vitro and demonstrate that stromal cells first mount an acute stress response before emerging as DC or senescent DC (snDC). In the absence of immune cell-mediated clearance of snDC, secondary senescence transforms DC into progesterone-resistant cells that abundantly express extracellular matrix remodelling factors. Additional single-cell analysis of midluteal endometrium identified DIO2 and SCARA5 as marker genes of a diverging decidual response in vivo. Finally, we report a conspicuous link between a pro-senescent decidual response in peri-implantation endometrium and recurrent pregnancy loss, suggesting that pre-pregnancy screening and intervention may reduce the burden of miscarriage.
Keyphrases
- single cell
- extracellular matrix
- induced apoptosis
- dendritic cells
- pregnancy outcomes
- preterm birth
- cell cycle arrest
- rna seq
- randomized controlled trial
- pregnant women
- liver failure
- oxidative stress
- endothelial cells
- endoplasmic reticulum stress
- gene expression
- signaling pathway
- respiratory failure
- stress induced
- hepatitis b virus
- dna methylation
- extracorporeal membrane oxygenation
- transcription factor
- physical activity
- body mass index
- risk factors