| Literature DB >> 31465303 |
Giovanni A Carosso1,2, Leandros Boukas1,2,3, Jonathan J Augustin2,4,5, Ha Nam Nguyen6, Briana L Winer2, Gabrielle H Cannon2, Johanna D Robertson2, Li Zhang2, Kasper D Hansen2,3, Loyal A Goff2,5, Hans T Bjornsson2,7,8,9.
Abstract
Chromatin modifiers act to coordinate gene expression changes critical to neuronal differentiation from neural stem/progenitor cells (NSPCs). Lysine-specific methyltransferase 2D (KMT2D) encodes a histone methyltransferase that promotes transcriptional activation and is frequently mutated in cancers and in the majority (>70%) of patients diagnosed with the congenital, multisystem intellectual disability disorder Kabuki syndrome 1 (KS1). Critical roles for KMT2D are established in various non-neural tissues, but the effects of KMT2D loss in brain cell development have not been described. We conducted parallel studies of proliferation, differentiation, transcription, and chromatin profiling in KMT2D-deficient human and mouse models to define KMT2D-regulated functions in neurodevelopmental contexts, including adult-born hippocampal NSPCs in vivo and in vitro. We report cell-autonomous defects in proliferation, cell cycle, and survival, accompanied by early NSPC maturation in several KMT2D-deficient model systems. Transcriptional suppression in KMT2D-deficient cells indicated strong perturbation of hypoxia-responsive metabolism pathways. Functional experiments confirmed abnormalities of cellular hypoxia responses in KMT2D-deficient neural cells and accelerated NSPC maturation in vivo. Together, our findings support a model in which loss of KMT2D function suppresses expression of oxygen-responsive gene programs important to neural progenitor maintenance, resulting in precocious neuronal differentiation in a mouse model of KS1.Entities:
Keywords: Adult stem cells; Epigenetics; Genetics; Neurological disorders; Neuroscience
Year: 2019 PMID: 31465303 PMCID: PMC6824316 DOI: 10.1172/jci.insight.129375
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708