Drugs

Question 1

Warfarin

Therapeutic Use, Mechanism of Action, Side Effects, Therapeutic Index, Metabolism, Pharmacogenomics, TDM

Answer 1

Therapeutic Use: Increases clotting time (anticoagulant) to prevent thrombi/stroke
Mechanism of Action: suppresses VKORC1 - reduces vitamin K regeneration - blocks carboxylation of coagulation factors
Side Effect: Increases bleeding if dose is too high
TI: ~1 - very narrow sweet spot
Metabolism: CYP2C9
Pharmacogenomics: CYP2C92/3 have reduced function - poor metabolizers need more days to determine if anticoagulation is stable & TDM via INR (international normalized ratio of patient prothrombin time - how long it takes to clot - adjust dose based on this number)
Pharmacodynamics: VKORC1 haplotype A - more sensitive to drug than wild-type G - higher risk of hemorrhagic activity
Dosage scheme depends on genetics of CYP2C9 and VKORC1

Question 2

Benzodiazepines [-azepam + -azolam]
Diazepam [Valium]
Midazolam [Versed]

(Therapeutic Use, Mechanism of Action, Side Effect, TI, Metabolism)

Answer 2

Therapeutic Use: sedation, improve sleep, treat anxiety + muscle spasms
Mechanism of Action: allosteric activator of GABA-a receptors (binds b/w b+g subunits) - increase IPSP, increase Cl- current by increasing frequency of channel openings
Side Effect: over-sedation, dizziness, confusion, memory loss
TI: ~100+ (safer)
Metabolism: CYP3A4 hydroxylation [CYP2C19 helps with -azepams] (reduce 90% activity) & Glucuronidation (very water soluble and inactive form)

Question 3

Sulfonylureas

Mechanism of Action

Answer 3

inhibit K-ATP channels, resulting in depolarized Vrest, allowing V-gated Ca channels to open and cause insulin secretion in pancreas and vasoconstriction in SMC

Question 4

Minoxidil

Therapeutic Use, Mechanism of Action

Answer 4

Therapeutic Use: Treat HT
Mechanism of action: activates K-ATP receptors in SMC - hyperpolarized Vrest - v-gated Ca channels harder to open - more vasodilatation

Question 5

Local Anaesthetics 
(Therapeutic Use, Mechanism of Action, and Special Characteristic)

Answer 5

Therapeutic Use: Localized pain reduction
Mechanism of Action: Block V-gated Na Channels by enhancing inactivation (preferential binding to inactivated state);
Use-Dependent Block: inhibition intensifies with use as more Na channels get inactivated after every AP (good for neurons that fire frequently - pain nerves + epilepsy); weak base than enters channel from cytosolic side through fenestrations

Question 6

Tetrodotoxin (TTX)

Therapeutic Use, Mechanism of Action

Answer 6

Use: Eating pufferfish, should be just enough to make your fingertips tingle, POISON
Mechanism of Action: Potent Na Channel Blocker; acts like plug on EC side of channel (Pre-synaptic Transmission NMJ), also EC block on nicotinic receptor (Post-synaptic Transmission NMJ)

Question 7

Drug Class: L-Type Ca++ Channel Blockers (Mechanism of Action, Therapeutic Uses)

Answer 7

Mechanism of Action: shorten cardiac AP plateau (phase II) = shorten AP
Use: treat angina, HT (inhibit SMC VC), Arrythmia

Question 8

Drug Class: Na+ Channel Blockers (Mechanism of Action, Therapeutic Uses)

Answer 8

Mechanism of Action: Decrease/Attenuate depolarization upstroke (blunts rate of rise) - slows AP conduction through heart - prevents re-entry loops
Therapeutic Uses: local anaesthesia, arrhythmia, epilepsy/migraines

Question 9

Drug Class: K+ Channel Blockers

Mechanism of Action, Therapeutic Uses, Side Effect

Answer 9

Mechanism of Action: impair repolarization in phase III - longer cardiac AP
Therapeutic Uses: arrhythmia
Side Effect: Drug Induced LQTS, pro-arrhythmic

Question 10

Ondansetron (Zofran) and -setrons

Mechanism of Action, Therapeutic Use

Answer 10

Mechanism of Action: Competitive Antagonist at 5-HT3 Serotonin Receptors
Therapeutic Uses: Treat nausea + vomiting (that typically occurs because of cancer chemotherapy agents)

Question 11

Zolpidem (Ambien)

