Scientific Reports (Jun 2017)

Ohmyungsamycins promote antimicrobial responses through autophagy activation via AMP-activated protein kinase pathway

  • Tae Sung Kim,
  • Yern-Hyerk Shin,
  • Hye-Mi Lee,
  • Jin Kyung Kim,
  • Jin Ho Choe,
  • Ji-Chan Jang,
  • Soohyun Um,
  • Hyo Sun Jin,
  • Masaaki Komatsu,
  • Guang-Ho Cha,
  • Han-Jung Chae,
  • Dong-Chan Oh,
  • Eun-Kyeong Jo

DOI
https://doi.org/10.1038/s41598-017-03477-3
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 14

Abstract

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Abstract The induction of host cell autophagy by various autophagy inducers contributes to the antimicrobial host defense against Mycobacterium tuberculosis (Mtb), a major pathogenic strain that causes human tuberculosis. In this study, we present a role for the newly identified cyclic peptides ohmyungsamycins (OMS) A and B in the antimicrobial responses against Mtb infections by activating autophagy in murine bone marrow-derived macrophages (BMDMs). OMS robustly activated autophagy, which was essentially required for the colocalization of LC3 autophagosomes with bacterial phagosomes and antimicrobial responses against Mtb in BMDMs. Using a Drosophila melanogaster–Mycobacterium marinum infection model, we showed that OMS-A-induced autophagy contributed to the increased survival of infected flies and the limitation of bacterial load. We further showed that OMS triggered AMP-activated protein kinase (AMPK) activation, which was required for OMS-mediated phagosome maturation and antimicrobial responses against Mtb. Moreover, treating BMDMs with OMS led to dose-dependent inhibition of macrophage inflammatory responses, which was also dependent on AMPK activation. Collectively, these data show that OMS is a promising candidate for new anti-mycobacterial therapeutics by activating antibacterial autophagy via AMPK-dependent signaling and suppressing excessive inflammation during Mtb infections.