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๏ฝ Histamine: a chemical messenger mostly generated
in mast cells
๏ฝ Mediates a wide range of cellular responses
โ—ฆ Allergic and inflammatory reactions
โ—ฆ Gastric acid secretion
โ—ฆ Neurotransmission in parts of the brain.
๏ฝ Histamine is present in practically all tissues, with
significant amounts in the lungs, skin, blood
vessels, and GI tract
๏ฝ Found at high concentration in mast cells and
basophils
๏ฝ A neurotransmitter in the brain
๏ฝ Also occurs as a component of venoms and in
secretions from insect stings
Synthesis
๏ฝ Histamine is formed by the decarboxylation of
histidine by histidine decarboxylase
๏ฝ In mast cells, histamine is stored in granules
๏ฝ If histamine is not stored, it is rapidly inactivated
by the enzyme amine oxidase
Release of histamine
๏ฝ Most often, histamine is just one of several
chemical mediators released in response to stimuli
๏ฝ The stimuli for release of histamine from tissues
may include destruction of cells as a result of cold,
toxins from organisms, venoms from insects and
spiders, and trauma
๏ฝ Allergies and anaphylaxis can also trigger
significant release of histamine.
๏ฝ Azelastine
๏ฝ Bepotastine
๏ฝ Brompheniramine
๏ฝ Cetirizine
๏ฝ Chlorpheniramine
๏ฝ Clemastine
๏ฝ Cyclizine
๏ฝ Cyproheptadine
๏ฝ Desloratadine
๏ฝ Diphenhydramine
๏ฝ Dimenhydrinate
๏ฝ Doxylamine
๏ฝ Fexofenadine
๏ฝ Hydroxyzine
๏ฝ Ketotifen
๏ฝ Levocetirizine
๏ฝ Loratadine
๏ฝ Meclizine
๏ฝ Promethazine
Mechanism of action
๏ฝ Released in response to certain stimuli and binds to various types
of histamine receptors (H1, H2, H3, and H4)
๏ฝ H1 and H2 receptors are widely expressed and are the targets of
clinically useful drugs
๏ฝ H1 receptors are important in producing smooth muscle
contraction and increasing capillary permeability
๏ฝ Histamine promotes vasodilation of small blood vessels by
causing the vascular endothelium to release nitric oxide
๏ฝ Can enhance secretion of proinflammatory cytokines in several
cell types and in local tissues
๏ฝ H1 receptors mediate many pathological processes, including
allergic rhinitis, atopic dermatitis, conjunctivitis, urticaria,
bronchoconstriction, asthma, and anaphylaxis
๏ฝ Histamine stimulates the parietal cells in the stomach, causing an
increase in acid secretion via the activation of H2 receptors.
๏ฝ Histamine causes contraction of airway smooth
muscle, stimulation of secretions, dilation and
increased permeability of the capillaries, and
stimulation of sensory nerve endings
๏ฝ If the release of histamine is slow enough to permit
its inactivation before it enters the bloodstream, a
local allergic reaction results
๏ฝ If histamine release is too fast for inactivation, a
full-blown anaphylactic reaction occurs.
๏ฝ The H1-receptor blockers can be divided into first-
and second generation drugs.
