Материал: MasterPass _ Pharmacology in 7 Days for Medical Students
PHARMACOLOGY IN 7 DAYS FOR MEDICAL STUDENTS
Table 3.1
Receptor activated |
Effects |
|
α2- GABAA → Inhibition of neuronal circuits in |
Reduction in anxiety (anxiolytic effect) |
|
the limbic system |
|
|
α2- GABAA → increased pre-synaptic |
Skeletal muscle relaxation |
|
inhibition in the spinal cord (at higher doses) |
|
|
α1- GABA A |
¥ |
Hypnosis (artiÞcially produced sleep) |
|
¥ |
Anterograde amnesia (temporary |
|
|
impairment of memory) |
|
¥ |
Anticonvulsant effect |
BDZs do not affect the autonomic nervous system. Also, they lack any antipsychotic or analgesic activity.
Local anaesthetics
As we know that Na+ influx is necessary for depolarisation to take place. It is also necessary for conduction of the wave of depolarisation. Local anaesthetics, by blocking the voltage-gated Na+ channels, block both generation and conduction of the action potential and in this way produce a membrane-stabilising effect.
Location of receptor sites: Local anaesthetics block the Na+ channels from the cytosolic side. They must, therefore, cross the lipid membrane and diffuse into the cytoplasm before they could reach their receptor sites in the Na+ channel.
Two forms of local anaesthetic molecules: Local anaesthetic molecules are available both in the nonionised (uncharged) and ionised (charged) forms. The nonionised molecules are more lipid-soluble and thus have greater ability to diffuse across the lipid membrane and reach effective intracellular concentrations within the cytoplasm. The ionised molecules, however, have greater affinity for the receptor sites. Thus availability of both the nonionised and ionised forms is important for the functioning of the local anaesthetics.
Effects of ECF K+ and Ca++ on local anaesthetic activity:
•↑ ECF K+ → ↑ local anaesthetic activity.
•↑ ECF Ca++ → ↓ local anaesthetic activity.
Order of loss of sensations: Autonomic sensations are lost first after local anaesthetic injection followed by pain, touch, vibration and deep pressure sensations (in this order) and finally motor activity.
The order of loss of sensations depends on:
1Diameter of the nerve fibres: Smaller fibres are blocked more easily than the larger fibres.
2Myelination of the nerve fibres: Myelinated fibres are blocked more easily than the unmyelinated fibres.
3Physiologic firing rate of the nerve fibres: Rapidly firing fibres are usually blocked before the slowly firing fibres.
Ketamine
Ketamine is a short-acting, non-barbiturate anaesthetic. It characteristically produces ‘dissociative anaesthesia’ in which patient appears to be awake but is immobile, doesn’t feel pain and is amnesic.
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MECHANISMS OF ACTION
Ketamine antagonises the actions of glutamic acid (an excitatory neurotransmitter) on the N-methyl-D-aspartate (NMDA) receptor. It also increases the central sympathetic outflow (→ bronchodilatation, ↑ cardiac output and ↑ BP). Because of this property, Ketamine is especially beneficial in cases of asthma and shock (cardiogenic; hypovolemic). Because of the same property it is not recommended in cases of hypertension and stroke.
Haloperidol
Haloperidol is a typical (traditional) neuroleptic agent used in the treatment of schizophrenia and other psychoses.
Dopamine hypothesis of schizophrenia: It appears that schizophrenia, at least in part, is caused by an excess of dopamine in the mesolimbic pathway of the brain (regulates mood and mentation).
Types of dopamine receptors: Five types of dopamine receptors have been identified (D1-D5). D1 and D5 receptors activate adenylyl cyclase, whereas, D2, D3 and D4 receptors inhibit adenylyl cyclase.
Table 3.2 Location of dopamine receptors
Location of dopamine |
Responsible for |
Effect of dopamine |
receptors |
|
receptor blockade |
Mesolimbic pathway |
Regulates mood and mentation |
Antipsychotic effect |
Nigrostriatal pathway |
Extrapyramidal function |
Extrapyramidal symptoms |
Tuberoinfundibular pathway |
Control of prolactin release |
Hyperprolactinemia |
Chemoreceptor trigger zone |
Emesis |
Anti-emetic effect |
|
|
|
Receptors affected by haloperidol:
1Haloperidol exerts its antipsychotic effect by primarily blocking the D2 receptors present in caudate, putamen, nucleus accumbens, cerebral cortex and hypothalamus.
2Antipsychotic effect is also in part produced by haloperidol-induced α1 receptor blockade.
3Many of the newer atypical antipsychotic agents also block 5-HT2, H1 and M
receptors. Haloperidol lacks effect on any of these receptors.
