Which of the following statements is true regarding competitive reversible antagonism?

Efficacy and Vmax remain unchanged.

ED50 remains unchanged in competitive reversible antagonism.

Potency remains unchanged in the presence of a competitive antagonist.

Affinity (Kd) remains unchanged in competitive reversible antagonism.

What does the therapeutic index of a drug signify?

Dose which produces maximum effect

Maximum response that can be elicited by a drug

The therapeutic index of a drug is defined as the ratio between the toxic dose and the effective dose.

Ratio of toxic dose to effective dose

A shift to the right in the biological activity dose- response curve for a hormone with no accompanying change in the maximal response indicates:

Increased sensitivity and decreased responsiveness

Decreased responsiveness and decreased sensitivity

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

In treatment of Parkinsonism, L-Dopa is combined with carbidopa mainly to:

To decrease side effects of L–Dopa

To decrease dose requirement of L–Dopa

To decrease effectiveness of L–Dopa

To increase crossing of L–Dopa through BBB

Dose-Response Relationships for FMGE: High-Yield Pharmacology Lessons

DRC Basics & Curve Types - Dose Makes the Difference

Dose: Amount of drug. Response: Effect observed.
Dose-Response Relationship: Correlates dose with effect magnitude.
Graded Response:
- Effect intensity varies with dose in an individual.
- Example: Blood pressure change.
- Curve: Hyperbolic (linear dose) or sigmoid (log dose).
Quantal Response:
- All-or-none effect in a population (e.g., sleep/cure).
- Shows frequency of response.
- Curve: Typically sigmoid.
DRC Shapes (General):
- Hyperbolic: Response vs. linear dose.
- Sigmoid (S-shaped): Response vs. log dose; for $ED_{50}$, $E_{max}$ analysis.

⭐ Graded dose-response curves depict the intensity of effect in an individual, while quantal curves show the frequency of response in a population.

Graded Dose-Response Curves - Efficacy vs. Might-acy

Graded DRCs plot drug effect (response) against dose or concentration.
Efficacy ($E_{max}$): Maximum effect a drug can produce. Represents the drug's maximal therapeutic potential. Higher $E_{max}$ = ↑ efficacy.
Potency ($EC_{50}$ or $ED_{50}$): Dose/concentration required to produce 50% of $E_{max}$. Lower $EC_{50}$/$ED_{50}$ = ↑ potency.
- Primarily reflects drug-receptor binding affinity.
Slope of DRC: Indicates the range of doses over which response changes; steep slope = narrow therapeutic window.
📌 Mnemonic: Potency = Position (on X-axis, Left is more potent); Efficacy = Effect (Max Y-axis value).

⭐ Efficacy (maximum effect) is often clinically more important than potency (amount of drug needed for an effect).

Quantal DRCs & Drug Safety - Safety Numbers Game

Quantal DRCs: Dose vs. % population with all-or-none effect.
Key Metrics:
- $ED_{50}$: Effective dose in 50% of population.
- $TD_{50}$: Toxic dose in 50% of population.
- $LD_{50}$: Lethal dose in 50% (animals).
Drug Safety Indices (Margin of Safety indicators):
- Therapeutic Index ($TI$): $TI = \frac{TD_{50}}{ED_{50}}$ or $TI = \frac{LD_{50}}{ED_{50}}$.
  - 📌 TILE: Toxic Is Lethal / Effective.
  - Low $TI$ (narrow margin, requires monitoring): Warfarin, Lithium, Digoxin, Phenytoin, Theophylline.
  - 📌 "Warning: These Drugs Can Leak Poison".
- Certain Safety Factor ($CSF$): $CSF = \frac{LD_1}{ED_{99}}$ (stricter; $LD_1$: lethal 1%, $ED_{99}$: effective 99%).

⭐ A higher Therapeutic Index indicates a wider margin of safety for a drug.

Receptor Interactions & Response Variation - Receptor Roulette

Agonists: Bind & activate receptors.
- Full: Elicits maximal response ($E_{max}$); high intrinsic activity.
- Partial: Submaximal response; lower intrinsic activity. Can act as antagonist with full agonist.
- Inverse: Opposite effect to agonist; reduces basal receptor activity.

Antagonists: Bind receptors, block agonist. 📌 Competitive Right-shifts $EC_{50}$ ($E_{max}$ same); Non-competitive Lowers $E_{max}$ (NCLM).

Type	$EC_{50}$	$E_{max}$	Overcome by ↑ Agonist?	Site of Action
Competitive (Reversible)	↑ (Right shift)	Unchanged	Yes	Active
Non-competitive	Unchanged/↑	↓ (Down shift)	No	Allosteric/Active
Irreversible	Unchanged/↑	↓ (Down shift)	No (covalent bond)	Active

⭐ Competitive antagonists increase $EC_{50}$ (shift DRC right) but do not change $E_{max}$, while non-competitive antagonists decrease $E_{max}$ and may or may not change $EC_{50}$.

Response Variation:
- Spare Receptors: $E_{max}$ achieved with fractional receptor occupancy (e.g., insulin).
- Tachyphylaxis: Rapid ↓ drug response on repeated dosing (acute tolerance; e.g., ephedrine).
- Tolerance: Gradual ↓ drug effectiveness with chronic use.
- Desensitization: ↓ Receptor responsiveness (e.g., downregulation, uncoupling).
- Idiosyncrasy: Genetically determined abnormal drug reaction (e.g., G6PD deficiency).

High‑Yield Points - ⚡ Biggest Takeaways

Graded Dose-Response Curves (DRCs) relate drug dose to effect intensity.

Efficacy (Emax) is the maximum possible effect a drug can produce.

Potency (ED50): dose for 50% of Emax; lower ED50 means higher potency.

Quantal DRCs show population response (all-or-none) to varying doses.

Therapeutic Index (TI) = TD50/ED50; a wider TI indicates greater drug safety.

Spare receptors allow Emax with submaximal receptor occupancy.

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