自体抗原 TRIM21 (Ro52) 在细胞溶解性死亡后形成促炎免疫复合物

Esther L Jones, Benjamin Demarco, Madelon ML de Jong, Han Cai, Sarah Hill, Ryan E. Glass, Gemma Harris, Saba Nayar, Benjamin A Fisher, Audrey Gerard, Jelena S Bezbradica, Lynn B Dustin
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摘要

斯约格伦病(SjD)会引起局部和全身性炎症,这是由于针对细胞内蛋白(如 TRIM21/Ro52)的自身抗体产生所致。TRIM21 是一种 E3 泛素连接酶,它能与蛋白溶解的病原体上的抗体 Fc 结构域结合,这些病原体逃过了细胞外免疫,进入了细胞溶质;TRIM21 对这些病原体进行泛素化,促使其蛋白酶体降解。TRIM21如何以及为何成为自身抗原仍不清楚。我们的研究表明,TRIM21会在细胞溶解性死亡(热凋亡/坏死)时释放,但不会在细胞凋亡时释放。释放的 TRIM21 与循环抗体 Fc 结构域结合,形成大型免疫复合物(IC)。这些复合物与 TRIM21/Ro52 血清阳性 SjD 血浆抗体结合后会进一步增强,其中的相互作用是通过 Fc 和 F(ab')2 结构域介导的。TRIM21-IC 被巨噬细胞吸收,在高干扰素环境中,巨噬细胞会驱动促炎反应、抗原呈递以及炎症和代谢转录变化。虽然死亡细胞会释放出许多细胞膜蛋白,但由于 TRIM21 与抗体的高亲和力,它能产生大量的 IC。这可能会使炎症和抗原呈递永久化,导致 TRIM21 成为高度自身免疫原。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Autoantigen TRIM21 (Ro52) assembles pro-inflammatory immune complexes following lytic cell death
Sjögren's disease (SjD) causes localised and systemic inflammation due to autoantibody production against intracellular proteins, such as TRIM21/Ro52. TRIM21 is an E3 ubiquitin ligase which binds antibody Fc domains on opsonised pathogens, which have escaped extracellular immunity and entered cytosols; TRIM21 ubiquitinates these, driving their proteasomal degradation. How and why TRIM21 becomes an autoantigen remains unclear. We show that TRIM21 is released upon lytic cell death (pyroptosis/necroptosis) but not apoptosis. Released TRIM21 binds circulating antibody Fc domains, and forms large immune complexes (ICs). These are further enhanced with TRIM21/Ro52 seropositive SjD plasma antibodies, where interactions are mediated via both Fc and F(ab')2 domains. TRIM21-ICs are taken up by macrophages, which in high interferon environments drive pro-inflammatory responses, antigen presentation, and inflammatory and metabolic transcriptional changes. Whilst many cytosolic proteins are released by dead cells, due to its high affinity for antibodies, TRIM21 can generate large ICs. This may perpetuate inflammation and antigen presentation, causing TRIM21 to be highly autoimmunogenic.
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