Jove
Visualize
联系我们
JoVE
x logofacebook logolinkedin logoyoutube logo
关于 JoVE
概览领导团队博客JoVE 帮助中心
作者
出版流程编辑委员会范围与政策同行评审常见问题投稿
图书馆员
用户评价订阅访问资源图书馆顾问委员会常见问题
研究
JoVE JournalMethods CollectionsJoVE Encyclopedia of Experiments存档
教育
JoVE CoreJoVE BusinessJoVE Science EducationJoVE Lab Manual教师资源中心教师网站
使用条款与条件
隐私政策
政策

相关概念视频

Drug Concentration Versus Time Correlation01:15

Drug Concentration Versus Time Correlation

775
The plasma drug concentration-time curve is a crucial tool in pharmacokinetics, representing the drug's concentration in plasma at different time intervals post-administration. This curve illustrates the drug's journey from absorption into the systemic circulation, distribution to body tissues, and eventual elimination through excretion or biotransformation.
Two pivotal parameters are the minimum effective concentration (MEC) and the minimum toxic concentration (MTC). The MEC is the...
775
Analysis of Population Pharmacokinetic Data01:12

Analysis of Population Pharmacokinetic Data

257
Analysis of population pharmacokinetic data involves studying the behavior of drugs within diverse populations to understand their pharmacokinetic parameters. Traditional pharmacokinetic methods typically involve collecting samples from a few individuals and estimating these parameters. While these methods are commonly used, they have limitations in capturing the variability in drug response among individuals or heterogeneous populations. Population pharmacokinetics is employed to address these...
257
Dose-Response Relationship: Overview01:03

Dose-Response Relationship: Overview

3.1K
Agonists can bind with and activate receptors, resulting in the formation of drug-receptor complexes. Once formed, these complexes catalyze many biochemical processes at the cellular level and subsequently induce a pharmacologic response. The degree of response is directly proportional to the fraction of activated receptors, which in turn, depends on the concentration of the drug at the receptor site as well as the sensitivity of the receptor. An increase in the administered dose contributes to...
3.1K
Dose-Response Relationship: Potency and Efficacy01:22

Dose-Response Relationship: Potency and Efficacy

4.4K
The potency of a drug is the measure of its ability to produce a biological response and can be compared by looking at the half-maximum effective concentration or EC50 values of different drugs. A lower EC50 value indicates higher potency of the drug. In the dose–response curve of two antihypertensive drugs, candesartan and irbesartan, a significant difference is observed in their EC50 values. A lower EC50 value for candesartan indicates that it is more potent than irbesartan, as it...
4.4K

您也可能阅读

相关文章

通过共同作者、期刊和引用图与本文相关的文章。

排序
Same author

"Dual-Boosting" Strategy to Enhance Radical Generation of Photosensitizer for Mitochondria-Targeted Phototherapy.

Research (Washington, D.C.)·2026
Same author

Dynamic Manipulation Skill Learning for Tactile Myoelectric Prosthetic Hands in Tool Handling.

Cyborg and bionic systems (Washington, D.C.)·2026
Same author

A Multi-Scenario Coupled Simulation of Diet-Land Systems: Diet-Land Supply-Demand Matching and Responses from the Historical-to-Future.

Foods (Basel, Switzerland)·2026
Same author

SPD-DANN: An SPD manifold unsupervised domain adaptation method for cross subject motor imagery EEG decoding.

Neural networks : the official journal of the International Neural Network Society·2026
Same author

Updated subnational estimates of Water, Sanitation and Hygiene access in Low- and Middle-Income countries: a spatially referenced hierarchical ordinal multinomial modeling analysis using R template model builder.

Research square·2026
Same author

Trends and future of the disease burden of malignant neoplasms of bone and articular cartilage in China from 1990 to 2023: An analysis based on the Global Burden of Disease 2023.

European journal of surgical oncology : the journal of the European Society of Surgical Oncology and the British Association of Surgical Oncology·2026
Same journal

PACEff Builder: An Efficient Platform for Constructing PACE Hybrid-Resolution Models for Molecular Dynamics Simulations of Aqueous Protein, Peptide Assembly, and Membrane Protein Systems.

Journal of chemical information and modeling·2026
Same journal

TransKla: A Local-Global Cross-Attention Based Transformer Approach for Prediction of Lysine Lactylation Sites.

