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Literature DB >> 16460734

Blind docking of drug-sized compounds to proteins with up to a thousand residues.

Abstract

Blind docking was introduced for the detection of possible binding sites and modes of peptide ligands by scanning the entire surface of protein targets. In the present study, the method is tested on a group of drug-sized compounds and proteins with up to a thousand amino acid residues. Both proteins from complex structures and ligand-free proteins were used as targets. Robustness, limitations and future perspectives of the method are discussed. It is concluded that blind docking can be used for unbiased mapping of the binding patterns of drug candidates.

Mesh：

Substances：
Ligands
Proteins

Year: 2006 PMID： 16460734 DOI： 10.1016/j.febslet.2006.01.074

Source DB: PubMed Journal: FEBS Lett ISSN： 0014-5793 Impact factor: 4.124

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Cited

66 in total

1. Design and synthesis of Hsp90 inhibitors: exploring the SAR of Sansalvamide A derivatives.

Authors: Robert P Sellers; Leslie D Alexander; Victoria A Johnson; Chun-Chieh Lin; Jeremiah Savage; Ricardo Corral; Jason Moss; Tim S Slugocki; Erinprit K Singh; Melinda R Davis; Suchitra Ravula; Jamie E Spicer; Jenna L Oelrich; Andrea Thornquist; Chung-Mao Pan; Shelli R McAlpine
Journal: Bioorg Med Chem Date: 2010-07-22 Impact factor: 3.641

2. Exploring the landscape of protein-ligand interaction energy using probabilistic approach.

Authors: Marcin Pacholczyk; Marek Kimmel
Journal: J Comput Biol Date: 2010-11-20 Impact factor: 1.479

3. The studies on substrate, product and inhibitor binding to a wild-type and neuronopathic form of human acid-beta-glucosidase.

Authors: Igor Z Zubrzycki; Agnieszka Borcz; Magdalena Wiacek; Wojciech Hagner
Journal: J Mol Model Date: 2007-08-23 Impact factor: 1.810

Blind docking of drug-sized compounds to proteins with up to a thousand residues.

1. Design and synthesis of Hsp90 inhibitors: exploring the SAR of Sansalvamide A derivatives.

2. Exploring the landscape of protein-ligand interaction energy using probabilistic approach.

3. The studies on substrate, product and inhibitor binding to a wild-type and neuronopathic form of human acid-beta-glucosidase.

4. A threading-based method (FINDSITE) for ligand-binding site prediction and functional annotation.

5. Affinity and specificity of levamlodipine-human serum albumin interactions: insights into its carrier function.

6. Improving accuracy and efficiency of blind protein-ligand docking by focusing on predicted binding sites.

Review 7. FINDSITE: a combined evolution/structure-based approach to protein function prediction.

8. Potentiation of alpha7 nicotinic acetylcholine receptors via an allosteric transmembrane site.

9. Comparison of structure-based and threading-based approaches to protein functional annotation.

10. Novel ligands that target the mitochondrial membrane protein mitoNEET.