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Identifying mechanism-of-action targets for drugs and probes.

Authors :
Gregori-Puigjané, Elisabet
Gregori-Puigjané, Elisabet
Setola, Vincent
Hert, Jérôme
Crews, Brenda A
Irwin, John J
Lounkine, Eugen
Marnett, Lawrence
Roth, Bryan L
Shoichet, Brian K
Gregori-Puigjané, Elisabet
Gregori-Puigjané, Elisabet
Setola, Vincent
Hert, Jérôme
Crews, Brenda A
Irwin, John J
Lounkine, Eugen
Marnett, Lawrence
Roth, Bryan L
Shoichet, Brian K
Source :
Proceedings of the National Academy of Sciences of the United States of America; vol 109, iss 28, 11178-11183; 0027-8424
Publication Year :
2012

Abstract

Notwithstanding their key roles in therapy and as biological probes, 7% of approved drugs are purported to have no known primary target, and up to 18% lack a well-defined mechanism of action. Using a chemoinformatics approach, we sought to "de-orphanize" drugs that lack primary targets. Surprisingly, targets could be easily predicted for many: Whereas these targets were not known to us nor to the common databases, most could be confirmed by literature search, leaving only 13 Food and Drug Administration-approved drugs with unknown targets; the number of drugs without molecular targets likely is far fewer than reported. The number of worldwide drugs without reasonable molecular targets similarly dropped, from 352 (25%) to 44 (4%). Nevertheless, there remained at least seven drugs for which reasonable mechanism-of-action targets were unknown but could be predicted, including the antitussives clemastine, cloperastine, and nepinalone; the antiemetic benzquinamide; the muscle relaxant cyclobenzaprine; the analgesic nefopam; and the immunomodulator lobenzarit. For each, predicted targets were confirmed experimentally, with affinities within their physiological concentration ranges. Turning this question on its head, we next asked which drugs were specific enough to act as chemical probes. Over 100 drugs met the standard criteria for probes, and 40 did so by more stringent criteria. A chemical information approach to drug-target association can guide therapeutic development and reveal applications to probe biology, a focus of much current interest.

Details

Database :
OAIster
Journal :
Proceedings of the National Academy of Sciences of the United States of America; vol 109, iss 28, 11178-11183; 0027-8424
Notes :
application/pdf, Proceedings of the National Academy of Sciences of the United States of America vol 109, iss 28, 11178-11183 0027-8424
Publication Type :
Electronic Resource
Accession number :
edsoai.on1377976944
Document Type :
Electronic Resource