Nature Communications (Oct 2024)

Reversible covalent c-Jun N-terminal kinase inhibitors targeting a specific cysteine by precision-guided Michael-acceptor warheads

  • Dániel Bálint,
  • Ádám Levente Póti,
  • Anita Alexa,
  • Péter Sok,
  • Krisztián Albert,
  • Lili Torda,
  • Dóra Földesi-Nagy,
  • Dániel Csókás,
  • Gábor Turczel,
  • Tímea Imre,
  • Eszter Szarka,
  • Ferenc Fekete,
  • Isabel Bento,
  • Márton Bojtár,
  • Roberta Palkó,
  • Pál Szabó,
  • Katalin Monostory,
  • Imre Pápai,
  • Tibor Soós,
  • Attila Reményi

DOI
https://doi.org/10.1038/s41467-024-52573-2
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 19

Abstract

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Abstract There has been a surge of interest in covalent inhibitors for protein kinases in recent years. Despite success in oncology, the off-target reactivity of these molecules is still hampering the use of covalent warhead-based strategies. Herein, we disclose the development of precision-guided warheads to mitigate the off-target challenge. These reversible warheads have a complex and cyclic structure with optional chirality center and tailored steric and electronic properties. To validate our proof-of-concept, we modified acrylamide-based covalent inhibitors of c-Jun N-terminal kinases (JNKs). We show that the cyclic warheads have high resilience against off-target thiols. Additionally, the binding affinity, residence time, and even JNK isoform specificity can be fine-tuned by adjusting the substitution pattern or using divergent and orthogonal synthetic elaboration of the warhead. Taken together, the cyclic warheads presented in this study will be a useful tool for medicinal chemists for the deliberate design of safer and functionally fine-tuned covalent inhibitors.