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7R8R

Physachenolide C with Bromodomain (BRD3-BD1)

7R8R の概要
エントリーDOI10.2210/pdb7r8r/pdb
関連するPDBエントリー3s92
分子名称Bromodomain-containing protein 3, Physachenolide C (3 entities in total)
機能のキーワードbromodomain 3, physachenolide c, prostate cancer, signaling protein
由来する生物種Homo sapiens (Human)
タンパク質・核酸の鎖数1
化学式量合計14915.22
構造登録者
Fromme, R.,Sivinski, J.,Zerio, C.,Gunatilaka, A.A.L.,Chapman, E. (登録日: 2021-06-27, 公開日: 2022-09-21, 最終更新日: 2023-10-25)
主引用文献Zerio, C.J.,Sivinski, J.,Wijeratne, E.M.K.,Xu, Y.M.,Ngo, D.T.,Ambrose, A.J.,Villa-Celis, L.,Ghadirian, N.,Clarkson, M.W.,Zhang, D.D.,Horton, N.C.,Gunatilaka, A.A.L.,Fromme, R.,Chapman, E.
Physachenolide C is a Potent, Selective BET Inhibitor.
J.Med.Chem., 66:913-933, 2023
Cited by
PubMed Abstract: 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.
PubMed: 36577036
DOI: 10.1021/acs.jmedchem.2c01770
主引用文献が同じPDBエントリー
実験手法
X-RAY DIFFRACTION (1.8 Å)
構造検証レポート
Validation report summary of 7r8r
検証レポート(詳細版)ダウンロードをダウンロード

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件を2024-10-30に公開中

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