Lothstein - Anti-Histamines

Question 1

What are the sites of histamine sythesis?

Answer 1

• L-histidine -> histamine
• Mast cells and basophils have ability to store large amts of histamine (in granules) for its release, when needed
• Control of release in many other cells, but only at the level of conversion of histidine to histamine:
  1. Epidermal cells, intestinal mucosa, CNS neurons, rapidly-dividing cells

Question 2

What are the 4 primary functional sites of histamine?

Answer 2

• Stomach: stimulate production of HCl
• Brain: neurotransmitter -> regulates sleep, hormonal secretion, memory formation, brain arousal (absence of histamine in brain can make you sleepy)
• Immune system: acts as vasodilator in allergies/immune system response
• Role in vasculature and smooth mm focus of the lecture

Question 3

Briefly describe the importance of the histamine receptors.

Answer 3

• Histamine, by itself, has no function -> it has to bind to a receptor
• H1 was the first to be identified
• Roles of histamine can be segregated by the type of receptor it is interacting with (see attached):
  1. H3 believed to control release of histamine from a number of cells
  2. H1/2 also involved in CNS
  3. Focus on H1 antagonists -> no FDA approved drugs out for H3-H4 antagonism yet (H2 antagonists used for GI biz)

Question 4

What are the functions of the different histamine receptors?

Answer 4

• Distinct and overlapping functions
• All 4 receptors can be linked to a variety of nasal symptoms in rhinitis and allergies -> H1 is most important in this regard

Question 5

How can one ligand target multiple receptors?

Answer 5

• Molecules in the body have a complex topology that can often be recognized by different types of receptors
• Histamine can bind 4 different histamine receptors, and other receptors as well -> basis of AE’s and side effects

Question 6

How is histamine release by mast cells controlled?

Answer 6

• Latticework of (-) charged carbs bound to the (+) charged histamine (and other pro-inflammatory cytokines, i.e., LT’s)
• Histamine has a short half-life (prevents systemic effect) -> time-release capsule whereby sodium exchanges with histamine, which is is gradually released
  1. Allows a broader release area of histamine in the body, producing a local-regional effect, rather than an extremely local effect
• Mast cell not destroyed by release -> granules fuse w/PM and release their contents
  1. Takes several days for mast cells to regenerate their supply of histamine

Question 7

Describe the effects of histamine on the vasculature.

Answer 7

• Histamine only has effect where there are histamine receptors -> none in the true capillary bed (permeability actually in the VENULES/ARTERIOLES: VASODILATION)
• H1 (aa and vv): constriction of vessel via smooth mm, but dilation at endothelial level -> net effect on LG VESSELS is VASOCONSTRICTION (smooth mm effect predominates)
  1. This is true in vasculature, and also bronchi (net effect in the lungs is BRONCHOCONSTRICTION)
• H2: slower onset, and more persistent VASODILATION in SM VESSELS -> allows immune system components to move into tissue and confront and destroy allergens (at consequence of itching, sneezing, and runny nose)

Question 8

What happens when a mast cell responds to an allergen?

Answer 8

• Mast cells sensitized by IgE, so when an allergen binds, there is a cross-linking of IgE bound to specific receptors, leading to activation of mast cell and histamine release
• Other substances involved/released from mast cells: LT’s, PG’s, tryptase (but about 1,000,000x more histamine)
• Histamine mostly involved in the early phase allergic response (sneezing, itching, runny nose/rhinorrhea, nasal obstruction -> fluid, swelling due to edema)
  1. This stage is the target of anti-histamines
• Late response: runny nose, watery eyes

Question 9

How do anti-histamine drugs work?

Answer 9

• Unclear, but the proposed mechanism is inverse agonism
• Receptors exist in active and inactive conformation, and activity depends on % of receptors in e/conformation
• Histamine stabilizes the # of receptors in the active conformation
  1. All H1 antagonists can bind the inactive form, and accumulate this conformation, decreasing histamine receptor activity
• Technical difference pharmacologically, but the same effect clinically as competitive inhibition

Question 10

What is the general H1 antagonist structure?

