مقایسهٔ روشها
روشهای انتخابی خود را کنار هم مرور کنید؛ ردیفهای متفاوت برجسته شدهاند.
| الکتروفیزیولوژی وصله-گیره (Patch-Clamp Electrophysiology)× | مدلسازی فارماکودینامیک جمعیتی× | تحلیل شیلد (Schild Analysis)× | |
|---|---|---|---|
| حوزه | داروشناسی | داروشناسی | داروشناسی |
| خانواده | Process / pipeline | Process / pipeline | Process / pipeline |
| سال پیدایش≠ | 1976 | 1992 | 1947 |
| پدیدآور≠ | Erwin Neher and Bert Sakmann | Lewis Sheiner and Stephen Roush | Henry Schild |
| نوع≠ | ion channel screening | dose-response modeling | antagonism quantification |
| منبع بنیادین≠ | Neher, E., & Sakmann, B. (1976). Single-channel currents recorded from membrane of denervated frog muscle fibres. Nature, 260(5554), 799-802. DOI ↗ | Dahlström, B., & Nyberg, L. (1993). Population pharmacokinetics and pharmacodynamics. Clinical Pharmacokinetics, 24(1), 45-57. link ↗ | Schild, H. O. (1947). pA, a new scale for the measurement of drug antagonism. Journal of Physiology, 106(3), 337-357. DOI ↗ |
| نامهای دیگر≠ | patch clamp, whole-cell recording, ion channel assay | PopPD, population PD, hierarchical PD modeling | Schild plot, pA2 |
| مرتبط | 3 | 3 | 3 |
| خلاصه≠ | Patch-clamp electrophysiology is a technique for measuring ionic currents through ion channels in cell membranes, developed by Neher and Sakmann in 1976. It enables direct observation of single-channel and whole-cell currents at millisecond resolution, making it essential for characterizing drug effects on ion channels and cardiac safety assessment. | Population pharmacodynamic (PopPD) modeling integrates pharmacokinetics with individual dose-response relationships across patient populations to characterize drug efficacy and tolerability. Pioneered by Lewis Sheiner and colleagues, PopPD accounts for inter-individual variability in drug effects and enables rational dose optimization and response prediction. | Schild analysis is a quantitative method for characterizing competitive receptor antagonism developed by Henry Schild in 1947. It uses dose-response curves in the presence and absence of antagonist to estimate the antagonist affinity constant (pA2), enabling standardized comparison of antagonist potency across drugs and experimental systems. |
| ScholarGateمجموعهداده ↗ |
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