Nitric oxide inhibits hypothalamic luteinizing hormone-releasing hormone release by releasing gamma-aminobutyric acid.

Seilicovich, Adriana; Duvilanski, Beatriz H.; Pisera, Daniel; Theas, María Susana; Gimeno, M.F.; Rettori, Valéria; McCann, S. M.

doi:10.1073/pnas.92.8.3421

Cited by 75 publications

(46 citation statements)

References 22 publications

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“…The fact that LPS and interferon treatment inhibits basal and stimulated ACTH secretion from AtT-20 cells is consistent with other studies which show that NO inhibits ACTH secretion (27)(28)(29)(30)(31)(32)(33)(34)(35)(36). The effect of LPS upon the pituitary is complex: in the whole animal LPS is often reported to stimulate ACTH secretion (87).…”

Section: Discussionsupporting

confidence: 76%

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Kalirin Inhibition of Inducible Nitric-oxide Synthase

Ratovitski¹,

Alam

Quick³

et al. 1999

Journal of Biological Chemistry

110

114

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Nitric oxide (NO) acts as a neurotransmitter. However, excess NO produced from neuronal NO synthase (nNOS) or inducible NOS (iNOS) during inflammation of the central nervous system can be neurotoxic, disrupting neurotransmitter and hormone production and killing neurons. A screen of a hippocampal cDNA library showed that a unique region of the iNOS protein interacts with Kalirin, previously identified as an interactor with a secretory granule peptide biosynthetic enzyme. Kalirin associates with iNOS in vitro and in vivo and inhibits iNOS activity by preventing the formation of iNOS homodimers. Expression of exogenous Kalirin in pituitary cells dramatically reduces iNOS inhibition of ACTH secretion. Thus Kalirin may play a neuroprotective role during inflammation of the central nervous system by inhibiting iNOS activity.

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Section: Discussionsupporting

confidence: 76%

“…Experimental evidence from neuronal cultures and animal models shows that NO can also inhibit specific secretory responses of neurons. For example, some but not all modes of stimulating hormone secretion from the pituitary are enhanced in the presence of NOS inhibitors (27)(28)(29)(30)(31)(32)(33)(34)(35)(36).…”

mentioning

confidence: 99%

Kalirin Inhibition of Inducible Nitric-oxide Synthase

Ratovitski¹,

Alam

Quick³

et al. 1999

Journal of Biological Chemistry

110

114

View full text Add to dashboard Cite

show abstract

“…The mechanisms proposed to explain the role of NO on the hypothalamic-pituitary-testicular axis involve effects at different levels (6). At the hypothalamic level, most studies have reported stimulatory effects (7)(8)(9), although inhibitory effects have been also reported (10). At the pituitary level, NO inhibits LH secretion (11).…”

Section: Introductionmentioning

confidence: 99%

Role of the testis in the response of the pituitary-testicular axis to nitric oxide-related agents

Gaytán

Bellido²,

Aguilar³

et al. 1997

European Journal of Endocrinology

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Nitric oxide (NO) is generated from the guanidine group of L-arginine by NO synthases (NOS) in a wide variety of tissues, including endocrine organs. In order to discriminate between central and local effects of NO-related agents on the pituitary-testicular axis, adult rats were injected intraperitoneally with 1 g/kg body weight (bw) L-arginine methyl ester (L-AME, an exogenous substrate of NOS), 0.5 mg/kg bw sodium nitroprusside (SNP, an NO donor) or vehicle (0.9% NaCl) or intratesticularly with 2 mg/testis L-AME, 2 mg/testis SNP or 25 ml vehicle, and killed at 60 or 120 min after treatment. Both intraperitoneal and intratesticular administration of L-AME had the same effects: a decrease in the serum concentrations of LH and testosterone and in those of testosterone in the testicular interstitial fluid. However, treatment with SNP was more effective when given intratesticularly, inducing a decrease in serum and interstitial fluid testosterone concentrations, without significant changes in LH concentrations. Furthermore, when rats were injected intraperitoneally with 4 mg L-AME (the same dose as that given intratesticularly), serum LH concentrations were not changed. In addition, L-AME administration was not effective in modifying serum LH concentrations in castrated rats. To test the possible role of Leydig cells, the effects of systemic administration of L-AME were studied in rats depleted of Leydig cells by treatment with ethylene dimethane sulphonate. In these animals L-AME significantly decreased serum LH concentrations. To study the role of macrophages in this system, rats depleted of testicular macrophages by the liposome-suicide approach were injected intraperitoneally (1 g/kg bw) or intratesticularly (2 mg/testis) with L-AME or vehicle, 10 days after macrophage depletion, and killed at 120 min after treatment. The effects of L-AME on serum LH concentrations were blocked when the drug was administered intratesticularly.