Antipsychotic effects of haloperidol: Haloperidol reduces the ‘positive’ symptoms of schizophrenia;1 it, however, has little effect on the ‘negative’ symptoms.2
Barbiturates
1There are multiple mechanisms of action of barbiturates at multiple sites in the brain. They act on GABAA receptor Cl– channel.
2Macromolecular complex.
3GABA-ergic at low doses, i.e. facilitation of action of GABA and prolongation of Cl– channels opening.
1 Positive symptoms of schizophrenia: hallucinations, delusions.
2Negative symptoms of schizophrenia: impaired attention, cognitive impairment, apathy, anhedonia (not getting pleasure from normally pleasurable stimuli).
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PHARMACOLOGY IN 7 DAYS FOR MEDICAL STUDENTS
4GABA-mimetic at high doses, i.e. directly activates Cl– channels.
5Barbiturates are less sedative in their action since they also depress the actions of excitatory neurotransmitters (NT), e.g. glutamic acid.
6Actions of excitatory NT, i.e. glutamic acid (at AMPA receptor subtype) depressed.
7Potentiation of inhibitory GABAA receptors.
8Inhibition of excitatory AMPA receptors leading to CND depressant effect.
9Higher concentration inhibits Ca++.
Carbamazepine
1Carbamazepine blocks voltage-dependent Na+ channels and inhibits the spread of discharge.
2Acts pre-synaptically to decrease the synaptic transmission.
3Post-synaptic actions of GABA may be potentiated.
4Also inhibits uptake and release of norepinephrine from the brain.
Phenytoin sodium
It is a membrane stabiliser and acts by:
1Decreasing the resting fluxes of Na+ ions as well as Na+ currents during the action potential.
2Decreasing the influx of Ca++ ions during depolarisation.
3Decreasing the efflux of K+ ions during action potential.
4Decrease in post-tetanic potentiation.
5Restoration of balance between excitatory glutamate and inhibitory GABA pathways.
6Decrease in the duration of after-discharge.
7Increase in the refractory period of the neurons.
8Causes stimulation of cerebellum, which in turn causes stimulation of inhibitory pathways from cerebellum to cerebral cortex.
The above-mentioned processes show that phenytoin sodium causes:
1A decrease in the development of maximal seizure activity from the epileptic focus.
2A decrease in the spread of seizure activity from an active focus.
Sodium valproate/valproic acid
GABA, which is the main inhibitory NT in the brain, is synthesised from glutamic acid (glutamate) in GABA-ergic neurons by an enzyme called glutamic acid decarboxylase. GABA is metabolised sequentially by GABA transaminase into succinic-semialdehyde, then into succinic acid by the enzyme succinic-semialdehyde dehydrogenase.
Main mechanism of action of sodium valproic is to raise GABA concentration in the CNS by inhibiting above-mentioned both enzymes responsible for the metabolism of GABA resulting in increased inhibition of neurons in the CNS. Sodium valproic also enhances GABA post-synaptic actions. It has a weak Na+ channels blocking effect and also causes small decrease in low threshold Ca++ channels.
Chlorpromazine (largactil)
It acts on a variety of CNS and peripheral receptors and causes:
1Post-synaptic dopamine (D2) receptor blockade.
25HT2A and 5HT2C serotinergic receptor blockade.
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MECHANISMS OF ACTION
3Muscarinic and ganglion receptor blockade.
4α1 adrenoceptor and H1 histaminic receptor blockade.
5Quinidine and local anaesthetic-like activity.
Effects on CNS
1 General psycho-physiological and behavioural effects:
aNeuroleptic syndrome: characterised by apathy and indifference, suppression of psychomotor and spontaneous activity, decreased hallucinations, decreased illusions, decrease in stereotype behaviour, decrease in incoherent thoughts
and suppression of conditioned avoidance behaviour (does not suppress unconditioned responses).
bCatalepsy: Cataleptic immobility means maintaining of abnormal posture in animals and humans.
c 5HT receptor blockade leads to disturbances in mood, behaviour and sleep.
2Effects on motor activity: Decreased spontaneous activity, extrapyramidal symptoms (Parkinsonism, acute dystonias, akathesias, tardive dyskinesia, perioral tremors [Rabbit syndrome]).
3Effects on chemoreceptor trigger zone (CTZ): It blocks CTZ in D2 receptor area in the medulla suppressing nausea and vomiting; hence used as anti-emetic.
4Hypothalamic and endocrine effects: By blocking α-1 receptors ADH, oestrogen, progesterone, corticosteroids and growth hormone levels are decreased.