Answer 10

Substitutions on these 3 sites for the drugs

Question 11

What are the therapeutic applications of H1 antagonists?

Answer 11

• Amelioration of allergy and hay fever symptoms
• Treatment of symptoms of insect bites and stings
• Treatment of symptoms of contact flora poisoning
• Attenuation of motion sickness and vertigo (1st gen -> NOT through interaction with histamine receptors, but rather via anti-cholinergic effects)

Question 12

Compare and contrast the 1st and 2nd gen anti-histamines (table).

Answer 12

• 1st gen: 4-6 hour duration, so pt compliance can be a limiting factor
  1. Anticholinergic effects can be beneficial or AE’s.
• 2nd gen: upwards of 24 hour duration

Question 13

What are the properties of the 1st gen H1 antagonists?

Answer 13

• Common functional effects: can almost ignore structural categories; some variations in sedation, but all are sedative
• Sedative effect: H1 receptors in hypothalamus; histamine is a potent regulator of wakefulness and sedation in the brain -> presence of histamine makes you more alert
  1. Drugs pass through BBB (uncharged) -> can bypass P-gp’s, and easily penetrate brain/have CNS effects
• Anti-cholinergic: no such thing as a truly specific agonist or antagonist -> as you INC dose, drug will be able to bind o/receptors, in this case, muscarinic
  1. GI effect is in H2 receptor domain (smooth muscle peristalsis -> mild effect of 1st generation meds)
  2. Contraindicated for the tx of asthma bc dry and thicken mucosal secretions (anti-cholinergic)
• No effect on histamine release from mast cells

Question 14

What are the names and indications of the ether/ethanolamine derivatives?

Answer 14

• Diphenhydramine and Dimenhydrinate: allergic rhinitis, anaphylaxis
  1. Adjunct, common cold, insomnia, motion sickness
  2. Highly sedating
• Clemastine: allergic rhinitis, cutaneous hypersensitivity, uticaria, and angioedema
  1. Highly sedating
• 1st gen: CONTRAINDICATED IN ASTHMA PATIENTS

Question 15

What are the names and indications of the alkylamine derivatives?

Answer 15

• Chlorpheniramine: allergic rhinitis, common cold
• Brompheniramine: allergic rhinitis, urticaria
• 1st gen: CONTRAINDICATED IN ASTHMA PATIENTS

Question 16

What are the indications for promethazine? Derivative of?

Answer 16

• Promethazine: allergic condition, motion sickness, nausea and vomiting
  1. Highly sedating
• Phenothiazine derivative
• 1st gen: CONTRAINDICATED IN ASTHMA PTS

Question 17

What are the names and indications of the piperazine derivatives?

Answer 17

• Cyclizine: motion sickness, nausea and vomiting
• Meclizine: motion sickness, vertigo
• Hydrxoxyzine: nausea and vomiting, pruritis
• 1st gen: CONTRAINDICATED IN ASTHMA PTS

Question 18

Which anti-histamines are contraindicated in asthma patients?

Answer 18

• 1st gen
• Diphenhydramine, Dimenhydrinate, and Clemastine
• Chlorpheniramine and Brompheniramine
• Promethazine
• Cyclizine, Meclizine, and Hydrxoxyzine

Question 19

What are the AE/side effects of the 1st H1 antagonists?

Answer 19

• 1st-generation antagonists are not only targeting the H1 receptor, but can bind, to a lesser extent, other receptors
• Motion sickness treatment is a consequence of muscarinic effects (not H1)
  1. CN VIII -> inner ear and vomit reflex -> block muscarinic transmission through this N
• Also have sedative effect

Question 20

What are the properties of the 2nd gen H1 antagonists?