Mechanism of Action, Therapeutic Use, Key Feature

Answer 11

Mechanism of Action: binds selectively to specific B[a]p sites involved in producing sleep
Therapeutic Use: help fall asleep
Allosteric Activator - reduces likelihood of receptor desensitization

Question 12

Penicillin

Side Effect, Mechanism of Action, Excretion

Answer 12

Major Side Effect: blocks open GABA-a receptor channels - induces seizures!
Mechanism of Action: uncompetitive antagonist to activated GABA-a channels - CONVULSANT
Excretion: Tubular Secretion (through OATs, competing pathway with Probenecid causes prolonged penicillin activity - GOOD)

Question 13

Strychnine

Mechanism of Action, Effect

Answer 13

Mechanism of Action: Post-synaptic inhibitor, competitive inhibitor of glycine receptors
Effect: causes excessive spasticity

Question 14

Tetanus Toxin 
(Mechanism of Action, Effect)

Answer 14

Mechanism of Action: Pre-synaptic inhibitor, blocks glycine release
Effect: causes excessive spasticity

Question 15

Memanite

Mechanism of Action, Effect

Answer 15

Mechanism of Action: binds to open NMDA channel (uncompetitive antagonist) and inhibits Ca2+ flow
Effect: May be used to treat Alzheimer’s and seizures
Acts like penicillin (uncompetitive antagonist)

Question 16

Fluticasone [-son- and -one drugs]

Mechanism of Action, Effect

Answer 16

Mechanism of Action: activates glucocorticoid receptors to inhibit inflammatory response

Question 17

Selective Serotonin Reuptake Inhibitors [SSRIs]

Mechanism of Action, Therapeutic Use

Answer 17

Mechanism of Action: blocks SLC6A4 serotonin reuptake SLC secondary active transporter
Therapeutic Use: anti-depressent (more serotonin lingering in synaptic cleft)

Question 18

Grapefruit Juice [Furanocoumarins]

Mechanism of Action, Effect, Low vs. High F, Oral vs. IV

Answer 18

Mechanism of Action: Inhibit CYP3A4 + PGP, increasing bioavailability of drugs
Effect: Toxic elevations of drug in systemic circulation
Large effects on drugs with low F - bigger boosts possible
Only affects orally ingested drugs

Question 19

Cimetidine [-idine]

Mechanism of Action, Key Feature, Metabolism Reaction, Problem

Answer 19

Mechanism of Action: Competitive Inhibitor (complementary shape) for H2 Histamine Receptor
Metabolized by S-oxidation
Inhibits many types of CYPs cause of drug:drug interaction toxic buildup
Desensitization: continual use causes GCPR receptor upregulation, over-inhibition suppresses internalization/degradation

Question 20

Caffeine

Use, Mechanism of Action, Metabolism Reaction, Family

Answer 20

Use: stimulant
Mechanism of Action: competitive inhibitor (complementary shape to adenosine) of adenosine receptor at low doses (disinhibition of cellular functions)
Minor Mechanism: inhibits phosphodiesterases at higher doses (increase cAMP and signaling through pathway)
Metabolism: N-dealkylation to active metabolite or theophylline
METHYLXANTHINE FAMILY WITH THEOPHYLLINE

Question 21

Theophylline

Use, Mechanism of Action, Metabolism Reaction, Family

Answer 21

Use: last resort to treat bronchiole disorders
Mechanism of Action: competitive inhibitor (complementary shape to adenosine) of adenosine receptor at low doses (disinhibition of cellular functions)
Minor Mechanism: inhibits phosphodiesterases at higher doses (increase cAMP and signaling through pathway)
Metabolism: N-dealkylation to inactive metabolite
METHYLXANTHINE FAMILY WITH CAFFEINE

Question 22

Ethanol

Pathway, Problem

Answer 22

Pathway: EtOH - alcohol dehydrogenase oxidizes to - acetaldehyde (TOXIC drunk guy) - aldehyde dehydrogenase oxidizes to - acetate
Problem: Role in Acetaminophen toxicity - high ethanol induces CYP2E1, which can metabolize acetaminophen into toxic NAPQI
Polymorphisms: “Asian Glow” Chinese more likely to have enhanced alcohol DH and reduced aldehyde DH = toxic buildup of aldehyde causes facial flushing

