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Disruption of GRIN2B Impairs Differentiation in Human Neurons.

Stem Cell Reports. 2018; 
Bell S, Maussion G, Jefri M, Peng H, Theroux JF, Silveira H, Soubannier V, Wu H, Hu P, Galat E, Torres-Platas SG, Boudreau-Pinsonneault C, O'Leary LA, Galat V, Turecki G, Durcan TM, Fon EA, Mechawar N, Ernst C.
Products/Services Used Details Operation
Recombinant Proteins Three days after the formation of EBs, a 70-mm Falcon cell strainer was used to collect aggregations, which were then re- suspended in a fresh low-bind/Petri dish in Neural Progenitor (NP) medium (DMEM/F12 supplemented with N2, B27 supple- ment, bFGF [20 ng/mL; GenScript], EGF [20 ng/mL; GenScript], Get A Quote

摘要

Heterozygous loss-of-function mutations in GRIN2B, a subunit of the NMDA receptor, cause intellectual disability and language impairment. We developed clonal models of GRIN2B deletion and loss-of-function mutations in a region coding for the glutamate binding domain in human cells and generated neurons from a patient harboring a missense mutation in the same domain. Transcriptome analysis revealed extensive increases in genes associated with cell proliferation and decreases in genes associated with neuron differentiation, a result supported by extensive protein analyses. Using electrophysiology and calcium imaging, we demonstrate that NMDA receptors are present on neural progenitor cells and that human mutation... More

关键词

CRISPR; CRISPR-Cas9; GRIN2B; NMDA; NMDAR2B; NPCs; glutamate; iPSCs; neural stem cell; neurodevelopment