Discovery of Carboranes as Inducers of 20S Proteasome Activity

被引:14
作者
Ban, Hyun Seung [1 ]
Minegishi, Hidemitsu [1 ]
Shimizu, Kazuki [1 ]
Maruyama, Minako [1 ]
Yasui, Yuka [1 ]
Nakamura, Hiroyuki [1 ]
机构
[1] Gakushuin Univ, Fac Sci, Dept Chem, Toshima Ku, Tokyo 1718588, Japan
来源
CHEMMEDCHEM | 2010年 / 5卷 / 08期
关键词
20S proteasome; activators; caspase-like activity; drug discovery; trypsin-like activity; MULTICATALYTIC PROTEINASE; BETULINIC ACID; INHIBITORS; ACTIVATION; UBIQUITIN; SYSTEM; POTENT; DEGRADATION; DERIVATIVES; PEPTIDES;
D O I
10.1002/cmdc.201000112
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
(Chemical Equation Presented) The carborane framework gives analogues able to induce 20S proteasome activities. A series of ortho-carboranylphenoxy derivatives were synthesized as 20S proteasome agonists, and carborane derivatives 11 a and 11 b were found to be potent inducers of the β1 and β2 activities of the 20S proteasome. Since small-molecule proteasome activators have not been developed, the carboranes described here have potential as chemical probes for the investigation of proteasome-dependent degradation pathways. © 2010 Wiley-VCH Verlag GmbH& Co. KGaA.
引用
收藏
页码:1236 / 1241
页数:6
相关论文
共 27 条
[1]   Potent and selective inhibitors of the proteasome: Dipeptidyl boronic acids [J].
Adams, J ;
Behnke, M ;
Chen, SW ;
Cruickshank, AA ;
Dick, LR ;
Grenier, L ;
Klunder, JM ;
Ma, YT ;
Plamondon, L ;
Stein, RL .
BIOORGANIC & MEDICINAL CHEMISTRY LETTERS, 1998, 8 (04) :333-338
[2]   A new structural class of proteasome inhibitors identified by microbial screening using yeast-based assay [J].
Asai, A ;
Tsujita, T ;
Sharma, SV ;
Yamashita, Y ;
Akinaga, S ;
Funakoshi, M ;
Kobayashi, H ;
Mizukami, T .
BIOCHEMICAL PHARMACOLOGY, 2004, 67 (02) :227-234
[3]   20S proteasome and its inhibitors: Crystallographic knowledge for drug development [J].
Borissenko, Ljudmila ;
Groll, Michael .
CHEMICAL REVIEWS, 2007, 107 (03) :687-717
[4]  
CHU-PING M, 1992, Journal of Biological Chemistry, V267, P10515
[5]   Intracellular protein degradation: From a vague idea, through the lysosome and the ubiquitin-proteasome system, and onto human diseases and drug targeting - (Nobel lecture) [J].
Ciechanover, A .
ANGEWANDTE CHEMIE-INTERNATIONAL EDITION, 2005, 44 (37) :5944-5967
[6]  
Ciechanover A., 2005, ANGEW CHEM, V117, P6095
[7]   ACTIVATION OF THE MULTICATALYTIC PROTEINASE FROM RAT SKELETAL-MUSCLE BY FATTY-ACIDS OR SODIUM DODECYL-SULFATE [J].
DAHLMANN, B ;
RUTSCHMANN, M ;
KUEHN, L ;
REINAUER, H .
BIOCHEMICAL JOURNAL, 1985, 228 (01) :171-177
[8]   KINETIC MECHANISM OF ACTIVATION BY CARDIOLIPIN (DIPHOSPHATIDYLGLYCEROL) OF THE RAT-LIVER MULTICATALYTIC PROTEINASE [J].
DEMENA, IR ;
MAHILLO, E ;
ARRIBAS, J ;
CASTANO, JG .
BIOCHEMICAL JOURNAL, 1993, 296 :93-97
[9]   Potent estrogen agonists based on carborane as a hydrophobic skeletal structure - A new medicinal application of boron clusters [J].
Endo, Y ;
Iijima, T ;
Yamakoshi, Y ;
Fukasawa, H ;
Miyaura, C ;
Inada, M ;
Kubo, A ;
Itai, A .
CHEMISTRY & BIOLOGY, 2001, 8 (04) :341-355
[10]   Potent estrogenic agonists bearing dicarba-closo-dodecaborane as a hydrophobic pharmacophore [J].
Endo, Y ;
Iijima, T ;
Yamakoshi, Y ;
Yamaguchi, M ;
Fukasawa, H ;
Shudo, K .
JOURNAL OF MEDICINAL CHEMISTRY, 1999, 42 (09) :1501-1504
123