PRACTICE QUIZZES on antimicrobial chemotherapy

ANTIBACTERIALS ANTIVIRAL AND ANTIFUNGAL DRUGS ANTIMALARIAL DRUGS ANTIPROTOZOAL AND ANTIHELMINTHIC DRUGS  

By Pharmacology Mentor

Inhalation Anesthetics

Introduction Inhalation anesthetics play a central role in modern anesthesia, enabling practitioners to achieve and maintain general anesthesia during surgical procedures. Unlike intravenous agents, which rapidly induce unconsciousness, inhalation anesthetics are administered via inhaled gases or vapors, typically using advanced anesthesia machines and vaporizers. These agents act on the central nervous system (CNS) to produce loss of consciousness, analgesia, and in many cases, muscle relaxation. Widely

By Pharmacology Mentor

Antimicrobial Resistance and its mechanisms

Antimicrobial resistance (AMR) is the process by which microorganisms evolve to withstand the effects of drugs that were once effective against them. Understanding the mechanisms of resistance is vital for clinicians, microbiologists, and policy makers in managing infections and designing stewardship interventions. What Is Antimicrobial Resistance? AMR occurs when previously susceptible microbes (bacteria, fungi, viruses, or parasites) acquire the ability

By Pharmacology Mentor
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Over-the-Counter (OTC) Drugs: A Comprehensive Overview

Main Takeaway: Over-the-counter (OTC) drugs are non-prescription medications available directly to consumers

By Pharmacology Mentor

Antimicrobial Stewardship: An Editorial Review

1. Introduction and Scope Antimicrobial stewardship (AMS) is a coordinated set of interventions

By anonymous

Pharmacology of Fibrinolytics

Introduction Fibrinolytics—also known as thrombolytics—are a specialized class of pharmacological agents that

By Pharmacology Mentor

Aspirin: A Comprehensive Pharmacological Overview

Aspirin, scientifically known as acetylsalicylic acid (ASA), is a cornerstone in the

By Pharmacology Mentor

Classification of Adrenergic Receptors: A Quick Overview

Introduction Adrenergic receptors play a pivotal role in regulating physiological processes and

By Pharmacology Mentor

Pharmacology of Antiplatelet Drugs

Antiplatelet drugs inhibit platelet activation and aggregation, thereby reducing the risk of

By Pharmacology Mentor

Antimalarial Drugs – A Comprehensive Guide

Antimalarial drugs are a class of medications specifically designed to prevent and

By Pharmacology Mentor

Pharmacology of Prostaglandin Analogues

I. Introduction Prostaglandins are autacoids derived from arachidonic acid via the cyclooxygenase

By Dr. Ambadasu Bharatha
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Pharmacology of GLP-1 Agonists

1. Introduction: The Incretin Effect To understand GLP-1 agonists, one must first understand the "Incretin Effect." This physiological phenomenon describes the observation that oral glucose administration elicits a much higher insulin response than an isoglycemic intravenous (IV) glucose infusion. In Type 2 Diabetes Mellitus (T2DM), the incretin effect is significantly blunted, predominantly due to a reduction in GLP-1 secretion or responsiveness. This provides the rationale for pharmacological replacement. Figure 1. The Incretin Effect. The graph demonstrates the difference in plasma insulin levels following oral glucose intake versus intravenous infusion, despite identical plasma glucose levels. This difference is attributed to the release of incretin hormones (GLP-1 and GIP). 2. Physiology of Endogenous GLP-1 Endogenous GLP-1 is rapidly degraded (half-life < 2 minutes) by the enzyme Dipeptidyl Peptidase-4 (DPP-4). This rapid degradation makes native GLP-1 unsuitable as a drug. Physiological Actions of GLP-1: 3. Classification of GLP-1 Receptor Agonists Pharmacological agents are structurally modified to resist degradation by DPP-4, prolonging their half-life. They are classified based on their structure and duration of action. 3.1 Based on Structure 3.2 Based on Duration of Action CategoryDrugsDosing FrequencyEffect on Fasting vs. Post-Prandial Glucose (PPG)Short-ActingExenatide (Standard), LixisenatideTwice Daily / DailyPredominantly lowers PPG (via delayed gastric emptying).Long-ActingLiraglutide, LixisenatideDailyLowers both Fasting and PPG.Ultra-Long ActingSemaglutide, Dulaglutide, Exenatide XROnce WeeklyStrong reduction in Fasting Glucose; sustained control. 4. Mechanism of Action GLP-1 agonists bind to the GLP-1 receptor, a G-protein coupled receptor (GPCR) on the surface of pancreatic beta-cells and other tissues. Intracellular Signaling: Figure 2. Molecular Mechanism. GLP-1 binds to its GPCR on the beta-cell, increasing cAMP. This pathway enhances glucose-dependent insulin secretion. Crucially, this pathway is only active when glucose enters the cell, minimizing the risk of hypoglycemia. Systemic Effects ( The "Pleiotropic" Effects): Figure 3. Systemic Effects of GLP-1 Agonists. Beyond the pancreas, these drugs act on the brain (satiety), stomach (delayed emptying), liver (reduced gluconeogenesis via lower glucagon), and heart (cardioprotection). 5. Individual Agents & Pharmacokinetics 5.1 Exenatide 5.2 Liraglutide 5.3 Semaglutide 5.4 Dulaglutide 5.5 Tirzepatide (The "Twincretin") 6. Clinical Uses & Guidelines 7. Adverse Effects 8. Contraindications 9. Comparison: GLP-1 Agonists vs. DPP-4 Inhibitors This comparison is a favorite topic for viva/board exams. FeatureGLP-1 Receptor AgonistsDPP-4 Inhibitors (Gliptins)ExamplesLiraglutide, SemaglutideSitagliptin, LinagliptinRouteSubcutaneous (mostly)OralMechanismPharmacological levels of GLP-1 activityIncreases endogenous GLP-1 (physiologic levels)HbA1c ReductionHigh (1.0 – 1.8%)Modest (0.5 – 0.8%)Weight EffectSignificant Weight LossWeight NeutralGastric EmptyingDelayed (causes nausea)No effectCV BenefitProven Benefit (Lira, Sema, Dula)Neutral (Saxagliptin risk of HF)Side EffectsNausea, VomitingWell tolerated (Rare joint pain)CostHighModerate 10. References

By Pharmacology Mentor

Skeletal Muscle Relaxants: A Quick Guide

Introduction Skeletal muscle relaxants are a class of medications commonly used to alleviate muscle spasms and spasticity. These drugs are often employed in the management of conditions like multiple sclerosis

By Pharmacology Mentor