๏ฝ First generation drugs
โ—ฆ Penetrate the CNS and cause sedation
โ—ฆ Interact with other receptors, producing a variety of unwanted
adverse effects
๏ฝ Second-generation agents
โ—ฆ Specific for peripheral H1 receptors
โ—ฆ Do not penetrate the BBB causing less CNS depression than the
first generation drugs
โ—ฆ Desloratadine, fexofenadine and loratadine show the least
sedation
โ—ฆ Cetirizine and levocetirizine are partially sedating
๏ฝ The action of all the H1-receptor blockers is qualitatively
similar
๏ฝ Block the receptor-mediated response of a target tissue
๏ฝ Much more effective in preventing symptoms than reversing
them
๏ฝ Have additional effects due to binding to cholinergic,
adrenergic, or serotonin receptors
๏ฝ Cyproheptadine also acts as a serotonin antagonist on the
appetite center, sometimes used off label as an appetite
stimulant and in treating anorgasmy associated SSRIs
๏ฝ Antihistamines such as azelastine and ketotifen also have
mast cellโ€“stabilizing effects
Therapeutic uses
1. Allergic and inflammatory conditions
2. Motion sickness and nausea
3. Somnifacients
Allergic and inflammatory conditions:
๏ฝ H1-receptor blockers are useful in treating and
preventing allergic reactions caused by antigens
acting on IgE antibody
๏ฝ Oral antihistamines are the drugs of choice in
controlling the symptoms of allergic rhinitis and
urticaria because histamine is the principal
mediator released by mast cells
๏ฝ Ophthalmic antihistamines are useful for the
treatment of allergic conjunctivitis
๏ฝ Not implicated in asthma
Motion sickness and nausea
๏ฝ Diphenhydramine, dimenhydrinate, cyclizine, meclizine
and promethazine are effective for prevention of the
symptoms of motion sickness
๏ฝ Not effective if symptoms are already present
๏ฝ Taken prior to expected travel
๏ฝ Antihistamines prevent or diminish nausea and
vomiting mediated by the chemoreceptor and
vestibular pathways
๏ฝ The antiemetic action is due to blockade of central H1
and M1 muscarinic receptors
๏ฝ Meclizine is useful for the treatment of vertigo
associated with vestibular disorders
Somnifacients
๏ฝ Many first-generation antihistamines, such as
diphenhydramine and doxylamine have strong
sedative properties
๏ฝ Used in the treatment of insomnia
๏ฝ Available OTC without a prescription
๏ฝ Use is contraindicated in individuals working in
jobs in which wakefulness is critical
๏ฝ Antihistamines are not the medications of choice
Pharmacokinetics
๏ฝ H1-receptor blockers are well absorbed after oral
administration, with maximum serum levels occurring at 1
to 2 hours
๏ฝ Average t1/2 is 4 to 6 hours, except for that of meclizine
and the second generation agents which is 12 to 24 hours
๏ฝ First-generation H1- receptor blockers are distributed in all
tissues, including CNS
๏ฝ Most are metabolized by the hepatic CYP450 system
๏ฝ Cetirizine and levocetirizine are excreted largely unchanged
in urine
๏ฝ Fexofenadine is excreted largely unchanged in feces
๏ฝ Some are available as ophthalmic or intranasal formulations
๏ฝ First-generation H1-receptor blockers have a low
specificity, interacting with histamine, muscarinic
cholinergic, ฮฑ-adrenergic and serotonin receptors
๏ฝ The extent of interaction with receptors varies
๏ฝ Some side effects may be undesirable, and others
may be of therapeutic value
๏ฝ Incidence and severity of adverse reactions for a
given drug varies between individual subjects
๏ฝ First-generation H1-receptor blockers have a low
specificity, interacting not only with histamine
receptors but also with muscarinic cholinergic
receptors, ฮฑ-adrenergic receptors, and serotonin
receptors
๏ฝ The extent of interaction with these receptors and
the nature of the side effects varies with the
structure of the drug
๏ฝ Some side effects may be undesirable, and others
may be of therapeutic value
๏ฝ Incidence and severity of adverse reactions for a
given drug varies between individual subjects
๏ฝ Sedation: (First-generation H1 antihistamines)
๏ฝ Diphenhydramine may cause paradoxical
hyperactivity in young children
๏ฝ Fatigue, dizziness, lack of coordination, and tremors
๏ฝ First-generation antihistamines exert anticholinergic
effects, Dryness, blurred vision and retention of
urine
๏ฝ The most common adverse reaction associated with
second-generation antihistamines is headache
๏ฝ Topical diphenhydramine can cause hypersensitivity
such as contact dermatitis when applied to the skin.
Drug interactions:
๏ฝ Potentiation of effects of other CNS depressants,
including alcohol
๏ฝ Patients taking MAOIs should not take
antihistamines
๏ฝ 1st generation antihistamines with anticholinergic
actions may decrease effectiveness of
cholinesterase inhibitors
Overdoses:
๏ฝ The margin of safety of H1-receptor blockers is
relatively high, and chronic toxicity is rare
๏ฝ Acute poisoning is relatively common, especially in
young children
๏ฝ The most common and dangerous effects of acute
poisoning are those on the CNS, including
hallucinations, excitement, ataxia, and convulsion
๏ฝ If untreated, the patient may experience a
deepening coma and collapse of the
cardiorespiratory system
๏ฝ Have little, if any, affinity for H1 receptors.
๏ฝ Clinical use: inhibitors of gastric acid secretion in
treatment of ulcers and heartburn
๏ฝ Include:
โ—ฆ Cimetidine
โ—ฆ Ranitidine
โ—ฆ Famotidine
โ—ฆ Nizatidine

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Antihistamines - Pharmacology

  • 1.
