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Rational drug repositioning guided by an integrated pharmacological network of protein, disease and drug.


ABSTRACT:

Background

The process of drug discovery and development is time-consuming and costly, and the probability of success is low. Therefore, there is rising interest in repositioning existing drugs for new medical indications. When successful, this process reduces the risk of failure and costs associated with de novo drug development. However, in many cases, new indications of existing drugs have been found serendipitously. Thus there is a clear need for establishment of rational methods for drug repositioning.

Results

In this study, we have established a database we call "PharmDB" which integrates data associated with disease indications, drug development, and associated proteins, and known interactions extracted from various established databases. To explore linkages of known drugs to diseases of interest from within PharmDB, we designed the Shared Neighborhood Scoring (SNS) algorithm. And to facilitate exploration of tripartite (Drug-Protein-Disease) network, we developed a graphical data visualization software program called phExplorer, which allows us to browse PharmDB data in an interactive and dynamic manner. We validated this knowledge-based tool kit, by identifying a potential application of a hypertension drug, benzthiazide (TBZT), to induce lung cancer cell death.

Conclusions

By combining PharmDB, an integrated tripartite database, with Shared Neighborhood Scoring (SNS) algorithm, we developed a knowledge platform to rationally identify new indications for known FDA approved drugs, which can be customized to specific projects using manual curation. The data in PharmDB is open access and can be easily explored with phExplorer and accessed via BioMart web service (http://www.i-pharm.org/, http://biomart.i-pharm.org/).

SUBMITTER: Lee HS 

PROVIDER: S-EPMC3443412 | biostudies-literature | 2012 Jul

REPOSITORIES: biostudies-literature

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Rational drug repositioning guided by an integrated pharmacological network of protein, disease and drug.

Lee Hee Sook HS   Bae Taejeong T   Lee Ji-Hyun JH   Kim Dae Gyu DG   Oh Young Sun YS   Jang Yeongjun Y   Kim Ji-Tea JT   Lee Jong-Jun JJ   Innocenti Alessio A   Supuran Claudiu T CT   Chen Luonan L   Rho Kyoohyoung K   Kim Sunghoon S  

BMC systems biology 20120702


<h4>Background</h4>The process of drug discovery and development is time-consuming and costly, and the probability of success is low. Therefore, there is rising interest in repositioning existing drugs for new medical indications. When successful, this process reduces the risk of failure and costs associated with de novo drug development. However, in many cases, new indications of existing drugs have been found serendipitously. Thus there is a clear need for establishment of rational methods for  ...[more]

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