Distinct pathogenic mutations in ARF1 allow dissection of its dual role in cGAS-STING signalling.

IF 6.5 1区生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY

EMBO Reports Pub Date : 2025-03-24 DOI:10.1038/s44319-025-00423-7

Johannes Lang, Tim Bergner, Julia Zinngrebe, Alice Lepelley, Katharina Vill, Steffen Leiz, Meinhard Wlaschek, Matias Wagner, Karin Scharffetter-Kochanek, Pamela Fischer-Posovszky, Clarissa Read, Yanick J Crow, Maximilian Hirschenberger, Konstantin M J Sparrer

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引用次数: 0

Abstract

Tight control of cGAS-STING-mediated DNA sensing is crucial to avoid auto-inflammation. The GTPase ADP-ribosylation factor 1 (ARF1) is crucial to maintain cGAS-STING homeostasis and various pathogenic ARF1 variants are associated with type I interferonopathies. Functional ARF1 inhibits STING activity by maintaining mitochondrial integrity and facilitating COPI-mediated retrograde STING trafficking and deactivation. Yet the factors governing the two distinct functions of ARF1 remained unexplored. Here, we dissect ARF1's dual role by a comparative analysis of disease-associated ARF1 variants and their impact on STING signalling. We identify a de novo heterozygous s.55 C > T/p.R19C ARF1 variant in a patient with type I interferonopathy symptoms. The GTPase-deficient variant ARF1 R19C selectively disrupts COPI binding and retrograde transport of STING, thereby prolonging innate immune activation without affecting mitochondrial integrity. Treatment of patient fibroblasts in vitro with the STING signalling inhibitors H-151 and amlexanox reduces chronic interferon signalling. Summarizing, our data reveal the molecular basis of a ARF1-associated type I interferonopathy allowing dissection of the two roles of ARF1, and suggest that pharmacological targeting of STING may alleviate ARF1-associated auto-inflammation.

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ARF1中不同的致病突变允许解剖其在cGAS-STING信号传导中的双重作用。

严格控制cgas - sting介导的DNA传感是避免自身炎症的关键。GTPase adp -核糖基化因子1 （ARF1）对维持cGAS-STING稳态至关重要，各种致病性ARF1变异与I型干扰素病变相关。功能性ARF1通过维持线粒体完整性和促进copi介导的逆行STING运输和失活来抑制STING活性。然而，控制ARF1两种不同功能的因素仍未被探索。在这里，我们通过比较分析疾病相关的ARF1变异及其对STING信号传导的影响来剖析ARF1的双重作用。我们鉴定了一种新的杂合菌株s.55c> T/p。1型干扰素病症状患者的R19C ARF1变异gtpase缺陷变体ARF1 R19C选择性地破坏COPI结合和STING的逆行运输，从而在不影响线粒体完整性的情况下延长先天免疫激活。体外用STING信号抑制剂H-151和氨lexanox治疗患者成纤维细胞可减少慢性干扰素信号。总之，我们的数据揭示了ARF1相关的I型干扰素病变的分子基础，允许分离ARF1的两个作用，并提示STING的药理靶向可能减轻ARF1相关的自身炎症。

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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来源期刊

EMBO Reports 生物-生化与分子生物学

CiteScore

11.20

自引率

1.30%

发文量

267

审稿时长

1 months

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