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An IL-13 inhibitor blocks the development of hepatic fibrosis during a T-helper type 2–dominated inflammatory response

机译:IL-13抑制剂在2型T辅助为主的炎症反应中阻止肝纤维化的发展

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摘要

In schistosomiasis, chronic parasite egg–induced granuloma formation can lead to tissue destruction and fibrosis, which causes much of the morbidity and mortality associated with this disease. Here we show the importance of IL-13 in the pathogenesis of schistosomiasis, and demonstrate, perhaps for the first time, the therapeutic efficacy of an IL-13 inhibitor, sIL-13Rα2-Fc, in the control of hepatic fibrosis. T-helper type 2 (Th2) cytokines dominate the immune response in mice infected with Schistosoma mansoni, yet the specific contributions of IL-13 and IL-4 to the development of fibrosis were not previously investigated. Our studies demonstrate that both cytokines play redundant roles in granuloma formation, which explains the ability of IL-4–deficient mice to form granulomas around eggs. More importantly, however, these studies demonstrate that IL-13 is the dominant Th2-type cytokine regulating fibrosis. IL-13 stimulated collagen production in fibroblasts, and procollagen I and procollagen III mRNA expression was decreased in sIL-13Rα2-Fc–treated mice. Moreover, the reduction in fibrosis observed in IL-4–deficient mice was much less pronounced than that in sIL-13Rα2-Fc–treated animals. Fibrosis is a major pathological manifestation of a number of allergic, autoimmune, and infectious diseases. Thus, our findings provide evidence that IL-13 inhibitors may be of general therapeutic benefit in preventing damaging tissue fibrosis resulting from Th2-dominated inflammatory responses.
机译:在血吸虫病中,慢性寄生虫卵诱导的肉芽肿形成可导致组织破坏和纤维化,从而导致与此病相关的许多发病率和死亡率。在这里,我们显示了IL-13在血吸虫病发病机理中的重要性,并首次证明了IL-13抑制剂sIL-13Rα2-Fc在控制肝纤维化中的疗效。 T型辅助2型(Th2)细胞因子在曼氏血吸虫感染的小鼠中的免疫反应中起主导作用,但先前尚未研究IL-13和IL-4对纤维化发展的特定作用。我们的研究表明,两种细胞因子在肉芽肿形成中都起着多余的作用,这解释了IL-4缺陷小鼠在卵周围形成肉芽肿的能力。但是,更重要的是,这些研究表明IL-13是主要的Th2型细胞因子调节纤维化。 IL-13刺激了成纤维细胞中胶原蛋白的产生,而经sIL-13Rα2-Fc治疗的小鼠中前胶原I和前胶原III mRNA表达下降。此外,与sIL-13Rα2-Fc治疗的动物相比,在缺乏IL-4的小鼠中观察到的纤维化减少没有那么明显。纤维化是许多过敏性,自身免疫性和感染性疾病的主要病理表现。因此,我们的发现提供了证据,即IL-13抑制剂在预防由Th2为主的炎症反应导致的破坏性组织纤维化中可能具有一般的治疗益处。

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