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Chemical transmission in the central nervous system

Chemical transmission in the central nervous system. Chemical transmission in the CNS. The basic processes of synaptic transmission in the CNS are essentially similar to those operating in the periphery

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Chemical transmission in the central nervous system

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  1. Chemical transmission in the central nervous system

  2. Chemical transmission in the CNS • The basic processes of synaptic transmission in the CNS are essentially similar to those operating in the periphery • Glial cells, particularly astrocytes, participate actively in chemical signalling, functioning essentially as 'inexcitable neurons'.

  3. The terms neurotransmitter, neuromodulator and neurotrophic factor refer to chemical mediators that operate over different timescales. In general: neurotransmitters are released by presynaptic terminals and produce rapid excitatory or inhibitory responses in postsynaptic neurons neuromodulators are released by neurons and by astrocytes and produce slower pre- or postsynaptic responses neurotrophic factors are released mainly by non-neuronal cells and act on tyrosine-kinase-linked receptors, which regulate gene expression, and control neuronal growth and phenotypic characteristics.

  4. Neurotransmitters fast neurotransmitters, operating through ligand-gated ion channels (e.g. glutamate, GABA) . slow neurotransmitters and neuromodulators operate mainly through G-protein-coupled receptors (e.g. dopamine, neuropeptides, prostanoids).

  5. The same agent (e.g. glutamate, 5-HT (5-hydroxytryptamine), acetylcholine) may act through both ligand-gated channels and G-protein-coupled receptors. Many chemical mediators, including glutamate, nitric oxide and arachidonic acid metabolites, are produced by glia as well as neurons. Many other mediators (e.g. cytokines, chemokines, growth factors, steroids) control long-term changes in the brain (e.g. synaptic plasticity, remodelling, etc.), mainly by affecting gene transcription

  6. Drug action in the CNS • The basic types of drug target (ion channels, receptors, enzymes and transporter proteins) apply in the CNS as elsewhere. • Most of these targets occur in many different molecular isoforms, the functional significance of which is, in most cases, unclear. • Many of the currently available neuroactive drugs are relatively non-specific, affecting several different targets, the principal ones being receptors, ion channels and transporters. • The relationship between the pharmacological profile and the therapeutic effect of neuroactive drugs is often unclear. • Slowly developing secondary responses to the primary interaction of the drug with its target are often important (e.g. the delayed efficacy of antidepressant drugs, tolerance and dependence with opiates, etc.).

  7. METABOLISM AND RELEASE OF AMINO ACIDS

  8. Transport of glutamate (Glu) and glutamine (Gln) by neurons and astrocytes. Released glutamate is captured partly by neurons and partly by astrocytes, which convert it to glutamine. Astrocytes release glutamine via a transporter, and neurons take it up and synthesise glutamate.

  9. Main sites of drug action on NMDA and GABAA-receptors

  10. SYNAPTIC PLASTICITY Synaptic plasticity is a general term to describe long-term changes in synaptic connectivity and efficacy, either following physiological alterations in neuronal activity (as in learning and memory) or resulting from pathological disturbances (as in epilepsy, chronic pain or drug dependence)..

  11. Broadly speaking, synaptic plasticity underlies much of what we call 'brain function', and understanding how it happens has been a holy grail for neurobiologists for decades. Needless to say, no single mechanism is responsible for the many phenomena that fall within the term; however, the discovery of long-term potentation (LTP), and the central role of glutamate and NMDA-receptors, represents a big step forward

  12. Excitatory amino acids (EAAs) EAAs, namely glutamate, aspartate, and possibly homocysteate, are the main fast excitatory transmitters in the CNS. Glutamate is formed mainly from the tricarboxylic acid cycle intermediate α-oxoglutarate, by the action of GABAaminotransferase .

  13. There are four main EAA receptor subtypes • NMDA • AMPA • kainate • metabotropic

  14. NMDA-, AMPA- and kainate-receptors are ionotropic receptors regulating cation channels; metabotropic receptors are G-protein-coupled receptors and act through intracellular second messengers. There are many molecular subtypes within each class. • The channels controlled by NMDA-receptors are highly permeable to Ca2+ and are blocked by Mg2+.

