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相关概念视频

Protein-protein Interfaces02:04

Protein-protein Interfaces

13.7K
Many proteins form complexes to carry out their functions, making protein-protein interactions (PPIs) essential for an organism's survival. Most PPIs are stabilized by numerous weak noncovalent chemical forces. The physical shape of the interfaces determines the way two proteins interact. Many globular proteins have closely-matching shapes on their surfaces, which form a large number of weak bonds. Additionally, many PPIs occur between two helices or between a surface cleft and a...
13.7K
Protein Networks02:26

Protein Networks

4.1K
An organism can have thousands of different proteins, and these proteins must cooperate to ensure the health of an organism. Proteins bind to other proteins and form complexes to carry out their functions. Many proteins interact with multiple other proteins creating a complex network of protein interactions.
These interactions can be represented through maps depicting protein-protein interaction networks, represented as nodes and edges. Nodes are circles that are representative of a protein,...
4.1K
Protein-Protein Interfaces02:04

Protein-Protein Interfaces

3.9K
3.9K
Ligand Binding Sites02:40

Ligand Binding Sites

13.5K
Proteins are dynamic macromolecules that carry out a wide variety of essential processes; however, the activities of most proteins depend on their interactions with other molecules or ions, known as ligands.
Protein-ligand interactions are quite specific; even though numerous potential ligands surround a cellular protein at any given time, only a particular ligand can bind to that protein. Moreover, a ligand binds only to a dedicated area on the surface of the protein, known as the...
13.5K
Conserved Binding Sites01:49

Conserved Binding Sites

4.4K
Many proteins’ biological role depends on their interactions with their ligands, small molecules that bind to specific locations on the protein known as ligand-binding sites. Ligand-binding sites are often conserved among homologous proteins as these sites are critical for protein function.
Binding sites are often located in large pockets, and if their location on a protein’s surface is unknown, it can be predicted using various approaches. The energetic method computationally...
4.4K
Protein-Drug Binding: Determination Methods01:22

Protein-Drug Binding: Determination Methods

325
Determining protein-drug binding can be achieved through indirect and direct methods, each providing valuable insights into the interaction between proteins and drugs.
Indirect methods involve isolating the bound drug from its free form in biological samples such as blood, serum, or plasma. These techniques aim to measure the percentage of drugs bound to proteins. Equilibrium dialysis is a commonly used method where the free drug concentration at equilibrium is measured by separating the bound...
325

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相关实验视频

Updated: Sep 18, 2025

Development of Inhibitors of Protein-protein Interactions through REPLACE: Application to the Design and Development Non-ATP Competitive CDK Inhibitors
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Development of Inhibitors of Protein-protein Interactions through REPLACE: Application to the Design and Development Non-ATP Competitive CDK Inhibitors

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从概念到抑制剂:针对蛋白质-蛋白质相互作用的蓝图

Seong Ho Hong1, Thu Nguyen1, Joseph F Ongkingco1

  • 1Department of Chemistry, New York University, New York, New York 10003, United States.

Chemical reviews
|June 24, 2025
PubMed
概括

通过合理的设计和选,现在可以实现针对蛋白质与蛋白质相互作用 (PPI). 计算方法和选技术的进步使得开发新型抑制剂能够用于以前无法治疗的目标.

科学领域:

  • 生物化学 生物化学
  • 药物发现 药物发现 药物发现
  • 结构生物学 结构生物学

背景情况:

  • 从历史上看,蛋白与蛋白相互作用 (PPI) 被认为是不可抗药的目标.
  • 最近在理性设计和高通量选方面的进展改变了这一范式.
  • 针对PPI对于各种疾病的治疗干预至关重要.

研究的目的:

  • 审查推动针对个人隐私保护措施取得进展的概念和方法.
  • 突出设计抑制剂对抗具有挑战性的蛋白质表面的策略.
  • 讨论计算方法的整合,天然产品的洞察力和新的选技术.

主要方法:

  • 蛋白质表面的计算剖析用于连接体设计.
  • 宏观循环和小蛋白质连接体的设计.
  • 作为模板,利用天然产品衍生的结合表位.
  • 开发蛋白质结构模拟用于合理的抑制剂设计.
  • 结合受约束和当代选方法.

主要成果:

  • 识别可处理的蛋白质表面,以 Ras. 的成功准为例.
  • 开发用于设计小分子和基抑制剂的计算策略.

更多相关视频

Biosensor-based High Throughput Biopanning and Bioinformatics Analysis Strategy for the Global Validation of Drug-protein Interactions
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Biosensor-based High Throughput Biopanning and Bioinformatics Analysis Strategy for the Global Validation of Drug-protein Interactions

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Protein WISDOM: A Workbench for In silico De novo Design of BioMolecules
10:58

Protein WISDOM: A Workbench for In silico De novo Design of BioMolecules

Published on: July 25, 2013

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相关实验视频

Last Updated: Sep 18, 2025

Development of Inhibitors of Protein-protein Interactions through REPLACE: Application to the Design and Development Non-ATP Competitive CDK Inhibitors
10:33

Development of Inhibitors of Protein-protein Interactions through REPLACE: Application to the Design and Development Non-ATP Competitive CDK Inhibitors

Published on: October 26, 2015

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Biosensor-based High Throughput Biopanning and Bioinformatics Analysis Strategy for the Global Validation of Drug-protein Interactions
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Biosensor-based High Throughput Biopanning and Bioinformatics Analysis Strategy for the Global Validation of Drug-protein Interactions

Published on: December 1, 2020

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Protein WISDOM: A Workbench for In silico De novo Design of BioMolecules
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Protein WISDOM: A Workbench for In silico De novo Design of BioMolecules

Published on: July 25, 2013

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  • 利用天然的蛋白质-蛋白质结合接口来指导抑制剂的设计.
  • 在创建具有形状控制的多种连接体支架方面取得了进展.
  • 结论:

    • 针对PPI是一个快速发展的领域,具有显著的治疗潜力.
    • 计算,生化和选方法的结合是成功的关键.
    • 未来的努力可能会集中在进一步完善设计原则和扩大PPI抑制剂的查能力.