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相关概念视频

Biopharmaceutics and Pharmacokinetics: Overview01:28

Biopharmaceutics and Pharmacokinetics: Overview

3.3K
Understanding drugs, drug products, and their performance in pharmaceutical science is pivotal. Drugs, whether simple molecules or complex compounds, are designed to interact with the body's biological systems to diagnose, treat, or prevent diseases. Drug products include various delivery systems such as tablets, capsules, injections, and inhalers. The performance of these drug products is gauged by their ability to deliver the active ingredient to the desired site of action at the...
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Dosage Regimens: Designs and Approaches01:28

Dosage Regimens: Designs and Approaches

258
Designing a dosage regimen, which refers to the manner of drug administration, is a complex process involving the selection of drug dose, route, and frequency. This process is underpinned by pharmacokinetic parameters derived from tests and population averages. These parameters are then tailored to patient-specific variables such as diagnosis, demographics, and allergy status. Once therapy commences, therapeutic response monitoring is critical and achieved through clinical and physical...
258
Pharmacodynamics: Overview and Principles01:21

Pharmacodynamics: Overview and Principles

2.8K
Pharmacodynamics is a scientific field that delves into drugs' intricate biochemical, cellular, and physiological effects on the human body. The study of pharmacodynamics helps us understand how drugs interact with the body and elicit various responses.
Most drugs' effects result from their interactions with drug receptors or targets within the body. These interactions trigger specific responses at the cellular or systemic level. Drug receptors can be found on the surfaces of cells or...
2.8K
Dosage Regimens: Partial Pharmacokinetic Parameters01:01

Dosage Regimens: Partial Pharmacokinetic Parameters

147
It is not uncommon for complete drug pharmacokinetic profiles to remain elusive in pharmacokinetics. This necessitates certain educated assumptions by pharmacokineticists to determine appropriate dosage regimens without comprehensive pharmacokinetic data from animal or human studies. One prevalent assumption is setting the bioavailability factor, denoted as F, to 1 or 100%. This assumption caters to the scenario where a drug doesn't achieve full systemic absorption, resulting in the patient...
147
Pharmaceutical Equivalents01:26

Pharmaceutical Equivalents

175
As defined by regulatory standards, pharmaceutical equivalents require generic drug products to have identical dosage forms and chemically identical active pharmaceutical ingredients (APIs). They must adhere to compendial or applicable standards for potency, content uniformity, disintegration times, and dissolution rates. In the case of modified-release dosage forms, variations in drug content are permissible as long as the delivered amount remains consistent with the innovator drug product.
175
Nonlinear Pharmacokinetics: Overview01:19

Nonlinear Pharmacokinetics: Overview

1.1K
Nonlinear or dose-dependent pharmacokinetics is a phenomenon that occurs when the pharmacokinetic parameters of certain drugs deviate from linear pharmacokinetics at higher doses. These drugs do not follow the expected first-order kinetics, where the rate of drug elimination is directly proportional to the drug concentration. Instead, they exhibit a nonlinear relationship, which can be attributed to several factors.
Nonlinearity can arise due to the saturation of plasma protein-binding or...
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相关实验视频

Updated: Jan 13, 2026

Author Spotlight: Microbial Control and Monitoring Strategies for Cleanroom Environments and Cellular Therapies
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Author Spotlight: Microbial Control and Monitoring Strategies for Cleanroom Environments and Cellular Therapies

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在2026年IUPHAR/BPS指南的药理学.

Simon D Harding1, Jane F Armstrong1, Elena Faccenda1

  • 1Institute for Neuroscience and Cardiovascular Research, University of Edinburgh, Edinburgh EH8 9XD, United Kingdom.

Nucleic acids research
|October 29, 2025
PubMed
概括

药理学指南数据库 (GtoPdb) 提供专家策划的药理学数据对目标和配体. 最近的更新增强了内容,包括抗菌药理学和天然产品,改善了药物发现资源.

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相关实验视频

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Synthesis of pH Dependent Pyrazole, Imidazole, and Isoindolone Dipyrrinone Fluorophores using a Claisen-Schmidt Condensation Approach
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科学领域:

  • 药理学 药理学是指药理学的学科.
  • 生物医学信息学 生物医学信息学
  • 药物发现 药物发现 药物发现

背景情况:

  • IUPHAR/BPS药理学指南 (GtoPdb) 是一个全面的,开放的数据库.
  • 它提供了专家策划的蛋白质标和配体分子的药理学数据.
  • 数据库包括已批准的药物,小分子,和抗体.

研究的目的:

  • 在GtoPdb资源中报告最近的改进和内容扩展.
  • 突出抗菌药理学和新疗法领域的发展.
  • 以外部链接展示GtoPdb作为一个符合FAIR的资源的价值.

主要方法:

  • 数据库由专家策划.
  • 整合来自合作的数据 (例如,抗生素DB).
  • 在两年多的时间里,跨多个版本的内容扩展.

主要成果:

  • 该数据库现在包括3103个蛋白质标和13260个连接物分子.
  • 抗菌药理,天然产品和核酸含量的显著扩张.
  • 改进了经批准的药物的呈现,具有新的治疗点和潜在的调节剂.

结论:

  • GtoPdb是一个不断更新的,有价值的药理学研究资源.
  • 它的FAIR合规性和与外部数据库的链接增强了它的实用性.
  • 扩展内容支持各种药理学领域的药物发现和研究.