Involvement of Nitric Oxide in Depolarization-Induced Suppression of Inhibition in Hippocampal Pyramidal Cells during Activation of Cholinergic Receptors

doi:10.1523/JNEUROSCI.2104-07.2007

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The Journal of Neuroscience, September 19, 2007, 27(38):10211-10222; doi:10.1523/JNEUROSCI.2104-07.2007

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Cellular/Molecular
Involvement of Nitric Oxide in Depolarization-Induced Suppression of Inhibition in Hippocampal Pyramidal Cells during Activation of Cholinergic Receptors
Judit K. Makara,¹ István Katona,¹ Gábor Nyíri,¹ Beáta Németh,¹ Catherine Ledent,² Masahiko Watanabe,³ Jan de Vente,⁴ Tamás F. Freund,¹ and Norbert Hájos¹
¹Department of Cellular and Network Neurobiology, Institute of Experimental Medicine, Hungarian Academy of Sciences, H-1083 Budapest, Hungary, ²Institut de Recherche Interdisciplinaire en Biologie Humaine et Moleculaire, Universite Libre de Bruxelles, 1070 Brussels, Belgium, ³Department of Anatomy, Hokkaido University School of Medicine, Sapporo 060-8638, Japan, and ⁴European Graduate School of Neuroscience, Department of Psychiatry and Neuropsychology, Division of Cellular Neuroscience, Maastricht University, 6200 MD Maastricht, The Netherlands
Correspondence should be addressed to Dr. Norbert Hájos, Department of Cellular and Network Neurobiology, Institute of Experimental Medicine, Hungarian Academy of Sciences, Budapest H-1450, Hungary. Email: hajos{at}koki.hu
Several types of neurons are able to regulate their synapticinputs via releasing retrograde signal molecules, such as endocannabinoidsor nitric oxide (NO). Here we show that, during activation ofcholinergic receptors, retrograde signaling by NO controls CB₁cannabinoid receptor (CB₁R)-dependent depolarization-inducedsuppression of inhibition (DSI). Spontaneously occurring IPSCswere recorded in CA1 pyramidal neurons in the presence of carbachol,and DSI was induced by a 1-s-long depolarization step. We foundthat, in addition to the inhibition of CB₁Rs, blocking the NOsignaling pathway at various points also disrupted DSI. Inhibitorsof NO synthase (NOS) or NO-sensitive guanylyl cyclase (NO-sGC)diminished DSI, whereas a cGMP analog or an NO donor inhibitedIPSCs and partially occluded DSI in a CB₁R-dependent manner.Furthermore, an NO scavenger applied extracellularly or postsynapticallyalso decreased DSI, whereas L-arginine, the precursor for NO,prolonged it. DSI of electrically evoked IPSCs was also blockedby an inhibitor of NOS in the presence, but not in the absence,of carbachol. In line with our electrophysiological data, doubleimmunohistochemical staining revealed an NO-donor-induced cGMPaccumulation in CB₁R-positive axon terminals. Using electronmicroscopy, we demonstrated the postsynaptic localization ofneuronal NOS at symmetrical synapses formed by CB₁R-positiveaxon terminals on pyramidal cell bodies, whereas NO-sGC wasfound in the presynaptic terminals. These electrophysiologicaland anatomical results in the hippocampus suggest that NO isinvolved in depolarization-induced CB₁R-mediated suppressionof IPSCs as a retrograde signal molecule and that operationof this cascade is conditional on cholinergic receptor activation.

Key words: synaptic plasticity; hippocampus; GABA; CB₁ receptor; cGMP; retrograde

Received Dec. 22, 2006; revised July 18, 2007; accepted July 22, 2007.

Correspondence should be addressed to Dr. Norbert Hájos, Department of Cellular and Network Neurobiology, Institute of Experimental Medicine, Hungarian Academy of Sciences, Budapest H-1450, Hungary. Email: hajos{at}koki.hu

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