| Literature DB >> 34256013 |
Michael Dominic Stutz1, Cody Charles Allison1, Samar Ojaimi1, Simon Peter Preston1, Marcel Doerflinger1, Philip Arandjelovic1, Lachlan Whitehead1, Stefanie M Bader1, Daniel Batey1, Marie-Liesse Asselin-Labat1, Marco J Herold1, Andreas Strasser1, Nicholas P West2, Marc Pellegrini3.
Abstract
Apoptosis can potently defend against intracellular pathogens by directly killing microbes and eliminating their replicative niche. However, the reported ability of Mycobacterium tuberculosis to restrict apoptotic pathways in macrophages in vitro has led to apoptosis being dismissed as a host-protective process in tuberculosis despite a lack of in vivo evidence. Here we define crucial in vivo functions of the death receptor-mediated and BCL-2-regulated apoptosis pathways in mediating protection against tuberculosis by eliminating distinct populations of infected macrophages and neutrophils and priming T cell responses. We further show that apoptotic pathways can be targeted therapeutically with clinical-stage compounds that antagonize inhibitor of apoptosis (IAP) proteins to promote clearance of M. tuberculosis in mice. These findings reveal that any inhibition of apoptosis by M. tuberculosis is incomplete in vivo, advancing our understanding of host-protective responses to tuberculosis (TB) and revealing host pathways that may be targetable for treatment of disease.Entities:
Keywords: IAP antagonist; Mycobacterium tuberculosis; apoptosis; caspase; cell death; macrophages; pyroptosis
Year: 2021 PMID: 34256013 DOI: 10.1016/j.immuni.2021.06.009
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745