June 3, 2026 · STEAM

Pharmacology basics

Introduction to pharmacology

What is pharmacology?

Pharmacology is the science that studies how drugs interact with living systems. It covers the origins, chemistry, therapeutic uses, and adverse effects of medicines, integrating elements from biology, chemistry, physiology, and medicine. The goal is to understand how drugs produce beneficial effects while minimizing harm to patients.

Why study pharmacology?

Studying pharmacology equips clinicians and researchers to select appropriate therapies, optimize dosing, and anticipate potential safety issues. It explains why a medication works in one patient but not another, guiding personalized treatment plans. A solid pharmacology foundation also supports patient education, adherence, and responsible prescribing practices that protect public health.

Key terms you should know

Pharmacokinetics and pharmacodynamics
MOA (mechanism of action)
Receptor, agonist, antagonist
Bioavailability and first-pass metabolism
Half-life and elimination
Therapeutic window
Adverse effects and contraindications
Drug interactions and hypersensitivity

Drug actions and targets

Receptors and effectors

Drugs interact with specific biological targets to modify physiological functions. Receptors are the primary binding sites, often located on the cell surface or inside cells. Effectors include ion channels, enzymes, transporters, and signaling molecules that translate receptor engagement into a cellular response. Understanding these interactions helps predict a drug’s potency, efficacy, and potential side effects.

Mechanisms of action (MOA)

The MOA describes how a drug produces its therapeutic effect at the molecular level. Common MOAs include receptor activation or blockade, enzyme inhibition, transporter modulation, and interference with signaling pathways. Some medications act directly on their targets, while others modify the environment around the target to influence outcomes.

Agonists vs antagonists

Agonists bind to receptors and activate them, producing a biological response. Antagonists bind without triggering a response, blocking the receptor and preventing other molecules from acting. Partial agonists generate a weaker response than full agonists, offering an option to balance efficacy and safety. The interplay between these agents shapes clinical choices, especially when precise control of receptor activity is needed.

Allosteric modulators

Allosteric modulators bind to sites distinct from the primary active site, changing receptor shape and function. They can enhance (positive allosteric modulators) or inhibit (negative allosteric modulators) the effect of the endogenous ligand or a co-administered drug. This mechanism allows fine-tuning of responses and can improve safety by reducing overactivation or excessive inhibition.

Pharmacokinetics and pharmacodynamics

ADME overview

ADME describes how the body handles a drug: Absorption (how the drug enters the bloodstream), Distribution (how it travels to tissues), Metabolism (how it is chemically altered, often in the liver), and Excretion (how it is eliminated). Route of administration, formulation, and patient factors influence each step, shaping onset, intensity, and duration of effect.

Dose-response relationships

Dose-response relationships describe how increasing doses of a drug affect the magnitude of the response. A typical sigmoidal curve captures potency (the concentration required for a given effect) and efficacy (the maximum effect achievable). Clinically, this informs choosing a dose that achieves desired benefit while limiting harm.

Therapeutic window

The therapeutic window is the range between the minimum effective concentration and the minimum toxic concentration. Drugs with a wide window are generally safer, while those with a narrow window require careful monitoring, dose adjustments, or therapeutic drug monitoring to prevent adverse outcomes.

Bioavailability

Bioavailability measures the fraction of an administered dose that reaches systemic circulation in an active form. It varies by route (oral, intravenous, subcutaneous, etc.) and is influenced by absorption, metabolism, and first-pass effects. Understanding bioavailability helps explain differences in dosing and onset among formulations.

Half-life and elimination

The half-life is the time needed for the drug’s plasma concentration to reduce by half. It informs dosing intervals and how quickly a steady state is reached with repeated dosing. Elimination pathways, including renal and hepatic routes, determine how long a drug remains active and how to adjust dosing in organ impairment.

Drug safety and ethics

Adverse effects and contraindications

Adverse effects are unintended drug effects that can range from mild to life-threatening. Contraindications identify situations where a drug should not be used due to potential harm. Clinicians monitor for risk factors, adjust regimens, and educate patients to recognize warning signs and seek timely care.

Drug interactions

Drug interactions occur when one medication alters the effect of another. Interactions can be pharmacokinetic (affecting absorption, distribution, metabolism, or excretion) or pharmacodynamic (changing the drug’s effect at its target). Factors such as polypharmacy, age, genetics, and food choices (for example, certain fruit juices) influence interaction risk.

Risk-benefit assessment

Risk-benefit assessment weighs potential therapeutic gains against possible harms for a given patient. This evaluation considers disease severity, alternatives, patient preferences, comorbidities, and monitoring needs. Shared decision-making helps align treatment choices with patient values and safety considerations.

Common therapeutic classes

Analgesics

Analgesics relieve pain and include non-opioid options (like acetaminophen and NSAIDs) and opioid analgesics. Non-opioids may have anti-inflammatory effects or fever-reducing properties, while opioids require careful titration due to tolerance, dependence, and respiratory risks. Dose, duration, and patient context guide safe use.

Antibiotics

Antibiotics treat bacterial infections by targeting bacterial growth or survival. Stewardship is essential to prevent resistance, so clinicians select appropriate spectra, durations, and dosing. Allergies, interactions, and adverse effects such as gastrointestinal upset or superinfections are considered in plan formation.

Cardiovascular drugs

This class includes agents that control blood pressure, heart rate, and lipid levels, as well as drugs that treat heart failure and arrhythmias. Therapy often combines multiple drug types, requiring attention to interactions, monitoring of vital signs, and lab parameters (for example, electrolytes and lipid profiles).

Psychotropic medications

Psychotropic drugs influence mood, perception, or behavior and include antidepressants, antipsychotics, and anxiolytics. They require ongoing assessment of efficacy and tolerability, awareness of metabolic or neurological side effects, and careful consideration of withdrawal or dependence risks when stopping treatment.

Antidiabetics

Antidiabetic medications regulate blood glucose and include insulin and oral agents such as metformin. Therapy aims for glycemic control while minimizing hypoglycemia risk. Individualized plans address disease duration, comorbidities, lifestyle, and monitoring strategies.

Study tips and resources

Key mnemonics for quick recall

Helpful memory aids include:

ADME — Absorption, Distribution, Metabolism, Excretion
MOA — Mechanism of Action
“Right Drug, Right Dose, Right Patient, Right Time” — a patient-safety reminder

Practice questions and case studies

Engage with practice questions to test understanding of mechanisms, dosing, and safety. Case studies help translate theory into clinical scenarios, reinforcing decision-making when faced with comorbidity, polypharmacy, and varying patient factors. Use explanations to identify gaps in knowledge and guide focused review.

Trusted Source Insight

Trusted Source: https://www.who.int

Trusted Summary: WHO emphasizes rational use of medicines, patient safety, and access to essential medicines. It highlights pharmacovigilance, evidence-based prescribing, and public health considerations in pharmacology.