8+ Novel Intramolecular Bivalent Glues for Targeted Protein Degradation

targeted protein degradation via intramolecular bivalent glues

8+ Novel Intramolecular Bivalent Glues for Targeted Protein Degradation

This emerging technology harnesses small molecules to induce highly specific elimination of disease-causing proteins. These molecules, functioning as “molecular bridges,” link a target protein to the cellular machinery responsible for protein degradation. This bridging mechanism allows for the targeted removal of proteins previously considered “undruggable” by traditional methods that typically inhibit protein function rather than eliminate the protein itself. For example, a bivalent molecule can be designed with one arm that binds to a specific protein targeted for degradation, and another arm that recruits an E3 ubiquitin ligase, a key component of the protein degradation system.

The ability to selectively eliminate proteins opens exciting new avenues for therapeutic intervention. This approach offers potential advantages over traditional drug modalities by addressing the root cause of diseases driven by problematic proteins, rather than just mitigating their effects. Historically, drug development has focused on inhibiting the function of disease-related proteins. However, many proteins lack suitable binding sites for effective inhibition. This new degradation technology overcomes this limitation, vastly expanding the range of potentially druggable targets and offering new hope for diseases currently lacking effective treatments.

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9+ Top Targeted Protein Degradation Conferences 2024

targeted protein degradation conference

9+ Top Targeted Protein Degradation Conferences 2024

Events focused on eliminating specific proteins within cells, typically through small-molecule induced proximity, represent a burgeoning area of research in drug discovery and development. These meetings bring together experts from diverse fields such as chemistry, biology, pharmacology, and clinical medicine. A typical gathering might involve presentations on novel degrader molecules, discussions of emerging therapeutic targets, and analyses of clinical trial results. For example, sessions could cover PROTACs (proteolysis-targeting chimeras), molecular glues, or other degradation technologies.

Such assemblies are crucial for advancing this rapidly evolving field. They foster collaboration and information exchange among researchers, accelerating the development of new therapies for a range of diseases, including cancer, neurodegenerative disorders, and infectious diseases. Historically, drug development has focused on inhibiting protein function. However, this approach is limited by the “druggability” of target proteins. Eliminating disease-causing proteins entirely offers a novel and potentially more effective therapeutic strategy.

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