Pharmacy — Pharmacokinetics, Drug Classes & Mechanisms

🎯 Module Objectives

Define and apply the four pharmacokinetic parameters: ADME
Calculate and interpret half-life, volume of distribution and bioavailability
Explain dose-response relationships, agonism and antagonism
Classify major drug categories by receptor/enzyme target and mechanism
Predict clinically relevant drug interactions using CYP450 knowledge
Identify common adverse effects by drug class

1. Pharmacokinetics — What the Body Does to a Drug

Pharmacokinetics (PK) describes how a drug moves through the body over time. Summarised by the ADME framework.

Absorption → Distribution → Metabolism → Excretion

Key PK Parameters

Parameter	Definition	Clinical Significance
Half-life (t½)	Time for plasma drug concentration to fall by 50%	Determines dosing frequency; after 5 t½, drug is effectively eliminated
Volume of Distribution (Vd)	Apparent volume in which drug is distributed in the body	High Vd = extensive tissue binding; low Vd = stays in plasma
Bioavailability (F)	Fraction of administered dose reaching systemic circulation unchanged	IV = 100%; oral often <100% due to first-pass metabolism
Clearance (CL)	Volume of plasma cleared of drug per unit time	Determines maintenance dose; affected by renal/hepatic function
Steady State (Css)	Plasma concentration plateau reached after ~5 half-lives of regular dosing	Target for therapeutic drug monitoring

2. ADME in Detail

Absorption

Routes: oral (PO), intravenous (IV), intramuscular (IM), subcutaneous (SC), transdermal, inhalation
First-pass effect: orally administered drugs absorbed from GI tract pass through the liver before reaching systemic circulation; extensive hepatic metabolism can significantly reduce bioavailability (e.g., nitroglycerin: ~1% oral bioavailability → given sublingually)
Lipid-soluble drugs are better absorbed passively; polar drugs require transporters

Distribution

Drug distributes from blood into tissues based on: lipid solubility, plasma protein binding, tissue affinity
Plasma protein binding: only free (unbound) drug is pharmacologically active; highly protein-bound drugs have smaller effective Vd
Blood-brain barrier (BBB): only lipid-soluble, unbound drugs readily cross; protective against many toxins but limits CNS drug delivery

Metabolism

Primary site: liver (also intestine, lungs, kidneys)
Phase I: oxidation, reduction, hydrolysis — often via CYP450 enzymes → creates more polar metabolite (may be active or inactive)
Phase II: conjugation (glucuronidation, sulfation, acetylation) → makes metabolite water-soluble for excretion
CYP450 enzymes: CYP3A4 (most common; ~50% of drugs), CYP2D6, CYP2C9, CYP2C19

Excretion

Renal: most common route; glomerular filtration + tubular secretion − tubular reabsorption
Biliary/faecal: large/polar molecules secreted into bile; some undergo enterohepatic recirculation
Dose reduction required in renal/hepatic impairment for renally/hepatically cleared drugs

📌 Clinical Pearl — Always check renal function before dosing renally-excreted drugs (e.g., metformin, digoxin, aminoglycosides). Check liver function before hepatically-metabolised drugs with narrow therapeutic indices.

3. Pharmacodynamics — What the Drug Does to the Body

Drug-Receptor Theory

Affinity: drug's ability to bind its receptor
Efficacy (intrinsic activity): ability to produce a maximal response once bound
Potency: amount of drug needed to produce 50% of maximal effect (EC₅₀). High potency = low EC₅₀.

Agonists and Antagonists

Drug Type	Binds Receptor?	Activates Receptor?	Example
Full Agonist	Yes	Yes (100%)	Morphine (μ-opioid receptor)
Partial Agonist	Yes	Yes (<100%)	Buprenorphine (μ-opioid receptor)
Antagonist	Yes	No	Naloxone (μ-opioid receptor)
Inverse Agonist	Yes	Reduces basal activity	Some antihistamines (H1 receptor)

Therapeutic Window

The range between the minimum effective dose and the minimum toxic dose. Drugs with a narrow therapeutic window (e.g., digoxin, warfarin, lithium, phenytoin) require careful monitoring.

