EMDB/PDB/SASBDBから引用されている文献のデータベース

キーワード
構造解析手法	All X線回折 NMR 電子顕微鏡小角散乱中性子線回折線維回折粉末回折赤外分光 EPR FRET 理論モデルハイブリッド
著者・登録者
ジャーナル
IF	>30 >20 >10 >5 all

タイトル	UM171 glues asymmetric CRL3-HDAC1/2 assembly to degrade CoREST corepressors.
ジャーナル・号・ページ	Nature, Vol. 639, Issue 8053, Page 232-240, Year 2025
掲載日	2025年2月12日
著者	Megan J R Yeo / Olivia Zhang / Xiaowen Xie / Eunju Nam / N Connor Payne / Pallavi M Gosavi / Hui Si Kwok / Irtiza Iram / Ceejay Lee / Jiaming Li / Nicholas J Chen / Khanh Nguyen / Hanjie Jiang / Zhipeng A Wang / Kwangwoon Lee / Haibin Mao / Stefan A Harry / Idris A Barakat / Mariko Takahashi / Amanda L Waterbury / Marco Barone / Andrea Mattevi / Steven A Carr / Namrata D Udeshi / Liron Bar-Peled / Philip A Cole / Ralph Mazitschek / Brian B Liau / Ning Zheng /
PubMed 要旨	UM171 is a potent agonist of ex vivo human haematopoietic stem cell self-renewal. By co-opting KBTBD4, a substrate receptor of the CUL3-RING E3 ubiquitin ligase (CRL3) complex, UM171 promotes the ...UM171 is a potent agonist of ex vivo human haematopoietic stem cell self-renewal. By co-opting KBTBD4, a substrate receptor of the CUL3-RING E3 ubiquitin ligase (CRL3) complex, UM171 promotes the degradation of the LSD1-CoREST corepressor complex, thereby limiting haematopoietic stem cell attrition. However, the direct target and mechanism of action of UM171 remain unclear. Here we show that UM171 acts as a molecular glue to induce high-affinity interactions between KBTBD4 and HDAC1/2 to promote corepressor degradation. Through proteomics and chemical inhibitor studies, we identify the principal target of UM171 as HDAC1/2. Cryo-electron microscopy analysis of dimeric KBTBD4 bound to UM171 and the LSD1-HDAC1-CoREST complex identifies an asymmetric assembly in which a single UM171 molecule enables a pair of KELCH-repeat propeller domains to recruit the HDAC1 catalytic domain. One KBTBD4 propeller partially masks the rim of the HDAC1 active site, which is exploited by UM171 to extend the E3-neosubstrate interface. The other propeller cooperatively strengthens HDAC1 binding through a distinct interface. The overall CoREST-HDAC1/2-KBTBD4 interaction is further buttressed by the endogenous cofactor inositol hexakisphosphate, which acts as a second molecular glue. The functional relevance of the quaternary complex interaction surfaces is demonstrated by base editor scanning of KBTBD4 and HDAC1. By delineating the direct target of UM171 and its mechanism of action, we reveal how the cooperativity offered by a dimeric CRL3 E3 can be leveraged by a small molecule degrader.
リンク	Nature / PubMed:39939761 / PubMed Central
手法	EM (単粒子)
解像度	3.77 - 3.83 Å
構造データ	43386 8voj EMDB-43386, PDB-8voj: The Cryo-EM structure of LSD1-CoREST-HDAC1 in complex with KBTBD4 enhanced by UM171 and IP6 手法: EM (単粒子) / 解像度: 3.77 Å 47155 9dtg EMDB-47155, PDB-9dtg: The cryo-EM structure of apo KBTBD4 手法: EM (単粒子) / 解像度: 3.83 Å
化合物	ChemComp-ZN: Unknown entry ChemComp-IHP: INOSITOL HEXAKISPHOSPHATE PDB-1acv: DSBA MUTANT H32S
由来	homo sapiens (ヒト)
キーワード	TRANSCRIPTION / molecular glue / protein degradation / E3 ligase / transcription and translation / LIGASE / targeted protein degradation / transcription and tranlation