Can we discover pharmacological promiscuity early in the drug discovery process?

Jens-Uwe Peters; Jérôme Hert; Caterina Bissantz; Alexander Hillebrecht; Grégori Gerebtzoff; Stefanie Bendels; Fabien Tillier; Jacques Migeon; Holger Fischer; Wolfgang Guba; Manfred Kansy

doi:10.1016/j.drudis.2012.01.001

Can we discover pharmacological promiscuity early in the drug discovery process?

Drug Discov Today. 2012 Apr;17(7-8):325-35. doi: 10.1016/j.drudis.2012.01.001. Epub 2012 Jan 16.

Authors

Jens-Uwe Peters¹, Jérôme Hert, Caterina Bissantz, Alexander Hillebrecht, Grégori Gerebtzoff, Stefanie Bendels, Fabien Tillier, Jacques Migeon, Holger Fischer, Wolfgang Guba, Manfred Kansy

Affiliation

¹ F Hoffmann-La Roche Ltd, pRED, Pharma Research & Early Development, Discovery Chemistry, CH-4070 Basel, Switzerland. jens-uwe.peters@roche.com

PMID: 22269136
DOI: 10.1016/j.drudis.2012.01.001

Abstract

The term 'pharmacological promiscuity' describes the activity of a single compound against multiple targets. When undesired, promiscuity is a major safety concern that needs to be detected as early as possible in the drug discovery process. The analysis of large datasets reveals that the majority of promiscuous compounds are characterized by recognizable molecular properties and structural motifs, the most important one being a basic center with a pK(a)(B)>6. These compounds interact with a small set of targets such as aminergic GPCRs; some of these targets attract surprisingly high hit rates. In this review, we discuss current trends in the assessment of pharmacological promiscuity and propose strategies to enable early detection and mitigation.

Publication types

Review

MeSH terms

Animals
Drug Discovery / methods*
Drug-Related Side Effects and Adverse Reactions*
Humans
Pharmaceutical Preparations / chemistry*
Pharmacology
Structure-Activity Relationship

Substances

Pharmaceutical Preparations