Mis-localization of endogenous TDP-43 leads to ALS-like early-stage metabolic dysfunction and progressive motor deficits

IF 14.9 1区医学 Q1 NEUROSCIENCES

Molecular Neurodegeneration Pub Date : 2024-06-20 DOI:10.1186/s13024-024-00735-7

Yiying Hu, Alexander Hruscha, Chenchen Pan, Martina Schifferer, Michael K. Schmidt, Brigitte Nuscher, Martin Giera, Sarantos Kostidis, Özge Burhan, Frauke van Bebber, Dieter Edbauer, Thomas Arzberger, Christian Haass, Bettina Schmid

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引用次数: 0

Abstract

The key pathological signature of ALS/ FTLD is the mis-localization of endogenous TDP-43 from the nucleus to the cytoplasm. However, TDP-43 gain of function in the cytoplasm is still poorly understood since TDP-43 animal models recapitulating mis-localization of endogenous TDP-43 from the nucleus to the cytoplasm are missing. CRISPR/Cas9 technology was used to generate a zebrafish line (called CytoTDP), that mis-locates endogenous TDP-43 from the nucleus to the cytoplasm. Phenotypic characterization of motor neurons and the neuromuscular junction was performed by immunostaining, microglia were immunohistochemically localized by whole-mount tissue clearing and muscle ultrastructure was analyzed by scanning electron microscopy. Behavior was investigated by video tracking and quantitative analysis of swimming parameters. RNA sequencing was used to identify mis-regulated pathways with validation by molecular analysis. CytoTDP fish have early larval phenotypes resembling clinical features of ALS such as progressive motor defects, neurodegeneration and muscle atrophy. Taking advantage of zebrafish’s embryonic development that solely relys on yolk usage until 5 days post fertilization, we demonstrated that microglia proliferation and activation in the hypothalamus is independent from food intake. By comparing CytoTDP to a previously generated TDP-43 knockout line, transcriptomic analyses revealed that mis-localization of endogenous TDP-43, rather than TDP-43 nuclear loss of function, leads to early onset metabolic dysfunction. The new TDP-43 model mimics the ALS/FTLD hallmark of progressive motor dysfunction. Our results suggest that functional deficits of the hypothalamus, the metabolic regulatory center, might be the primary cause of weight loss in ALS patients. Cytoplasmic gain of function of endogenous TDP-43 leads to metabolic dysfunction in vivo that are reminiscent of early ALS clinical non-motor metabolic alterations. Thus, the CytoTDP zebrafish model offers a unique opportunity to identify mis-regulated targets for therapeutic intervention early in disease progression.

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内源性 TDP-43 定位错误导致类似渐冻人症的早期代谢功能障碍和进行性运动障碍

ALS/FTLD的主要病理特征是内源性TDP-43从细胞核向细胞质的错误定位。然而，人们对TDP-43在细胞质中的功能增益仍然知之甚少，因为目前还没有再现内源性TDP-43从细胞核向细胞质错误定位的TDP-43动物模型。我们利用CRISPR/Cas9技术生成了一种斑马鱼品系（称为CytoTDP），它能将内源性TDP-43从细胞核错误定位到细胞质。运动神经元和神经肌肉接头的表型特征是通过免疫染色法进行的，小胶质细胞是通过全装组织清除法进行免疫组织化学定位的，肌肉的超微结构是通过扫描电子显微镜分析的。通过视频跟踪和游泳参数的定量分析对行为进行了研究。利用 RNA 测序来识别调控不当的通路，并通过分子分析进行验证。CytoTDP 鱼的早期幼体表型与渐冻症的临床特征相似，如进行性运动缺陷、神经变性和肌肉萎缩。斑马鱼的胚胎发育在受精后 5 天前完全依赖卵黄的使用，利用这一优势，我们证明了下丘脑中小胶质细胞的增殖和激活与食物摄入无关。通过将 CytoTDP 与之前产生的 TDP-43 基因敲除系进行比较，转录组分析表明，内源性 TDP-43 的错误定位，而不是 TDP-43 核功能缺失，导致了早发性代谢功能障碍。新的TDP-43模型模拟了渐进性运动功能障碍（ALS/FTLD）的特征。我们的研究结果表明，新陈代谢调节中枢下丘脑的功能障碍可能是导致 ALS 患者体重减轻的主要原因。内源性 TDP-43 的细胞质功能获得导致体内代谢功能障碍，这让人联想到 ALS 早期临床非运动性代谢改变。因此，CytoTDP 斑马鱼模型提供了一个独特的机会，可在疾病进展早期确定治疗干预的误调靶点。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Molecular Neurodegeneration 医学-神经科学

CiteScore

23.00

自引率

4.60%

发文量

审稿时长

6-12 weeks

期刊介绍： Molecular Neurodegeneration, an open-access, peer-reviewed journal, comprehensively covers neurodegeneration research at the molecular and cellular levels. Neurodegenerative diseases, such as Alzheimer's, Parkinson's, Huntington's, and prion diseases, fall under its purview. These disorders, often linked to advanced aging and characterized by varying degrees of dementia, pose a significant public health concern with the growing aging population. Recent strides in understanding the molecular and cellular mechanisms of these neurodegenerative disorders offer valuable insights into their pathogenesis.