Structural Analysis of Spiro β-Lactone Proteasome Inhibitors

被引：38

作者：

Groll, Michael ^{[2
]}

Balskus, Emily P. ^{[1
]}

Jacobsen, Eric N. ^{[1
]}

机构：

[1] Harvard Univ, Dept Chem & Chem Biol, Cambridge, MA 02138 USA

[2] Tech Univ Munich, Lehrstuhl Biochem, Dept Chem, Ctr Integrated Prot Sci, D-85747 Garching, Germany

来源：

JOURNAL OF THE AMERICAN CHEMICAL SOCIETY | 2008年 / 130卷 / 45期

基金：

美国国家科学基金会;

关键词：

D O I：

10.1021/ja806059t

中图分类号：

O6 [化学];

学科分类号：

0703 ;

摘要：

Spiro beta-lactone-based proteasome inhibitors were discovered in the context of an asymmetric catalytic total synthesis of the natural product (+)-lactacystin (1). Lactone 4 was found to be a potent inhibitor of the 26S proteasome, while its C-6 epimer (5) displayed weak activity. Crystallographic studies of the two analogues covalently bound to the 20S proteasome permitted characterization of the important stabilizing interactions between each inhibitor and the proteasome's key catalytic N-terminal threonine residue. This structural data support the hypothesis that the discrepancy in potency between 4 and 5 may be due to differences in the hydrolytic stabilities of the resulting acyl enzyme complexes.

引用

页码：14981 / +

页数：4

共 26 条

[1] α,β-unsaturated β-silyl imide substrates for catalytic, enantioselective conjugate additions:: A total synthesis of (+)-lactacystin and the discovery of a new proteasome inhibitor [J].

Balskus, Emily P. ;

Jacobsen, Eric N. .

JOURNAL OF THE AMERICAN CHEMICAL SOCIETY, 2006, 128 (21) :6810-6812

[2] 20S proteasome and its inhibitors: Crystallographic knowledge for drug development [J].

Borissenko, Ljudmila ;

Groll, Michael .

CHEMICAL REVIEWS, 2007, 107 (03) :687-717

[3] Crystallography & NMR system:: A new software suite for macromolecular structure determination [J].

Brunger, AT ;

Adams, PD ;

Clore, GM ;

DeLano, WL ;

Gros, P ;

Grosse-Kunstleve, RW ;

Jiang, JS ;

Kuszewski, J ;

Nilges, M ;

Pannu, NS ;

Read, RJ ;

Rice, LM ;

Simonson, T ;

Warren, GL .

ACTA CRYSTALLOGRAPHICA SECTION D-BIOLOGICAL CRYSTALLOGRAPHY, 1998, 54 :905-921

[4]

Dick LR, 1997, J BIOL CHEM, V272, P182

[5] Mechanistic studies on the inactivation of the proteasome by lactacystin A central role for clasto-lactacystin beta-lactone [J].

Dick, LR ;

Cruikshank, AA ;

Grenier, L ;

Melandri, FD ;

Nunes, SL ;

Stein, RL .

JOURNAL OF BIOLOGICAL CHEMISTRY, 1996, 271 (13) :7273-7276

[6] Salinosporamide A:: A highly cytotoxic proteasome inhibitor from a novel microbial source, a marine bacterium of the new genus Salinospora [J].

Feling, RH ;

Buchanan, GO ;

Mincer, TJ ;

Kauffman, CA ;

Jensen, PR ;

Fenical, W .

ANGEWANDTE CHEMIE-INTERNATIONAL EDITION, 2003, 42 (03) :355-+

[7]

FENTEANY G, 1995, SCIENCE, V268, P725

[8] Functions of the proteasome: from protein degradation and immune surveillance to cancer therapy [J].

Goldberg, A. L. .

BIOCHEMICAL SOCIETY TRANSACTIONS, 2007, 35 :12-17

[9] Crystal structures of salinosporamide A (NPI-0052) and B (NPI-0047) in complex with the 20S proteasome reveal important consequences of β-lactone ring opening and a mechanism for irreversible binding [J].

Groll, M ;

Huber, R ;

Potts, BCM .

JOURNAL OF THE AMERICAN CHEMICAL SOCIETY, 2006, 128 (15) :5136-5141

[10] Inhibitor-binding mode of homobelactosin C to proteasomes: New insights into class I MHC ligand generation [J].

Groll, M ;

Larionov, OV ;

Huber, R ;

de Meijere, A .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 2006, 103 (12) :4576-4579

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