Treffer: Pharmacogenomic analysis: correlating molecular substructure classes with microarray gene expression data.

Title:
Pharmacogenomic analysis: correlating molecular substructure classes with microarray gene expression data.
Authors:
Blower PE; Leadscope Inc, Columbus, OH 43212, USA. Pblower@leadscope.com, Yang C, Fligner MA, Verducci JS, Yu L, Richman S, Weinstein JN
Source:
The pharmacogenomics journal [Pharmacogenomics J] 2002; Vol. 2 (4), pp. 259-71.
Publication Type:
Journal Article
Language:
English
Journal Info:
Publisher: Nature Pub. Group Country of Publication: United States NLM ID: 101083949 Publication Model: Print Cited Medium: Print ISSN: 1470-269X (Print) Linking ISSN: 1470269X NLM ISO Abbreviation: Pharmacogenomics J Subsets: MEDLINE
Imprint Name(s):
Original Publication: Avenet, NJ : Nature Pub. Group, c2001-
MeSH Terms:
Oligonucleotide Array Sequence Analysis*, Gene Expression/*genetics , Pharmacogenetics/*methods, Algorithms ; Antineoplastic Agents/pharmacology ; Cells ; Databases, Genetic ; Drug Design ; Humans ; Quinones/pharmacology ; Tumor Cells, Cultured
Substance Nomenclature:
0 (Antineoplastic Agents)
0 (Quinones)
Entry Date(s):
Date Created: 20020828 Date Completed: 20030210 Latest Revision: 20041117
Update Code:
20250114
DOI:
10.1038/sj.tpj.6500116
PMID:
12196914
Database:
MEDLINE

Weitere Informationen

Genomic studies are producing large databases of molecular information on cancers and other cell and tissue types. Hence, we have the opportunity to link these accumulating data to the drug discovery processes. Our previous efforts at 'information-intensive' molecular pharmacology have focused on the relationship between patterns of gene expression and patterns of drug activity. In the present study, we take the process a step further-relating gene expression patterns, not just to the drugs as entities, but to approximately 27,000 substructures and other chemical features within the drugs. This coupling of genomic information with structure-based data mining can be used to identify classes of compounds for which detailed experimental structure-activity studies may be fruitful. Using a systematic substructure analysis coupled with statistical correlations of compound activity with differential gene expression, we have identified two subclasses of quinones whose patterns of activity in the National Cancer Institute's 60-cell line screening panel (NCI-60) correlate strongly with the expression patterns of particular genes: (i) The growth inhibitory patterns of an electron-withdrawing subclass of benzodithiophenedione-containing compounds over the NCI-60 are highly correlated with the expression patterns of Rab7 and other melanoma-specific genes; (ii) the inhibitory patterns of indolonaphthoquinone-containing compounds are highly correlated with the expression patterns of the hematopoietic lineage-specific gene HS1 and other leukemia genes. As illustrated by these proof-of-principle examples, we introduce here a set of conceptual tools and fluent computational methods for projecting directly from gene expression patterns to drug substructures and vice versa. The analysis is presented in terms of the NCI-60 cell lines and microarray-based gene expression patterns, but the concept and methods are broadly applicable to other large-scale pharmacogenomic database sets as well. The approach (SAT for Structure-Activity-Target) provides a systematic way to mine databases for the design of further structure-activity studies, particularly to aid in target and lead identification.