  15. AMPA- and kainate-receptors are involved in fast excitatory transmission; NMDA-receptors mediate slower excitatory responses and, through their effect in controlling Ca2+ entry, play a more complex role in controlling synaptic plasticity (e.g. long-term potentiation).

  16. Competitive NMDA-receptor antagonists include AP5 and other experimental compounds; the NMDA-operated ion channel is blocked by dizocilpine, as well as by the psychotomimetic drugs ketamine and phencyclidine. • CNQX is a selective AMPA receptor antagonist

  17. NMDA-receptor activation is increased by endogenous polyamines, such as spermine, acting on a modulatory site that is blocked by ifenprodil. • The entry of excessive amounts of Ca2+ produced by NMDA-receptor activation can result in cell death: excitotoxicity • Metabotropic receptors are G-protein-coupled receptors, linked to inositol trisphosphate formation and intracellular Ca2+ release. They play a part in glutamate-mediated synaptic plasticity and excitotoxicity. Specific agonists and antagonists are known. • EAA receptor antagonists have yet to be developed

  18. LTP (Bliss & Collingridge, 1993; Bennett, 2000) • is the term used to describe a long-lasting (hours in vitro, days or weeks in vivo) enhancement of synaptic transmission that occurs at various CNS synapses following a short (conditioning) burst of presynaptic stimulation, typically at about 100 Hz for 1 second. Its counterpart is long-term depression (LTD), which is produced by a longer train of stimuli at lower frequency.

  19. These phenomena have been studied in great detail in the hippocampus which plays a central role in learning and memory. It has been argued that 'learning', in the synaptic sense, can occur if synaptic strength is enhanced following simultaneous activity in both pre- and postsynaptic neurons. LTP shows this characteristic; it does not occur if presynaptic activity fails to excite the postsynaptic neuron, or if the latter is activated independently, for instance by different presynaptic input. Thus LTP initiation involves both the presynaptic and postsynaptic components, and it results from enhanced activation of AMPA-receptors at EAA synapses.

  20. The facilitatory process also appears to involve both pre- and postsynaptic elements ,the release of glutamate is increased, and so is the response of postsynaptic AMPA-receptors to glutamate. Increased expression and trafficking of AMPA-receptors to synaptic sites also occurs.

  21. learning and memory • Though LTP is well established as a synaptic phenomenon, its relationship to learning and memory remains controversial, though the evidence is suggestive. For example, NMDA-receptor antagonists applied to the hippocampus impair learning in rats; also, 'saturation' of LTP by electrical stimulation of the hippocampus has been found to impair the ability of rats to learn a maze.

  22. Furthermore, LTP-like changes have been detected after learning has taken place. Thus there is hope that drugs capable of enhancing LTP may improve learning and memory. LTP is just one manifestation of synaptic plasticity whereby neuronal connections respond to changes in the activity of the nervous system. Other phenomena, including short-term potentiation and LTD also occur, and they too appear to involve glutamate receptors

  23. AGONISTS AND POSITIVE MODULATORS • Various agonists at EAA-receptors that are theoretically are positive AMPA-receptor modulators, which act by reducing receptor desensitization, may improve memory and cognitive performance. Cyclothiazide acts in this way but is toxic; drugs such as piracetam and aniracetam, which are used in dementia,also sensitize AMPA-receptors, though it is not certain that this accounts for their psychotropic effects.

  24. GAMMA-AMINOBUTYRIC ACID

  25. GABA is the main inhibitory transmitter in the brain. In the spinal cord and brainstem, glycine is also important

  26. Inhibitory amino acids: GABA and glycine • GABA is the main inhibitory transmitter in the brain. • It is present fairly uniformly throughout the brain; there is very little in peripheral tissues. • GABA is formed from glutamate, by the action of GAD (glutamic acid decarboxylase). Its action is terminated mainly by reuptake, but also by deamination, catalysed by GABA transaminase.

