AI Article Synopsis
- Intracellular bacterial pathogens manipulate host cell processes to create a suitable environment for their survival, with the Q fever bacterium using its Type 4 secretion system to form a specialized vacuole known as a CCV.
- The study identifies that the bacterial effector protein Vice interacts with specific lipids (like phosphatidylserine) and triggers the formation of compartments similar to CCVs in host cells, demonstrating its role in both vacuole formation and stabilization.
- Vice performs dual functions: first aiding in the internalization of vacuoles through macropinocytosis, and then disrupting the ESCRT machinery to maintain these compartments, highlighting its key role in bacterial replication and survival.
Article Abstract
Intracellular bacterial pathogens divert multiple cellular pathways to establish their niche and persist inside their host. , the causative agent of Q fever, secretes bacterial effector proteins via its Type 4 secretion system to generate a -containing vacuole (CCV). Manipulation of lipid and protein trafficking by these effectors is essential for bacterial replication and virulence. Here, we have characterized the lipid composition of CCVs and found that the effector Vice interacts with phosphoinositides and membranes enriched in phosphatidylserine and lysobisphosphatidic acid. Remarkably, eukaryotic cells ectopically expressing Vice present compartments that resemble early CCVs in both morphology and composition. We found that the biogenesis of these compartments relies on the double function of Vice. The effector protein initially localizes at the plasma membrane of eukaryotic cells where it triggers the internalization of large vacuoles by macropinocytosis. Then, Vice stabilizes these compartments by perturbing the ESCRT machinery. Collectively, our results reveal that Vice is an essential effector protein capable of hijacking two major cellular pathways to shape the bacterial replicative niche.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11194487 | PMC |
| http://dx.doi.org/10.1073/pnas.2315481121 | DOI Listing |
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