Therapeutic index (TI) = TD₅₀ / ED₅₀. Higher TI = safer drug.
MEC (Minimum Effective Concentration) and MTC (Minimum Toxic Concentration) define the therapeutic window in plasma

4. Major Drug Classes

Class	Mechanism	Key Examples	Primary Use
β-Blockers	Competitive antagonism of β-adrenergic receptors (β1 > β2)	Metoprolol, Atenolol, Propranolol	Hypertension, angina, arrhythmia, heart failure
ACE Inhibitors	Inhibit ACE → ↓ angiotensin II + ↓ aldosterone	Lisinopril, Enalapril, Ramipril	Hypertension, heart failure, diabetic nephropathy
Statins	Competitive inhibition of HMG-CoA reductase → ↓ cholesterol synthesis	Atorvastatin, Rosuvastatin, Simvastatin	Hypercholesterolaemia, cardiovascular risk reduction
NSAIDs	Reversible inhibition of COX-1 and COX-2 → ↓ prostaglandins	Ibuprofen, Naproxen, Diclofenac	Pain, inflammation, fever
Antibiotics (Penicillins)	Inhibit bacterial cell wall synthesis (β-lactam binds PBP)	Amoxicillin, Flucloxacillin, Piperacillin	Gram-positive and some gram-negative bacterial infections
SSRIs	Block serotonin reuptake transporter (SERT) → ↑ synaptic serotonin	Fluoxetine, Sertraline, Escitalopram	Depression, anxiety disorders, OCD
Metformin	Activates AMPK → ↓ hepatic gluconeogenesis; ↑ peripheral glucose uptake	Metformin	Type 2 diabetes; first-line therapy
Warfarin	Inhibits vitamin K epoxide reductase → ↓ clotting factors II, VII, IX, X	Warfarin	Anticoagulation (atrial fibrillation, DVT/PE prevention)
Opioids	Agonists at μ, δ, κ opioid receptors → inhibit pain signalling	Morphine, Oxycodone, Fentanyl, Codeine	Moderate-severe pain; high addiction potential

5. Drug Interactions

CYP450-Mediated Interactions

CYP inhibitors — reduce metabolism of co-administered drugs → ↑ plasma levels → risk of toxicity
Examples: fluconazole, erythromycin, grapefruit juice (CYP3A4 inhibitors)
CYP inducers — increase metabolism → ↓ plasma levels → risk of treatment failure
Examples: rifampicin, carbamazepine, St John's Wort (CYP3A4 inducers)

Pharmacodynamic Interactions

Additive — effects of two drugs sum (e.g., two CNS depressants → greater sedation)
Synergistic — combined effect greater than sum (e.g., β-lactam + aminoglycoside against gram-negative bacteria)
Antagonistic — one drug reduces effect of another (e.g., naloxone reverses opioid effects)

⚠️ High-Risk Combination — Warfarin + any CYP2C9 inhibitor (e.g., fluconazole, amiodarone) dramatically increases bleeding risk by reducing warfarin metabolism. Requires immediate INR monitoring and dose adjustment.

Knowledge Check

1. A drug has a half-life of 8 hours. How long until it reaches steady state with regular dosing?

Steady state is reached after approximately 5 half-lives. 5 × 8 hours = 40 hours (~1.7 days). This is true regardless of the dose or dosing interval — it's determined solely by the half-life.

2. Why is the oral bioavailability of nitroglycerin very low and how is this overcome?

Nitroglycerin undergoes extensive first-pass metabolism in the liver (~99%), so almost none of an oral dose reaches systemic circulation. This is overcome by sublingual (under the tongue) administration, which allows direct absorption into the systemic circulation via the rich sublingual vasculature, bypassing first-pass metabolism.

3. A patient on warfarin is started on rifampicin for TB. What do you expect to happen and why?

Rifampicin is a potent CYP450 inducer (particularly CYP2C9, which metabolises warfarin). Induction increases warfarin metabolism → lower warfarin plasma levels → reduced anticoagulation → risk of thrombosis. The warfarin dose will need to be significantly increased. When rifampicin is later stopped, the dose must be reduced again to avoid bleeding.

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Pharmacokinetics · Pharmacodynamics · Drug Classes