Role of Nitric Oxide on Motor Behavior

Ea, Del Bel; Guimarães, F.S.; Echeverry, Marcela Bermúdez; Mz, Gomes; Schiaveto-de-Souza, A.; Padovan-Neto, Fernando E.; Tumas,; Ap, Barion-Cavalcanti; Lazzarini, Márcio; Nucci-da-Silva, LP; Sa, D. De

doi:10.1007/s10571-005-3065-8

Cited by 111 publications

(77 citation statements)

References 145 publications

(201 reference statements)

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“…Nevertheless, sub-chronic 7-NI treatment induced an even stronger regularization of temporal structure of nigral spiking activity reducing burst firing of about 60% when compared with the control group. These findings are in line with the evidence that NOS inhibitors induce catalepsy in rodents [62,63] and decrease exploratory behaviour in rats [64] while both effects disappear after only 4 days of NOS inhibition [36,[64][65][66][67]. Therefore, the increase in DA neurotransmission after 7-NI sub-chronic treatment showed by Di Matteo et al [47] might be the mechanism involved in the rapid tolerance development after chronic NOS inhibition.…”

Section: Fig (1) Effect Of Nitric Oxide Drugs On the Firing Rate Ofsupporting

confidence: 85%

“…It has been proposed that NO modulates motor behaviour [43,66,165] and considerable data indicate a direct NO-DA interaction either in normal BG function (as explained above) or in BG related movement disorders such as PD. For instance the DA agonists, cocaine, morphine, substance P or methamphetamine-induced hyperlocomotion could be impeded by NOS inhibitors in mice and rats [166][167][168].…”

Section: No Implication On Bg Dysfunctionmentioning

confidence: 99%

“…For instance the DA agonists, cocaine, morphine, substance P or methamphetamine-induced hyperlocomotion could be impeded by NOS inhibitors in mice and rats [166][167][168]. Yet, inhibition of NOS also induces catalepsy after systemic or intrastriatal injection [65,66], in agreement with the finding that striatal NOS activity is depressed in parkinsonian animal models [136,137] and in human PD [24,169]. NO synthesis seems to be under the control of the phasic/synaptic striatal DA transmission [70,71] and extracellular increase of NO tone within the GPi, motor putamen and SNr are correlated with transient clinical transition in PD patients [122,170,171].…”

Section: No Implication On Bg Dysfunctionmentioning

confidence: 99%

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Nitric Oxide Modulation of the Basal Ganglia Circuitry: Therapeutic Implication for Parkinson's Disease and Other Motor Disorders

Pierucci

Galati

Valentino

et al. 2011

CNSNDDT

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Several recent studies have emphasized a crucial role for the nitrergic system in movement control and the pathophysiology of the basal ganglia (BG). These observations are supported by anatomical evidence demonstrating the presence of nitric oxide synthase (NOS) in all the basal ganglia nuclei. In fact, nitrergic terminals have been reported to make synaptic contacts with both substantia nigra dopamine-containing neurons and their terminal areas such as the striatum, the globus pallidus and the subthalamus. These brain areas contain a high expression of nitric oxide (NO)-producing neurons, with the striatum having the greatest number, together with important NO afferent input. In this paper, the distribution of NO in the BG nuclei will be described. Furthermore, evidence demonstrating the nitrergic control of BG activity will be reviewed. The new avenues that the increasing knowledge of NO in motor control has opened for exploring the pathophysiology and pharmacology of Parkinson's disease and other movement disorders will be discussed. For example, inhibition of striatal NO/guanosine monophosphate signal pathway by phosphodiesterases seems to be effective in levodopa-induced dyskinesia. However, the results of experimental studies have to be interpreted with caution given the complexities of nitrergic signalling and the limitations of animal models. Nevertheless, the NO system represents a promising pharmacological intervention for treating Parkinson's disease and related disorders.

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Section: Fig (1) Effect Of Nitric Oxide Drugs On the Firing Rate Ofsupporting

confidence: 85%

Section: No Implication On Bg Dysfunctionmentioning

confidence: 99%

Section: No Implication On Bg Dysfunctionmentioning

confidence: 99%

See 1 more Smart Citation

Nitric Oxide Modulation of the Basal Ganglia Circuitry: Therapeutic Implication for Parkinson's Disease and Other Motor Disorders

Pierucci

Galati

Valentino

et al. 2011

CNSNDDT

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“…The underlying mechanism for the increased locomotion in eNOS Ϫ/Ϫ mice needs further study but could represent an adaptive response to decreased energy consumption or be related to a central neural effect of eNOS deletion (21). In line with this latter concept, chronic NO inhibition increases locomotion activity in rats (22). Energy expenditure, normalized for ambulatory activity, was Ͼ30% lower in eNOS Ϫ/Ϫ mice than in control mice, suggesting decreased FFA oxidation in skeletal muscle of eNOS Ϫ/Ϫ mice.…”

