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CARBON MONOXIDE A novel neurotransmitter Prabhat kumar Padhi V-2005-30-12 M.V.Sc. Student Dept of Pharmacology & Toxicology College of Veterinary & Animal Sciences CSKHPKV, Palampur. Carbon monoxide & neurotransmission ?!$%@?.
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CARBON MONOXIDEA novel neurotransmitterPrabhat kumar PadhiV-2005-30-12M.V.Sc. StudentDept of Pharmacology & ToxicologyCollege of Veterinary & Animal SciencesCSKHPKV, Palampur
Carbon monoxide & neurotransmission ?!$%@? The word carbon monoxide brings to our mind the thought of a heavily polluted world, deaths of unsuspicious people inside closed rooms and all the bad names that it has earned until now.
Even more interesting is the possibility that this highly toxic molecule may act as a transmitter in the nervous system! • This discovery was triggered by the elucidation of the neurotransmitter role of the more toxic Nitrogen monoxide (NO). • Recent advances in the neuroscience field have suggested diverse roles for CO in the nervous system.
Brief history of toxic CO • In Greek and roman times the role of carbon monoxide as a poisonous gas was Known. It was used for executions. • Claude Bernard first described the mechanism of toxicity of CO in 1857. • In 1927 the effect of CO on tissue uptake of O2 was demonstrated. • Warburg used yeast tissue cultures to show that cellular uptake of O2 was decreased by large doses of CO.
Brief history of neurotransmitter CO • 1952 Sjöstrand reported the endogenous synthesis of CO. • 1968 heme oxygeanse was identified. • Mid 1980 isoforms of HO were discovered. • 1993 role of CO as neurotransmitter by Verma et al. • In 1997 HO3 was discovered.
Brief history of neurotransmitter CO • On the right is the photograph of Solomon H. Snyder (Johns Hopkins University School of Medicine). • He is one among the foremost authorities in this field.
Mechanism of toxicity • 210 times more affinity for Hb than O2. • Oxyhemoglobin dissociation curve shifted to left. • Decreases tissue uptake of O2. • Decreases function of cytochromeP450
Signs of toxicity • Colorless, odourless gas not detected by human senses. • Low conc- cardiovascular and neurobehavioural effects • High conc- coma and death • Treatment hyperbaric O2. (Haldane 1895)
Synthesis of CO • For the endogenous synthesis of CO heme is the substrate. • Also required for this process are • NADPH • cytochrome P450 • enzyme heme oxygenase (HO). • Endogenous heme is localized in neurons. In fact heme is synthesized in every nucleated cell of the body.
Synthesis of CO There are 3 isoforms of HO • HO1 (inducible), found in many tissues like lungs, spleen ageing RBC etc. • HO2 (constitutive) found in brain, neurons in GIT, blood , testes. • HO3 (constitutive) found in rats. It does not have potent enzymatic activity
Regulation of HO1 Transcriptionally upregulated by • Synergistic induction. Induction and function of HO1 parallels with physiological activity of a given stimulus. Ex: IL-1, Caffeic acid, Curcumine • Antagonistic induction of HO1 is to counteract the action of the stimuli in a feed back mechanism. Ex: Serum, Angiotensin
mGluR1 Phosphorylation C. Calcium-calmodulin Regulation of HO2
Fate of endogenous Carbon monoxide in the body Endogenously produced CO is removed by the following means • Expiration • Scavenging • Oxidation
Work on Olfactory receptor neurons HO inhibitors reduce basal cGMP levels & block generation of cGMP in response to odorants in the olfactory receptor neurons. This presents the strongest evidence favoring the role of CO in the nervous system. Findings that support role of CO as a neurotransmitter
Other findings Hyperpolarizing factor in the GIT • HO2 null mice have depolarized smooth muscle cells and the membrane potential in the gut is abolished. • Regions of the canine GIT that are more hyperpolarized generate more CO and exhibit more HO2 activity. • Genomic deletion of biosynthetic enzymes, Antiserum against HO, inhibition of enzyme HO have also demonstrated the possible roles of CO as a neurotransmitter.
