Structural basis of inhibition of cysteine proteases by E-64 and its derivatives

This paper focuses on the inhibitory mechanism of E‐64 and its derivatives (epoxysuccinyl‐based inhibitors) with some cysteine proteases, based on the binding modes observed in the x‐ray crystal structures of their enzyme–inhibitor complexes. E‐64 is a potent irreversible inhibitor against general c...

Full description

Saved in:
Bibliographic Details
Published inBIOPOLYM Vol. 51; no. 1; pp. 99 - 107
Main Authors Matsumoto, Keita, Mizoue, Kazutoshi, Kitamura, Kunihiro, Tse, Wai-Ching, Huber, Carol P., Ishida, Toshimasa
Format Journal Article
LanguageEnglish
Published New York John Wiley & Sons, Inc 1999
Subjects
actinidin
binding mode
Binding Sites
cathepsin B
cathepsin K
cathepsin L
Crystal structure
Crystallography, X-Ray
Cysteine Endopeptidases - chemistry
Cysteine Endopeptidases - metabolism
cysteine protease
Cysteine Proteinase Inhibitors - chemical synthesis
Cysteine Proteinase Inhibitors - chemistry
Cysteine Proteinase Inhibitors - pharmacology
Drug Design
E-64
E-64 derivative
Epoxy Compounds
inhibitory mechanism
Leucine - analogs & derivatives
Leucine - chemical synthesis
Leucine - chemistry
Leucine - pharmacology
Models, Molecular
Molecular dynamics
Molecular structure
papain
Protein Conformation
Static Electricity
Structure-Activity Relationship
Succinic Acid
Online AccessGet full text

Cover

More Information
Summary:This paper focuses on the inhibitory mechanism of E‐64 and its derivatives (epoxysuccinyl‐based inhibitors) with some cysteine proteases, based on the binding modes observed in the x‐ray crystal structures of their enzyme–inhibitor complexes. E‐64 is a potent irreversible inhibitor against general cysteine proteases, and its binding modes with papain, actinidin, cathepsin L, and cathepsin K have been reviewed at the atomic level. E‐64 interacts with the Sn subsites of cysteine proteases. Although the Sn–Pn (n = 1 ∼ 3) interactions of the inhibitor with the main chains of the active site residues are similar in respective complexes, the significant difference is observed in the side‐chain interactions of S2–P2 and S3–P3 pairs because of different residues constituting the respective subsites. E‐64‐c and CA074 are representative derivatives developed from E‐64 as a clinical usable and a cathepsin B‐specific inhibitors, respectively. In contrast with similar binding/inhibitory modes of E‐64‐c and E‐64 for cysteine proteases, the inhibitory mechanism of cathepsin B‐specific CA074 results from the binding to the Sn′ subsite. © 1999 John Wiley & Sons, Inc. Biopoly 51: 99–107, 1999
Bibliography:ark:/67375/WNG-0LK4BM1H-2
ArticleID:BIP11
istex:755D2B124B0F3A48870653BC59C365634541D5AF
ObjectType-Article-1
SourceType-Scholarly Journals-1
ObjectType-Feature-2
content type line 23
ObjectType-Article-2
ObjectType-Feature-1
ISSN:0006-3525
1097-0282
DOI:10.1002/(SICI)1097-0282(1999)51:1<99::AID-BIP11>3.0.CO;2-R