Discovery of Potent and Orally Active p53-MDM2 InhibitorsRO5353 and RO2468 for Potential Clinical Development

机译：发现有效和口服活性的p53-MDM2抑制剂RO5353和RO2468用于潜在的临床开发

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The development of small-molecule MDM2 inhibitors to restore dysfunctional p53 activities represents a novel approach for cancer treatment. In a previous communication, the efforts leading to the identification of a non-imidazoline MDM2 inhibitor, RG7388, was disclosed and revealed the desirable in vitro and in vivo pharmacological properties that this class of pyrrolidine-based inhibitors possesses. Given this richness and the critical need for a wide variety of chemical structures to ensure success in the clinic, research was expanded to evaluate additional derivatives. Here we report two new potent, selective, and orally active p53-MDM2 antagonists, RO5353 and RO2468, as follow-ups with promising potential for clinical development.

机译：开发小分子MDM2抑制剂以恢复功能异常的p53活性代表了一种新的癌症治疗方法。在先前的通讯中，公开了导致鉴定非咪唑啉MDM2抑制剂RG7388的努力，并揭示了这类基于吡咯烷酮的抑制剂所具有的理想的体外和体内药理特性。考虑到这种丰富性以及对确保临床成功的多种化学结构的迫切需求，研究已扩展到评估其他衍生物。在这里，我们报告了两种新的有效，选择性和口服活性的p53-MDM2拮抗剂RO5353和RO2468，作为具有临床开发潜力的后续药物。

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期刊名称 ACS Medicinal Chemistry Letters
作者
Zhuming Zhang; *; ⊥; Xin-Jie Chu; *; ⊥; Jin-Jun Liu; Qingjie Ding; Jing Zhang; David Bartkovitz; Nan Jiang; Prabha Karnachi; Sung-Sau So; Christian Tovar; ZoranM. Filipovic; Brian Higgins; Kelli Glenn; Kathryn Packman; Lyubomir Vassilev; Bradford Graves;
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年(卷),期 2014(5),2
年度 2014
页码 124–127
总页数 4
原文格式 PDF
正文语种
中图分类药物化学;
关键词
MDM2 p53 wild-type small molecule apoptosis cancer;

机译：MDM2;p53;野生型;小分子;细胞凋亡;癌症;

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专利

1. Discovery of Potent and Orally Active p53-MDM2 Inhibitors RO5353 and RO2468 for Potential Clinical Development [J] . Zhuming Zhang, Xin-Jie Chu, Jin-Jun Liu ACS medicinal chemistry letters . 2014,第2期

机译：发现有效和口服活性的p53-MDM2抑制剂RO5353和RO2468用于潜在的临床开发
2. Discovery of DS-5272 as a promising candidate: A potent and orally active p53-MDM2 interaction inhibitor [J] . Miyazaki Masaki, Uoto Kouichi, Sugimoto Yuuichi, Bioorganic and medicinal chemistry . 2015,第10期

机译：发现DS-5272作为有前途的候选药物：一种有效且口服的p53-MDM2相互作用抑制剂
3. Discovery of RG7388, a potent and selective p53-MDM2 inhibitor in clinical development [J] . Ding Q., Zhang Z., Liu J.-J., Journal of Medicinal Chemistry . 2013,第14期

机译：在临床开发中发现了有效的选择性p53-MDM2抑制剂RG7388
4. Estimation of active myocardial force development: a feasibility study in a potentially clinical setting [C] . Claus, P., McLaughlin, Engineering in Medicine and Biology Society, 2003. Proceedings of the 25th Annual International Conference of the IEEE . 2003

机译：估计活跃的心肌力量发展：在潜在的临床环境中的可行性研究
5. Development of Orally Bioavailable 4(1H)-Quinolones and 1,2,3,4-Tetrahydroacridin-9(10H)-ones with Potent Anti-malarial Activity [D] . Maignan, Jordany R. 2015

机译：具有有效抗疟疾活性的口服生物可利用的4（1H）-喹诺酮和1,2,3,4-Tetrahydroacridin-9（10H）-ones的开发
6. Discovery of 4-((3′R4′S5′R)-6″-Chloro-4′-(3-chloro-2-fluorophenyl)-1′-ethyl-2″-oxodispirocyclohexane-12′-pyrrolidine-3′3″-indoline-5′-carboxamido)bicyclo2.2.2octane-1-carboxylicAcid (AA-115/APG-115): A Potent and Orally Active Murine Double Minute2 (MDM2) Inhibitor in Clinical Development [O] . Angelo Aguilar, Jianfeng Lu, Liu Liu, -1

机译：发现4-（（3R4S5R）-6-Chloro-4-（3-氯-2-氟苯基）-1-乙基-2-氧二螺环己烷-1 2′-吡咯烷-3′3″-二氢吲哚 -5′-羧酰胺基）双环2.2.2辛烷-1-羧酸酸（AA-115 / APG-115）：有力且口服活跃的小鼠双分钟2（MDM2）临床开发中的抑制剂
7. Discovery of Potent and Orally Active p53-MDM2 Inhibitors RO5353 and RO2468 for Potential Clinical Development [O] . Zhuming Zhang, Xin-Jie Chu, Jin-Jun Liu, 2014

机译：有效和口服活性P53-MDM2抑制剂RO5353和RO2468的发现，用于潜在的临床发展
8. Development of Potent Orally Active Agents for Prevention and Treatment of Poxvirus Infection. [R] . Hostetler, K. Y. 2003

机译：开发强效口服活性剂预防和治疗痘病毒感染。

Discovery of Potent and Orally Active p53-MDM2 InhibitorsRO5353 and RO2468 for Potential Clinical Development

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