Salmonella effector SseL induces PD-L1 up-regulation and T cell inactivation via β-catenin signalling axis

The Journal of Infectious Diseases Pub Date : 2025-03-19 DOI:10.1093/infdis/jiaf131

Umesh Chopra, Maria Kondooparambil Sabu, Raju S Rajmani, Ayushi Devendrasingh Chaudhary, Shashi Kumar Gupta, Dipshikha Chakravortty

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Abstract

The upregulation of PD-L1 by various pathogens is a recognized strategy to evade the adaptive immune response. Salmonella infection also upregulates PD-L1 levels; however, the underlying mechanism remains unclear. Our study reveals that this upregulation is mediated by Salmonella pathogenicity island 2 (SPI-2) effectors, as PFA-fixed and STMΔssaV fail to alter PD-L1 levels. We have further investigated the role of the SPI-2 effector SseL (a deubiquitinase) in PD-L1 upregulation, and our study reveals SseL to be crucial for upregulating PD-L1 in vitro as well as in vivo murine models. STMΔsseL exhibits colonization defects in secondary infection sites such as the liver and spleen. Notably, STMΔsseL-infected mice show earlier mortality associated with heightened inflammation. Mechanistically, SseL stabilizes β-catenin, which translocates to the nucleus and leads to PD-L1 transcription, which is abrogated by the β-catenin/TCF inhibitor FH535. Collectively, our study elucidates the mechanism by which Salmonella mediates immune suppression through PD-L1 upregulation.

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沙门氏菌效应物SseL通过β-catenin信号轴诱导PD-L1上调和T细胞失活

各种病原体上调PD-L1是一种公认的逃避适应性免疫反应的策略。沙门氏菌感染也会上调PD-L1水平；然而，其潜在机制尚不清楚。我们的研究表明，这种上调是由沙门氏菌致病性岛2 （SPI-2）效应物介导的，因为pfa固定和STMΔssaV不能改变PD-L1的水平。我们进一步研究了SPI-2效应物SseL（一种去泛素酶）在PD-L1上调中的作用，我们的研究表明SseL在体外和体内小鼠模型中对PD-L1上调至关重要。STMΔsseL显示继发感染部位如肝脏和脾脏的定植缺陷。值得注意的是，STMΔsseL-infected小鼠显示出与炎症加剧相关的早期死亡率。从机制上讲，SseL稳定β-catenin， β-catenin易位到细胞核并导致PD-L1转录，而这一转录被β-catenin/TCF抑制剂FH535所消除。总之，我们的研究阐明了沙门氏菌通过上调PD-L1介导免疫抑制的机制。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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The Journal of Infectious Diseases

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