Efficient targeted oncogenic KRASG12C degradation via first reversible-covalent PROTAC

被引:56
|
作者
Yang, Fang [1 ]
Wen, Yalei [1 ]
Wang, Chaofan [1 ]
Zhou, Yuee [1 ]
Zhou, Yang [1 ]
Zhang, Zhi-Min [1 ]
Liu, Tongzheng [1 ]
Lu, Xiaoyun [1 ]
机构
[1] Jinan Univ, Coll Pharm, 601 Huangpu Ave West, Guangzhou 510632, Peoples R China
来源
EUROPEAN JOURNAL OF MEDICINAL CHEMISTRY | 2022年 / 230卷
基金
中国国家自然科学基金;
关键词
KRAS(G12C); Reversible-covalent inhibitors; PROTAC; Anticancer; Warheads; PROTEIN-DEGRADATION; AMG; 510; KRAS; INHIBITORS; DISCOVERY; CANCER;
D O I
10.1016/j.ejmech.2021.114088
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
KRAS is the most frequently mutated oncogene and plays a predominant role in driving initiation and progression of multiple cancers. Attempts to degrade the oncogene KRAS(G12C) with PROTAC strategy have been considered as an alternative strategy to combate cancers. However, the irreversible PROTACs may compromise the substoichiometric activity to decrease the potency. Herein, we report the development of YF135, the first reversible-covalent PROTAC capable of recruiting VHL mediated proteasomal degradation of KRAS(G12C). YF135 induces the rapid and sustained degradation of endogenous KRAS(G12C) and attenuates pERK signaling in H358 and H23 cells in a reversible manner. (C) 2022 Elsevier Masson SAS. All rights reserved.
引用
收藏
页数:13
相关论文
共 50 条
  • [31] Covalent inhibitor targets KRasG12C: A new paradigm for drugging the undruggable and challenges ahead
    Li, Hui-yu
    Qi, Wei-liang
    Wang, Yu-xiang
    Meng, Ling-hua
    GENES & DISEASES, 2023, 10 (02) : 403 - 414
  • [32] Contribution of Noncovalent Recognition and Reactivity to the Optimization of Covalent Inhibitors: A Case Study on KRasG12C
    Peczka, Nikolett
    Randelovic, Ivan
    Orgovan, Zoltan
    Csorba, Noemi
    Egyed, Attila
    Petri, Laszlo
    Abranyi-Balogh, Peter
    Gadanecz, Marton
    Perczel, Andras
    Tovari, Jozsef
    Schlosser, Gitta
    Takacs, Tamas
    Mihalovits, Levente M.
    Ferenczy, Gyorgy G.
    Buday, Laszlo
    Keseru, Gyorgy M.
    ACS CHEMICAL BIOLOGY, 2024, 19 (08) : 1743 - 1756
  • [33] Development of covalent KRASG12C inhibitor APG-1842 for the treatment of solid tumors
    Gu, Shaoulai
    Li, Qiang
    Li, Chao
    Wang, Qixin
    Fang, Douglas D.
    Wang, Shaomeng
    Yang, Dajun
    Zhai, Yifan
    CANCER RESEARCH, 2022, 82 (12)
  • [34] The discovery and preclinical characterization of the potent covalent KRASG12C inhibitor UCT-001024
    Rose, Tristin E.
    O'Boyle, Brendan M.
    Hilf, Justin A.
    Baker-Tripp, Emma L.
    Feng, Zhengao
    Yang, Kevin
    Bartberger, Michael D.
    Loson, Oliver C.
    O'Brien, Neil A.
    McDermott, Martina S.
    Kamranpour, Naeimeh
    Jia, Weiping
    Luo, Tong
    Ayala, Raul
    Glasby, John
    Stoltz, Brian M.
    Slamon, Dennis J.
    CANCER RESEARCH, 2023, 83 (07)
  • [35] Reversible Covalent PROTACs: Novel and Efficient Targeted Degradation Strategy
    Yuan, Minghua
    Chu, Yanan
    Duan, Yongtao
    FRONTIERS IN CHEMISTRY, 2021, 9
  • [36] TEAD Inhibitors Sensitize KRASG12C Inhibitors via Dual Cell Cycle Arrest in KRASG12C-Mutant NSCLC
    Tammaccaro, Salvina Laura
    Prigent, Philippe
    Le Bail, Jean-Christophe
    Dos-Santos, Odette
    Dassencourt, Laurent
    Eskandar, Myriam
    Buzy, Armelle
    Venier, Olivier
    Guillemot, Jean-Claude
    Veeranagouda, Yaligara
    Didier, Michel
    Spanakis, Emmanuel
    Kanno, Tokuwa
    Cesaroni, Matteo
    Mathieu, Stephane
    Canard, Luc
    Casse, Alhassan
    Windenberger, Fanny
    Calvet, Loreley
    Noblet, Laurence
    Sidhu, Sukhvinder
    Debussche, Laurent
    Moll, Jurgen
    Valtingojer, Iris
    PHARMACEUTICALS, 2023, 16 (04)
  • [37] Design, Structure Optimization, and Preclinical Characterization of JAB-21822, a Covalent Inhibitor of KRASG12C
    Li, Amin
    Li, Sujing
    Wang, Peng
    Dang, Chaojie
    Fan, Xinrui
    Chen, Mengran
    Liu, Dan
    Li, Fu
    Liu, Huan
    Zhang, Wei
    Wang, Yanping
    Wang, Yinxiang
    JOURNAL OF MEDICINAL CHEMISTRY, 2025, 68 (03) : 2422 - 2436
  • [38] Discovery of novel covalent KRASG12C inhibitors that display high potency and selectivity in vitro and in vivo
    Li, Liansheng
    Janes, Matthew R.
    Zhang, Jingchuan
    Hansen, Rasmus
    Peters, Ulf
    Guo, Xin
    Chen, Yuching
    Babbar, Anjali
    Firdaus, Sarah J.
    Feng, Jun
    Chen, Jeffrey H.
    Li, Shuangwei
    Li, Shisheng
    Thach, Carol
    Liu, Yuan
    Zarieh, Ata
    Kucharski, Jeff M.
    Wu, Tao
    Yu, Ke
    Wang, Yi
    Yao, Yvonne
    Deng, Xiaohu
    Zarrinkar, Patrick P.
    Dhanak, Dashyant
    Lorenzi, Matthew V.
    Hu-Lowe, Dana
    Ren, Pingda
    Liu, Yi
    CANCER RESEARCH, 2018, 78 (13)
  • [39] Synthesis of Adagrasib (MRTX849), a Covalent KRASG12C Inhibitor Drug for the Treatment of Cancer
    Chen, Cheng-yi
    Lu, Zhichao
    Scattolin, Thomas
    Chen, Chengsheng
    Gan, Yonghong
    McLaughlin, Mark
    ORGANIC LETTERS, 2023, : 944 - 949
  • [40] Revealing the mechanism of action of a fi rst-in-class covalent inhibitor of KRASG12C (ON) and other functional properties of oncogenic KRAS by 31 P NMR
    Sharma, Alok K.
    Pei, Jun
    Yang, Yue
    Dyba, Marcin
    Smith, Brian
    Rabara, Dana
    Larsen, Erik K.
    Lightstone, Felice C.
    Esposito, Dominic
    Stephen, Andrew G.
    Wang, Bin
    Beltran, Pedro J.
    Wallace, Eli
    Nissley, Dwight V.
    McCormick, Frank
    Maciag, Anna E.
    JOURNAL OF BIOLOGICAL CHEMISTRY, 2024, 300 (02)
12345