Target validation and drug discovery using genomic and protein-protein interaction technologies

After the successful completion of the human genome project, mapping of the human proteome has become the next important challenge facing the biotech and pharmaceutical industries. Identification of the 'right' target(s) is now a critical part of the process because of the cost of drug dis...

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Bibliographic Details
Published inExpert opinion on therapeutic targets Vol. 6; no. 4; p. 517
Main Authors Pillutla, Renuka C, Fisher, Paul B, Blume, Arthur J, Goldstein, Neil I
Format Journal Article
LanguageEnglish
Published England 01.08.2002
Subjects
Animals
Cells, Cultured - drug effects
Cloning, Molecular - methods
Combinatorial Chemistry Techniques
DNA, Complementary - genetics
Drug Delivery Systems
Drug Design
Drug Evaluation, Preclinical - methods
Gene Expression Profiling - methods
Gene Library
Genomics
HeLa Cells - drug effects
Humans
Mammals
Nucleic Acid Hybridization - methods
Peptide Library
Polymerase Chain Reaction - methods
Protein Interaction Mapping
Proteomics
Subtraction Technique
Two-Hybrid System Techniques
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Summary:After the successful completion of the human genome project, mapping of the human proteome has become the next important challenge facing the biotech and pharmaceutical industries. Identification of the 'right' target(s) is now a critical part of the process because of the cost of drug discovery. Compounding this situation is the fact that the pharmaceutical industry faces a further challenge of being able to sustain current and historical growth rates. Hence, the discovery of new drug targets is important for developing new drug leads that can become preclinical drug candidates. Proteomics is the next phase of the effort whereby the human genome can be understood. However, mapping the human proteome presents a daunting challenge. Proteomics involves several essential components with the most significant being the discovery and description of all protein-protein interactions. Once this compendium is available, a secondary and equally important initiative will be to decipher proteins that are differentially expressed in any given disease condition. At this point, the critical focus will be to select the most relevant proteins, understand their partner interactions and then further winnow them to the point where they are relevant pharmaceutical target candidates. This paradigm can be compared to finding the relevant 'needle in the proteome haystack'. This review describes the use of genomic and protein-protein interaction technologies to identify and validate these 'needles' as the first step in the drug discovery process.
ISSN:1744-7631
DOI:10.1517/14728222.6.4.517