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Itaconate transport across the plasma membrane and Salmonella-containing vacuole via MCT1/4 modulates macrophage antibacterial activity

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作者

    Qingcai Meng,  Chengxi Li,  Yuping Cai,  Ying Chen,  Xiaoqing Chen,  Xin Wang,  Biling Zhang,  Yue Zhang,  Feng Liu,  Meixin Chen
    Meixin Chen
分类
关键词
bidirectional transport of itaconate; bacterial infection; macrophage

摘要

Itaconate accumulates and manifests antibacterial activity in macrophages upon bacterial infection. Convincing evidence substantiates that itaconate transports across the plasma membrane and vacuolar membrane. But the molecular bases underlying the bidirectional transport of itaconate across membranes and how it affects intracellular bacterial replication remain elusive. Here, we identify MCT1 and MCT4 as bidirectional transporters of itaconate. In addition to modulating itaconate concentration as transporters at the plasma membrane, MCT1 and MCT4 function as itaconate transporters at Salmonella-containing vacuole (SCV). Upon Salmonella infection, MCT1 and MCT4 transport itaconate into SCV facilitated by RAB32. Itaconate is also secreted out of cells through MCT1 and MCT4 as the infection persists. The suppression of MCT1 and MCT4-dependent itaconate secretion generally increases the concentration of itaconate and the prevalence of itaconate-targeted Salmonella intracellularly, consequently inhibiting Salmonella replication. Our study offers valuable insights into itaconate transport during bacterial infection and sheds light on the development of itaconate-dependent therapeutic strategies.

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DOI:

Submission ID:

12

下载次数

已发布

2025-11-19

如何引用

Meng, Q., Li, C., Cai, Y., Chen, Y., Chen, X., Wang, X., Zhang, B., Zhang, Y., Liu, F., & Chen, M. (2025). Itaconate transport across the plasma membrane and Salmonella-containing vacuole via MCT1/4 modulates macrophage antibacterial activity. 浪淘沙预印本平台. https://doi.org/10.65215/k8ndfn18

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