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Interneuronal Mechanism for Tinbergen’s Hierarchical Model of Behavioral Choice

Recent studies of behavioral choice support the notion that the decision to carry out one behavior rather than another depends on the reconfiguration of shared interneuronal networks [1]. We investigated another decision-making strategy, derived from the classical ethological literature [2, 3], whic...

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Autores principales: Pirger, Zsolt, Crossley, Michael, László, Zita, Naskar, Souvik, Kemenes, György, O’Shea, Michael, Benjamin, Paul R., Kemenes, Ildikó
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cell Press 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4159561/
https://www.ncbi.nlm.nih.gov/pubmed/25155505
http://dx.doi.org/10.1016/j.cub.2014.07.044
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author Pirger, Zsolt
Crossley, Michael
László, Zita
Naskar, Souvik
Kemenes, György
O’Shea, Michael
Benjamin, Paul R.
Kemenes, Ildikó
author_facet Pirger, Zsolt
Crossley, Michael
László, Zita
Naskar, Souvik
Kemenes, György
O’Shea, Michael
Benjamin, Paul R.
Kemenes, Ildikó
author_sort Pirger, Zsolt
collection PubMed
description Recent studies of behavioral choice support the notion that the decision to carry out one behavior rather than another depends on the reconfiguration of shared interneuronal networks [1]. We investigated another decision-making strategy, derived from the classical ethological literature [2, 3], which proposes that behavioral choice depends on competition between autonomous networks. According to this model, behavioral choice depends on inhibitory interactions between incompatible hierarchically organized behaviors. We provide evidence for this by investigating the interneuronal mechanisms mediating behavioral choice between two autonomous circuits that underlie whole-body withdrawal [4, 5] and feeding [6] in the pond snail Lymnaea. Whole-body withdrawal is a defensive reflex that is initiated by tactile contact with predators. As predicted by the hierarchical model, tactile stimuli that evoke whole-body withdrawal responses also inhibit ongoing feeding in the presence of feeding stimuli. By recording neurons from the feeding and withdrawal networks, we found no direct synaptic connections between the interneuronal and motoneuronal elements that generate the two behaviors. Instead, we discovered that behavioral choice depends on the interaction between two unique types of interneurons with asymmetrical synaptic connectivity that allows withdrawal to override feeding. One type of interneuron, the Pleuro-Buccal (PlB), is an extrinsic modulatory neuron of the feeding network that completely inhibits feeding when excited by touch-induced monosynaptic input from the second type of interneuron, Pedal-Dorsal12 (PeD12). PeD12 plays a critical role in behavioral choice by providing a synaptic pathway joining the two behavioral networks that underlies the competitive dominance of whole-body withdrawal over feeding.
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spelling pubmed-41595612014-09-10 Interneuronal Mechanism for Tinbergen’s Hierarchical Model of Behavioral Choice Pirger, Zsolt Crossley, Michael László, Zita Naskar, Souvik Kemenes, György O’Shea, Michael Benjamin, Paul R. Kemenes, Ildikó Curr Biol Report Recent studies of behavioral choice support the notion that the decision to carry out one behavior rather than another depends on the reconfiguration of shared interneuronal networks [1]. We investigated another decision-making strategy, derived from the classical ethological literature [2, 3], which proposes that behavioral choice depends on competition between autonomous networks. According to this model, behavioral choice depends on inhibitory interactions between incompatible hierarchically organized behaviors. We provide evidence for this by investigating the interneuronal mechanisms mediating behavioral choice between two autonomous circuits that underlie whole-body withdrawal [4, 5] and feeding [6] in the pond snail Lymnaea. Whole-body withdrawal is a defensive reflex that is initiated by tactile contact with predators. As predicted by the hierarchical model, tactile stimuli that evoke whole-body withdrawal responses also inhibit ongoing feeding in the presence of feeding stimuli. By recording neurons from the feeding and withdrawal networks, we found no direct synaptic connections between the interneuronal and motoneuronal elements that generate the two behaviors. Instead, we discovered that behavioral choice depends on the interaction between two unique types of interneurons with asymmetrical synaptic connectivity that allows withdrawal to override feeding. One type of interneuron, the Pleuro-Buccal (PlB), is an extrinsic modulatory neuron of the feeding network that completely inhibits feeding when excited by touch-induced monosynaptic input from the second type of interneuron, Pedal-Dorsal12 (PeD12). PeD12 plays a critical role in behavioral choice by providing a synaptic pathway joining the two behavioral networks that underlies the competitive dominance of whole-body withdrawal over feeding. Cell Press 2014-09-08 /pmc/articles/PMC4159561/ /pubmed/25155505 http://dx.doi.org/10.1016/j.cub.2014.07.044 Text en © 2014 The Authors https://creativecommons.org/licenses/by/3.0/This work is licensed under a Creative Commons Attribution 3.0 Unported License (https://creativecommons.org/licenses/by/3.0/) .
spellingShingle Report
Pirger, Zsolt
Crossley, Michael
László, Zita
Naskar, Souvik
Kemenes, György
O’Shea, Michael
Benjamin, Paul R.
Kemenes, Ildikó
Interneuronal Mechanism for Tinbergen’s Hierarchical Model of Behavioral Choice
title Interneuronal Mechanism for Tinbergen’s Hierarchical Model of Behavioral Choice
title_full Interneuronal Mechanism for Tinbergen’s Hierarchical Model of Behavioral Choice
title_fullStr Interneuronal Mechanism for Tinbergen’s Hierarchical Model of Behavioral Choice
title_full_unstemmed Interneuronal Mechanism for Tinbergen’s Hierarchical Model of Behavioral Choice
title_short Interneuronal Mechanism for Tinbergen’s Hierarchical Model of Behavioral Choice
title_sort interneuronal mechanism for tinbergen’s hierarchical model of behavioral choice
topic Report
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4159561/
https://www.ncbi.nlm.nih.gov/pubmed/25155505
http://dx.doi.org/10.1016/j.cub.2014.07.044
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