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Protein Degradation via CRL4CRBN Ubiquitin Ligase: Discovery and Structure-Activity Relationships of Novel Glutarimide Analogs That Promote Degradation of Aiolos and/or GSPT1.

Joshua D HansenKevin CondroskiMatthew CorreaGeorge MullerHon-Wah ManAlexander RuchelmanWeihong ZhangFan VocansonTim CreaWei LiuGang LuFrans BaculiLaurie LeBrunAfshin MahmoudiGilles CarmelMatt HickmanChin-Chun Lu
Published in: Journal of medicinal chemistry (2017)
We previously disclosed the identification of cereblon modulator 3 (CC-885), with potent antitumor activity mediated through the degradation of GSPT1. We describe herein the structure-activity relationships for analogs of 3 with exploration of the structurally related dioxoisoindoline class. The observed activity of protein degradation could in part be rationalized through docking into the previously disclosed 3-CRBN-GSPT1 cocrystal ternary complex. For SAR that could not be rationalized through the cocrystal complex, we sought to predict SAR through a QSAR model developed in house. Through these analyses, selective protein degradation could be achieved between the two proteins of interest, GSPT1 and Aiolos.
Keyphrases
  • protein protein
  • molecular docking
  • small molecule
  • molecular dynamics
  • amino acid
  • high throughput