Question 23

Succinylcholine

Mechanism of Action, Metabolism

Answer 23

Mechanism of Action: prevents ACh excitation of skeletal muscle; depolarizing blocker - fastest known ACh blocker b/c you can overload dose and it’ll be degraded
Metabolism: Degraded twice via ester hydrolysis by pseudocholinesterases

Question 24

Acetaminophen

Therapeutic Use, Mechanism of Action, Metabolism, Treatment for Metabolism Problems

Answer 24

Therapeutic Use: analgesic & antipyretic
Mechanism of Action: inhibits cyclooxygenases (housekeeping COX1 + painful COX2)
Metabolism: no phase I reaction because already hydroxylated, many possible pathways:
A. Sulfation to nontoxic inactivated form (LOW DOSES)
B. Glucuronidation to nontoxic inactivated form (LOW DOSES)
C. HIGH DOSES: CYP2E1 + CYP3A4 make NAPQI (reactive toxic intermediate electrophile kills hepatocytes) - metabolized again via GLUTATHIONE GSTs - requires glutathione
*If HIGH DOSE AND LOW GLUTATHIONE - NAPQI reacts with nucleophilic macromoleculs, triggering liver cell death
Treatment: N-acetylcysteine - complementary shape to glutathione, but less polar so it can diffuse through lipid bilayer (anti-inflammatory and antioxidant)

Question 25

Albuterol

Therapeutic Use, Mechanism of Action

Answer 25

Therapeutic Use: rescue inhaler for asthma, treats COPD

Mechanism of action: beta-2 receptor agonist (relax SMC)

Question 26

Codeine

Therapeutic Use, Metabolism, Key Feature, Pharmacogenomics

Answer 26

Therapeutic Use: Pro-drug analgesic
Metabolism: via O-dealkylation by CYP2D6 (Phase I) to Morphine (activated Drug)
Key Feature: Morphine involved in Enterohepatic Cycle (Antibiotics cause increased half-life)
Pharmacogenomics: Affects Biotransformation, CYP2D6 polymorphisms create poor metabolizers (ineffective doses) and ultra-rapid metabolizers (toxicity)

Question 27

Hydrocodone

Therapeutic Use, Metabolism

Answer 27

Therapeutic Use: active analgesic, also a pro-drug to become even more active
Metabolism: via O-dealkylation by CYP2D6 (Phase I) to Hydrophorphone (even more activated)
(poor metabolizers need more and rapid metabolizers need less)

Question 28

Metoprolol

Therapeutic Use, Mechanism of Action, Metabolism

Answer 28

Therapeutic Use: anti-HT, anti-anginal, antiarrhythmic (like propanolol but MORE selective)
Mechanism of Action: Selectively blocks beta-1 receptors (inhibiting causes decrease in HR and contractility) - good beta blockers for asthmatics b/c doesn’t block airway
Metabolism: CYP2D6 inactivates (poor metabolizers need less and rapid metabolizers need more)

Question 29

Omeprazole (-prazoles)

Therapeutic Use, Mechanism of Action, Metabolism

Answer 29

PROTON PUMP INHIBITOR
Therapeutic Use: treat excess acid secretion disorders (ulcers)
Mechanism of Action: irreversibly blocks proton pump + prevents acid secretion
Metabolism: CYP2C19

Question 30

Clopidogrel [Plavix]

Therapeutic Use, Metabolism, Pharmacogenomics - KNOW THE VARIANTS

Answer 30

Therapeutic Use: Anti-platelet Activity
Metabolism: Pro-drug activated by twice metabolism through CYP2C19
Pharmacogenomics: CYP2C192/3 variants cause reduced function, impaired anti-platelet effects - high risk of thrombosis/stroke - even in carriers with one of these variants!

Question 31

Ibuprofen

Family, Therapeutic Use, Mechanism of Action, Metabolism

Answer 31

NSAIDs - non-steroidal anti-inflammatory drugs
Therapeutic Use: pain-reliever + anti-inflammatory
Mechanism of Action: inhibits both housekeeping COX1 and painful COX2 enzymes
Metabolism: CYP2C9 - polymorphic poor metabolizers have reduced clearance

Question 32

Celecoxib

Family, Therapeutic Use, Mechanism of Action, Metabolism

Answer 32

NSAIDs - non-steroidal anti-inflammatory drugs
Therapeutic Use: pain-reliver + anti-inflammatory - used more than Ibuprofen in treating post-operative pain
Mechanism of Action: Selectively inhibits painful COX2
Metabolism: CYP2C9 - polymorphic poor metabolizers have reduced clearance

