Application of industrial scale genomics to discovery of therapeutic targets in heart failure

doi:10.1016/S1388-9842(01)00203-3

European Journal of Heart Failure 2001 3(6):641-650; doi:10.1016/S1388-9842(01)00203-3

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Application of industrial scale genomics to discovery of therapeutic targets in heart failure

Fuad Mehraban^a^,* and James E. Tomlinson^b

^a CuraGen Corporation 555 Long Wharf Drive, New Haven, CT 06511, USA
^b COR Therapeutics Inc 256 E Grand Avenue, South San Francisco, CA 94080, USA

^* Corresponding author. Tel.: +1-203-974-6297; fax: +1-203-401-3351. E-mail address: fmehraba{at}curagen.com (F. Mehraban).

Abstract

In recent years intense activity in both academic and industrialsectors has provided a wealth of information on the human genomewith an associated impressive increase in the number of novelgene sequences deposited in sequence data repositories and patentapplications. This genomic industrial revolution has transformedthe way in which drug target discovery is now approached. Inthis article we discuss how various differential gene expression(DGE) technologies are being utilized for cardiovascular disease(CVD) drug target discovery. Other approaches such as sequencingcDNA from cardiovascular derived tissues and cells coupled withbioinformatic sequence analysis are used with the aim of identifyingnovel gene sequences that may be exploited towards target discovery.Additional leverage from gene sequence information is obtainedthrough identification of polymorphisms that may confer diseasesusceptibility and/or affect drug responsiveness. Pharmacogenomicstudies are described wherein gene expression-based techniquesare used to evaluate drug response and/or efficacy. Industrial-scalegenomics supports and addresses not only novel target gene discoverybut also the burgeoning issues in pharmaceutical and clinicalcardiovascular medicine relative to polymorphic gene responses.

Key Words: Genomics • Expression profiling • Cardiovascular disease • Drug discovery

Received April 13, 2001; Revised May 30, 2001; Accepted August 14, 2001

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