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干细胞衍生的脊髓中间神经元的亚型多样化和突触特异性。

Subtype Diversification and Synaptic Specificity of Stem Cell-Derived Spinal Interneurons.

机构信息

Departments of Pathology and Cell Biology, Neuroscience, Rehabilitation & Regenerative Medicine, and Neurology, Center for Motor Neuron Biology and Disease, Columbia Stem Cell Initiative, Columbia University Irving Medical Center, New York, NY 10032, USA.

Departments of Pathology and Cell Biology and Neurology, Center for Motor Neuron Biology and Disease, Columbia University Irving Medical Center, New York, NY 10032, USA.

出版信息

Neuron. 2018 Oct 10;100(1):135-149.e7. doi: 10.1016/j.neuron.2018.09.016.

Abstract

Neuronal diversification is a fundamental step in the construction of functional neural circuits, but how neurons generated from single progenitor domains acquire diverse subtype identities remains poorly understood. Here we developed an embryonic stem cell (ESC)-based system to model subtype diversification of V1 interneurons, a class of spinal neurons comprising four clades collectively containing dozens of molecularly distinct neuronal subtypes. We demonstrate that V1 subtype diversity can be modified by extrinsic signals. Inhibition of Notch and activation of retinoid signaling results in a switch to MafA clade identity and enriches differentiation of Renshaw cells, a specialized MafA subtype that mediates recurrent inhibition of spinal motor neurons. We show that Renshaw cells are intrinsically programmed to migrate to species-specific laminae upon transplantation and to form subtype-specific synapses with motor neurons. Our results demonstrate that stem cell-derived neuronal subtypes can be used to investigate mechanisms underlying neuronal subtype specification and circuit assembly.

摘要

神经元的多样化是构建功能性神经回路的一个基本步骤,但人们对单个祖细胞来源的神经元如何获得不同的亚型身份仍知之甚少。在这里,我们开发了一种基于胚胎干细胞(ESC)的系统来模拟 V1 中间神经元的亚型多样化,V1 中间神经元是一类脊髓神经元,包含四个分支,总共包含数十种具有不同分子特征的神经元亚型。我们证明,外部信号可以改变 V1 亚型的多样性。抑制 Notch 并激活视黄酸信号会导致向 MafA 分支身份转变,并富集中间神经元的分化,中间神经元是一种专门的 MafA 亚型,它介导脊髓运动神经元的反复抑制。我们表明,中间神经元在移植后会被内在编程以迁移到特定物种的层,并与运动神经元形成特定亚型的突触。我们的结果表明,干细胞衍生的神经元亚型可用于研究神经元亚型特化和回路组装的机制。

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