Question 33

Imatinib [Gleevec]

Mechanism of Action, Therapeutic Use

Answer 33

Mechanism of Action: binds to ATP-binding site of constitutively active BCR-ABL Tyrosine Kinase to prevent ATP binding and phosphorylation
Therapeutic Use: Treat specific type of CML

Question 34

Digoxin

What is it, Complications

Answer 34

Cardiac Medication
Transport: Uses OCT on basolateral side in Tubular Secretion
Competes with: Quinidine (another cardiac medication) - Prolonged half-lives, toxic build-up
Key Drug in Enterohepatic Cycle (Antibiotics kill gut bacteria - decrease drug’s half life)

Question 35

Estradiol

What is it, Complications

Answer 35

Birth Control

Key Drug in Enterohepatic Cycle (Antibiotics kill gut bacteria - decrease drug’s half life - cause unplanned pregancies)

Question 36

Statins

Mechanism of Action, Complications

Answer 36

Mechanism of Action: Inhibit HMG CoA Reductase - prevent cholesterol biosynthesis - treat familial hypercholesterolemia
Transport: Biliary Drug Excretion through SLC01B1 (OATP1B1)* polymorphisms cause increased sensitivity and toxicity - myotoxicity + muscle injury

Question 37

Tacrolimus

Therapeutic Use, TI, F, Metabolism, Pharmacogenomics

Answer 37

Therapeutic Use: Immunosuppressant, prevents organ rejection in transplants, treats inflammatory/autoimmune disorders
TI: NARROW requires TDM
F: Low F due to high first pass metabolism
Metabolism: by CYP3A4 (no polymorphisms) + CYP3A5 (polymorphisms significant!)
Pharmacogenomics: CYP3A5 variants have 1nc change in splice site that makes enzyme NON-functional - extremely common in Caucasians
Poor Metabolizers: Non-functional diplotype - most prevalent in Caucasians - considered norm - use standard dose and monitor with TDM
Intermediate/Extensive Metabolizers: increase starting dose

Question 38

Thiopurines

Therapeutic Use, Pharmacogenomics

Answer 38

Therapeutic Use: Pro-Drugs require conversion to THIOGUANINES for anti-cancer cytotoxicity
Pathway: Thiopurine - 6-MP - Thioguanine
TPMT: Enzyme that converts intermediate 6-MP into inactive form
Pharmacogenomics: variants have impaired TPMT function
Poor metabolizers: less elimination - increased risk for bone marrow suppression - need to give lower doses for variant carriers

Question 39

Mg2+ and other polyvalent cations (Mn, Co, La)

Mechanism of Action

Answer 39

Block pre-synaptic Calcium ion entry into nerve terminal at NMJ

Question 40

Botulinum Toxin Type A

Mechanism of Action, Therapeutic Use

Answer 40

1. cleaves SNAP-25 in fusion machinery - inhibits priming of secretion and release of ACh at NMJ
2. Therapeutic Use: Treats blepharospasm

Question 41

-curoniums

Mechanism of Action

Answer 41

1. Most popular non-depolarizing competitive inhibitors of nicotinic ACh receptors at NMJ

Question 42

Neostigmine [-stigmines]

Mechanism of Action, Therapeutic Use

Answer 42

1. reversible inhibitor of AChE at NMJ - prolongs effects of ACh
2. speeds recovery from -curoniums after surgery, treats Myasthenic Gravus

Question 43

Atropine

Mechanism of Action, Therapeutic Use

Answer 43

1. competitive inhibitor of ACh at mAChR’s in heart (parasympathetic), blocks vagal slowing
2. Increases HR during spinal anesthesia

Question 44

Ipratropium, Tiotropium [-tropiums]

Mechanism of Action, Therapeutic Use

Answer 44

1. competitive inhibitor of ACh at mAChR’s in bronchioles (parasympathetic), reduces constriction to open airway
2. Treat airway disorders (Asthma, COPD)

Question 45

Norepinephrine, Epinephrine, Phenylephrine

Mechanism of Action, Therapeutic Use

Answer 45

1. a-1 agonist - increase BP through smooth muscle constriction
2. phenylephrine also decreases nasal congestion by constricting mucosal layers

Question 46

Propanolol

Mechanism of Action, Therapeutic Uses, Metabolism

Answer 46

1. b-1 + b-2 competitive antagonist of norepinephrine
2. anti-arrhythmia, anti-HT, anti-HF
3. metabolized by CYP3A4