共 26 条
Tasiamide F, a potent inhibitor of cathepsins D and E from a marine cyanobacterium
被引:28
作者:

Al-Awadhi, Fatma H.
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机构:
Univ Florida, Dept Med Chem, Gainesville, FL 32611 USA
Univ Florida, Ctr Nat Prod Drug Discovery & Dev CNPD3, Gainesville, FL 32611 USA Univ Florida, Dept Med Chem, Gainesville, FL 32611 USA

Ratnayake, Ranjala
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h-index: 0
机构:
Univ Florida, Dept Med Chem, Gainesville, FL 32611 USA
Univ Florida, Ctr Nat Prod Drug Discovery & Dev CNPD3, Gainesville, FL 32611 USA Univ Florida, Dept Med Chem, Gainesville, FL 32611 USA

Paul, Valerie J.
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h-index: 0
机构:
Smithsonian Marine Stn, Ft Pierce, FL USA Univ Florida, Dept Med Chem, Gainesville, FL 32611 USA

Luesch, Hendrik
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h-index: 0
机构:
Univ Florida, Dept Med Chem, Gainesville, FL 32611 USA
Univ Florida, Ctr Nat Prod Drug Discovery & Dev CNPD3, Gainesville, FL 32611 USA Univ Florida, Dept Med Chem, Gainesville, FL 32611 USA
机构:
[1] Univ Florida, Dept Med Chem, Gainesville, FL 32611 USA
[2] Univ Florida, Ctr Nat Prod Drug Discovery & Dev CNPD3, Gainesville, FL 32611 USA
[3] Smithsonian Marine Stn, Ft Pierce, FL USA
基金:
美国国家卫生研究院;
关键词:
Natural products;
Marine cyanobacteria;
Protease inhibitors;
Cathepsins D and E;
Molecular docking;
BIOLOGICAL EVALUATION;
ELASTASE INHIBITORS;
AMINO-ACIDS;
DESIGN;
ACTIVATION;
PEPSTATIN;
PEPTIDE;
D O I:
10.1016/j.bmc.2016.04.062
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:
In search of novel protease inhibitors with therapeutic potential, our efforts exploring the marine cyanobacterium Lyngbya sp. have led to the discovery of tasiamide F (1), which is an analogue of tasiamide B (2). The structure was elucidated using a combination of NMR spectroscopy and mass spectrometry. The key structural feature in 1 is the presence of the Phe-derived statine core, which contributes to its aspartic protease inhibitory activity. The antiproteolytic activity of 1 and 2 was evaluated in vitro against cathepsins D and E, and BACE1. Tasiamide F (1) displayed IC50 values of 57 nM, 23 nM, and 0.69 mu M, respectively, indicating greater selectivity for cathepsins over BACE1 compared with tasiamide B (2). Molecular docking experiments were carried out for compounds 1 and 2 against cathepsins D and E to rationalize their activity towards these proteases. The dysregulated activities of cathepsins D and E have been implicated in cancer and modulation of immune responses, respectively, and these proteases represent potential therapeutic targets. (C) 2016 Elsevier Ltd. All rights reserved.
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页码:3276 / 3282
页数:7
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