neuronal specification
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Biology Open ◽  
2021 ◽  
Author(s):  
Konstantina Filippopoulou ◽  
Carole Couillault ◽  
Vincent Bertrand

Neural bHLH transcription factors play a key role in the early steps of neuronal specification in many animals. We have previously observed that the Achaete-Scute HLH-3, the Olig HLH-16 and their binding partner the E protein HLH-2 activate the terminal differentiation program of a specific class of cholinergic neurons, AIY, in C. elegans. Here we identify a role for a fourth bHLH, the Neurogenin NGN-1, in this process, raising the question of why so many neural bHLHs are required for a single neuronal specification event. Using quantitative imaging we show that the combined action of different bHLHs is needed to activate the correct level of expression of the terminal selector transcription factors TTX-3 and CEH-10 that subsequently initiate and maintain the expression of a large battery of terminal differentiation genes. Surprisingly, the different bHLHs have an antagonistic effect on another target, the proapoptotic BH3-only factor EGL-1, normally not expressed in AIY and otherwise detrimental for its specification. We propose that the use of multiple neural bHLHs allows robust neuronal specification while, at the same time, preventing spurious activation of deleterious genes.


Science ◽  
2018 ◽  
Vol 362 (6411) ◽  
pp. 176-180 ◽  
Author(s):  
Isabel Holguera ◽  
Claude Desplan

To understand how neurons assemble to form functional circuits, it is necessary to obtain a detailed knowledge of their diversity and to define the developmental specification programs that give rise to this diversity. Invertebrates and vertebrates appear to share common developmental principles of neuronal specification in which cascades of transcription factors temporally pattern progenitors, while spatial cues modify the outcomes of this temporal patterning. Here, we highlight these conserved mechanisms and describe how they are used in distinct neural structures. We present the questions that remain for a better understanding of neuronal specification. Single-cell RNA profiling approaches will potentially shed light on these questions, allowing not only the characterization of neuronal diversity in adult brains, but also the investigation of the developmental trajectories leading to the generation and maintenance of this diversity.


2018 ◽  
Vol 295 ◽  
pp. S109-S110
Author(s):  
D. Lupu ◽  
M. Varshney ◽  
I. Nalvarte ◽  
J. Insunza ◽  
F. Loghin ◽  
...  

2018 ◽  
Vol 8 (1) ◽  
Author(s):  
Tomás Armenteros ◽  
Zoraida Andreu ◽  
Rafael Hortigüela ◽  
D. Chichung Lie ◽  
Helena Mira

Neuron ◽  
2018 ◽  
Vol 97 (3) ◽  
pp. 520-537.e6 ◽  
Author(s):  
Siraj K. Zahr ◽  
Guang Yang ◽  
Hilal Kazan ◽  
Michael J. Borrett ◽  
Scott A. Yuzwa ◽  
...  

eLife ◽  
2017 ◽  
Vol 6 ◽  
Author(s):  
Esteban Hoijman ◽  
L Fargas ◽  
Patrick Blader ◽  
Berta Alsina

Neural patterning involves regionalised cell specification. Recent studies indicate that cell dynamics play instrumental roles in neural pattern refinement and progression, but the impact of cell behaviour and morphogenesis on neural specification is not understood. Here we combine 4D analysis of cell behaviours with dynamic quantification of proneural expression to uncover the construction of the zebrafish otic neurogenic domain. We identify pioneer cells expressing neurog1 outside the otic epithelium that migrate and ingress into the epithelialising placode to become the first otic neuronal progenitors. Subsequently, neighbouring cells express neurog1 inside the placode, and apical symmetric divisions amplify the specified pool. Interestingly, pioneer cells delaminate shortly after ingression. Ablation experiments reveal that pioneer cells promote neurog1 expression in other otic cells. Finally, ingression relies on the epithelialisation timing controlled by FGF activity. We propose a novel view for otic neurogenesis integrating cell dynamics whereby ingression of pioneer cells instructs neuronal specification.


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