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Ephrin-B在中间神经元迁移中的自主和非自主作用。

Autonomous and non-autonomous roles for ephrin-B in interneuron migration.

作者信息

Talebian Asghar, Britton Rachel, Ammanuel Simon, Bepari Asim, Sprouse Francis, Birnbaum Shari G, Szabó Gábor, Tamamaki Nobuaki, Gibson Jay, Henkemeyer Mark

机构信息

Department of Neuroscience, University of Texas Southwestern Medical Center, Dallas, TX 75390, USA; Kent Waldrep Center for Basic Research on Nerve Growth and Regeneration, University of Texas Southwestern Medical Center, Dallas, TX 75390, USA.

Department of Neuroscience, University of Texas Southwestern Medical Center, Dallas, TX 75390, USA.

出版信息

Dev Biol. 2017 Nov 15;431(2):179-193. doi: 10.1016/j.ydbio.2017.09.024. Epub 2017 Sep 22.

Abstract

While several studies indicate the importance of ephrin-B/EphB bidirectional signaling in excitatory neurons, potential roles for these molecules in inhibitory neurons are largely unknown. We identify here an autonomous receptor-like role for ephrin-B reverse signaling in the tangential migration of interneurons into the neocortex using ephrin-B (EfnB1/B2/B3) conditional triple mutant (TM) mice and a forebrain inhibitory neuron specific Cre driver. Inhibitory neuron deletion of the three EfnB genes leads to reduced interneuron migration, abnormal cortical excitability, and lethal audiogenic seizures. Truncated and intracellular point mutations confirm the importance of ephrin-B reverse signaling in interneuron migration and cortical excitability. A non-autonomous ligand-like role was also identified for ephrin-B2 that is expressed in neocortical radial glial cells and required for proper tangential migration of GAD65-positive interneurons. Our studies thus define both receptor-like and ligand-like roles for the ephrin-B molecules in controlling the migration of interneurons as they populate the neocortex and help establish excitatory/inhibitory (E/I) homeostasis.

摘要

虽然多项研究表明 Ephrin-B/EphB 双向信号在兴奋性神经元中具有重要作用,但这些分子在抑制性神经元中的潜在作用在很大程度上仍不清楚。我们利用 Ephrin-B(EfnB1/B2/B3)条件性三突变(TM)小鼠和前脑抑制性神经元特异性 Cre 驱动子,在此确定了 Ephrin-B 反向信号在中间神经元向新皮层切向迁移中的自主受体样作用。三个 EfnB 基因的抑制性神经元缺失导致中间神经元迁移减少、皮层兴奋性异常以及致命的听源性癫痫发作。截短突变和细胞内点突变证实了 Ephrin-B 反向信号在中间神经元迁移和皮层兴奋性中的重要性。还确定了在新皮层放射状胶质细胞中表达的 Ephrin-B2 具有非自主配体样作用,它是 GAD65 阳性中间神经元正常切向迁移所必需的。因此,我们的研究确定了 Ephrin-B 分子在控制中间神经元向新皮层迁移并帮助建立兴奋性/抑制性(E/I)稳态方面的受体样和配体样作用。

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