Journal of chemical information and modeling·2026
Same journal

CondenSimAdapter: A Versatile Builder for Multiscale Simulations of Protein Condensates with Broad Force-Field Compatibility and Robust Dense-Phase Relaxation.

Journal of chemical information and modeling·2026
Same journal

Simulation Guided Design of a Potentially Hyperactive Ice Nucleating Protein.

Journal of chemical information and modeling·2026
Same journal

Setting the Bases of the Photogenotoxicity of <i>p</i>-Aminobenzoic Acid.

Journal of chemical information and modeling·2026
Same journal

Probing Charge-Controlled Inter-Domain Flexibility: Integrating Experimental and Coarse-Grained Approaches.

Journal of chemical information and modeling·2026
查看所有相关文章

相关实验视频

Updated: Jul 4, 2025

Author Spotlight: Cost-Effective Transcriptomic Drug Screening - Unlocking New Targets
06:40

Author Spotlight: Cost-Effective Transcriptomic Drug Screening - Unlocking New Targets

Published on: February 23, 2024

1.3K

复合活动预测与剂量依赖的转录基因特征和深度学习.

William J Godinez1, Vladimir Trifonov2, Bin Fang2

  • 1Novartis Institutes for BioMedical Research, Emeryville, California 94608, United States.

Journal of chemical information and modeling
|January 31, 2024
PubMed
概括
此摘要是机器生成的。

转录组学到活动转换器 (TAT) 模型使用基因表达特征预测化合物生物活性. 这些计算模型成功识别了疟疾抑制剂,证明了药物发现的成本高效方法.

更多相关视频

Author Spotlight: Impact of Intergenic Interactions on Disease-Identifying Dark Biomarkers
03:37

Author Spotlight: Impact of Intergenic Interactions on Disease-Identifying Dark Biomarkers

Published on: March 1, 2024

727
Author Spotlight: Advancing Alzheimer's Research &#8211; Exploring Early Detection and Multi-Omics Approaches
09:47

Author Spotlight: Advancing Alzheimer's Research – Exploring Early Detection and Multi-Omics Approaches

Published on: December 15, 2023

1.0K

相关实验视频

Last Updated: Jul 4, 2025

Author Spotlight: Cost-Effective Transcriptomic Drug Screening - Unlocking New Targets
06:40

Author Spotlight: Cost-Effective Transcriptomic Drug Screening - Unlocking New Targets

Published on: February 23, 2024

1.3K
Author Spotlight: Impact of Intergenic Interactions on Disease-Identifying Dark Biomarkers
03:37

Author Spotlight: Impact of Intergenic Interactions on Disease-Identifying Dark Biomarkers

Published on: March 1, 2024

727
Author Spotlight: Advancing Alzheimer's Research &#8211; Exploring Early Detection and Multi-Omics Approaches
09:47

Author Spotlight: Advancing Alzheimer's Research – Exploring Early Detection and Multi-Omics Approaches

Published on: December 15, 2023

1.0K

科学领域:

  • 计算生物学是一种计算生物学.
  • 药物发现 药物发现
  • 系统药理学 系统药理学

背景情况:

  • 预测各种测试中的化合物活性在药物发现中至关重要.
  • 来自分析分析的基因表达特征可以预测其他分析中的化合物活性.
  • 应用包括预测作用机制 (MoA),非目标效应和多药学.

研究的目的:

  • 引入转录组学到活动变压器 (TAT) 模型,用于预测生物化学和细胞分析中的化合物活性.
  • 为了利用多种化合物度的基因表达特征,提高预测准确度.

主要方法:

  • 使用RASL-seq试验中的基因表达数据开发了TAT模型.
  • 训练模型预测262个剂量反应测试中的2692种化合物的活性.
  • 使用持有数据集和前性实验测试验证实模型实用性.

主要成果:

  • 在51%的测试中获得了有用的预测模型.
  • 在疟疾抑制试验中对TAT预测进行了前性验证,达到63%的成功率.
  • 通过前性验证确定了几种亚微分子疟疾抑制剂.

结论:

  • 通过TAT建模的跨化合物度的转录基因反应提供了一个强大的预测框架.
  • TAT模型提供了一种具有成本效益的方法,用于在各种测试中识别化合物生物活性.
  • 这种方法具有加速药物发现和开发的巨大潜力.