Research Group Biomarkers for Infectious Diseases, TWINCORE, Centre for Experimental and Clinical Infection Research, Hannover, Germany.
Research Group Biomarkers for Infectious Diseases, Helmholtz Centre for Infection Research, Braunschweig, Germany.
Clin Transl Med. 2022 Jul;12(7):e931. doi: 10.1002/ctm2.931.
Congenital ISG15 deficiency is a rare autoinflammatory disorder that is driven by chronically elevated systemic interferon levels and predominantly affects central nervous system and skin.
We have developed induced pluripotent stem cell-derived macrophages and endothelial cells as a model to study the cellular phenotype of ISG15 deficiency and identify novel treatments. ISG15 macrophages exhibited the expected hyperinflammatory responses, but normal phagocytic function. In addition, they displayed a multifaceted pathological phenotype featuring increased apoptosis/pyroptosis, oxidative stress, glycolysis, and acylcarnitine levels, but decreased glutamine uptake, BCAT1 expression, branched chain amino acid catabolism, oxidative phosphorylation, β-oxidation, and NAD(P)H-dependent oxidoreductase activity. Furthermore, expression of genes involved in mitochondrial biogenesis and respiratory chain complexes II-V was diminished in ISG15 cells. Defective mitochondrial respiration was restored by transduction with wild-type ISG15, but only partially by a conjugation-deficient variant, suggesting that some ISG15 functions in mitochondrial respiration require ISGylation to cellular targets. Treatment with itaconate, dimethyl-itaconate, 4-octyl-itaconate, and the JAK1/2 inhibitor ruxolitinib ameliorated increased inflammation, propensity for cell death, and oxidative stress. Furthermore, the treatments greatly improved mitochondria-related gene expression, BCAT1 levels, redox balance, and intracellular and extracellular ATP levels. However, efficacy differed among the compounds according to read-out and cell type, suggesting that their effects on cellular targets are not identical. Indeed, only itaconates increased expression of anti-oxidant genes NFE2L2, HMOX1, and GPX7, and dimethyl-itaconate improved redox balance the most. Even though itaconate treatments normalized the elevated expression of interferon-stimulated genes, ISG15 macrophages maintained their reduced susceptibility to influenza virus infection.
These findings expand the cellular phenotype of human ISG15 deficiency and reveal the importance of ISG15 for regulating oxidative stress, branched chain amino acid metabolism, and mitochondrial function in humans. The results validate ruxolitinib as treatment for ISG15 deficiency and suggest itaconate-based medications as additional therapeutics for this rare disorder.
先天性 ISG15 缺乏症是一种罕见的自身炎症性疾病,由慢性系统性干扰素水平升高驱动,主要影响中枢神经系统和皮肤。
我们已经开发了诱导多能干细胞衍生的巨噬细胞和内皮细胞作为研究 ISG15 缺乏症细胞表型的模型,并确定了新的治疗方法。ISG15 巨噬细胞表现出预期的过度炎症反应,但正常的吞噬功能。此外,它们表现出多方面的病理表型,包括增加的细胞凋亡/细胞焦亡、氧化应激、糖酵解和酰基辅酶 A 水平,但减少谷氨酰胺摄取、BCAT1 表达、支链氨基酸分解代谢、氧化磷酸化、β-氧化和 NAD(P)H 依赖性氧化还原酶活性。此外,ISG15 细胞中线粒体生物发生和呼吸链复合物 II-V 相关基因的表达减少。野生型 ISG15 的转导恢复了缺陷的线粒体呼吸,但部分由缀合缺陷变体恢复,表明 ISG15 在线粒体呼吸中的一些功能需要 ISGylation 到细胞靶标。用衣康酸、二甲基衣康酸、4-辛基衣康酸和 JAK1/2 抑制剂鲁索利替尼治疗可改善炎症增加、细胞死亡倾向和氧化应激。此外,这些治疗方法大大改善了与线粒体相关的基因表达、BCAT1 水平、氧化还原平衡以及细胞内和细胞外 ATP 水平。然而,根据读出和细胞类型,化合物的疗效不同,这表明它们对细胞靶标的作用并不相同。事实上,只有衣康酸增加了抗氧化基因 NFE2L2、HMOX1 和 GPX7 的表达,而二甲基衣康酸最能改善氧化还原平衡。尽管衣康酸治疗使干扰素刺激基因的表达升高正常化,但 ISG15 巨噬细胞仍保持对流感病毒感染的低易感性。
这些发现扩展了人类 ISG15 缺乏症的细胞表型,并揭示了 ISG15 对调节人类氧化应激、支链氨基酸代谢和线粒体功能的重要性。结果验证了鲁索利替尼是治疗 ISG15 缺乏症的方法,并表明衣康酸盐类药物是治疗这种罕见疾病的额外治疗方法。
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