Answer 20

• Don’t cross BBB nearly as much as 1st gen (bc charged): 70% 1st gen to 20% 2nd gen -> limited to no sedation
• All have the same effect
• Comparable potency to 1st gen for H1 receptor blocking, but NO sedative or anti-cholinergic effect
  1. Little effect on smooth mm peristalsis in the GI tract
• NO effect on bronchial secretions, so can be taken safely by asthma patients (but not first-line asthma drugs).
• Single dose over 24 hours due to pharmacokinetics; un-metabolized (or metabolized to another active form) by liver and secreted in feces or urine
• Note: 2 no longer on market due to interaction with anti-fungals/macrolides leading to fatal cardiac arrhythmias (K channel binding) -> always think about drug combos
  1. Short hx of FDA warnings for use of 2nd gen anti-histamines, but most were IV abuse drugs -> no drug is absolutely safe bc every individual has potential to be different in terms of their response to a drug

Question 21

What are the indications for Loratadine, Fexofenadine, Desloratadine, Acrivastine, and Cetirizine?

Answer 21

Urticaria, seasonal allergic rhinitis

2nd/3rd gen H1 antagonists

Non-sedating

Question 22

What are the indications for Olopatadine, Levocabastine, and Azelastine?

Answer 22

Allergic conjunctivitis, seasonal allergic rhinitis

2nd/3rd gen H1 antagonists

Non-sedating

Question 23

What are the side effects of the 1st gen vs. 2nd gen H1 antagonists?

Answer 23

• 1st gen: sedation, impaired cognition, DEC alertness, slowed rxn time, confusion, dizziness, dystonia, potentiation of nasal congestion
• 2nd gen: mild cognitive disturbance

Question 24

What are the goals of 3rd gen H1 antagonist drug development?

Answer 24

Question 25

Desloratidine (Clarinex)

Answer 25

• Greater H1 specificty: 14 to 17x greater binding to H1 receptors than Loratadine
• 15 to 50x lower affinity for muscarinic receptors (M1, 2, 4, and 5) compared to H1-receptors
• Relatively long elimination half-life (27 hours)
• Not going to blow others off market, but is competitive
• Non-sedating, 3rd gen H1 receptor antagonist (reverse agonist)
  1. Indicated for urticaria, seasonal allergic rhinitis

Question 26

What are the clinical uses of the H1 antagonists, 1st gen vs. 2nd/3rd?

Answer 26

• Note: role of cholinergic receptors in itching dermatosis, so first generation have more of an effect

Question 27

Olopatadine

Answer 27

• Selectivity for H1 receptor > other ocular antihistamines
• Inhibits release of histamine from mast cells
  1. May block activities of some additional mediators of ophthalmic inflammation by INH release of tryptase and prostaglandin D2 from same granules
• Prevents or reduces ocular inflammation rxns induced by a variety of common allergens
  1. Used to treat ocular rhinitis, allergic conjunctivitis, seasonal allergic rhinitis
• Non-sedating, 3rd gen H1 receptor antagonist (reverse agonist)

Question 28

Levocabastine

Answer 28

• Rapid-acting agent for as needed-use against nasal and ocular effects of rhinitis
• Piperidine derivative: 1250 times more potent than chlorpheniramine
• 40,000x effective dose exhibits no other pharmacological effects -> perhaps most specific H1 antagonist developed so far
• Indications: allergic conjunctivitis, seasonal allergic rhinitis
• Non-sedating, 3rd gen H1 receptor antagonist (reverse agonist)

Question 29

Azelastine

Answer 29

• Phthalazinone derivative that INH histamine + LT activity
• Blocks Ca mobilization and the 5-lipoxygenase pathway
• INH PAF (platelet activating factor) through receptor antagonism
  1. PAF and LT’s are principal mediators of asthmatic attacks, so blocking these actions was hoped to help with asthmatic attacks, but none of these drugs have been approved primarily for the tx of asthma
  2. Anti-histamines that are safe for asthmatics to take, and may be used as adjunctive therapy
• Indications: allergic conjunctivitis, seasonal allergic rhinitis
• Non-sedating, 3rd gen H1 receptor antagonist (reverse agonist)
• Emedastine, Mizolastine, and Ebastine all similar