Design of intrinsically disordered region binding proteins

  1. Kejia Wu
  2. Hanlun Jiang
  3. Derrick R. Hicks
  4. Caixuan Liu
  5. Edin Muratspahić
  6. Theresa A. Ramelot
  7. Yuexuan Liu
  8. Kerrie McNally
  9. Sebastian Kenny
  10. Andrei Mihut
  11. Amit Gaur
  12. Brian Coventry
  13. Wei Chen
  14. Asim K. Bera
  15. Alex Kang
  16. Stacey Gerben
  17. Mila Ya-Lan Lamb
  18. Analisa Murray
  19. Xinting Li
  20. Madison A. Kennedy
  21. Wei Yang
  22. Zihao Song
  23. Gudrun Schober
  24. Stuart M. Brierley
  25. John O’Neill
  26. Michael H. Gelb
  27. Gaetano T. Montelione
  28. Emmanuel Derivery
  29. David Baker
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Abstract

Intrinsically disordered proteins and peptides play key roles in biology, but a lack of defined structures and high variability in sequence and conformational preferences have made targeting such systems challenging. We describe a general approach for designing proteins that bind intrinsically disordered protein regions in diverse extended conformations with side chains fitting into complementary binding pockets. We used the approach to design binders for 39 highly diverse unstructured targets, including polar targets, and obtained designs with 100-picomolar to 100-nanomolar affinities in 34 cases, testing ~22 designs per target. The designs function in cells and as detection reagents and are specific for their intended targets in all-by-all binding experiments. Our approach is a major step toward a general solution to the intrinsically disordered protein and peptide recognition problem.

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  1. Version published to 10.1126/science.adr8063
  2. Version published to 10.1101/2024.07.15.603480 on bioRxiv