विधियों की तुलना करें
चुनी हुई विधियों की आमने-सामने समीक्षा करें; भिन्नता वाली पंक्तियाँ रेखांकित हैं।
| फार्माकोकाइनेटिक कम्पार्टमेंट मॉडल× | जैव-समतुल्यता विश्लेषण (दो एक-तरफ़ा परीक्षण)× | |
|---|---|---|
| क्षेत्र | औषधमिति | औषधमिति |
| परिवार≠ | Regression model | Hypothesis test |
| उद्भव वर्ष≠ | 1982 | 1987 |
| प्रवर्तक≠ | Gibaldi & Perrier | Donald J. Schuirmann |
| प्रकार≠ | Deterministic ODE-based pharmacokinetic model | Parametric equivalence test |
| मौलिक स्रोत≠ | Gibaldi, M., & Perrier, D. (1982). Pharmacokinetics (2nd ed.). Marcel Dekker. ISBN: 978-0-8247-1042-2 | Schuirmann, D. J. (1987). A comparison of the two one-sided tests procedure and the power approach for assessing the equivalence of average bioavailability. Journal of Pharmacokinetics and Biopharmaceutics, 15(6), 657–680. DOI ↗ |
| उपनाम | Mammillary Compartment Model, Multi-Compartment PK Model, Compartmental Analysis, Farmakokinetik Kompartman Modeli | TOST Procedure, Average Bioequivalence, BE Analysis, Biyoeşdeğerlik Analizi |
| संबंधित≠ | 3 | 2 |
| सारांश≠ | The pharmacokinetic compartment model represents the body as one or more hypothetical compartments interconnected by first-order rate processes, describing how a drug is absorbed, distributed, and eliminated over time. Systematized by Gibaldi and Perrier in 1982, these models use ordinary differential equations to characterize plasma concentration-time profiles. They are the cornerstone of drug development, dosage regimen design, and regulatory submission pharmacokinetic analyses. | Bioequivalence Analysis is a regulatory-grade statistical framework used to determine whether a test drug formulation (generic or reformulated) delivers the active ingredient to the systemic circulation at a rate and extent comparable to a reference product. Introduced by Donald J. Schuirmann in 1987, the method operationalizes equivalence through the Two One-Sided Tests (TOST) procedure, replacing the ambiguous absence-of-difference paradigm with an explicit equivalence margin evaluated on log-transformed pharmacokinetic endpoints such as AUC and C_max. |
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