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Drugs Affecting the Central Nervous System

Drugs Affecting the Central Nervous System. Disease states of Central Nervous System. Typically caused by too much, or too little neurotransmission Too much Hyperexcitable neurons fire in absence of stimuli (e.g. seizure disorders)

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Drugs Affecting the Central Nervous System

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  1. Drugs Affecting the Central Nervous System

  2. Disease states of Central Nervous System • Typically caused by too much, or too little neurotransmission • Too much • Hyperexcitable neurons fire in absence of stimuli (e.g. seizure disorders) • Too many neurotransmitter molecules binding to post-synapse receptors • psychoses

  3. Too little • Too few neurotransmitters binding to post-synapse receptors

  4. Major Parts of the Brain • Cerebrum • Brainstem • Cerebellum

  5. Cerebrum • Largest and uppermost part of the brain • Divided into right and left hemispheres • Controls all the higher intellectual and motor functions of the body • Cerebrum composed of an outer cortex and an inner medulla

  6. Cerebral Cortex • Contains neuronal cell bodies (gray matter) that control all voluntary activities of the body • Divided up into 4 lobes: frontal, parietal, temporal, and occipital, each controlling specific brain functions • Electroencephalogram (EEG) is a recording of the electrical activity of the cortex

  7. Cerebral Medulla • Referred to as the “white matter” and is composed of myelinated nerve axons • Functions to conduct nerve impulses to and from different parts of the nervous system • Basal ganglia are neuronal cell bodies (gray matter) located within the cerebral medulla that function in the regulation of motor activity

  8. Brainstem and Spinal Cord • Located below the cerebrum and is continuous with the spinal cord • Brainstem divided into the thalamus, hypothalamus, pons, and medulla oblongata • Spinal cord is a collection of all the sensory and motor nerves going to and from the brain

  9. Reticular Formation • A network of nerves and brain areas involved in regulating alertness, wakefulness, and sleep • Composed of both inhibitory and excitatory nerves • Excitatory nerves collectively referred to as the reticular activating system (RAS) • Many stimulants (amphetamines) and depressants (alcohol, barbiturates) affect the RAS

  10. Limbic System • Network of nerves and brain areas involved in emotional and behavioral responses • Associated with emotional responses to fear, anger, anxiety, sexual behavior, and reward and punishment • Affected by drugs of abuse and involved in the development of drug dependency

  11. Neurotransmitters

  12. Norepinephrine • Adrenergic hormone released at the effector organ by sympathetic neurons • Monamine • Depression thought be caused by impaired monoamine transmission • Drugs that stimulate monoamine release are indicated for ADD or narcolepsy

  13. Dopamine • Another monoamine derived from the amino acid tyrosine • Binds dopamine receptors (D1 or D2) • Antipsychotics prevent signals activated by dopamine binding • Parkinson’s disease also caused by altered dopamine binding

  14. Serotonin (5-HT) • Monoamine hormone derived from the amino acid tryptophan • Typically released by inhibitory neurons • Lysergic acid diethylamide binds to serotonin receptors • Depression, ADD and headaches associated with serotonin imbalance

  15. Gamma-amino butyric acid (GABA) • Inhibitory neurotransmitter of the brain and central nervous system • Synthesized from the amino acid glutamate • Cause Ca2+ influx into the neuron resulting in hyperpolarization • More difficult to excite • Benzodiazepines and barbituates enhance GABA effects

  16. Excitatory Amino Acids • Amino acid glutamate or structurally related chemicals • Important for learning and memory • Abnormal increased activity will result in toxicity • Alzheimers, ALS, stroke, Huntington’s

  17. Antidepressants

  18. Mental Depression • Exogenous or reactive depression usually occurs in response to some external factor or adverse life event • Endogenous depression usually originates from within the psyche of the individual and the causes are less well understood • Bipolar mood disorder involves alternating cycles of depression and mania

  19. Causes of Mental Depression • Exact causes not well understood • Mental depression appears to involve the development of low levels of the brain monoamine neurotransmitters, serotonin (SER) and norepinephrine (NE) • This explanation is referred to as the “Monoamine Theory of Mental Depression”