Peripheral effects
1Effects on ANS: By blocking muscarinic receptors, atropine-like effects are seen, e.g. dryness of mouth, tachycardia, blurring of vision, etc.
2Effects on CVS:
aα-1 receptor blockade results in decreased blood pressure, decreased resting heart rate, vasodilatation and decrease in peripheral resistance (causing orthostatic hypotension).
bECG changes like ↑ QT-PT interval; flattening or notching of P wave; ST segment depression; ventricular tachycardia (VT) – caused by local anaesthetic effect; quinidine-like effects.
3Miscellaneous effects: Local anaesthetic effect; hypothermia; renal effects (e.g. ↓ ADH secretion → ↓ Na+ and Cl– absorption); hepatic effects (e.g. cholestatic jaundice because of swelling of canaliculi); antihistaminic like effects (e.g. sedation); skeletal muscle relaxant effect (no effect is produced on the neuromuscular junction).
Lithium carbonate
Effects on electrolytes and ion transport: Lithium is closely related to Na+ in its properties. It can substitute for Na+ in generating action potentials and in Na+-Na+ exchange across the membrane. It inhibits the latter process, i.e. Li-Na+ exchange is gradually slowed after lithium is introduced into the body. At therapeutic concentrations (around 1mmol/L), it does not significantly effect the Na+/Ca++ exchange process or Na+/K+ ATPase pump.
Effects on neurotransmitters: Lithium appears to enhance some of the actions of serotonin though findings have been contradictory. Its effects on norepinephrine are variable. The drug may decrease norepinephrine and dopamine turnover and these effects, if confirmed, might be relevant to its antimanic actions. Lithium also appears
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PHARMACOLOGY IN 7 DAYS FOR MEDICAL STUDENTS
to block the development of dopamine receptor supersensitivity that may accompany chronic therapy with antipsychotic agents. Finally lithium may augment the synthesis of acetylcholine perhaps by increasing choline uptake into nerve terminals.
Effects on second messengers: One of the best defined effects of lithium is its action on inositol phosphates. Inositol-1, 4, 5-triphosphate (IP3) and diacylglycerol (DAG) are important second messengers for both α-adrenergic and muscarinic transmission. Lithium inhibits several important enzymes in the normal recycling of the membrane phosphoinositides including the conversion of IP2 to IP1 (inositolmonophosphate) and the conversion of IP1 to inositol. This block leads to the depletion of phosphatidylinositol-4,5-biphosphate (PIP2), which is the membrane precursor of IP3 and DAG. Over time the effects of transmitters on the cell diminish in proportion to the amount of activity in the PIP2-dependent pathways. Before therapy, such activity might be greatly increased in mania. Thus lithium could cause a selective depression of the overactive circuits.
Effects on adenylyl cyclase: Studies of noradrenergic effects in isolated brain tissue indicate that lithium can inhibit norepinephrine sensitive adenylyl cyclase. Such an effect could relate to both its antidepressant and its antimanic effects.
Tricyclic antidepressants (TCAs)
These drugs block the reuptake of serotonin (5HT) and noradrenaline by blocking 5HT and α2 presynaptic receptors respectively and by stimulating the presynaptic β1 receptors present on the serotinergic and noradrenergic terminals. They do not affect the storage or synthesis of these amines. As a result of blockade of reuptake of these amines, their deficiency is made up in the brain relieving the symptoms of depression. Biochemical deficiency of these monoamines is made up within 24–48hrs during the treatment; however, therapeutic effects appear after 2–3 weeks. During this lag period, adaptive changes in the adrenergic, serotinergic and histaminic receptors takes place, which include:
Presynaptic receptor adaptive changes:
APresynaptic α2 and 5HT1 receptors are downregulated increasing the release of noradrenaline and 5HT respectively by knocking out negative feedback on the release of these hormones.
BPresynaptic β1 receptors are upregulated increasing positive feed back on release
of noradrenaline.
Postsynaptic receptor adaptive changes:
Aβ1, β2 and 5HT2 receptors are downregulated while H2 receptors are either blocked or downregulated in the CNS.
Bα1 receptors in the CNS may be upregulated or no change occurs in them. However, α1 receptors in blood vessels may be blocked leading to postural hypotension.
Precautions with the use of TCAs:
1TCAs undergo variable first-pass metabolism in the liver with resultant inconsistent bioavailability. Because of this, their dose needs off-and-on adjustment.
2TCAs have a narrow therapeutic index (a dose 5–6 times greater than the maximum daily dose of imipramine can be lethal). Therefore, depressed patients with suicidal tendency should not be given TCAs, or be given TCAs in low doses with vigilant monitoring.
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