Release of 50 new, drug-like compounds and their computational target predictions for open source anti-tubercular drug discovery Articles uri icon

authors

  • REBOLLO-LOPEZ, MARÍA JOSE
  • LELIÈVRE, JOËL
  • ÁLVAREZ GÓMEZ, DANIEL
  • CASTRO PICHEL, JULIA
  • MARTÍNEZ-JIMÉNEZ, FRANCISCO
  • PAPADATOS, GEORGE
  • KUMAR, VINOD
  • COLMENAREJO, GONZALO
  • MUGUMBATE, GRACE
  • HURLE, MARK
  • BARROSO, VANESSA
  • YOUNG, ROB J.
  • MARTÍNEZ HOYOS, MARÍA
  • GONZÁLEZ DEL RÍO, RUBÉN
  • BATES, ROBERT H.
  • LOPEZ-ROMAN, EVA MARIA
  • MENDOZA LOSANA, ALFONSO
  • BROWN, JAMES R.
  • ÁLVAREZ RUIZ, EMILIO
  • MARTI-RENOM, MARC A.
  • OVERINGTON, JOHN P.
  • CAMMACK, NICHOLAS
  • BARROS-AGUIRE, DAVID

publication date

  • December 2015

start page

  • 1

end page

  • 18

issue

  • 12

volume

  • 10

International Standard Serial Number (ISSN)

  • 1932-6203

abstract

  • As a follow up to the antimycobacterial screening exercise and the release of GSK's first Tres Cantos Antimycobacterial Set (TCAMS-TB), this paper presents the results of a second antitubercular screening effort of two hundred and fifty thousand compounds recently added to the GSK collection. The compounds were further prioritized based on not only antitubercular potency but also on physicochemical characteristics. The 50 most attractive compounds were then progressed for evaluation in three different predictive computational biology algorithms based on structural similarity or GSK historical biological assay data in order to determine their possible mechanisms of action. This effort has resulted in the identification of novel compounds and their hypothesized targets that will hopefully fuel future TB drug discovery and target validation programs alike.

subjects

  • Biology and Biomedicine