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Retinoid-independent motor neurogenesis from human embryonic stem cells reveals a medial columnar ground state

机译:来自人类胚胎干细胞的类视黄醇独立运动神经发生揭示了内侧柱状基态

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摘要

A major challenge in neurobiology is to understand mechanisms underlying human neuronal diversification. Motor neurons (MNs) represent a diverse collection of neuronal subtypes, displaying differential vulnerability in different human neurodegenerative diseases. The ability to manipulate cell subtype diversification is critical to establish accurate, clinically relevant in vitro disease models. Retinoid signalling contributes to caudal precursor specification and subsequent MN subtype diversification. Here we investigate the necessity for retinoic acid in motor neurogenesis from human embryonic stem cells. We show that activinodal signalling inhibition, followed by sonic hedgehog agonist treatment, is sufficient for MN precursor specification, which occurs even in the presence of retinoid pathway antagonists. Importantly, precursors mature into HB9/ChAT-expressing functional MNs. Furthermore, retinoid-independent motor neurogenesis results in a ground state biased to caudal, medial motor columnar identities from which a greater retinoid-dependent diversity of MNs, including those of lateral motor columns, can be selectively derived in vitro.
机译:神经生物学的主要挑战是了解人类神经元多样化的潜在机制。运动神经元(MN)代表了神经元亚型的各种集合,在不同的人类神经退行性疾病中表现出不同的脆弱性。操作细胞亚型多样化的能力对于建立准确的,临床相关的体外疾病模型至关重要。类维生素A信号有助于尾巴前体规范和随后的MN亚型多样化。在这里,我们研究了维甲酸在人类胚胎干细胞运动神经发生中的必要性。我们表明,激活素/节点信号转导抑制,然后进行声波刺猬激动剂治疗,对于MN前体指标就足够了,即使在存在类维生素A途径拮抗剂的情况下也是如此。重要的是,前体成熟为表达HB9 / ChAT的功能性MN。此外,与类维生素A无关的运动神经发生导致基态偏向尾,内侧运动柱状身份,从中可以选择性地在体外衍生出更大的类视黄醇依赖性MN(包括外侧运动柱)。

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