What would happen to the half-life and plasma concentration of a drug which follows first-order kinetics, if the dose is doubled?

Half - life remains the same and plasma concentration doubles

Half - life and plasma concentration remains the same

Half - life doubles and plasma concentration remains the same

Half - life and plasma concentration doubles

Low apparent volume of distribution of drug indicates that:

Drug is not extensively distributed to tissue

Tubular secretion of a drug can be confirmed if its renal clearance is:

More than the glomerular filtration rate (GFR)

Equal to the glomerular filtration rate (GFR)

Less than the glomerular filtration rate (GFR)

More than the volume of distribution

Compartment Models for INI-CET: High-Yield Pharmacology Lessons

Compartment Model Basics - Drug's Imaginary Homes

Theoretical pharmacokinetic spaces, not literal anatomical regions, where a drug is assumed to distribute uniformly.
Purpose: Simplify complex ADME processes to mathematically predict drug concentration ($C_p$) over time and optimize dosing regimens.
Key Assumptions:
- Body acts as a system of one or more interconnected compartments.
- Drug distribution within any compartment is instantaneous and homogenous (well-stirred).
- Drug transfer between compartments and elimination from the body typically follow first-order kinetics (rate proportional to drug amount).
Central Compartment ($V_c$): Includes plasma, extracellular fluid, and highly perfused tissues (e.g., heart, lungs, liver, kidneys); rapid drug equilibration.
Peripheral Compartment(s) ($V_p$): Includes less perfused tissues (e.g., muscle, fat, bone); slower drug equilibration.

One, Two, and Three Compartment Models

⭐ The number of exponential phases in the plasma drug concentration-time curve after an IV bolus dose determines the number of compartments in the model (e.g., two phases suggest a two-compartment model).

One-Compartment Model - The Simple Story

Body treated as a single, uniform compartment where drug distributes instantaneously and homogeneously.
Elimination typically follows first-order kinetics; rate of elimination is proportional to the drug amount.
Assumptions:
- Rapid mixing of drug throughout the compartment.
- Linear pharmacokinetics (processes are not saturated).
Key Parameters:
- Volume of Distribution ($V_d$): Apparent volume into which drug distributes.
  - $V_d = ext{Dose (IV bolus)} / C_0$ (where $C_0$ is initial plasma concentration)
- Elimination Rate Constant ($k_e$ or $k$): Fraction of drug eliminated per unit time.
- Half-life ($t_{1/2}$): Time for drug concentration to reduce by 50%.
  - $t_{1/2} = 0.693 / k_e$
- Clearance (CL): Volume of plasma cleared of drug per unit time.
  - $CL = k_e imes V_d$
Graphical Representation:
- A semi-log plot (log plasma concentration vs. time) yields a straight line after IV bolus.
Clinical Relevance:
- Simplifies dose calculations for drugs that rapidly distribute (e.g., some aminoglycosides after IV administration).

⭐ Following an IV bolus, drug concentration ($C_p$) declines monoexponentially: $C_p(t) = C_0 imes e^{-k_e imes t}$. The slope of the natural log plasma concentration versus time plot is $-k_e$. For log base 10, slope is $-k_e / 2.303$.

Two-Compartment Model - The Complex Tale

Drug initially in Central Compartment (blood, highly perfused organs like heart, lungs, kidneys, brain), then distributes to Peripheral Compartment (less perfused tissues, e.g., muscle, fat).
Plasma concentration ($C_p$) shows biexponential decline: 📌 Two compartments, two phases.
- $\alpha$-phase (Distribution): Rapid $C_p$ fall; drug central $\rightarrow$ peripheral.
- $\beta$-phase (Elimination): Slower $C_p$ fall; drug eliminated from central compartment post-distribution equilibrium. $\beta < \alpha$.
Equation: $C_p(t) = A \cdot e^{-\alpha t} + B \cdot e^{-\beta t}$.
Key Volumes of Distribution:
- $V_c$: Central compartment volume; for initial concentration after IV bolus.
- $V_{dss}$: Volume of distribution at steady state ($V_c + V_p$); reflects total drug after distribution.
- $V_{d\beta}$: Volume of distribution during $\beta$-phase; used for clearance: $CL = V_{d\beta} \cdot \beta$.
Rate Constants: $k_{12}$ (central $\rightarrow$ peripheral), $k_{21}$ (peripheral $\rightarrow$ central), $k_{10}$ (elimination from central).
Clinical Significance:
- Explains drug effect termination by redistribution (e.g., Thiopental: rapid IV anesthetic onset, short action due to redistribution to fat/muscle).
- Crucial for dosing drugs with slow tissue equilibration or narrow therapeutic index (e.g., Digoxin, Vancomycin).
- Loading dose often targets $V_c$; maintenance dose considers total clearance and $V_{dss}$ or $V_{d\beta}$.
Examples: Lidocaine, Vancomycin, Digoxin, Diazepam.

Semi-log plot of 1- and 2-compartment models

⭐ For drugs exhibiting two-compartment kinetics, the terminal elimination half-life ($t_{1/2\beta} = 0.693/\beta$) is longer than the distribution half-life ($t_{1/2\alpha} = 0.693/\alpha$) and is the primary determinant of dosing intervals once distribution is complete.

High‑Yield Points - ⚡ Biggest Takeaways

One-compartment model: Body as a single, uniform unit; drug distribution is instantaneous.

Two-compartment model: Central (blood, highly perfused) & peripheral (tissues) compartments.

Vd (Volume of Distribution): Relates drug amount in body to its plasma concentration.

Kel (Elimination Rate Constant): Fraction of drug eliminated per unit time.

t½ (Half-life): Time for drug concentration to decrease by 50%; inversely related to Kel.

Loading Dose: Achieves target plasma concentration rapidly, especially for large Vd.

Maintenance Dose: Maintains steady-state concentration within therapeutic range.

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