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Viser: Targeting Protein-Protein Interactions for Drug Discovery

Targeting Protein-Protein Interactions for Drug Discovery, 1. udgave
Søgbar e-bog

Targeting Protein-Protein Interactions for Drug Discovery Vital Source e-bog

Jian Zhang
(2025)
John Wiley & Sons
1.544,00 kr.
Leveres umiddelbart efter køb
Targeting Protein-Protein Interactions for Drug Discovery

Targeting Protein-Protein Interactions for Drug Discovery

Jian Zhang
(2025)
Sprog: Engelsk
John Wiley & Sons, Incorporated
1.625,00 kr.
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Detaljer om varen

  • 1. Udgave
  • Vital Source E-book
  • Udgiver: John Wiley & Sons (September 2025)
  • ISBN: 9783527845811

Up-to-date reference surveying the latest advances in the structural understanding of protein-protein interactions and developments in drug discovery and therapeutics

Targeting Protein–Protein Interactions for Drug Discovery provides a systematic and comprehensive overview of protein-protein interactions (PPIs), reviewing foundational concepts, advanced methodologies, and emerging therapeutic strategies, reflecting the multidisciplinary nature of PPI research.

This book discusses computational methods for predicting PPI structures, with a special emphasis on protein docking and deep learning-based approaches, diverse chemical scaffolds for PPI modulation, including foldamers as inhibitors of aberrant PPIs and sulfonyl-³-AApeptides as novel modulators, and the development and application of stapled peptides as modulators of intracellular PPIs, offering enhanced stability, binding affinity, and cellular permeability.

Readers will also find information on cyclic peptides, focusing on their unique conformational stabilization and therapeutic potential across a range of diseases, small molecule inhibitors targeting BCL-family proteins, revealing their potential in cancer therapy, molecular glues as activators for PPIs, categorized into degraders, stabilizers, and inhibitors based on their biological effects, and the targeting of the APC–Asef interaction for drug discovery in colorectal cancer therapy, offering a case study of specificity and clinical relevance.

Targeting Protein–Protein Interactions for Drug Discovery explores sample topics including:

  • Challenges and strategies of drug discovery targeting PPIs, including high-throughput screening and structure-based drug design
  • Fluorescence resonance energy transfer (FRET) technology, a powerful tool for real-time analysis of molecular interactions in live cells
  • Utility of mass spectrometry (MS) for large-scale mapping of PPI networks with high sensitivity and resolution
  • Proximity ligation assays (PLA) for detecting PPIs in situ, emphasizing spatial precision and adaptability for multiplexed detection
  • Application of surface plasmon resonance (SPR) for characterizing PPI specificity, affinity, and kinetics

Exploring both classical and novel approaches to PPI characterization and modulation, Targeting Protein–Protein Interactions for Drug Discovery offers a comprehensive reference for researchers aiming to unlock the therapeutic potential of PPIs along with educators and students engaged in the study of cellular mechanisms, drug discovery, and biotechnology.

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Detaljer om varen

  • Hardback: 432 sider
  • Udgiver: John Wiley & Sons, Incorporated (November 2025)
  • ISBN: 9783527353606

Up-to-date reference surveying the latest advances in the structural understanding of protein-protein interactions and developments in drug discovery and therapeutics

Targeting Protein-Protein Interactions for Drug Discovery provides a systematic and comprehensive overview of protein-protein interactions (PPIs), reviewing foundational concepts, advanced methodologies, and emerging therapeutic strategies, reflecting the multidisciplinary nature of PPI research.

This book discusses computational methods for predicting PPI structures, with a special emphasis on protein docking and deep learning-based approaches, diverse chemical scaffolds for PPI modulation, including foldamers as inhibitors of aberrant PPIs and sulfonyl-γ-AApeptides as novel modulators, and the development and application of stapled peptides as modulators of intracellular PPIs, offering enhanced stability, binding affinity, and cellular permeability.

Readers will also find information on cyclic peptides, focusing on their unique conformational stabilization and therapeutic potential across a range of diseases, small molecule inhibitors targeting BCL-family proteins, revealing their potential in cancer therapy, molecular glues as activators for PPIs, categorized into degraders, stabilizers, and inhibitors based on their biological effects, and the targeting of the APC-Asef interaction for drug discovery in colorectal cancer therapy, offering a case study of specificity and clinical relevance.

Targeting Protein-Protein Interactions for Drug Discovery explores sample topics including:

  • Challenges and strategies of drug discovery targeting PPIs, including high-throughput screening and structure-based drug design
  • Fluorescence resonance energy transfer (FRET) technology, a powerful tool for real-time analysis of molecular interactions in live cells
  • Utility of mass spectrometry (MS) for large-scale mapping of PPI networks with high sensitivity and resolution
  • Proximity ligation assays (PLA) for detecting PPIs in situ, emphasizing spatial precision and adaptability for multiplexed detection
  • Application of surface plasmon resonance (SPR) for characterizing PPI specificity, affinity, and kinetics

Exploring both classical and novel approaches to PPI characterization and modulation, Targeting Protein-Protein Interactions for Drug Discovery offers a comprehensive reference for researchers aiming to unlock the therapeutic potential of PPIs along with educators and students engaged in the study of cellular mechanisms, drug discovery, and biotechnology.

1. Overview of protein-protein interaction (PPI) systems
2. Overview of drug discovery targeting PPI systems
3. Bioluminescence resonance energy transfer (BRET) assay for PPI study
4. Mass spectrometry (MS) for PPI study
5. Proximity ligation assay (PLA) for PPI study
6. Surface plasma resonance (SPR) assay for PPI study
7. Computational methods for PPI study
8. Peptidomimetics for PPI drug discovery
9. AApeptides for PPI drug discovery
10. Stapled peptides for PPI drug discovery
11. Cyclic peptides for PPI drug discovery
12. PPI drug discovery targeting B cell lymphoma (BCL) family
13. PPI drug discovery targeting MDM2-p53
14. PPI drug discovery targeting APC-Asef
15. Computational methods applied to drug discovery for PPI systems
16. Allosteric modulation of PPI systems for drug discovery
17. Current Challenges and Future Directions
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