The anti-mycobacterial activity of the cytochrome bcc inhibitor Q203 can be enhanced by small-molecule inhibition of cytochrome bd.

Sci Rep

Department of Molecular Cell Biology, Amsterdam Institute for Molecules, Medicines and Systems, Faculty of Earth- and Life Sciences, Vrije Universiteit Amsterdam, De Boelelaan 1108, 1081 HZ, Amsterdam, The Netherlands.

Published: February 2018

AI Article Synopsis

  • Mycobacterial energy metabolism is emerging as a key focus for new anti-tuberculosis drug development, with Q203 targeting the cytochrome bcc complex but not killing the bacteria.
  • Inhibition of cytochrome bd by aurachin D enhances Q203's bactericidal activity, addressing its limitations.
  • Combining inhibitors targeting both cytochrome bcc and cytochrome bd may be an effective strategy against Mycobacterium tuberculosis.

Article Abstract

Mycobacterial energy metabolism currently attracts strong attention as new target space for development of anti-tuberculosis drugs. The imidazopyridine Q203 targets the cytochrome bcc complex of the respiratory chain, a key component in energy metabolism. Q203 blocks growth of Mycobacterium tuberculosis at nanomolar concentrations, however, it fails to actually kill the bacteria, which may limit the clinical applicability of this candidate drug. In this report we show that inhibition of cytochrome bd, a parallel branch of the mycobacterial respiratory chain, by aurachin D invoked bactericidal activity of Q203. In biochemical assays using inverted membrane vesicles from Mycobacterium tuberculosis and Mycobacterium smegmatis we found that inhibition of respiratory chain activity by Q203 was incomplete, but could be enhanced by inactivation of cytochrome bd, either by genetic knock-out or by inhibition with aurachin D. These results indicate that simultaneously targeting the cytochrome bcc and the cytochrome bd branch of the mycobacterial respiratory chain may turn out as effective strategy for combating M. tuberculosis.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5805707PMC
http://dx.doi.org/10.1038/s41598-018-20989-8DOI Listing

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