  20. Treatment of Depression • Treatment involves a combination of psychotherapy and antidepressant drugs • Antidepressant drugs act to increase NE and SER levels in the brain • Tricyclic antidepressants (TCA) and selective serotonin reuptake inhibitors (SSRI) are the two most important antidepressant drug classes • Monoamine oxidase inhibitors (MAOI) are less frequently used and require dietary restriction

  21. Monoamine Oxidase Inhibitors (MAOI) • Monoamine oxidase is the enzyme that metabolizes the monoamines NE and SER • Inhibition of MAO increases SER and NE levels and functional activity in the brain • Requires 2–4 weeks for maximum effects • Foods containing tyramine must be avoided • Tyramine stimulates the release of NE and may cause a hypertensive crisis • MAOIs are indicated for patients who cannot tolerate TCAs and SSRIs

  22. Tricyclic Antidepressants (TCA) • Mechanism of action of TCAs is to block reuptake of NE and SER into nerve endings • Blockage of reuptake increases NE and SER levels and stimulation of NE and SER receptors • Requires 2–4 weeks for maximum effect • TCAs are divided into secondary amines which increase NE more than SER and are less sedating than tertiary amines which increase SER more than NE

  23. Autonomic Effects of TCAs • TCAs possess anticholinergic activity which can cause dry mouth, visual disturbances, constipation, and urinary retention • TCAs also possess alpha blocking activity that can lower blood pressure • TCAs can also affect cardiac rhythm and may cause cardiac arrhythmias

  24. Selective Serotonin Reuptake Inhibitors (SSRI) • Selectively block the reuptake of SER • Cause little if any anticholinergic and alpha blocking effects • Are generally not sedating, and in some cases cause CNS stimulation • Common adverse effects include nausea, agitation, restlessness, and less frequently seizures

  25. Psychomotor Stimulants • Generally referred to as the amphetamines • Produce CNS stimulation more than an antidepressant effect, little used for depression • Act by increasing NE and DA activity • Clinical use for narcolepsy and treatment of hyperkinetic children • Amphetamines have a high abuse potential • Adverse effects due to excessive CNS and autonomic stimulation

  26. Lithium • Lithium is an elemental ion similar to sodium • Acts to depress nerve excitability that helps prevent mood swings and manic behavior • Common adverse effects include nausea, diarrhea, tremors, increased thirst, ringing in the ears (tinnitis), and more seriously kidney and heart damage • Periodic blood levels to prevent overdosage

  27. Sedatives and Hypnotics • Sedatives are drugs used to induce a mild state of CNS depression characterized by both mental and physical calmness • Hypnotics are drugs used to induce and maintain sleep • The same drugs are used to induce both sedation and hypnosis; however, the dosage for inducing sedation is lower

  28. Classification of Sedative- Hypnotic Drugs • Barbiturates – a drug family of chemically similar drugs with similar actions and features • Benzodiazepines – a drug family of chemically similar drugs with similar actions and features • Miscellaneous nonbarbiturates – a group of drugs with dissimilar chemical structures and pharmacologic features

  29. Pharmacology of Barbiturates • Drugs classified as short, intermediate, and long-acting sedative-hypnotics • At low doses they increase the inhibitory effects of GABA • At high doses they act like general anesthetics, and can cause profound CNS depression and death in overdosage • Barbiturates are also anticonvulsants

  30. Effects of Barbiturates on the Sleep Cycle • Decrease stage 1, falling asleep • Increase stage 2, a lighter stage of sleep • Decrease stages 3 and 4 referred to as deep sleep or slow-wave sleep • Decrease REM sleep, and may cause REM rebound

  31. Adverse Features of Barbiturates • Cause drug tolerance with chronic use and drug dependency with abuse • Can cause a severe type of physical drug addiction when chronically abused • The withdrawal reaction from barbiturates can be serious, resulting in convulsions and death • Drug interactions, induce microsomal enzymes to increase the rate of drug metabolism of all drugs metabolized by the microsomal enzymes

  32. Pharmacology of Benzodiazepines • Drugs classified as short, intermediate, and long-acting sedative-hypnotics • Drugs also produce antianxiety, skeletal muscle relaxing, and anticonvulsant effects • Act by increasing the inhibitory effects of GABA • Drugs do not induce the drug metabolizing microsomal enzymes

