Intracellular Salmonella hijacks the mitochondrial citrate carrier to evade host oxidative defenses.
Journal
Nature Communications
Journal Volume
16
Journal Issue
1
Start Page
Article Number : 9806
ISSN
2041-1723
Date Issued
2025-11-06
Author(s)
Fu, Chieh-Hua
Hsu, Yu-Ting
Hsu, Shao-Chun
Chen, Nai-Shu
Hu, Hsueh-Wen
Wu, Ting-Yin
Huang, Yi-Jou
Chen, Ying-Chu
Luo, An-Chi
Abstract
Intracellular vacuolar pathogens replicate within membrane-bound compartments known as pathogen-containing vacuoles (PCVs). Maintaining the integrity of these vacuoles is essential for creating a permissive niche that supports pathogen survival and proliferation. In this study, we show that Salmonella enterica serovar Typhimurium co-opts the host mitochondrial citrate carrier (CIC) to promote its intracellular replication by detoxifying the Salmonella-containing vacuole (SCV). Loss of CIC significantly impairs Salmonella growth within host cells, as CIC recruitment to SCVs regulates local citrate levels and mitigates the production of reactive oxygen species (ROS), thereby reducing oxidative stress. Mechanistically, we identify the SPI-2 effector SseF as a critical factor that interacts with CIC and the GTPase RAB7, enabling CIC recruitment to the SCV membrane. These findings reveal a previously unrecognized strategy by which an intracellular pathogen hijacks a mitochondrial metabolite transporter to modulate the vacuolar environment and evade host antimicrobial defenses. Notably, pharmacological inhibition of CIC sensitizes Salmonella to host immune pressures, highlighting CIC as a potential target for host-directed antimicrobial therapy.
Publisher
Nature Research
Type
journal article