Section: Enos Knockout Mice and ␤-Oxidationmentioning

confidence: 81%

Endothelial Nitric Oxide Synthase (eNOS) Knockout Mice Have Defective Mitochondrial β-Oxidation

et al. 2007

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OBJECTIVE-Recent observations indicate that the delivery of nitric oxide by endothelial nitric oxide synthase (eNOS) is not only critical for metabolic homeostasis, but could also be important for mitochondrial biogenesis, a key organelle for free fatty acid (FFA) oxidation and energy production. Because mice deficient for the gene of eNOS (eNOS Ϫ/Ϫ ) have increased triglycerides and FFA levels, in addition to hypertension and insulin resistance, we hypothesized that these knockout mice may have decreased energy expenditure and defective ␤-oxidation.RESEARCH DESIGN AND METHODS-Several markers of mitochondrial activity were assessed in C57BL/6J wild-type or eNOS Ϫ/Ϫ mice including the energy expenditure and oxygen consumption by indirect calorimetry, in vitro ␤-oxidation in isolated mitochondria from skeletal muscle, and expression of genes involved in fatty acid oxidation. RESULTS-eNOSϪ/Ϫ mice had markedly lower energy expenditure (Ϫ10%, P Ͻ 0.05) and oxygen consumption (Ϫ15%, P Ͻ 0.05) than control mice. This was associated with a roughly 30% decrease of the mitochondria content (P Ͻ 0.05) and, most importantly, with mitochondrial dysfunction, as evidenced by a markedly lower ␤-oxidation of subsarcolemmal mitochondria in skeletal muscle (Ϫ30%, P Ͻ 0.05). Finally, impaired mitochondrial ␤-oxidation was associated with a significant increase of the intramyocellular lipid content (30%, P Ͻ 0.05) in gastrocnemius muscle. CONCLUSIONS-These data indicate that elevated FFA and triglyceride in eNOSϪ/Ϫ mice result in defective mitochondrial ␤-oxidation in muscle cells. Diabetes

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“…NO has recently been implicated in the regulation of motor behavior including locomotory and respiratory activity Del Bel et al, 2005;Hedrick et al, 2005). NO modulates locomotor activity via actions at multiple levels along the neuroaxis from the cortex (Del Bel et al, 2005), to the brainstem and the spinal cord Sillar, 2002, 2004).…”

Section: Introductionmentioning

confidence: 99%

Nitric Oxide Potentiation of Locomotor Activity in the Spinal Cord of the Lamprey

Kyriakatos¹,

Molinari²,

Mahmood³

et al. 2009

J. Neurosci.

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To understand the intrinsic operation of spinal networks generating locomotion, we need to not only characterize the constituent neurons and their connectivity, but also determine the role of intrinsic modulation in shaping the final motor output. We have focused on the effects of nitric oxide (NO) on the locomotor frequency and the underlying synaptic mechanisms in the lamprey spinal cord. To identify the source of NO, we used NADPH-diaphorase histochemistry and nNOS immunocytochemistry. Gray matter and sensory neurons were positively labeled using both methods. Preparations preincubated with NO synthase inhibitors displayed slower locomotor frequency that increased upon washout of the inhibitors, suggesting that NO is an endogenous neuromodulator in the spinal cord. Application of NO donors increased the locomotor frequency that was blocked by an NO scavenger and partially reduced by an inhibitor of sGC. To analyze the synaptic modulation underlying the NO-induced increase of the locomotor frequency we performed intracellular recordings from motoneurons and interneurons. The NO-induced increase in locomotor frequency was associated with a decrease in the midcycle inhibition and an increase in on-cycle excitation. To determine the site of action of NO, we examined the effect of NO donors on miniature PSCs. NO increased both the frequency and amplitude of mEPSCs while it only decreased the frequency of mIPSCs, suggesting the increased excitation is mediated by both presynaptic and postsynaptic mechanisms, while the decrease in inhibition involves only presynaptic mechanisms. Our results demonstrate a significant role of NO in adult vertebrate motor control which, via modulation of both excitatory and inhibitory transmission, increases the locomotor burst frequency.

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Role of Nitric Oxide on Motor Behavior

Cited by 111 publications

References 145 publications

Nitric Oxide Modulation of the Basal Ganglia Circuitry: Therapeutic Implication for Parkinson's Disease and Other Motor Disorders

Nitric Oxide Modulation of the Basal Ganglia Circuitry: Therapeutic Implication for Parkinson's Disease and Other Motor Disorders

Endothelial Nitric Oxide Synthase (eNOS) Knockout Mice Have Defective Mitochondrial β-Oxidation

Nitric Oxide Potentiation of Locomotor Activity in the Spinal Cord of the Lamprey

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