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Literature DB >> 10483532

DREAM++: flexible docking program for virtual combinatorial libraries.

Abstract

We present a set of programs, DREAM+2 (Docking and Reaction programs using Efficient seArch Methods written in C++), for docking computationally generated ligands into macromolecular binding sites. DREAM++ is composed of three programs: ORIENT++, REACT++ and SEARCH++. The program ORIENT++ positions molecules in a binding site with the DOCK algorithm. Its output can be used as input to REACT++ and SEARCH+2. The program REACT++ performs user-specific chemical reactions on a docked molecule, so that reaction products can be evaluated for three dimensional complementarity with the macromolecular site. The program SEARCH++ performs an efficient conformation search on the reaction products using a hybrid backtrack and incremental construction algorithm. We have applied the programs to HIV protease-inhibitor complexes as test systems. We found that we can differentiate high-affinity ligands based on several measures: interaction energies, occupancy of protein subsites and the number of successfully docked conformations for each product. Encouraged by the results in the test case, we applied the programs to propose novel inhibitors of HIV protease. These inhibitors can be generated by organic reactions using commercially available reagents. They are alternatives to the inhibitors synthesized by Glaxo.

Entities: Chemical Disease Gene

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Year: 1999 PMID： 10483532 DOI： 10.1023/a:1008066310669

Source DB: PubMed Journal: J Comput Aided Mol Des ISSN： 0920-654X Impact factor: 3.686

43 in total

1. CONCERTS: dynamic connection of fragments as an approach to de novo ligand design.

Authors: D A Pearlman; M A Murcko
Journal: J Med Chem Date: 1996-04-12 Impact factor: 7.446

2. Towards the automatic design of synthetically accessible protein ligands: peptides, amides and peptidomimetics.

Authors: H J Böhm
Journal: J Comput Aided Mol Des Date: 1996-08 Impact factor: 3.686

3. Hammerhead: fast, fully automated docking of flexible ligands to protein binding sites.

Authors: W Welch; J Ruppert; A N Jain
Journal: Chem Biol Date: 1996-06

4. Docking flexible ligands to macromolecular receptors by molecular shape.

Authors: R L DesJarlais; R P Sheridan; J S Dixon; I D Kuntz; R Venkataraghavan
Journal: J Med Chem Date: 1986-11 Impact factor: 7.446

5. Flexible ligand docking using a genetic algorithm.

Authors: C M Oshiro; I D Kuntz; J S Dixon
Journal: J Comput Aided Mol Des Date: 1995-04 Impact factor: 3.686

6. BUILDER v.2: improving the chemistry of a de novo design strategy.

Authors: D C Roe; I D Kuntz
Journal: J Comput Aided Mol Des Date: 1995-06 Impact factor: 3.686

7. SPROUT: recent developments in the de novo design of molecules.

Authors: V J Gillet; W Newell; P Mata; G Myatt; S Sike; Z Zsoldos; A P Johnson
Journal: J Chem Inf Comput Sci Date: 1994 Jan-Feb

8. Hydroxyethylene isostere inhibitors of human immunodeficiency virus-1 protease: structure-activity analysis using enzyme kinetics, X-ray crystallography, and infected T-cell assays.

Authors: G B Dreyer; D M Lambert; T D Meek; T J Carr; T A Tomaszek; A V Fernandez; H Bartus; E Cacciavillani; A M Hassell; M Minnich
Journal: Biochemistry Date: 1992-07-28 Impact factor: 3.162

9. A series of penicillin derived C2-symmetric inhibitors of HIV-1 proteinase: synthesis, mode of interaction, and structure-activity relationships.

Authors: D C Humber; M J Bamford; R C Bethell; N Cammack; K Cobley; D N Evans; N M Gray; M M Hann; D C Orr; J Saunders
Journal: J Med Chem Date: 1993-10-15 Impact factor: 7.446

10. Structure of HIV-1 protease with KNI-272, a tight-binding transition-state analog containing allophenylnorstatine.

Authors: E T Baldwin; T N Bhat; S Gulnik; B Liu; I A Topol; Y Kiso; T Mimoto; H Mitsuya; J W Erickson
Journal: Structure Date: 1995-06-15 Impact factor: 5.006

9 in total

1. A comparative docking study and the design of potentially selective MMP inhibitors.

Authors: S Hanessian; N Moitessier; E Therrien
Journal: J Comput Aided Mol Des Date: 2001-10 Impact factor: 3.686

2. Discovery of a novel serine protease inhibitor utilizing a structure-based and experimental selection of fragments technique.

Authors: S Makino; T Kayahara; K Tashiro; M Takahashi; T Tsuji; M Shoji
Journal: J Comput Aided Mol Des Date: 2001-06 Impact factor: 3.686

DREAM++: flexible docking program for virtual combinatorial libraries.

1. CONCERTS: dynamic connection of fragments as an approach to de novo ligand design.

2. Towards the automatic design of synthetically accessible protein ligands: peptides, amides and peptidomimetics.

3. Hammerhead: fast, fully automated docking of flexible ligands to protein binding sites.

4. Docking flexible ligands to macromolecular receptors by molecular shape.

5. Flexible ligand docking using a genetic algorithm.

6. BUILDER v.2: improving the chemistry of a de novo design strategy.

7. SPROUT: recent developments in the de novo design of molecules.

8. Hydroxyethylene isostere inhibitors of human immunodeficiency virus-1 protease: structure-activity analysis using enzyme kinetics, X-ray crystallography, and infected T-cell assays.

9. A series of penicillin derived C2-symmetric inhibitors of HIV-1 proteinase: synthesis, mode of interaction, and structure-activity relationships.

10. Structure of HIV-1 protease with KNI-272, a tight-binding transition-state analog containing allophenylnorstatine.

1. A comparative docking study and the design of potentially selective MMP inhibitors.

2. Discovery of a novel serine protease inhibitor utilizing a structure-based and experimental selection of fragments technique.

3. Surrogate docking: structure-based virtual screening at high throughput speed.

Review 4. Hierarchical docking of databases of multiple ligand conformations.

Review 5. From laptop to benchtop to bedside: structure-based drug design on protein targets.

Review 6. Towards the development of universal, fast and highly accurate docking/scoring methods: a long way to go.

7. Combinatorial library-based design with Basis Products.

8. Drug design for ever, from hype to hope.

9. Incorporating Virtual Reactions into a Logic-based Ligand-based Virtual Screening Method to Discover New Leads.