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D1R- and D2R-Medium-Sized Spiny Neurons Diversity: Insights Into Striatal Vulnerability to Huntington’s Disease Mutation

机译:D1R和D2R-中等大小的刺神经元多样性:对亨廷顿疾病突变的威胁脆弱性洞察

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摘要

Huntington’s disease (HD) is a devastating neurodegenerative disorder caused by an aberrant expansion of the CAG tract within the exon 1 of the HD gene, HTT. HD progressively impairs motor and cognitive capabilities, leading to a total loss of autonomy and ultimate death. Currently, no cure or effective treatment is available to halt the disease. Although the HTT gene is ubiquitously expressed, the striatum appears to be the most susceptible district to the HD mutation with Medium-sized Spiny Neurons (MSNs) (D1R and D2R) representing 95% of the striatal neuronal population. Why are striatal MSNs so vulnerable to the HD mutation? Particularly, why do D1R- and D2R-MSNs display different susceptibility to HD? Here, we highlight significant differences between D1R- and D2R-MSNs subpopulations, such as morphology, electrophysiology, transcriptomic, functionality, and localization in the striatum. We discuss possible reasons for their selective degeneration in the context of HD. Our review suggests that a better understanding of cell type-specific gene expression dysregulation within the striatum might reveal new paths to therapeutic intervention or prevention to ameliorate HD patients’ life expectancy.
机译:亨廷顿病(HD)是引起CAG道的HD基因,HTT的外显子1中的异常膨胀破坏性神经退行性病症。 HD逐步损害运动和认知能力,导致自主性和最终死亡的总损失。目前,还没有治愈或有效的治疗方法,以阻止疾病。虽然HTT基因广泛表达,纹状体似乎是最容易区与中型棘神经元(MSN中)(D1R和D2R)表示纹状体神经元群的95%的HD突变。为什么纹状体的MSN如此脆弱的HD突变?特别是,为什么D1R-和D2R-的MSN显示不同的易感性HD?在这里,我们强调D1R-和D2R-的MSN亚群之间的显著差异,如形态,电生理,转录组学,功能和定位在纹状体。我们讨论了在HD的情况下他们选择变性的可能原因。我们的审查表明,纹状体内更好地了解细胞类型特异性基因表达的失调可能揭示干预治疗或预防改善HD患者的预期寿命的新路径。

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