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An Optimized Workflow to Generate and Characterize iPSC-Derived Motor Neuron (MN) Spheroids
An Optimized Workflow to Generate and Characterize iPSC-Derived Motor Neuron (MN) Spheroids
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An Optimized Workflow to Generate and Characterize iPSC-Derived Motor Neuron (MN) Spheroids
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An Optimized Workflow to Generate and Characterize iPSC-Derived Motor Neuron (MN) Spheroids
An Optimized Workflow to Generate and Characterize iPSC-Derived Motor Neuron (MN) Spheroids

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An Optimized Workflow to Generate and Characterize iPSC-Derived Motor Neuron (MN) Spheroids
An Optimized Workflow to Generate and Characterize iPSC-Derived Motor Neuron (MN) Spheroids
Journal Article

An Optimized Workflow to Generate and Characterize iPSC-Derived Motor Neuron (MN) Spheroids

2023
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Overview
A multitude of in vitro models based on induced pluripotent stem cell (iPSC)-derived motor neurons (MNs) have been developed to investigate the underlying causes of selective MN degeneration in motor neuron diseases (MNDs). For instance, spheroids are simple 3D models that have the potential to be generated in large numbers that can be used across different assays. In this study, we generated MN spheroids and developed a workflow to analyze them. To start, the morphological profiling of the spheroids was achieved by developing a pipeline to obtain measurements of their size and shape. Next, we confirmed the expression of different MN markers at the transcript and protein levels by qPCR and immunocytochemistry of tissue-cleared samples, respectively. Finally, we assessed the capacity of the MN spheroids to display functional activity in the form of action potentials and bursts using a microelectrode array approach. Although most of the cells displayed an MN identity, we also characterized the presence of other cell types, namely interneurons and oligodendrocytes, which share the same neural progenitor pool with MNs. In summary, we successfully developed an MN 3D model, and we optimized a workflow that can be applied to perform its morphological, gene expression, protein, and functional profiling over time.