| Literature DB >> 32320667 |
Ke Zhang1, Fang Yu1, Jian Zhu2, Sue Han3, Jiehui Chen1, Xuanyuan Wu4, Yingying Chen1, Tingyu Shen3, Jiaoyang Liao1, Wenke Guo1, Xianfa Yang5, Ran Wang1, Yun Qian1, Jiaxin Yang2, Leping Cheng6, Yun Zhao1, Chi-Chung Hui7, Jinsong Li1, Guangdun Peng8, Shuijin He9, Naihe Jing10, Ke Tang11.
Abstract
Recent studies have revealed an essential role for embryonic cortical development in the pathophysiology of neurodevelopmental disorders, including autism spectrum disorder (ASD). However, the genetic basis and underlying mechanisms remain unclear. Here, we generate mutant human embryonic stem cell lines (Mut hESCs) carrying an NR2F1-R112K mutation that has been identified in a patient with ASD features and investigate their neurodevelopmental alterations. Mut hESCs overproduce ventral telencephalic neuron progenitors (ventral NPCs) and underproduce dorsal NPCs, causing the imbalance of excitatory/inhibitory neurons. These alterations can be mainly attributed to the aberrantly activated Hedgehog signaling pathway. Moreover, the corresponding Nr2f1 point-mutant mice display a similar excitatory/inhibitory neuron imbalance and abnormal behaviors. Antagonizing the increased inhibitory synaptic transmission partially alleviates their behavioral deficits. Together, our results suggest that the NR2F1-dependent imbalance of excitatory/inhibitory neuron differentiation caused by the activated Hedgehog pathway is one precursor of neurodevelopmental disorders and may enlighten the therapeutic approaches.Entities:
Keywords: E/I imbalance; Hedgehog signaling pathway; NR2F1; autism spectrum disorders; dorsal neuron progenitor cell; excitatory neuron; inhibitory neuron; neurodevelopmental disorders; ventral neuron progenitor cell
Mesh:
Substances:
Year: 2020 PMID: 32320667 DOI: 10.1016/j.celrep.2020.03.085
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423