Drug X has an affinity for albumin, while drug Y has 150 times greater affinity. Which of the following statements is MOST accurate?

The free concentration of drug X in blood is higher, facilitating tissue distribution.

Drug X will be more available in tissues

Drug Y will be less available in tissues

Toxicity of drug Y may be influenced by multiple factors, not just its binding.

Which of the following describes the first-pass metabolism?

Drug given orally is metabolized by the liver before entering the circulation.

Drug given intravenously bypasses the liver initially.

Gastric acids primarily affect the stability of drugs.

Absorption of a drug occurs in the intestines.

Brand A of liposomal amphotericin B is of innovator company and brand B is of a generic company. AUC of Brand A is 124 mg.h/L and AUC of brand B is 115 mg.h/L. Which of the following statements is correct?

Brand A is bioequivalent to brand B

Brand A is not bioequivalent to brand B

Brand A has higher volume of distribution than brand B

Brand B has higher volume of distribution than brand A

Low apparent volume of distribution of drug indicates that:

Drug is not extensively distributed to tissue

Pharmacokinetics: Absorption and Distribution for UPSC-CMS: High-Yield Pharmacology Lessons

Membrane Transport & Absorption - Getting In!

Cell Membrane: Phospholipid bilayer, proteins; fluid mosaic model.
Passive Transport Mechanisms:
- Simple Diffusion:
  - Major route.
  - Down conc. gradient; no energy.
  - Favors lipid-soluble, unionized drugs.
  - Fick's Law: Rate $\propto \frac{\text{Surface Area} \times (\text{C}_1-\text{C}_2) \times \text{Permeability}}{\text{Thickness}}$
  - pH & Ionization: Henderson-Hasselbalch eq. for ionization.
    - Acids: $pH - pKa = \log([\text{Ionized A}^-]/[\text{Unionized HA}])$
    - Bases: $pKa - pH = \log([\text{Ionized BH}^+]/[\text{Unionized B}])$
  - 📌 Unionized form is lipid-soluble & absorbed.
    - Acidic drugs (Aspirin): ↑ unionized in acidic pH (stomach).
    - Basic drugs (Morphine): ↑ unionized in alkaline pH (intestine).
- Filtration: Small water-soluble drugs (< 100-200 Da) via aqueous pores.
Carrier-Mediated Transport: Uses transporters; specific, saturable, competitive.
- Facilitated Diffusion: Down gradient, no energy (e.g., GLUT for glucose).
- Active Transport: Against gradient, needs ATP (e.g., Na+/K+ ATPase, SGLT1).
  - Efflux: P-glycoprotein (MDR1) pumps out drugs, ↓ absorption.
Vesicular Transport (Endo/Exocytosis): Large molecules (e.g., Vit B12-IF).

⭐ P-glycoprotein (MDR1), an efflux pump, significantly impacts drug absorption and bioavailability, contributing to multidrug resistance.

Cell membrane transport mechanisms

Routes & Bioavailability - The Entry Game

Routes of Administration:
- Enteral: Oral (PO), Sublingual (SL), Rectal (PR).
  - PO: Common, convenient; subject to first-pass.
  - SL/Buccal: Bypasses first-pass (Nitroglycerin); rapid.
  - Rectal: Partial (≈50%) first-pass bypass; useful if N/V.
- Parenteral: IV, IM, SC.
  - IV: 100% bioavailability; immediate effect.
  - IM/SC: Depot possible; variable absorption.
- Inhalational: Rapid onset (anaesthetics, bronchodilators); large SA.
- Transdermal: Sustained delivery, bypasses first-pass (Fentanyl patch).
Bioavailability (F): Fraction of drug reaching systemic circulation unchanged.
- $F = (\frac{AUC_{oral}}{AUC_{IV}}) \times 100%$ (for same dose).
- IV route: $F = \textbf{100}%$.
- ↓F due to: First-pass metabolism, poor absorption, instability, formulation.
First-Pass Metabolism: Pre-systemic metabolism (liver, gut wall) ↓F.
- Affects: Propranolol, Lignocaine, Nitroglycerin (oral).
- 📌 "LMNOP": Lignocaine, Morphine, Nitroglycerin, Oestrogens, Propranolol (high first-pass).

⭐ Drugs with high first-pass metabolism (e.g., Lignocaine) require significantly higher oral doses than IV doses to achieve comparable therapeutic effects due to extensive pre-systemic elimination.

Drug Distribution - Spreading Out!

Drug movement: Blood → Tissues.
Key Factors:
- Lipid Solubility: ↑ solubility → ↑ distribution.
- Ionization (pH-pKa): Non-ionized form crosses membranes.
- Plasma Protein Binding (PPB):
  - Albumin (acidic drugs: warfarin), α1-acid glycoprotein (basic drugs: lidocaine).
  - Only unbound drug is active & distributes. High PPB → ↓ $V_d$, longer $t_{1/2}$.
- Blood Flow/Perfusion: Brain, liver, kidney (rapid); Fat, bone (slow).
- Tissue Affinity: E.g., Iodine (thyroid), Digoxin (heart), Chloroquine (liver, retina).
Volume of Distribution ($V_d$):
- Apparent volume drug occupies if concentration throughout body equals plasma concentration.
- Formula: $V_d = \frac{\text{Total amount of drug in body (Dose)}}{\text{Plasma drug concentration } (C_0)}$
- Low $V_d$ (< 5L): Confined to plasma (e.g., Heparin).
- Intermediate $V_d$ (15-20L): ECF (e.g., Aminoglycosides).
- High $V_d$ (> 40L): Accumulates in tissues (e.g., Chloroquine, Digoxin).
- Clinical use: Calculate Loading Dose ($LD = V_d \times C_{target}$).
Redistribution: Highly lipid-soluble IV drugs (e.g., Thiopental) initially to brain, then to muscle/fat → rapid termination of CNS effect.
Special Barriers:
- Blood-Brain Barrier (BBB): Tight junctions; P-glycoprotein efflux. Restricts polar drugs. Lipid-soluble drugs pass.
- Placental Barrier: Most drugs cross to some extent, especially lipid-soluble.

⭐ Drugs with a very high $V_d$ (e.g., Chloroquine, Amiodarone) are not effectively removed by hemodialysis because they are extensively sequestered in tissues, away from the blood being dialyzed.

High‑Yield Points - ⚡ Biggest Takeaways

Lipid solubility (↑) & low ionization favor drug absorption.

First-pass metabolism (liver/gut) ↓ oral bioavailability.

Bioavailability (F) = fraction of drug reaching systemic circulation unchanged.

Volume of distribution (Vd) reflects tissue drug distribution; high Vd = more in tissues.

Plasma protein binding: acidic drugs to albumin, basic drugs to α1-acid glycoprotein.

Only unbound drug is active, distributed, metabolized, excreted.

P-glycoprotein (MDR1): efflux pump, ↓ absorption, limits brain/placental entry_

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