  27. METABOLISM AND RELEASE OF AMINO ACIDS

  28. There are two types of GABA receptor, GABAA and GABAB. • GABAA-receptors, which occur mainly postsynaptically, are directly coupled to chloride channels, opening of which reduces membrane excitability. • Muscimol is a specific GABA agonist, and the convulsant bicuculline is an antagonist.

  29. Other drugs that interact with GABAA-receptors and channels include: • benzodiazepine tranquillizers, which act at an accessory binding site to facilitate the action of GABA • convulsants such as picrotoxin, which block the anion channel • neurosteroids, including endogenous progesterone metabolites, and other CNS depressants, such as barbiturates, which facilitate the action of GABA.

  30. GABAB receptors are G-protein-coupled receptors, linked to inhibition of cAMP formation. They cause pre- and postsynaptic inhibition by inhibiting calcium channel opening and increasing K+ conductance. Baclofen is a GABAB-receptor agonist used to treat spasticity. GABAB antagonists are not yet in clinical use.

  31. Glycine is an inhibitory transmitter mainly in the spinal cord, acting on its own receptor, structurally and functionally similar to the GABAA-receptor. • The convulsant drug strychnine is a competitive glycine antagonist. Tetanus toxin acts mainly by interfering with glycine release.

  32. Other transmitters and modulators

  33. Noradrenaline in the CNS • Mechanisms for synthesis, storage, release and reuptake of noradrenaline in the CNS are essentially the same as in the periphery, as are the receptors • Noradrenergic cell bodies occur in discrete clusters, mainly in the pons and medulla, one important such cell group being the locus ceruleus. • Noradrenergic pathways, running mainly in the medial forebrain bundle, and descending spinal tracts, terminate diffusely in the cortex, hippocampus, hypothalamus, cerebellum and spinal cord. • The actions of noradrenaline are mainly inhibitory (β-adrenoceptors), but some are excitatory (α- or β-adrenoceptors).

  34. Noradrenergic transmission is believed to be important in • the 'arousal' system, controlling wakefulness and alertness • blood pressure regulation • control of mood (functional deficiency contributing to depression). • Psychotropic drugs that act partly or mainly on noradrenergic transmission in the CNS include antidepressants, cocaine, amphetamine. Some antihypertensive drugs (e.g. clonidine, methyldopa ) act mainly on noradrenergic transmission in the CNS.

  35. Dopamine in the CNS • Dopamine is a neurotransmitter as well as being the precursor for noradrenaline. It is degraded in a similar fashion to noradrenaline, giving rise mainly to DOPAC and HVA , which are excreted in the urine. • There are three main dopaminergic pathways: • nigrostriatal pathway, important in motor control • mesolimbic/mesocortical pathways, running from groups of cells in the midbrain to parts of the limbic system, especially the nucleus accumbens, and to the cortex; they are involved in emotion and drug-induced reward systems • tuberohypophyseal neurons running from the hypothalamus to the pituitary gland, the secretions of which they regulate

  36. There are five dopamine receptor subtypes. D1- and D5-receptors are linked to stimulation of adenylate cyclase. D2-, D3- and D4-receptors are linked to inhibition of adenylate cyclase. Most known functions of dopamine appear to be mediated mainly by receptors of the D2 family. • Receptors of the D2 family may be implicated in schizophrenia. The D4-receptor shows marked polymorphism in humans. • Parkinson's disease is associated with a deficiency of nigrostriatal dopaminergic neurons.

  37. Behavioural effects of an excess of dopamine activity consist of stereotyped behaviour patterns and can be produced by dopamine-releasing agents (e.g. amphetamine) and dopamine agonists (e.g. apomorphine). • Hormone release from the anterior pituitary gland is regulated by dopamine, especially prolactin release (inhibited) and growth hormone release (stimulated). • Dopamine acts on the chemoreceptor trigger zone to cause nausea and vomiting.

  38. Thank you

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