Litcius/Paper detail

SALL3 mediates the loss of neuroectodermal differentiation potential in human embryonic stem cells with chromosome 18q loss

Yingnan Lei, Diana Al Delbany, Nuša Krivec, Marius Regin, Edouard Couvreu de Deckersberg, Charlotte Janssens, Manjusha Ghosh, Karen Sermon, Claudia Spits

2024Stem Cell Reports13 citationsDOIOpen Access PDF

Abstract

Human pluripotent stem cell (hPSC) cultures are prone to genetic drift, because cells that have acquired specific genetic abnormalities experience a selective advantage in vitro. These abnormalities are highly recurrent in hPSC lines worldwide, but their functional consequences in differentiating cells are scarcely described. In this work, we show that the loss of chromosome 18q impairs neuroectoderm commitment and that downregulation of SALL3, a gene located in the common 18q loss region, is responsible for this failed neuroectodermal differentiation. Knockdown of SALL3 in control lines impaired differentiation in a manner similar to the loss of 18q, and transgenic overexpression of SALL3 in hESCs with 18q loss rescued the differentiation capacity of the cells. Finally, we show that loss of 18q and downregulation of SALL3 leads to changes in the expression of genes involved in pathways regulating pluripotency and differentiation, suggesting that these cells are in an altered state of pluripotency.

Topics & Concepts

BiologyNeuroectodermEmbryonic stem cellGene knockdownInduced pluripotent stem cellDownregulation and upregulationCellular differentiationCell biologyStem cellGeneticsMolecular biologyCell cultureGeneMesodermRenal and related cancersPluripotent Stem Cells ResearchCRISPR and Genetic Engineering
SALL3 mediates the loss of neuroectodermal differentiation potential in human embryonic stem cells with chromosome 18q loss | Litcius