Login / Signup

Physachenolide C is a Potent, Selective BET Inhibitor.

Christopher J ZerioJared SivinskiE M Kithsiri WijeratneYa-Ming XuDuc T NgoAndrew J AmbroseLuis Villa-CelisNiloofar GhadirianMichael W ClarksonDonna D ZhangNancy C HortonA A Leslie GunatilakaRaimund FrommeEli Chapman
Published in: Journal of medicinal chemistry (2022)
A pulldown using a biotinylated natural product of interest in the 17β-hydroxywithanolide (17-BHW) class, physachenolide C (PCC), identified the bromodomain and extra-terminal domain (BET) family of proteins (BRD2, BRD3, and BRD4), readers of acetyl-lysine modifications and regulators of gene transcription, as potential cellular targets. BROMOscan bromodomain profiling and biochemical assays support PCC as a BET inhibitor with increased selectivity for bromodomain (BD)-1 of BRD3 and BRD4, and X-ray crystallography and NMR studies uncovered specific contacts that underlie the potency and selectivity of PCC toward BRD3-BD1 over BRD3-BD2. PCC also displays characteristics of a molecular glue, facilitating proteasome-mediated degradation of BRD3 and BRD4. Finally, PCC is more potent than other withanolide analogues and gold-standard pan-BET inhibitor (+)-JQ1 in cytotoxicity assays across five prostate cancer (PC) cell lines regardless of androgen receptor (AR)-signaling status.
Keyphrases
  • prostate cancer
  • high resolution
  • high throughput
  • gene expression
  • mass spectrometry
  • single cell
  • computed tomography
  • risk assessment
  • anti inflammatory
  • climate change
  • case control
  • structure activity relationship