Lateral parabrachial nucleus and opioid mechanisms of the central nucleus of the amygdala in the control of sodium intake

Lateral parabrachial nucleus and opioid mechanisms of the central nucleus of the amygdala in the control of sodium intake

•CeA facilitatory and LPBN inhibitory mechanisms interact to control NaCl intake.•Naloxone in the CeA blocks NaCl intake by euhydrated rats with muscimol into the LPBN.•Naloxone in the CeA blocks NaCl intake by hyperosmotic rats with LPBN moxonidine.•Opioids in the CeA are important for sodium intak...

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Veröffentlicht in:Behavioural brain research 2017-01, Vol.316, p.11-17
Hauptverfasser: Andrade-Franzé, Gláucia M.F., Gasparini, Silvia, De Luca, Laurival A., De Paula, Patrícia M., Colombari, Débora S.A., Colombari, Eduardo, Andrade, Carina A.F., Menani, José V.
Format: Artikel
Sprache:eng
Schlagworte:
Adrenergic receptors
Analgesics, Opioid - metabolism
Animals
Antihypertensive Agents - pharmacology
Central Amygdaloid Nucleus - drug effects
Central Amygdaloid Nucleus - physiology
Dehydration
Drinking - drug effects
Drinking - physiology
GABA
GABA-A Receptor Agonists - pharmacology
Imidazoles - pharmacology
Male
Muscimol - pharmacology
Naloxone - pharmacology
Narcotic Antagonists - pharmacology
Neural Pathways - drug effects
Neural Pathways - physiology
Opioid receptors
Parabrachial Nucleus - drug effects
Parabrachial Nucleus - physiology
Rats
Rats, Sprague-Dawley
Sodium - metabolism
Sodium appetite
Sodium, Dietary
Thirst
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Zusammenfassung:•CeA facilitatory and LPBN inhibitory mechanisms interact to control NaCl intake.•Naloxone in the CeA blocks NaCl intake by euhydrated rats with muscimol into the LPBN.•Naloxone in the CeA blocks NaCl intake by hyperosmotic rats with LPBN moxonidine.•Opioids in the CeA are important for sodium intake induced by LPBN deactivation.•Connection between LPBN and CeA mechanisms may depend on opioids action in the CeA. Facilitatory and inhibitory mechanisms in the central nucleus of the amygdala (CeA) and the lateral parabrachial nucleus (LPBN), respectively, are important for the control of sodium and water intake. Here we investigated the importance of the opioid mechanisms in the CeA for water and 0.3M NaCl intake in euhydrated or hyperosmotic rats treated with injections of muscimol (GABAA agonist) or moxonidine (α2 adrenergic/imidazoline agonist) into the LPBN, respectively. Male Holtzman rats (n=4–8/group) with stainless steel cannulas implanted bilaterally in the CeA and in the LPBN were used. The ingestion of 0.3M NaCl and water by euhydrated rats treated with muscimol (0.5nmol/0.2μl) into the LPBN (29.4±2.7 and 15.0±2.4ml/4h, respectively) was abolished by the previous injections of naloxone (opioid antagonist, 40μg/0.2μl) into the CeA (0.7±0.3 and 0.3±0.1ml/4h, respectively). The ingestion of 0.3M NaCl by rats treated with intragastric 2M NaCl (2ml/rat) combined with moxonidine (0.5nmol/0.2μl) into the LPBN (17.0±3.8ml/2h) was also strongly reduced by the previous injections of naloxone into the CeA (3.2±2.5ml/2h). Sucrose intake was not affected by naloxone injections into the CeA, which minimized the possibility of non-specific inhibition of ingestive behaviors with this treatment. The present results suggest that opioid mechanisms in the CeA are essential for hypertonic NaCl intake when the LPBN inhibitory mechanisms are deactivated or attenuated with injections of muscimol or moxonidine in this area.
ISSN:0166-4328
1872-7549
DOI:10.1016/j.bbr.2016.08.035