  • 2. ๏ฝ Histamine: a chemical messenger mostly generated in mast cells ๏ฝ Mediates a wide range of cellular responses โ—ฆ Allergic and inflammatory reactions โ—ฆ Gastric acid secretion โ—ฆ Neurotransmission in parts of the brain.
  • 3. ๏ฝ Histamine is present in practically all tissues, with significant amounts in the lungs, skin, blood vessels, and GI tract ๏ฝ Found at high concentration in mast cells and basophils ๏ฝ A neurotransmitter in the brain ๏ฝ Also occurs as a component of venoms and in secretions from insect stings
  • 4. Synthesis ๏ฝ Histamine is formed by the decarboxylation of histidine by histidine decarboxylase ๏ฝ In mast cells, histamine is stored in granules ๏ฝ If histamine is not stored, it is rapidly inactivated by the enzyme amine oxidase
  • 5. Release of histamine ๏ฝ Most often, histamine is just one of several chemical mediators released in response to stimuli ๏ฝ The stimuli for release of histamine from tissues may include destruction of cells as a result of cold, toxins from organisms, venoms from insects and spiders, and trauma ๏ฝ Allergies and anaphylaxis can also trigger significant release of histamine.
  • 6. ๏ฝ Azelastine ๏ฝ Bepotastine ๏ฝ Brompheniramine ๏ฝ Cetirizine ๏ฝ Chlorpheniramine ๏ฝ Clemastine ๏ฝ Cyclizine ๏ฝ Cyproheptadine ๏ฝ Desloratadine ๏ฝ Diphenhydramine ๏ฝ Dimenhydrinate ๏ฝ Doxylamine ๏ฝ Fexofenadine ๏ฝ Hydroxyzine ๏ฝ Ketotifen ๏ฝ Levocetirizine ๏ฝ Loratadine ๏ฝ Meclizine ๏ฝ Promethazine
  • 7. Mechanism of action ๏ฝ Released in response to certain stimuli and binds to various types of histamine receptors (H1, H2, H3, and H4) ๏ฝ H1 and H2 receptors are widely expressed and are the targets of clinically useful drugs ๏ฝ H1 receptors are important in producing smooth muscle contraction and increasing capillary permeability ๏ฝ Histamine promotes vasodilation of small blood vessels by causing the vascular endothelium to release nitric oxide ๏ฝ Can enhance secretion of proinflammatory cytokines in several cell types and in local tissues ๏ฝ H1 receptors mediate many pathological processes, including allergic rhinitis, atopic dermatitis, conjunctivitis, urticaria, bronchoconstriction, asthma, and anaphylaxis ๏ฝ Histamine stimulates the parietal cells in the stomach, causing an increase in acid secretion via the activation of H2 receptors.
  • 8. ๏ฝ Histamine causes contraction of airway smooth muscle, stimulation of secretions, dilation and increased permeability of the capillaries, and stimulation of sensory nerve endings ๏ฝ If the release of histamine is slow enough to permit its inactivation before it enters the bloodstream, a local allergic reaction results ๏ฝ If histamine release is too fast for inactivation, a full-blown anaphylactic reaction occurs.
  • 9.
  • 10. ๏ฝ The H1-receptor blockers can be divided into first- and second generation drugs. ๏ฝ First generation drugs โ—ฆ Penetrate the CNS and cause sedation โ—ฆ Interact with other receptors, producing a variety of unwanted adverse effects ๏ฝ Second-generation agents โ—ฆ Specific for peripheral H1 receptors โ—ฆ Do not penetrate the BBB causing less CNS depression than the first generation drugs โ—ฆ Desloratadine, fexofenadine and loratadine show the least sedation โ—ฆ Cetirizine and levocetirizine are partially sedating
  • 11.
  • 12. ๏ฝ The action of all the H1-receptor blockers is qualitatively similar ๏ฝ Block the receptor-mediated response of a target tissue ๏ฝ Much more effective in preventing symptoms than reversing them ๏ฝ Have additional effects due to binding to cholinergic, adrenergic, or serotonin receptors ๏ฝ Cyproheptadine also acts as a serotonin antagonist on the appetite center, sometimes used off label as an appetite stimulant and in treating anorgasmy associated SSRIs ๏ฝ Antihistamines such as azelastine and ketotifen also have mast cellโ€“stabilizing effects
  • 13.