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“…In vitro studies demonstrated that EtOH, as well as THC, increases GABA content in the MBH (21,22). It has been shown that GABA inhibits the release of LHRH (11) and that stimulatory neurotransmitters such as norepinephrine act through cAMP to increase the release of LHRH (23). Because the mechanism of action of a cannabinoid acting on its receptors is by the inhibition of AC with a consequent decrease of cAMP, in the present study we investigated whether EtOH would use the same pathway used by endocannabinoids to inhibit the release of LHRH.…”

mentioning

confidence: 99%

“…The primary action of GABA appears to be to inhibit the nitric oxidergic activation of cyclooxygenase (11). Therefore, lower levels of prostaglandins decrease AC activity with the consequent decrease of LHRH release.…”

mentioning

confidence: 99%

Alcohol inhibits luteinizing hormone-releasing hormone release by activating the endocannabinoid system

Fernández‐Solari

Scorticati

Mohn

et al. 2004

Proc. Natl. Acad. Sci. U.S.A.

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We hypothesized that ethanol (EtOH) might act through the endocannabinoid system to inhibit luteinizing hormone-releasing hormone (LHRH) release. Therefore, we examined the mechanism by which EtOH and anandamide (AEA), an endogenous cannabinoid, inhibit LHRH release from incubated medial basal hypothalamic explants. In previous work, we demonstrated that EtOH inhibits the N-methyl-D-aspartic acid-stimulated release of LHRH by increasing the release of two neurotransmitters: ␤-endorphin and ␥-aminobutyric acid (GABA). In the present work, bicuculline, a GABAergic antagonist, completely prevented the inhibition of AEA (10 ؊9 M) on N-methyl-D-aspartic acid-induced LHRH release, but naltrexone, a -opioid receptor antagonist, had no effect. AEA also significantly increased GABA release but had no effect on ␤-endorphin release. Therefore, AEA could inhibit LHRH release by increasing GABA but not ␤-endorphin release. Because EtOH and AEA acted similarly to inhibit LHRH release, we investigated whether both substances would affect the adenylate cyclase activity acting through the same GTP-coupled receptors, the cannabinoid receptors 1 (CB1-rs). AEA and EtOH (10 ؊1 M) reduced the forskolin-stimulated accumulation of cAMP, but AM251, a specific antagonist of CB1-r, significantly blocked that inhibition. Additionally we investigated whether CB1-r is involved in the inhibition of LHRH by EtOH and AEA. AEA and EtOH reduced forskolin-stimulated LHRH release, but AM251 significantly blocked that inhibition. Also, we demonstrated that EtOH did not act by increasing AEA synthase activity to inhibit LHRH release in our experimental conditions. Therefore, our results indicate that EtOH inhibits the release of LHRH acting through the endocannabinoid system. anandamide ͉ cannabinoid receptor 1 ͉ cyclic adenosine monophosphate ͉ ␥-amino butyric acid

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Nitric oxide inhibits hypothalamic luteinizing hormone-releasing hormone release by releasing gamma-aminobutyric acid.

Cited by 75 publications

References 22 publications

Kalirin Inhibition of Inducible Nitric-oxide Synthase

Kalirin Inhibition of Inducible Nitric-oxide Synthase

Role of the testis in the response of the pituitary-testicular axis to nitric oxide-related agents

Alcohol inhibits luteinizing hormone-releasing hormone release by activating the endocannabinoid system

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