Essential but Not Vulnerable: Indazole Sulfonamides Targeting Inosine Monophosphate Dehydrogenase as Potential Leads against Mycobacterium tuberculosis. Academic Article uri icon

Overview

abstract

  • A potent, noncytotoxic indazole sulfonamide was identified by high-throughput screening of >100,000 synthetic compounds for activity against Mycobacterium tuberculosis (Mtb). This noncytotoxic compound did not directly inhibit cell wall biogenesis but triggered a slow lysis of Mtb cells as measured by release of intracellular green fluorescent protein (GFP). Isolation of resistant mutants followed by whole-genome sequencing showed an unusual gene amplification of a 40 gene region spanning from Rv3371 to Rv3411c and in one case a potential promoter mutation upstream of guaB2 (Rv3411c) encoding inosine monophosphate dehydrogenase (IMPDH). Subsequent biochemical validation confirmed direct inhibition of IMPDH by an uncompetitive mode of inhibition, and growth inhibition could be rescued by supplementation with guanine, a bypass mechanism for the IMPDH pathway. Beads containing immobilized indazole sulfonamides specifically interacted with IMPDH in cell lysates. X-ray crystallography of the IMPDH-IMP-inhibitor complex revealed that the primary interactions of these compounds with IMPDH were direct pi-pi interactions with the IMP substrate. Advanced lead compounds in this series with acceptable pharmacokinetic properties failed to show efficacy in acute or chronic murine models of tuberculosis (TB). Time-kill experiments in vitro suggest that sustained exposure to drug concentrations above the minimum inhibitory concentration (MIC) for 24 h were required for a cidal effect, levels that have been difficult to achieve in vivo. Direct measurement of guanine levels in resected lung tissue from tuberculosis-infected animals and patients revealed 0.5-2 mM concentrations in caseum and normal lung tissue. The high lesional levels of guanine and the slow lytic, growth-rate-dependent effect of IMPDH inhibition pose challenges to developing drugs against this target for use in treating TB.

authors

  • Park, Yumi
  • Pacitto, Angela
  • Bayliss, Tracy
  • Cleghorn, Laura A T
  • Wang, Zhe
  • Hartman, Travis E.
  • Arora, Kriti
  • Ioerger, Thomas R
  • Sacchettini, Jim
  • Rizzi, Menico
  • Donini, Stefano
  • Blundell, Tom L
  • Ascher, David B
  • Rhee, Kyu Y.
  • Breda, Ardala
  • Zhou, Nian
  • Dartois, Veronique
  • Jonnala, Surendranadha Reddy
  • Via, Laura E
  • Mizrahi, Valerie
  • Epemolu, Ola
  • Stojanovski, Laste
  • Simeons, Fred
  • Osuna-Cabello, Maria
  • Ellis, Lucy
  • MacKenzie, Claire J
  • Smith, Alasdair R C
  • Davis, Susan H
  • Murugesan, Dinakaran
  • Buchanan, Kirsteen I
  • Turner, Penelope A
  • Huggett, Margaret
  • Zuccotto, Fabio
  • Rebollo-Lopez, Maria Jose
  • Lafuente-Monasterio, Maria Jose
  • Sanz, Olalla
  • Diaz, Gracia Santos
  • Lelièvre, Joël
  • Ballell, Lluis
  • Selenski, Carolyn
  • Axtman, Matthew
  • Ghidelli-Disse, Sonja
  • Pflaumer, Hannah
  • Bösche, Markus
  • Drewes, Gerard
  • Freiberg, Gail M
  • Kurnick, Matthew D
  • Srikumaran, Myron
  • Kempf, Dale J
  • Green, Simon R
  • Ray, Peter C
  • Read, Kevin
  • Wyatt, Paul
  • Barry, Clifton E
  • Boshoff, Helena I

publication date

  • October 17, 2016

Research

keywords

  • Antitubercular Agents
  • IMP Dehydrogenase
  • Mycobacterium tuberculosis
  • Sulfonamides

Identity

PubMed Central ID

  • PMC5972394

Scopus Document Identifier

  • 85018480535

Digital Object Identifier (DOI)

  • 10.1021/acsinfecdis.6b00103

PubMed ID

  • 27704782

Additional Document Info

volume

  • 3

issue

  • 1