Target deconvolution strategies in drug discovery

被引:308
作者
Terstappen, Georg C. [1 ]
Schluepen, Christina [1 ]
Raggiaschi, Roberto [1 ]
Gaviraghi, Giovanni [1 ]
机构
[1] Siena Biotech SPA, I-53100 Siena, Italy
来源
NATURE REVIEWS DRUG DISCOVERY | 2007年 / 6卷 / 11期
关键词
D O I
10.1038/nrd2410
中图分类号
Q81 [生物工程学(生物技术)]; Q93 [微生物学];
学科分类号
071005 ; 0836 ; 090102 ; 100705 ;
摘要
Recognition of some of the limitations of target-based drug discovery has recently led to the renaissance of a more holistic approach in which complex biological systems are investigated for phenotypic changes upon exposure to small molecules. The subsequent identification of the molecular targets that underlie an observed phenotypic response-termed target deconvolution - is an important aspect of current drug discovery, as knowledge of the molecular targets will greatly aid drug development. Here, the broad panel of experimental strategies that can be applied to target deconvolution is critically reviewed.
引用
收藏
页码:891 / 903
页数:13
相关论文
共 77 条
[51]   Biochemical suppression of small-molecule inhibitors: A strategy to identify inhibitor targets and signaling pathway components [J].
Peterson, JR ;
Lebensohn, AM ;
Pelish, HE ;
Kirschner, MW .
CHEMISTRY & BIOLOGY, 2006, 13 (04) :443-452
[52]   Untitled [J].
Raggiaschi, R ;
Terstappen, G .
BIOSCIENCE REPORTS, 2005, 25 (1-2) :1-1
[53]   A phage display technique for a fast, sensitive, and systematic investigation of protein-protein interactions [J].
Rossenu, S ;
Dewitte, D ;
Vandekerckhove, J ;
Ampe, C .
JOURNAL OF PROTEIN CHEMISTRY, 1997, 16 (05) :499-503
[54]   Target-based drug discovery: is something wrong? [J].
Sams-Dodd, F .
DRUG DISCOVERY TODAY, 2005, 10 (02) :139-147
[55]   Polyproline-rod approach to isolating protein targets of bioactive small molecules: Isolation of a new target of indomethacin [J].
Sato, Shin-ichi ;
Kwon, Youngjoo ;
Kamisuki, Shinji ;
Srivastava, Neeta ;
Mao, Qian ;
Kawazoe, Yoshinori ;
Uesugi, Motonari .
JOURNAL OF THE AMERICAN CHEMICAL SOCIETY, 2007, 129 (04) :873-880
[56]   Display cloning: functional identification of natural product receptors using cDNA-phage display [J].
Sche, PP ;
McKenzie, KM ;
White, JD ;
Austin, DJ .
CHEMISTRY & BIOLOGY, 1999, 6 (10) :707-716
[57]  
Schuchardt Sven, 2007, EXS, V97, P141, DOI 10.1007/978-3-7643-7439-6_7
[58]  
SHALTIEL S, 1984, METHOD ENZYMOL, V104, P69
[59]   A new curcumin derivative, HBC, interferes with the cell cycle progression of colon cancer cells via antagonization of the Ca2+/calmodulin function [J].
Shim, JS ;
Lee, J ;
Park, HJ ;
Park, SJ ;
Kwon, HJ .
CHEMISTRY & BIOLOGY, 2004, 11 (10) :1455-1463
[60]   High-performance affinity beads for identifying drug receptors [J].
Shimizu, N ;
Sugimoto, K ;
Tang, JW ;
Nishi, T ;
Sato, I ;
Hiramoto, M ;
Aizawa, S ;
Hatakeyama, M ;
Ohba, R ;
Hatori, H ;
Yoshikawa, T ;
Suzuki, F ;
Oomori, A ;
Tanaka, H ;
Kawaguchi, H ;
Watanabe, H ;
Handa, H .
NATURE BIOTECHNOLOGY, 2000, 18 (08) :877-881
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