Litcius/Paper detail

Peroxisomal ROS control cytosolic <i>Mycobacterium tuberculosis</i> replication in human macrophages

Enrica Pellegrino, Beren Aylan, Claudio Bussi, Antony Fearns, Elliott M. Bernard, Natalia Athanasiadi, Pierre Santucci, Laure Botella, Maximiliano G. Gutiérrez

2023The Journal of Cell Biology30 citationsDOIOpen Access PDF

Abstract

Peroxisomes are organelles involved in many metabolic processes including lipid metabolism, reactive oxygen species (ROS) turnover, and antimicrobial immune responses. However, the cellular mechanisms by which peroxisomes contribute to bacterial elimination in macrophages remain elusive. Here, we investigated peroxisome function in iPSC-derived human macrophages (iPSDM) during infection with Mycobacterium tuberculosis (Mtb). We discovered that Mtb-triggered peroxisome biogenesis requires the ESX-1 type 7 secretion system, critical for cytosolic access. iPSDM lacking peroxisomes were permissive to Mtb wild-type (WT) replication but were able to restrict an Mtb mutant missing functional ESX-1, suggesting a role for peroxisomes in the control of cytosolic but not phagosomal Mtb. Using genetically encoded localization-dependent ROS probes, we found peroxisomes increased ROS levels during Mtb WT infection. Thus, human macrophages respond to the infection by increasing peroxisomes that generate ROS primarily to restrict cytosolic Mtb. Our data uncover a peroxisome-controlled, ROS-mediated mechanism that contributes to the restriction of cytosolic bacteria.

Topics & Concepts

PeroxisomeCytosolCell biologyBiologyReactive oxygen speciesMycobacterium tuberculosisBiogenesisMicrobiologyBiochemistryGeneTuberculosisEnzymePathologyMedicinePeroxisome Proliferator-Activated ReceptorsImmune cells in cancerPneumocystis jirovecii pneumonia detection and treatment