Conditional RARα Knockout Mice Reveal Acute Requirement for Retinoic Acid and RARα in Homeostatic Plasticity

Conditional RARα Knockout Mice Reveal Acute Requirement for Retinoic Acid and RARα in Homeostatic Plasticity

All-trans retinoic acid (RA) plays important roles in brain development through regulating gene transcription. Recently, a novel postdevelopmental role of RA in mature brain was proposed. Specifically, RA rapidly enhanced excitatory synaptic transmission independent of transcriptional regulation. RA...

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Bibliographic Details
Main Authors: Federica eSarti, Jessica eSchroeder, Jason eAoto, Lu eChen
Format: Article
Language:English
Published: Frontiers Media S.A. 2012-02-01
Series:Frontiers in Molecular Neuroscience
Subjects:
synaptic scaling
calcium-permeable AMPA receptor
homeostatic synaptic plasticity
Retinoic acid
conditional RARalpha knockout
dendritic protein translation
Online Access:http://journal.frontiersin.org/Journal/10.3389/fnmol.2012.00016/full
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spelling doaj-c67127821dc54791aeca16b960ff6dbb2020-11-24T23:03:47ZengFrontiers Media S.A.Frontiers in Molecular Neuroscience1662-50992012-02-01510.3389/fnmol.2012.0001617275Conditional RARα Knockout Mice Reveal Acute Requirement for Retinoic Acid and RARα in Homeostatic PlasticityFederica eSarti0Federica eSarti1Jessica eSchroeder2Jason eAoto3Lu eChen4Stanford University School of MedicineUniversity of California, BerkeleyStanford University School of MedicineStanford University School of MedicineStanford University School of MedicineAll-trans retinoic acid (RA) plays important roles in brain development through regulating gene transcription. Recently, a novel postdevelopmental role of RA in mature brain was proposed. Specifically, RA rapidly enhanced excitatory synaptic transmission independent of transcriptional regulation. RA synthesis was induced when excitatory synaptic transmission was chronically blocked, and RA then activated dendritic protein synthesis and synaptic insertion of homomeric GluA1 AMPA receptors, thereby compensating for the loss of neuronal activity in a homeostatic fashion. This action of RA was suggested to be mediated by its canonical receptor RARα but no genetic evidence was available. Thus, we here tested the fundamental requirement of RARα in homeostatic plasticity using conditional RARα knockout mice, and additionally performed a structure-function analysis of RARα. We show that acutely deleting RARα in neurons eliminated RA’s effect on excitatory synaptic transmission, and inhibited activity blockade-induced homeostatic synaptic plasticity. By expressing various RARα rescue constructs in RARα knockout neurons, we found that the DNA-binding domain of RARα was dispensable for its role in regulating synaptic strength, further supporting the notion that RA and RARα act in a non-transcriptional manner in this context. By contrast, the ligand-binding domain (LBD) and the mRNA-binding domain (F-domain) are both necessary and sufficient for the function of RARα in homeostatic plasticity. Furthermore, we found that homeostatic regulation performed by the LBD/F domains leads to insertion of calcium-permeable AMPA receptors. Our results confirm with unequivocal genetic approaches that RA and RARα perform essential non-transcriptional functions in regulating synaptic strength, and establish a functional link between the various domains of RARα and their involvement in regulating protein synthesis and excitatory synaptic transmission during homeostatic plasticity.http://journal.frontiersin.org/Journal/10.3389/fnmol.2012.00016/fullsynaptic scalingcalcium-permeable AMPA receptorhomeostatic synaptic plasticityRetinoic acidconditional RARalpha knockoutdendritic protein translation
collection DOAJ
language English
format Article
sources DOAJ
author Federica eSarti
Federica eSarti
Jessica eSchroeder
Jason eAoto
Lu eChen
spellingShingle Federica eSarti
Federica eSarti
Jessica eSchroeder
Jason eAoto
Lu eChen
Conditional RARα Knockout Mice Reveal Acute Requirement for Retinoic Acid and RARα in Homeostatic Plasticity
Frontiers in Molecular Neuroscience
synaptic scaling
calcium-permeable AMPA receptor
homeostatic synaptic plasticity
Retinoic acid
conditional RARalpha knockout
dendritic protein translation
author_facet Federica eSarti
Federica eSarti
Jessica eSchroeder
Jason eAoto
Lu eChen
author_sort Federica eSarti
title Conditional RARα Knockout Mice Reveal Acute Requirement for Retinoic Acid and RARα in Homeostatic Plasticity
title_short Conditional RARα Knockout Mice Reveal Acute Requirement for Retinoic Acid and RARα in Homeostatic Plasticity
title_full Conditional RARα Knockout Mice Reveal Acute Requirement for Retinoic Acid and RARα in Homeostatic Plasticity
title_fullStr Conditional RARα Knockout Mice Reveal Acute Requirement for Retinoic Acid and RARα in Homeostatic Plasticity
title_full_unstemmed Conditional RARα Knockout Mice Reveal Acute Requirement for Retinoic Acid and RARα in Homeostatic Plasticity
title_sort conditional rarα knockout mice reveal acute requirement for retinoic acid and rarα in homeostatic plasticity
publisher Frontiers Media S.A.
series Frontiers in Molecular Neuroscience
issn 1662-5099
publishDate 2012-02-01
description All-trans retinoic acid (RA) plays important roles in brain development through regulating gene transcription. Recently, a novel postdevelopmental role of RA in mature brain was proposed. Specifically, RA rapidly enhanced excitatory synaptic transmission independent of transcriptional regulation. RA synthesis was induced when excitatory synaptic transmission was chronically blocked, and RA then activated dendritic protein synthesis and synaptic insertion of homomeric GluA1 AMPA receptors, thereby compensating for the loss of neuronal activity in a homeostatic fashion. This action of RA was suggested to be mediated by its canonical receptor RARα but no genetic evidence was available. Thus, we here tested the fundamental requirement of RARα in homeostatic plasticity using conditional RARα knockout mice, and additionally performed a structure-function analysis of RARα. We show that acutely deleting RARα in neurons eliminated RA’s effect on excitatory synaptic transmission, and inhibited activity blockade-induced homeostatic synaptic plasticity. By expressing various RARα rescue constructs in RARα knockout neurons, we found that the DNA-binding domain of RARα was dispensable for its role in regulating synaptic strength, further supporting the notion that RA and RARα act in a non-transcriptional manner in this context. By contrast, the ligand-binding domain (LBD) and the mRNA-binding domain (F-domain) are both necessary and sufficient for the function of RARα in homeostatic plasticity. Furthermore, we found that homeostatic regulation performed by the LBD/F domains leads to insertion of calcium-permeable AMPA receptors. Our results confirm with unequivocal genetic approaches that RA and RARα perform essential non-transcriptional functions in regulating synaptic strength, and establish a functional link between the various domains of RARα and their involvement in regulating protein synthesis and excitatory synaptic transmission during homeostatic plasticity.
topic synaptic scaling
calcium-permeable AMPA receptor
homeostatic synaptic plasticity
Retinoic acid
conditional RARalpha knockout
dendritic protein translation
url http://journal.frontiersin.org/Journal/10.3389/fnmol.2012.00016/full
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AT jasoneaoto conditionalraraknockoutmicerevealacuterequirementforretinoicacidandrarainhomeostaticplasticity
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