Roslyn and Leslie Goldstein Laboratory for Stem Cell Biology and Regenerative Medicine.
Institute for Brain Disorders and Neural Regeneration.
J Neurosci. 2019 Mar 6;39(10):1892-1909. doi: 10.1523/JNEUROSCI.2443-18.2018. Epub 2019 Jan 9.
Emerging studies are providing compelling evidence that the pathogenesis of Huntington's disease (HD), a neurodegenerative disorder with frequent midlife onset, encompasses developmental components. Moreover, our previous studies using a hypomorphic model targeting huntingtin during the neurodevelopmental period indicated that loss-of-function mechanisms account for this pathogenic developmental component (Arteaga-Bracho et al., 2016). In the present study, we specifically ascertained the roles of subpallial lineage species in eliciting the previously observed HD-like phenotypes. Accordingly, we used the Cre-loxP system to conditionally ablate the murine huntingtin gene (Htt) in cells expressing the subpallial patterning markers Gsx2 (Gsx2-Cre) or Nkx2.1 (Nkx2.1-Cre) in Htt mice of both sexes. These genetic manipulations elicited anxiety-like behaviors, hyperkinetic locomotion, age-dependent motor deficits, and weight loss in both Htt;Gsx2-Cre and Htt;Nkx2.1-Cre mice. In addition, these strains displayed unique but complementary spatial patterns of basal ganglia degeneration that are strikingly reminiscent of those seen in human cases of HD. Furthermore, we observed early deficits of somatostatin-positive and Reelin-positive interneurons in both Htt subpallial null strains, as well as early increases of cholinergic interneurons, Foxp2 arkypallidal neurons, and incipient deficits with age-dependent loss of parvalbumin-positive neurons in Htt;Nkx2.1-Cre mice. Overall, our findings indicate that selective loss-of-huntingtin function in subpallial lineages differentially disrupts the number, complement, and survival of forebrain interneurons and globus pallidus GABAergic neurons, thereby leading to the development of key neurological hallmarks of HD during adult life. Our findings have important implications for the establishment and deployment of neural circuitries and the integrity of network reserve in health and disease. Huntington's disease (HD) is a progressive degenerative disorder caused by aberrant trinucleotide expansion in the gene. Mechanistically, this mutation involves both loss- and gain-of-function mechanisms affecting a broad array of cellular and molecular processes. Although huntingtin is widely expressed during adult life, the mutant protein only causes the demise of selective neuronal subtypes. The mechanisms accounting for this differential vulnerability remain elusive. In this study, we have demonstrated that loss-of-huntingtin function in subpallial lineages not only differentially disrupts distinct interneuron species early in life, but also leads to a pattern of neurological deficits that are reminiscent of HD. This work suggests that early disruption of selective neuronal subtypes may account for the profiles of enhanced regional cellular vulnerability to death in HD.
新兴研究提供了令人信服的证据,表明亨廷顿病(HD)的发病机制包含发育成分,HD 是一种具有频繁中年发病的神经退行性疾病。此外,我们之前使用神经发育期间靶向亨廷顿蛋白的低功能模型进行的研究表明,失能机制解释了这种致病的发育成分(Arteaga-Bracho 等人,2016 年)。在本研究中,我们特别确定了亚皮质谱系物种在引发先前观察到的 HD 样表型中的作用。因此,我们使用 Cre-loxP 系统在雄性和雌性 Htt 小鼠中表达亚皮质模式标记物 Gsx2(Gsx2-Cre)或 Nkx2.1(Nkx2.1-Cre)的细胞中条件性缺失小鼠的 huntingtin 基因(Htt)。这些遗传操作在 Htt;Gsx2-Cre 和 Htt;Nkx2.1-Cre 小鼠中引起焦虑样行为、多动运动、与年龄相关的运动缺陷和体重减轻。此外,这些品系显示出独特但互补的基底神经节退化的空间模式,这些模式与人类 HD 病例中观察到的模式非常相似。此外,我们观察到两种 Htt 亚皮质缺失品系中生长抑素阳性和 Reelin 阳性中间神经元的早期缺陷,以及在 Htt;Nkx2.1-Cre 小鼠中,早期增加胆碱能中间神经元、Foxp2 arkypallidal 神经元以及与年龄相关的缺失与年龄相关的失活伴随着年龄相关的缺失。总体而言,我们的研究结果表明,亚皮质谱系中选择性亨廷顿蛋白功能丧失会导致前脑中间神经元和苍白球 GABA 能神经元数量、互补性和存活率的差异破坏,从而导致成年期 HD 的关键神经标志的发展。我们的研究结果对于健康和疾病中的神经回路的建立和部署以及网络储备的完整性具有重要意义。亨廷顿病(HD)是一种由基因中三核苷酸扩展引起的进行性退行性疾病。从机制上讲,这种突变涉及失能和获得功能机制,影响广泛的细胞和分子过程。尽管亨廷顿蛋白在成年期广泛表达,但突变蛋白仅导致选择性神经元亚型的死亡。导致这种差异易感性的机制仍不清楚。在这项研究中,我们已经证明,亚皮质谱系中亨廷顿蛋白功能的丧失不仅在生命早期会导致不同的中间神经元物种发生差异破坏,而且还会导致类似于 HD 的神经缺陷模式。这项工作表明,选择性神经元亚型的早期破坏可能解释了 HD 中增强的区域细胞死亡易感性的特征。
