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AlteredGABAergicmarkers,increasedbinocularityandreducedplasticityinthevisualcortexofEngrailed-2knockoutmice

Academic Article
Publication Date:
2014
abstract:
ThematurationoftheGABAergicsystemisacrucialdeterminantofcorticaldevelopmentduringearlypostnatallife,whensensorycircuitsundergoaprocessofactivity-dependentrefinement.Analteredexcitatory/inhibitorybalancehasbeenproposedasapossiblepathogenicmechanismofautismspectrumdisorders(ASD).Thehomeobox-containingtranscriptionfactorEngrailed-2(En2)hasbeenassociatedtoASD,andEn2knockout(En2-/-)miceshowASD-likefeaturesaccompaniedbyapartiallossofcorticalGABAergicinterneurons.HerewestudiedGABAergicmarkersandcorticalfunctioninEn2-/-mice,byexploitingthewell-knownanatomicalandfunctionalfeaturesofthemousevisualsystem.En2isexpressedinthevisualcortexatpostnatalday30andduringadulthood.Whencomparedtoage-matchedEn2+/+controls,En2-/-miceshowedanincreasednumberofparvalbumin(PV+),somatostatin(SOM+),andneuropeptideY(NPY+)positiveinterneuronsinthevisualcortexatP30,andadecreasednumberofSOM+andNPY+interneuronsintheadult.Atbothages,thedifferencesindistinctinterneuronpopulationsobservedbetweenEn2+/+andEn2-/-micewerelayer-specific.AdultEn2-/-micedisplayedanormaleye-specificsegregationintheretino-geniculatepathway,andinvivoelectrophysiologicalrecordingsshowedanormaldevelopmentofbasicfunctionalproperties(acuity,responselatency,receptivefieldsize)oftheEn2-/-primaryvisualcortex.However,asignificantincreaseofbinocularitywasfoundinP30andadultEn2-/-mice,ascomparedtoage-matchedcontrols.DifferentlyfromwhatobservedinEn2+/+mice,theEn2-/-primaryvisualcortexdidnotrespondtoabriefmonoculardeprivationperformedbetweenP26andP29,duringtheso-called"criticalperiod."ThesedatasuggestthatalteredGABAergiccircuitsimpactbaselinebinocularityandplasticityinEn2-/-mice,whileleavingothervisualfunctionalpropertiesunaffected.
Iris type:
01.01 Articolo in rivista
Keywords:
plasticity; inhibition; monoculardeprivation; criticalperiod; neurodevelopmentaldisorder
List of contributors:
Caleo, Matteo; Bozzi, Yuri; Cenni, MARIA CRISTINA
Handle:
https://iris.cnr.it/handle/20.500.14243/286613
Published in:
FRONTIERS IN CELLULAR NEUROSCIENCE
Journal
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