Научная статья на тему 'Becoming a new neuron in the cerebral cortex'

Becoming a new neuron in the cerebral cortex Текст научной статьи по специальности «Биологические науки»

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Opera Medica et Physiologica
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Текст научной работы на тему «Becoming a new neuron in the cerebral cortex»

Section MOLECULAR NEUROSCIENCE

genomic, and cell biological tools including mouse genetics and live imaging. One major research direction focuses on post-transcriptional RNA regulation in neural progenitor behavior and function. A second research focus is aimed at understanding how human-specific enhancers contribute to unique features of human brain development, including progenitor proliferation. This seminar will discuss new discoveries from our lab including how mitosis impacts progenitor cell fate specification in the developing brain, and layers of dynamic RNA regulation in neural progenitors.

Becoming a New Neuron in the Cerebral Cortex

Denis Jabaudon*

Dpt. of Basic Neuroscience, University of Geneva, Switeerland. * Presenting e-mail: denis.jabaudon@unige.ch

During neocortical development, excitatory neurons are born in the ventricular zone and migrate to the cortex, where they form the circuits that underlie mammalian skilled processing abilities. While the genetic programs that specify distinct subtypes of neurons within the neocortex are increasingly understood, how neuronal identity is dynamically acquired upon progenitor division is largely unknown. Identifying these primordial transcriptional processes is critical to understand how progenitor behavior is coupled to neuronal fate, and to provide mechanical insights into postmitotic neuron plasticity. Here, we will discuss recent findings from our laboratory on the mitotic and early-postmitotic biology of progenitors and their daughter cells, and how they inform neuronal specification and circuit assembly in the developing neocortex.

Dynamic Control of Neural Stem Cells

Ryoichiro Kageyama*

Institute for Virus Research; WPI-iCeMS, Kyoto University, Kyoto 606-8507, Japan. * Presenting e-mail: rkageyam@virus.kyoto-u.ac.jp

During brain development, neural stem cells gradually change their competency, giving rise to various types of neurons first and glial cells later. It is thus very important to maintain neural stem cells until the final stage of development to generate a full diversity of cell types. The basic helix-loop-helix (bHLH) factor Hesl plays an important role in maintenance of neural stem cells by repressing proneural gene expression. We found that the Hes1 expression oscillates by negative feedback, and that this oscillation is important for proliferation of neural stem cells, as sustained Hes1 expression inhibits proliferation of these cells. Hes1 oscillation drives the cyclic expression of proneural factors such as Asd1/Mash1. During neuronal differentiation, Hes1 expression disappears and proneural factor expression becomes sustained. By contrast, during astrocyte differentiation, Hes1 expression becomes dominant while proneural factor expression disappears. These results suggest that the multipotency is a state controlled by multiple oscillating fate-determination factors such as Hes1 and Asd1/Mash1, and that one of them becomes dominant during fate choice. We further showed by optogenetic approach that sustained expression of Asd1/Mash1 promotes neuronal differentiation, whereas oscillatory expression of Ascl1/Mash1 activates proliferation of neural stem cells, suggesting that the expression dynamics is important for the function of fate-determination factors. We also found that the Notch ligand Delta-like1 (Dll1), a downstream of Ascl1/ Mashl and Hesl, is expressed in an oscillatory manner, and that this oscillation is important for Hesl oscillation and proliferation of neural stem cells. These results indicate that the oscillatory expression of these factors in neural stem cells is essential for neural development.

Evolution of Cortical Development

A. Goffinet*

Université catholique de Louvain, Belgium. * Presenting e-mail: andre.goffinet@uclouvain.be

OM&P

Opera Med Physiol 2016 Vol. 2 (S1) 27

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