Gu Xiaofeng, Li Chenjian, Wei Weizheng, Lo Victor, Gong Shiaoching, Li Shi-Hua, Iwasato Takuji, Itohara Shigeyoshi, Li Xiao-Jiang, Mody Istvan, Heintz Nathaniel, Yang X William
Center for Neurobehavioral Genetics, Neuropsychiatric Institute, Department of Psychiatry, David Geffen School of Medicine at UCLA, Los Angeles, California 90095, USA.
Neuron. 2005 May 5;46(3):433-44. doi: 10.1016/j.neuron.2005.03.025.
Expanded polyglutamine (polyQ) proteins in Huntington's disease (HD) as well as other polyQ disorders are known to elicit a variety of intracellular toxicities, but it remains unclear whether polyQ proteins can elicit pathological cell-cell interactions which are critical to disease pathogenesis. To test this possibility, we have created conditional HD mice expressing a neuropathogenic form of mutant huntingtin (mhtt-exon1) in discrete neuronal populations. We show that mhtt aggregation is a cell-autonomous process. However, progressive motor deficits and cortical neuropathology are only observed when mhtt expression is in multiple neuronal types, including cortical interneurons, but not when mhtt expression is restricted to cortical pyramidal neurons. We further demonstrate an early deficit in cortical inhibition, suggesting that pathological interactions between interneurons and pyramidal neurons may contribute to the cortical manifestation of HD. Our study provides genetic evidence that pathological cell-cell interactions elicited by neuropathogenic forms of mhtt can critically contribute to cortical pathogenesis in a HD mouse model.
亨廷顿舞蹈病(HD)以及其他多聚谷氨酰胺疾病中的扩展型多聚谷氨酰胺(polyQ)蛋白已知会引发多种细胞内毒性,但尚不清楚polyQ蛋白是否能引发对疾病发病机制至关重要的病理性细胞间相互作用。为了检验这种可能性,我们构建了条件性HD小鼠,在离散的神经元群体中表达突变型亨廷顿蛋白(mhtt-exon1)的神经致病形式。我们发现mhtt聚集是一个细胞自主过程。然而,只有当mhtt在包括皮质中间神经元在内的多种神经元类型中表达时,才会观察到进行性运动缺陷和皮质神经病理学变化,而当mhtt表达仅限于皮质锥体神经元时则不会出现。我们进一步证明了皮质抑制的早期缺陷,这表明中间神经元和锥体神经元之间的病理性相互作用可能导致HD的皮质表现。我们的研究提供了遗传学证据,表明mhtt的神经致病形式引发的病理性细胞间相互作用可在HD小鼠模型中对皮质发病机制起到关键作用。
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