Evaluation of spiropiperidine hydantoins as a novel class of antimalarial agents

被引:21
|
作者
Meyers, Marvin J. [1 ]
Anderson, Elizabeth J. [1 ]
McNitt, Sarah A. [1 ]
Krenning, Thomas M. [1 ]
Singh, Megh [1 ]
Xu, Jing [2 ]
Zeng, Wentian [2 ]
Qin, Limei [3 ]
Xu, Wanwan [3 ]
Zhao, Siting [3 ]
Qin, Li [3 ]
Eickhoff, Christopher S. [1 ]
Oliva, Jonathan [1 ]
Campbell, Mary A. [1 ]
Arnett, Stacy D. [1 ]
Prinsen, Michael J. [1 ]
Griggs, David W. [1 ]
Ruminski, Peter G. [1 ]
Goldberg, Daniel E. [4 ,5 ]
Ding, Ke [6 ]
Liu, Xiaorong [2 ]
Tu, Zhengchao [2 ]
Tortorella, Micky D. [2 ]
Sverdrup, Francis M. [1 ]
Chen, Xiaoping [3 ]
机构
[1] St Louis Univ, Sch Med, Ctr World Hlth & Med, St Louis, MO 63104 USA
[2] Chinese Acad Sci, Drug Discovery Pipeline Guangzhou Inst Biomed Hlt, Guangzhou, Guangdong, Peoples R China
[3] Chinese Acad Sci, Guangzhou Inst Biomed & Hlth, Lab Pathogen Biol, State Key Lab Resp Dis,Ctr Infect & Immun, Guangzhou 510530, Guangdong, Peoples R China
[4] Washington Univ, Dept Med, St Louis, MO USA
[5] Washington Univ, Dept Mol Microbiol, St Louis, MO 63110 USA
[6] Chinese Acad Sci, Guangzhou Inst Biomed & Hlth, Key Lab Regenerat Biol, Inst Chem Biol, Guangzhou 510530, Guangdong, Peoples R China
基金
美国国家卫生研究院; 中国国家自然科学基金;
关键词
Aspartic protease inhibitors; Spiropiperidine hydantoins; Antiplasmodial; Antimalarial; SIGNAL PEPTIDE PEPTIDASE; PLASMODIUM-FALCIPARUM; ARTEMISININ RESISTANCE; DRUG DISCOVERY; PLASMEPSIN V; INHIBITORS; PROTEINS; DESIGN; EXPORT;
D O I
10.1016/j.bmc.2015.02.050
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Given the rise of parasite resistance to all currently used antimalarial drugs, the identification of novel chemotypes with unique mechanisms of action is of paramount importance. Since Plasmodium expresses a number of aspartic proteases necessary for its survival, we have mined antimalarial datasets for drug-like aspartic protease inhibitors. This effort led to the identification of spiropiperidine hydantoins, bearing similarity to known inhibitors of the human aspartic protease beta-secretase (BACE), as new leads for antimalarial drug discovery. Spiropiperidine hydantoins have a dynamic structure-activity relationship profile with positions identified as being tolerant of a variety of substitution patterns as well as a key piperidine N-benzyl phenol pharmacophore. Lead compounds 4e (CWHM-123) and 12k (CWHM-505) are potent antimalarials with IC50 values against Plasmodium falciparum 3D7 of 0.310 mu M and 0.099 mu M, respectively, and the former features equivalent potency on the chloroquine-resistant Dd2 strain. Remarkably, these compounds do not inhibit human aspartic proteases BACE, cathepsins D and E, or Plasmodium plasmepsins II and IV despite their similarity to known BACE inhibitors. Although the current leads suffer from poor metabolic stability, they do fit into a drug-like chemical property space and provide a new class of potent antimalarial agents for further study. (C) 2015 Elsevier Ltd. All rights reserved.
引用
收藏
页码:5144 / 5150
页数:7
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