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Unlocking New E3 Ligases for Targeted Protein Degradation in Cancer Therapy

Pioneering the Use of Novel E3 Ligases for Precision Protein Degradation

  • Current therapies target only 400 out of over 4,000 disease-associated proteins, emphasizing the necessity for expanded E3 ligase applications.
  • Curated an extensive list of E3 ligases, analyzing their ligandability, expression patterns, and interactions using advanced tools like UbiHub, UbiBrowser, and E3Atlas.
  • Evaluated E3 ligase expression across various cancer types to identify optimal candidates for safe and effective cancer therapy.
  • Identified C10orf90 as a potential superior TP53-specific E3 ligase, marking a significant advancement in targeted protein degradation strategies.
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