Amber De Visscher, Marte Vandeput, Jessica Vandenhaute, Bert Malengier-Devlies, Eline Bernaerts, Kourosh Ahmadzadeh, Jessica Filtjens, Tania Mitera, Nele Berghmans, Philippe E. Van den Steen, Christin Friedrich, Georg Gasteiger, Carine Wouters, Patrick Matthys
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By utilizing a Toll-like receptor (TLR)9- and TLR3:4-triggered MAS model, we showed that ILC1s highly produce IFN-γ and TNF-α. However, activated ILC1s undergo apoptosis and are strongly reduced in numbers, while cNK cells resist inflammation-induced apoptosis. Signs of mitochondrial stress suggest that this ILC1 apoptosis may be driven by inflammation-induced mitochondrial impairment. To study whether early induction of highly cytokine-producing ILC1s influences MAS development, we used Hobit KO mice due to their paucity of liver ILC1s but unaffected cNK cell numbers. Nevertheless, neither the severity of MAS features nor the total inflammatory cytokine levels were affected in these Hobit KO mice, indicating that ILC1s are dispensable for MAS pathogenesis. 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引用次数: 0
摘要
巨噬细胞活化综合征(MAS)是一种伴有肝脏炎症的严重细胞因子风暴紊乱。在肝脏中,经典的自然杀伤细胞(cNK)和肝脏驻留的 1 型先天性淋巴细胞(ILC1s)在 ILC 群体中占主导地位。迄今为止,研究主要集中在 cNK 细胞的相应作用上。考虑到 MAS 中的肝脏炎症和细胞因子风暴,肝脏驻留的 ILC1s 是一个值得探索的群体,因为它们在环境触发时能迅速产生细胞因子。通过利用Toll样受体(TLR)9和TLR3:4触发的MAS模型,我们发现ILC1s能大量产生IFN-γ和TNF-α。然而,活化的 ILC1 细胞会发生凋亡,数量会大幅减少,而 cNK 细胞则能抵御炎症诱导的凋亡。线粒体应激迹象表明,这种 ILC1 细胞凋亡可能是由炎症诱导的线粒体损伤驱动的。为了研究早期诱导高细胞因子分泌的 ILC1 是否会影响 MAS 的发展,我们使用了 Hobit KO 小鼠,因为它们的肝脏 ILC1 数量很少,但 cNK 细胞数量不受影响。然而,在这些 Hobit KO 小鼠中,MAS 特征的严重程度和总的炎症细胞因子水平都没有受到影响,这表明 ILC1s 在 MAS 发病机制中是不可或缺的。总之,我们的数据表明,ILC1s 在 TLR 触发过程中会发生凋亡,对 MAS 的发病机制是不可或缺的。
Liver type 1 innate lymphoid cells undergo apoptosis in murine models of macrophage activation syndrome and are dispensable for disease
Macrophage activation syndrome (MAS) exemplifies a severe cytokine storm disorder with liver inflammation. In the liver, classical natural killer (cNK) cells and liver-resident type 1 innate lymphoid cells (ILC1s) dominate the ILC population. Thus far, research has primarily focused on the corresponding role of cNK cells. Considering the liver inflammation and cytokine storm in MAS, liver-resident ILC1s represent an interesting population to explore due to their rapid cytokine production upon environmental triggers. By utilizing a Toll-like receptor (TLR)9- and TLR3:4-triggered MAS model, we showed that ILC1s highly produce IFN-γ and TNF-α. However, activated ILC1s undergo apoptosis and are strongly reduced in numbers, while cNK cells resist inflammation-induced apoptosis. Signs of mitochondrial stress suggest that this ILC1 apoptosis may be driven by inflammation-induced mitochondrial impairment. To study whether early induction of highly cytokine-producing ILC1s influences MAS development, we used Hobit KO mice due to their paucity of liver ILC1s but unaffected cNK cell numbers. Nevertheless, neither the severity of MAS features nor the total inflammatory cytokine levels were affected in these Hobit KO mice, indicating that ILC1s are dispensable for MAS pathogenesis. Collectively, our data demonstrate that ILC1s undergo apoptosis during TLR-triggering and are dispensable for MAS pathogenesis.
期刊介绍:
The European Journal of Immunology (EJI) is an official journal of EFIS. Established in 1971, EJI continues to serve the needs of the global immunology community covering basic, translational and clinical research, ranging from adaptive and innate immunity through to vaccines and immunotherapy, cancer, autoimmunity, allergy and more. Mechanistic insights and thought-provoking immunological findings are of interest, as are studies using the latest omics technologies. We offer fast track review for competitive situations, including recently scooped papers, format free submission, transparent and fair peer review and more as detailed in our policies.