  • 14. Therapeutic uses 1. Allergic and inflammatory conditions 2. Motion sickness and nausea 3. Somnifacients
  • 15. Allergic and inflammatory conditions: ๏ฝ H1-receptor blockers are useful in treating and preventing allergic reactions caused by antigens acting on IgE antibody ๏ฝ Oral antihistamines are the drugs of choice in controlling the symptoms of allergic rhinitis and urticaria because histamine is the principal mediator released by mast cells ๏ฝ Ophthalmic antihistamines are useful for the treatment of allergic conjunctivitis ๏ฝ Not implicated in asthma
  • 16. Motion sickness and nausea ๏ฝ Diphenhydramine, dimenhydrinate, cyclizine, meclizine and promethazine are effective for prevention of the symptoms of motion sickness ๏ฝ Not effective if symptoms are already present ๏ฝ Taken prior to expected travel ๏ฝ Antihistamines prevent or diminish nausea and vomiting mediated by the chemoreceptor and vestibular pathways ๏ฝ The antiemetic action is due to blockade of central H1 and M1 muscarinic receptors ๏ฝ Meclizine is useful for the treatment of vertigo associated with vestibular disorders
  • 17. Somnifacients ๏ฝ Many first-generation antihistamines, such as diphenhydramine and doxylamine have strong sedative properties ๏ฝ Used in the treatment of insomnia ๏ฝ Available OTC without a prescription ๏ฝ Use is contraindicated in individuals working in jobs in which wakefulness is critical ๏ฝ Antihistamines are not the medications of choice
  • 18. Pharmacokinetics ๏ฝ H1-receptor blockers are well absorbed after oral administration, with maximum serum levels occurring at 1 to 2 hours ๏ฝ Average t1/2 is 4 to 6 hours, except for that of meclizine and the second generation agents which is 12 to 24 hours ๏ฝ First-generation H1- receptor blockers are distributed in all tissues, including CNS ๏ฝ Most are metabolized by the hepatic CYP450 system ๏ฝ Cetirizine and levocetirizine are excreted largely unchanged in urine ๏ฝ Fexofenadine is excreted largely unchanged in feces ๏ฝ Some are available as ophthalmic or intranasal formulations
  • 19. ๏ฝ First-generation H1-receptor blockers have a low specificity, interacting with histamine, muscarinic cholinergic, ฮฑ-adrenergic and serotonin receptors ๏ฝ The extent of interaction with receptors varies ๏ฝ Some side effects may be undesirable, and others may be of therapeutic value ๏ฝ Incidence and severity of adverse reactions for a given drug varies between individual subjects
  • 20. ๏ฝ First-generation H1-receptor blockers have a low specificity, interacting not only with histamine receptors but also with muscarinic cholinergic receptors, ฮฑ-adrenergic receptors, and serotonin receptors ๏ฝ The extent of interaction with these receptors and the nature of the side effects varies with the structure of the drug ๏ฝ Some side effects may be undesirable, and others may be of therapeutic value ๏ฝ Incidence and severity of adverse reactions for a given drug varies between individual subjects
  • 21. ๏ฝ Sedation: (First-generation H1 antihistamines) ๏ฝ Diphenhydramine may cause paradoxical hyperactivity in young children ๏ฝ Fatigue, dizziness, lack of coordination, and tremors ๏ฝ First-generation antihistamines exert anticholinergic effects, Dryness, blurred vision and retention of urine ๏ฝ The most common adverse reaction associated with second-generation antihistamines is headache ๏ฝ Topical diphenhydramine can cause hypersensitivity such as contact dermatitis when applied to the skin.
  • 22. Drug interactions: ๏ฝ Potentiation of effects of other CNS depressants, including alcohol ๏ฝ Patients taking MAOIs should not take antihistamines ๏ฝ 1st generation antihistamines with anticholinergic actions may decrease effectiveness of cholinesterase inhibitors
  • 23. Overdoses: ๏ฝ The margin of safety of H1-receptor blockers is relatively high, and chronic toxicity is rare ๏ฝ Acute poisoning is relatively common, especially in young children ๏ฝ The most common and dangerous effects of acute poisoning are those on the CNS, including hallucinations, excitement, ataxia, and convulsion ๏ฝ If untreated, the patient may experience a deepening coma and collapse of the cardiorespiratory system
  • 24. ๏ฝ Have little, if any, affinity for H1 receptors. ๏ฝ Clinical use: inhibitors of gastric acid secretion in treatment of ulcers and heartburn ๏ฝ Include: โ—ฆ Cimetidine โ—ฆ Ranitidine โ—ฆ Famotidine โ—ฆ Nizatidine