A NSC-34 cell line-derived spheroid model: Potential and challenges for in vitro evaluation of neurodegeneration.

IF 2 3区 工程技术 Q2 ANATOMY & MORPHOLOGY Microscopy Research and Technique Pub Date : 2024-07-11 DOI:10.1002/jemt.24651
Pietro Arnaldi, Elena Casarotto, Michela Relucenti, Grazia Bellese, Maria Cristina Gagliani, Valeria Crippa, Patrizio Castagnola, Katia Cortese
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Abstract

Three-dimensional (3D) spheroid models aim to bridge the gap between traditional two-dimensional (2D) cultures and the complex in vivo tissue environment. These models, created by self-clustering cells to mimic a 3D environment with surrounding extracellular framework, provide a valuable research tool. The NSC-34 cell line, generated by fusing mouse spinal cord motor neurons and neuroblastoma cells, is essential for studying neurodegenerative diseases like amyotrophic lateral sclerosis (ALS), where abnormal protein accumulation, such as TAR-DNA-binding protein 43 (TDP-43), occurs in affected nerve cells. However, NSC-34 behavior in a 3D context remains underexplored, and this study represents the first attempt to create a 3D model to determine its suitability for studying pathology. We generated NSC-34 spheroids using a nonadhesive hydrogel-based template and characterized them for 6 days. Light microscopy revealed that NSC-34 cells in 3D maintained high viability, a distinct round shape, and forming stable membrane connections. Scanning electron microscopy identified multiple tunnel-like structures, while ultrastructural analysis highlighted nuclear bending and mitochondria alterations. Using inducible GFP-TDP-43-expressing NSC-34 spheroids, we explored whether 3D structure affected TDP-43 expression, localization, and aggregation. Spheroids displayed nuclear GFP-TDP-43 expression, albeit at a reduced level compared with 2D cultures and generated both TDP-35 fragments and TDP-43 aggregates. This study sheds light on the distinctive behavior of NSC-34 in 3D culture, suggesting caution in the use of the 3D model for ALS or TDP-43 pathologies. Yet, it underscores the spheroids' potential for investigating fundamental cellular mechanisms, cell adaptation in a 3D context, future bioreactor applications, and drug penetration studies. RESEARCH HIGHLIGHTS: 3D spheroid generation: NSC-34 spheroids, developed using a hydrogel-based template, showed high viability and distinct shapes for 6 days. Structural features: advanced microscopy identified tunnel-like structures and nuclear and mitochondrial changes in the spheroids. Protein dynamics: the study observed how 3D structures impact TDP-43 behavior, with altered expression but similar aggregation patterns to 2D cultures. Research implications: this study reveals the unique behavior of NSC-34 in 3D culture, suggests a careful approach to use this model for ALS or TDP-43 pathologies, and highlights its potential in cellular mechanism research and drug testing applications.

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NSC-34细胞系衍生球体模型:体外评估神经退化的潜力与挑战。
三维(3D)球形模型旨在弥补传统二维(2D)培养与复杂体内组织环境之间的差距。这些模型通过自聚细胞来模拟具有周围细胞外框架的三维环境,为研究提供了宝贵的工具。NSC-34细胞系由小鼠脊髓运动神经元和神经母细胞瘤细胞融合而成,是研究肌萎缩性脊髓侧索硬化症(ALS)等神经退行性疾病的重要工具,受影响的神经细胞中会出现TAR-DNA结合蛋白43(TDP-43)等异常蛋白积累。然而,NSC-34在三维环境中的行为仍未得到充分探索,本研究首次尝试创建一个三维模型,以确定其是否适合用于病理学研究。我们使用非粘性水凝胶模板生成了 NSC-34 球体,并对其进行了 6 天的表征。光镜观察发现,三维模型中的 NSC-34 细胞保持了较高的存活率、明显的圆形,并形成了稳定的膜连接。扫描电子显微镜发现了多个隧道状结构,而超微结构分析则强调了核弯曲和线粒体的改变。利用诱导型 GFP-TDP-43 表达的 NSC-34 球形体,我们探索了三维结构是否会影响 TDP-43 的表达、定位和聚集。与二维培养物相比,球体显示了核GFP-TDP-43表达,但水平较低,并产生了TDP-35片段和TDP-43聚集体。这项研究揭示了 NSC-34 在三维培养中的独特行为,建议在 ALS 或 TDP-43 病理学中谨慎使用三维模型。不过,它强调了球形培养物在研究基本细胞机制、细胞在三维环境中的适应性、未来的生物反应器应用以及药物渗透研究方面的潜力。研究亮点:三维球体的生成:使用基于水凝胶的模板生成的 NSC-34 球形体在 6 天内显示出很高的存活率和独特的形状。结构特征:先进的显微镜在球体内发现了隧道状结构以及核和线粒体的变化。蛋白质动态:研究观察到三维结构如何影响 TDP-43 的行为,其表达发生了改变,但聚集模式与二维培养物相似。研究意义:这项研究揭示了 NSC-34 在三维培养中的独特行为,建议谨慎使用该模型来研究 ALS 或 TDP-43 病理,并强调了其在细胞机制研究和药物测试应用方面的潜力。
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来源期刊
Microscopy Research and Technique
Microscopy Research and Technique 医学-解剖学与形态学
CiteScore
5.30
自引率
20.00%
发文量
233
审稿时长
4.7 months
期刊介绍: Microscopy Research and Technique (MRT) publishes articles on all aspects of advanced microscopy original architecture and methodologies with applications in the biological, clinical, chemical, and materials sciences. Original basic and applied research as well as technical papers dealing with the various subsets of microscopy are encouraged. MRT is the right form for those developing new microscopy methods or using the microscope to answer key questions in basic and applied research.
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