Objective: Several melanocortin peptides have a prompt and sustained resuscitating effect in conditions of hemorrhagic shock. The transcription nuclear factor kB (NF-kB) triggers a potentially lethal systemic inflammatory response, with marked production of tumor necrosis factor-alpha (TNF-alpha), in hemorrhagic shock. Here we investigated whether the hemorrhagic shock reversal produced by the melanocortin ACTH-(1-24) (adrenocorticotropin) depends on the activation of the recently recognized, vagus nerve-mediated, brain cholinergic anti-inflammatory pathway. Methods and results: Anesthetized rats were stepwise bled until mean arterial pressure (MAP) atabilized at 20-25 turn Hg. The severe hypovolemia was incompatible with survival, and all saline-treated animals died within 30 min. In rats intravenously (i.v.) treated with ACTH-(1-24), neural efferent activity along vagus nerve (monitored by means of a standard system for extracellular recordings) was markedly increased, and the restoration of cardiovascular and respiratory functions was associated with blunted NF-kB activity and with decreased TNF-alpha mRNA liver content and TNF-alpha plasma levels. Bilateral cervical vagotomy, pretreatment with the melanocortin MC4 receptor antagonist HS014, atropine sulfate or chlorisondamine, but not with atropine methylbromide, prevented the life-saving effect of ACTH-(1-24) and the associated effects on NF-kB activity and TNF-alpha levels. HS014 and atropine sulfate prevented, too, the ACTH-(1-24)-induced increase in neural efferent vagal activity, and accelerated the evolution of shock in saline-treated rats. Conclusions: The present data show, for the first time, that the melanocortin ACTH-(I -24) suppresses the NF-kB-dependent systemic inflammatory response triggered by hemorrhage, and reverses shock condition, by brain activation (in real-time) of the cholinergic anti-inflammatory pathway, this pathway seeming to be melanocortin-dependent. (C) 2004 European Society of Cardiology. Published by Elsevier B.V. All rights reserved.
Adrenocorticotropin reverses hemorrhagic shock in anesthetized rats through the rapid activation of a vagal anti-inflammatory pathway / Guarini, Salvatore; Cainazzo, Maria Michela; Giuliani, Daniela; Mioni, Chiara; D., Altavilla; H., Marini; Bigiani, Albertino; Ghiaroni, Valeria; M., Passaniti; Leone, Sheila; Bazzani, Carla; Ap, Caputi; F., Squadrito; Bertolini, Alfio. - In: CARDIOVASCULAR RESEARCH. - ISSN 0008-6363. - STAMPA. - 63:(2004), pp. 357-365. [10.1016/j.cardiores.2004.03.029]
Adrenocorticotropin reverses hemorrhagic shock in anesthetized rats through the rapid activation of a vagal anti-inflammatory pathway
GUARINI, Salvatore;CAINAZZO, Maria Michela;GIULIANI, Daniela;MIONI, Chiara;BIGIANI, Albertino;GHIARONI, Valeria;LEONE, Sheila;BAZZANI, Carla;BERTOLINI, Alfio
2004
Abstract
Objective: Several melanocortin peptides have a prompt and sustained resuscitating effect in conditions of hemorrhagic shock. The transcription nuclear factor kB (NF-kB) triggers a potentially lethal systemic inflammatory response, with marked production of tumor necrosis factor-alpha (TNF-alpha), in hemorrhagic shock. Here we investigated whether the hemorrhagic shock reversal produced by the melanocortin ACTH-(1-24) (adrenocorticotropin) depends on the activation of the recently recognized, vagus nerve-mediated, brain cholinergic anti-inflammatory pathway. Methods and results: Anesthetized rats were stepwise bled until mean arterial pressure (MAP) atabilized at 20-25 turn Hg. The severe hypovolemia was incompatible with survival, and all saline-treated animals died within 30 min. In rats intravenously (i.v.) treated with ACTH-(1-24), neural efferent activity along vagus nerve (monitored by means of a standard system for extracellular recordings) was markedly increased, and the restoration of cardiovascular and respiratory functions was associated with blunted NF-kB activity and with decreased TNF-alpha mRNA liver content and TNF-alpha plasma levels. Bilateral cervical vagotomy, pretreatment with the melanocortin MC4 receptor antagonist HS014, atropine sulfate or chlorisondamine, but not with atropine methylbromide, prevented the life-saving effect of ACTH-(1-24) and the associated effects on NF-kB activity and TNF-alpha levels. HS014 and atropine sulfate prevented, too, the ACTH-(1-24)-induced increase in neural efferent vagal activity, and accelerated the evolution of shock in saline-treated rats. Conclusions: The present data show, for the first time, that the melanocortin ACTH-(I -24) suppresses the NF-kB-dependent systemic inflammatory response triggered by hemorrhage, and reverses shock condition, by brain activation (in real-time) of the cholinergic anti-inflammatory pathway, this pathway seeming to be melanocortin-dependent. (C) 2004 European Society of Cardiology. Published by Elsevier B.V. All rights reserved.
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