  33. Effect of Benzodiazepines on the Sleep Cycle • Decrease stage 1, falling asleep • Increase stage 2 • Decrease stages 3 and 4 • Do not significantly decrease REM sleep • Benzodiazepines are considered safer drugs than the barbiturates, especially in overdosage

  34. Miscellaneous Nonbarbiturates • Zolpidem and zaleplon are short-acting hypnotics that do not disrupt the sleep cycle • These drugs increase the inhibitory effects of GABA but differently than other drugs • Both drugs are considered to be safer than other hypnotics and are at low risk for abuse • Side effects include dizziness, headache, GI disturbances, and mental confusion

  35. Alcohol • Classified as a CNS depressant drug • Unlike other drugs, alcohol provides nutritional calories • Like other drugs of abuse, alcohol causes development of drug tolerance, dependency, and withdrawal reactions • Most of the pharmacology of alcohol centers around its chronic use, abuse, and toxicology

  36. Disulfiram • Used to treat alcoholism and deter drinking • Disulfiram inhibits metabolism of alcohol, allowing acetaldehyde to accumulate • Increased acetaldehyde produces severe nausea, vomiting, headache, and hypotension • Alcoholics take the drug on a daily basis, knowing that if they drink any alcohol they will become violently ill

  37. Parkinson’s Disease • A neurological movement disorder of the brain involving the basal ganglia • Symptoms include tremor, muscular rigidity, and disturbances of movement • Major cause is a deficiency of the inhibitory neurotransmitter dopamine (DA) and the resulting excessive activity of the excitatory neurotransmitter acetylcholine (ACH)

  38. Drug Therapy • Primary therapy is the administration of drugs that increase the levels of DA in the basal ganglia • Secondary therapy is the administration of anticholinergic drugs that decrease ACH activity in the basal ganglia • Goal is to restore the balance between DA and ACH activity

  39. Drugs that Increase Dopamine • Levodopa • Dopamine agonists • Amantadine • Enzyme inhibiting drugs that slow the metabolic breakdown of dopamine

  40. Levodopa • The precursor of DA that is taken orally and converted into DA in the basal ganglia • Administered in combination with carbidopa that increases the amount of DA that enters the brain • Levodopa and carbidopa drug combination known as Sinemet • Levodopa is considered the most effectivedrug for the treatment of Parkinson’s disease

  41. Adverse Effects of Levodopa • Nausea, vomiting, and loss of appetite • Hypotension, and rapid/irregular heart rate • Dystonias, slow or weak movements that usually occur when levels of DA are low • Dyskinesias, uncontrolled or involuntary movements when DA levels are too high • “On-off” phenomenon when drug effects suddenly increase or decrease due to fluctuating levels of DA in the basal ganglia • Behavioral and mental disturbances

  42. Dopamine Agonists • Drugs: bromocriptine, pergolide, pramipexole, and ropinirole • Stimulate DA receptors in the basal ganglia • Used alone or in combination with levodopa • Adverse effects similar to levodopa: nausea, hypotension, dyskinesias, and mental disturbances

  43. Amantadine (Symmetrel) • An antiviral drug that additionally increases the release of DA in the brain • Used in early stages of treatment and in combination with other drugs • Effectiveness usually decreases in 6–12 months • Adverse effects include nausea, mental disturbances, and occasionally skin discoloration

  44. Enzyme Inhibitors • Selegiline (Eldepryl) inhibits MAO-B enzyme that slows metabolism of DA in the brain, increases DA levels; used alone or with levodopa • Tolcapone (Tasmar) and entacapone (Comtan) inhibit another enzyme, COMT, that also slows metabolism of DA; usually used with levodopa

  45. Anticholinergic Drugs • Used to decrease the activity of ACH and restore the normal balance between DA and ACH • Benztropine (Cogentin)and trihexyphenidyl (Artane) most widely used drugs • Antihistamine drugs, diphenhydramine (Benadryl), with high anticholinergic activity occasionally used • Used alone early in treatment or in combination with other drugs

  46. Central Analgesics

  47. Clinical Indication Produce a state of unconsciousness to prevent painful stimulation during surgical and dental procedures Types of anesthetics • Inhalation gases & volatile liquids: chloroform, halothane, nitrous oxide • Injectable: fentanyl, ketamine, midazolam, propofol

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