自闭症相关基因胰岛大脑 2 缺失的小鼠的行为和小脑传递缺陷。
Behavioral and cerebellar transmission deficits in mice lacking the autism-linked gene islet brain-2.
机构信息
Department of Biological Sciences, Hunter College, City University of New York, New York, New York 10065, USA.
出版信息
J Neurosci. 2010 Nov 3;30(44):14805-16. doi: 10.1523/JNEUROSCI.1161-10.2010.
Abstract
Deletion of the human SHANK3 gene near the terminus of chromosome 22q is associated with Phelan-McDermid syndrome and autism spectrum disorders. Nearly all such deletions also span the tightly linked IB2 gene. We show here that IB2 protein is broadly expressed in the brain and is highly enriched within postsynaptic densities. Experimental disruption of the IB2 gene in mice reduces AMPA and enhances NMDA receptor-mediated glutamatergic transmission in cerebellum, changes the morphology of Purkinje cell dendritic arbors, and induces motor and cognitive deficits suggesting an autism phenotype. These findings support a role for human IB2 mutation as a contributing genetic factor in Chr22qter-associated cognitive disorders.
摘要
人类 SHANK3 基因在染色体 22q 末端附近的缺失与 Phelan-McDermid 综合征和自闭症谱系障碍有关。几乎所有此类缺失也跨越紧密连锁的 IB2 基因。我们在这里表明,IB2 蛋白在大脑中广泛表达,并在突触后密度内高度富集。在小鼠中实验性破坏 IB2 基因可减少 AMPA 并增强小脑内 NMDA 受体介导的谷氨酸能传递,改变浦肯野细胞树突状分支的形态,并引起运动和认知缺陷,提示自闭症表型。这些发现支持人类 IB2 突变作为 Chr22qter 相关认知障碍的遗传因素的作用。
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