Enzymatically derived NO and extracellular ATP are receiving greater attention due to their role as messengers in the CNS during different physiological and pathological processes. Ionotropic (P2XR) and metabotropic (P2YR) purinergic receptors mediate ATP effects and are present throughout the body. Particularly P2XR are crucial for brain plasticity mechanisms, and are involved in the pathogenesis of different CNS illnesses. NO does not have a specific receptor and its actions are directly dependent on the production on demand by different nitric oxide synthase isoforms. NO synthesizing enzymes are present virtually in all tissues, and NO influences multifarious physiological and pathological functions. Interestingly, various are the tissue and organs modulated by both ATP and NO, such as the immune, brain and vascular systems. Moreover, direct interactions between purinergic and nitrergic mechanisms outside the CNS are well documented, with several studies also indicating that ATP and NO do participate to the same CNS functions. In the past few years, further experimental evidence supported the physiological and pathological relevance of ATP and NO direct interactions in the CNS. The aim of the present review is to provide an account of the available information on the interplay between purinergic and nitrergic systems, focussing on the CNS. The already established relevance of ATP and NO in different pathological processes would predict that the knowledge of ATP/NO cross-talk mechanisms would support pharmacological approaches toward the development of novel ATP/NO combined pharmacological agents. (C) 2007 Elsevier Ltd. All rights reserved.

Florenzano, F., Viscomi, M.t., Amadio, S., D'Ambrosi, N., Volonté, C., Molinari, M. (2008). Do ATP and NO interact in the CNS?. PROGRESS IN NEUROBIOLOGY, 84(1), 40-56 [10.1016/j.pneurobio.2007.10.004].

Do ATP and NO interact in the CNS?

Viscomi, M T;Amadio, S;D'Ambrosi, N;
2008-01-01

Abstract

Enzymatically derived NO and extracellular ATP are receiving greater attention due to their role as messengers in the CNS during different physiological and pathological processes. Ionotropic (P2XR) and metabotropic (P2YR) purinergic receptors mediate ATP effects and are present throughout the body. Particularly P2XR are crucial for brain plasticity mechanisms, and are involved in the pathogenesis of different CNS illnesses. NO does not have a specific receptor and its actions are directly dependent on the production on demand by different nitric oxide synthase isoforms. NO synthesizing enzymes are present virtually in all tissues, and NO influences multifarious physiological and pathological functions. Interestingly, various are the tissue and organs modulated by both ATP and NO, such as the immune, brain and vascular systems. Moreover, direct interactions between purinergic and nitrergic mechanisms outside the CNS are well documented, with several studies also indicating that ATP and NO do participate to the same CNS functions. In the past few years, further experimental evidence supported the physiological and pathological relevance of ATP and NO direct interactions in the CNS. The aim of the present review is to provide an account of the available information on the interplay between purinergic and nitrergic systems, focussing on the CNS. The already established relevance of ATP and NO in different pathological processes would predict that the knowledge of ATP/NO cross-talk mechanisms would support pharmacological approaches toward the development of novel ATP/NO combined pharmacological agents. (C) 2007 Elsevier Ltd. All rights reserved.
gen-2008
Pubblicato
Rilevanza internazionale
Articolo
Esperti anonimi
Settore BIO/10 - BIOCHIMICA
English
purinergic receptor
nitric oxide synthase
brain injury
neuron-glia interactions
Florenzano, F., Viscomi, M.t., Amadio, S., D'Ambrosi, N., Volonté, C., Molinari, M. (2008). Do ATP and NO interact in the CNS?. PROGRESS IN NEUROBIOLOGY, 84(1), 40-56 [10.1016/j.pneurobio.2007.10.004].
Florenzano, F; Viscomi, Mt; Amadio, S; D'Ambrosi, N; Volonté, C; Molinari, M
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2108/324748
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