The orphan nuclear receptor NR4A3 is dispensable for resident memory CD8+ T cell generation

Livia Odagiu, Salix Boulet, Dave Maurice-De Sousa, Jean-François Daudelin, Nathalie Labrecque
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Abstract

Different memory CD8+ T cell subsets are generated following acute responses: central, effector and resident (Trm). CD8+ Trm cells established residency at the sites of infection and provide an efficient and rapid frontline defense against re-infection. The NR4A family members (NR4A1, NR4A2 and NR4A3) of orphan nuclear receptor are transiently expressed following TCR signaling and NR4As were shown to influence CD8+ T cell response. Interestingly, Nr4a1, Nr4a2 and Nr4a3 have been reported to be transcribed by CD8+ Trm cells. In absence of NR4A1, less CD8+ Trm cells are present in the liver, lungs, small intestine intra-epithelial lymphocytes (IELs) and Peyers patches. NR4A2 was shown to play a role in the generation of small intestine IEL CD8+ Trm cells. However, evidence is still lacking for the contribution of NR4A3 during CD8+ Tm cell differentiation. In this study, we evaluated the role of NR4A3 in the differentiation and maintenance of CD8+ Trm cells. Our data demonstrate that in contrast to the other family members NR4A1 and NR4A2, NR4A3 is dispensable for the generation of CD8+ Trm cells in both epithelial and non-epithelial sites.
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孤儿核受体 NR4A3 对于常驻记忆 CD8+ T 细胞的生成是不可或缺的
急性反应后会产生不同的记忆性 CD8+ T 细胞亚群:中心细胞、效应细胞和常驻细胞(Trm)。CD8+ Trm 细胞在感染部位建立了驻留,为防止再次感染提供了高效、快速的前线防御。孤儿核受体 NR4A 家族成员(NR4A1、NR4A2 和 NR4A3)在 TCR 信号传导后瞬时表达,NR4As 被证明会影响 CD8+ T 细胞的反应。有趣的是,据报道,Nr4a1、Nr4a2 和 Nr4a3 可被 CD8+ Trm 细胞转录。在缺乏 NR4A1 的情况下,肝脏、肺、小肠上皮内淋巴细胞(IELs)和 Peyers 斑块中的 CD8+ Trm 细胞数量较少。研究表明,NR4A2 在小肠 IEL CD8+ Trm 细胞的生成中发挥作用。然而,NR4A3 在 CD8+ Tm 细胞分化过程中的作用仍缺乏证据。在这项研究中,我们评估了 NR4A3 在 CD8+ Tm 细胞分化和维持过程中的作用。我们的数据表明,与其他家族成员 NR4A1 和 NR4A2 不同,NR4A3 对于上皮和非上皮部位 CD8+ Tm 细胞的生成是不可或缺的。
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