Localization of HO2 HO2 is extensively localised in • Olfactory bulb, Hippocampus area • Gastrointestinal tract. • Genitourinary tract • Blood vessels, Glomus cells of carotid body • Trachea
Targets of CO • Soluble Guanylyl cyclase (sGC) • Ion channels • K+ Channels (KCa and KATP) • Na+ channels • Ca2+ channels • Hemoprotein targets and others • P38 MAPK
Physiological roles In the circulatory system • Carbon monoxide mediates endothelial derived vasorelaxation. • It acts in concert with NO in inducing vasorelaxation.
Physiological role Urogenital system • HO2 occurs throughout the autonomic nervous system. HO2 neuronal staining occurs in the pelvic ganglion and nerve fibers that innervate the bulbospongiosus and related muscles. • CO also plays a role in micturition. It is localised in detrussor muscle of bladder, urethral sphincter.
Physiological role Gastrointestinal tract • HO2 activity is prominent in internal anal sphincter area. • Also prominent in the myenteric plexus. • Also in the Interstitial cells of Cajal (ICC), the pace maker of the small intestine. • Also found in ganglionic cells located near islets of Langerhans and in liver.
CO plays a role in NANC transmission in the GIT. • Role in pacemaker activity,choleresis, insulin release. • It is an endogenous hyperpolarizing factor in the GIT. • It mediates the VIP associated NANC neurotransmission
Physiological role In the nervous system CO plays roles in the following functions • Odor response • Vision • Hearing • Thermal regulation • Nociception • Chemoreception • LTP, memory
Physiological role Hormones • Mediates release of GnRH, Neuropeptide Y from hypothalamus. • Release of Insulin from islets of Langerhans. Neuromuscular junction • The presence of HO2 immunoreactivity in the rat neuromuscular junction suggests that it may act as a post and pre-synaptic neurotransmitter in the NMJ.
Physiological role Circadian rhythm • CO acts on NPAS2 a mammalian transcription factor that regulates circadian rhythm. • It has also been linked to the suprachiasmatic nucleus in the brain. • CO has gotantiinflamatory(acts on COX) andanti-apoptoticactivities. These activities can be exploited in preventing graft rejection.
Cotransmission with NO CO and NO act together additively in the • Gastrointestinal system • Nervous system • Genitourinary system Many of the functions of NO are dependent upon the presence of CO.
Pathophysiology Neurodegeneration and brain disorders • HO/CO system has been implicated in various neurodegenerative diseases like • Alzheimer's disease • Parkinson's disease • Amyotrophic lateral sclerosis • This system has also been found altered in seizure disorders.
Pathophysiology CO in cardiovascular pathophysiology • Hypertension In hypertension CO/HO system plays a role in following conditions • Hypertension induced by HO inhibitors • Spontaneously hypertensive rats • Salt induced hypertension • Angiotensin-II induced hypertension • Renovascular hypertension • Portal hypertension • Cardiac hypertrophy and heart failure
Pathophysiology In addition role of CO/HO system can be traced to disorders like • Neurotoxicity • Genitourinary diseases • GIT disorders
Pathophysiology • Carbon monoxide in transplantation • Survival of Allograft • Survival of Xenograft • Carbon monoxide in apoptosis and cell proliferation • Vascular smooth muscles • Endothelial cells • Other types of cell
Therapeutic applications of carbon monoxide Carbon monoxide can be applied for therapeutic purposes by • Up regulation of enzyme HO • Down regulation of enzyme HO • Inhalation of CO • Use of CO releasing compounds • Use of prodrugs to release CO
Roles for future • Prevention of graft rejection • Fight against inflammation • Correction of hypertension and lung diseases. • Treatment of diseases of urogenital system. • Treatment of GIT diseases (Irritable bowel syndrome)
