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NOTCH3 signalling controls human trophoblast stem cell expansion and differentiation

Bianca Dietrich, Victoria Kunihs, Andreas Ian Lackner, Gudrun Meinhardt, Bon‐Kyoung Koo, Jürgen Pollheimer, Sandra Haider, Martin Knöfler

2023Development22 citationsDOIOpen Access PDF

Abstract

Failures in growth and differentiation of the early human placenta are associated with severe pregnancy disorders such as pre-eclampsia and fetal growth restriction. However, regulatory mechanisms controlling development of placental epithelial cells, the trophoblasts, remain poorly elucidated. Using trophoblast stem cells (TSCs), trophoblast organoids (TB-ORGs) and primary cytotrophoblasts (CTBs) of early pregnancy, we herein show that autocrine NOTCH3 signalling controls human placental expansion and differentiation. The NOTCH3 receptor was specifically expressed in proliferative CTB progenitors and its active form, the nuclear NOTCH3 intracellular domain (NOTCH3-ICD), interacted with the transcriptional co-activator mastermind-like 1 (MAML1). Doxycycline-inducible expression of dominant-negative MAML1 in TSC lines provoked cell fusion and upregulation of genes specific for multinucleated syncytiotrophoblasts, which are the differentiated hormone-producing cells of the placenta. However, progenitor expansion and markers of trophoblast stemness and proliferation were suppressed. Accordingly, inhibition of NOTCH3 signalling diminished growth of TB-ORGs, whereas overexpression of NOTCH3-ICD in primary CTBs and TSCs showed opposite effects. In conclusion, the data suggest that canonical NOTCH3 signalling plays a key role in human placental development by promoting self-renewal of CTB progenitors.

Topics & Concepts

BiologyTrophoblastCell biologyProgenitor cellCytotrophoblastSyncytiotrophoblastStem cellPlacentationSyncytiotrophoblastsCellular differentiationImmunologyCTBSPlacentaReceptorGeneticsFetusGeneSynaptic plasticityMetaplasticityPregnancyPregnancy and preeclampsia studiesRenal and related cancersReproductive System and Pregnancy
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