TY - JOUR T1 - Ebselen attenuates mycobacterial virulence through inhibition of ESX-1 secretion JF - bioRxiv DO - 10.1101/828574 SP - 828574 AU - Morwan M. Osman AU - Malte L. Pinckert AU - Sew Peak-Chew AU - Mark A. Troll AU - William H. Conrad AU - Lalita Ramakrishnan Y1 - 2021/01/01 UR - http://biorxiv.org/content/early/2021/12/13/828574.abstract N2 - The type VII secretion system ESX-1 mediates virulence in Mycobacterium tuberculosis and Mycobacterium marinum. We find that in M. marinum, the synthetic organoselenium compound ebselen inhibits secretion of ESAT-6, a major ESX-1 substrate. We find that ebselen inhibits the in vitro activity of the ESX-1 AAA+ ATPase EccA1, which potentiates ESX-1 substrate secretion and function. Ebselen modifies a cysteine in its N-terminal tetratricopeptide repeat domain that is required for EccA1’s in vitro ATPase activity. Surprisingly, mutational analyses show this this cysteine is not required for ESX-1 secretion or ebselen’s activity, showing that ebselen inhibits ESX-1 secretion independently of inhibiting EccA1 activity in vitro. While the mechanism by which ebselen inhibits ESX-1 secretion remains elusive, we show that it attenuates ESX-1-mediated damage of M. marinum-containing macrophage phagosomes and inhibits intramacrophage growth. Extending our studies to M. tuberculosis, we find that ebselen inhibits ESX-1 secretion and phagosomal membrane damage in this organism. This work provides insight into EccA1 biology. Ebselen is an orally active drug in clinical trials for other conditions and this work suggests its potential in tuberculosis therapy.Competing Interest StatementThe authors have declared no competing interest. ER -