The discovery of steroids and other novel FKBP inhibitors using a molecular docking program

被引：57

作者：

Burkhard, P ^{[1
]}

Hommel, U ^{[1
]}

Sanner, M ^{[1
]}

Walkinshaw, MD ^{[1
]}

机构：

[1] Univ Edinburgh, Struct Biochem Unit, Edinburgh EH9 3JR, Midlothian, Scotland

来源：

JOURNAL OF MOLECULAR BIOLOGY | 1999年 / 287卷 / 05期

关键词：

D O I：

10.1006/jmbi.1999.2621

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：

The molecular docking computer program SANDOCK was used to screen small molecule three-dimensional databases in the hunt for novel FKBP inhibitors. Spectroscopic measurements confirmed binding of over 20 compounds to the target protein, some with dissociation constants in the low micromolar range. The discovery that FK506 binding protein is a steroid binding protein may be of wider biological significance. Two-dimensional NMR was used to determine the steroid binding mode and confirmed the interactions predicted by the docking program. (C) 1999 Academic Press.

引用

页码：853 / 858

页数：6

共 25 条

[1]

AJAY MMA, 1995, J MED CHEM, V38, P4953

[2] THE DEVELOPMENT OF VERSION-3 AND VERSION-4 OF THE CAMBRIDGE STRUCTURAL DATABASE SYSTEM [J].

ALLEN, FH ;

DAVIES, JE ;

GALLOY, JJ ;

JOHNSON, O ;

KENNARD, O ;

MACRAE, CF ;

MITCHELL, EM ;

MITCHELL, GF ;

SMITH, JM ;

WATSON, DG .

JOURNAL OF CHEMICAL INFORMATION AND COMPUTER SCIENCES, 1991, 31 (02) :187-204

[3]

Bohm HJ, 1996, ANGEW CHEM INT EDIT, V35, P2589

[4] Towards the automatic design of synthetically accessible protein ligands: Peptides, amides and peptidomimetics [J].

Bohm, HJ .

JOURNAL OF COMPUTER-AIDED MOLECULAR DESIGN, 1996, 10 (04) :265-272

[5] LUDI - RULE-BASED AUTOMATIC DESIGN OF NEW SUBSTITUENTS FOR ENZYME-INHIBITOR LEADS [J].

BOHM, HJ .

JOURNAL OF COMPUTER-AIDED MOLECULAR DESIGN, 1992, 6 (06) :593-606

[6] An example of a protein ligand found by database mining:: Description of the docking method and its verification by a 2.3 Å X-ray structure of a thrombin-ligand complex [J].

Burkhard, P ;

Taylor, P ;

Walkinshaw, MD .

JOURNAL OF MOLECULAR BIOLOGY, 1998, 277 (02) :449-466

[7] USING SHAPE COMPLEMENTARITY AS AN INITIAL SCREEN IN DESIGNING LIGANDS FOR A RECEPTOR-BINDING SITE OF KNOWN 3-DIMENSIONAL STRUCTURE [J].

DESJARLAIS, RL ;

SHERIDAN, RP ;

SEIBEL, GL ;

DIXON, JS ;

KUNTZ, ID ;

VENKATARAGHAVAN, R .

JOURNAL OF MEDICINAL CHEMISTRY, 1988, 31 (04) :722-729

[8] PEPTIDYLPROLINE CIS/TRANS ISOMERASES [J].

GALAT, A ;

METCALFE, SM .

PROGRESS IN BIOPHYSICS & MOLECULAR BIOLOGY, 1995, 63 (01) :67-118

[9] A COMPUTATIONAL-PROCEDURE FOR DETERMINING ENERGETICALLY FAVORABLE BINDING-SITES ON BIOLOGICALLY IMPORTANT MACROMOLECULES [J].

GOODFORD, PJ .

JOURNAL OF MEDICINAL CHEMISTRY, 1985, 28 (07) :849-857

[10] AN INTEGRATED APPROACH TO 3-DIMENSIONAL INFORMATION MANAGEMENT WITH MACCS-3D [J].

GUNER, OF ;

HUGHES, DW ;

DUMONT, LM .

JOURNAL OF CHEMICAL INFORMATION AND COMPUTER SCIENCES, 1991, 31 (03) :408-414

← 1 2 3 →