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Involvement of NF-κBIZ and related cytokines in age-associated renal fibrosis

机译:NF-κBIZ和相关细胞因子参与与年龄相关的肾纤维化

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摘要

Chronic inflammation is a major contributor to age-related nephropathic changes, including renal fibrosis. In this study, various experimental paradigms were designed to delineate the role played by NF-?BIZ (also known as I?B?) in age-associated renal fibrosis. Analyses based on RNA-sequencing findings obtained by next generation sequencing (NGS) revealed the upregulations of NF-?BIZ and of IL-6 and MCP-1 (both known to be regulated by NF-?BIZ) during aging. The up-regulation of NF-?BIZ in aged rat kidneys coincided with increased macrophage infiltration. In LPS-treated macrophages, oxidative stress was found to play a pivotal role in NF-?BIZ expression, suggesting age-related oxidative stress is associated with NF-?BIZ activation. Furthermore, these in vitro findings were confirmed in LPS-treated old rats, which showed higher levels of oxidative stress and NF-?BIZ in kidneys than LPS-treated young rats. Additional in vitro experiments using macrophages and kidney fibroblasts demonstrated NF-?BIZ and related cytokines participate in fibrosis. In particular, increased levels of NF-?BIZ-associated cytokines in macrophages significantly up-regulated TGF-β induced kidney fibroblast activation. Moreover, experiments with NF-?BIZ knocked down macrophages showed reduced TGF-β- induced kidney fibroblast activation. The findings of the present study provide evidence regarding an involvement of NF-?BIZ in age-associated progressive renal fibrosis and provides potential targets for its prevention.
机译:慢性炎症是与年龄相关的肾病性变化的主要因素,包括肾脏纤维化。在这项研究中,设计了各种实验范式来描述NF-?BIZ(也称为I?B?)在与年龄相关的肾纤维化中的作用。基于下一代测序(NGS)获得的RNA测序发现的分析表明,衰老过程中NF-?BIZ以及IL-6和MCP-1(均已知受NF-?BIZ调节)的上调。衰老大鼠肾脏中NF-?BIZ的上调与巨噬细胞浸润的增加相吻合。在经LPS处理的巨噬细胞中,发现氧化应激在NF-?BIZ表达中起关键作用,这表明与年龄相关的氧化应激与NF-?BIZ活化有关。此外,这些体外研究结果在LPS治疗的老年大鼠中得到证实,与LPS治疗的年轻大鼠相比,肾脏中的氧化应激和NF-κBIZ水平更高。使用巨噬细胞和肾成纤维细胞进行的其他体外实验证明NF-?BIZ和相关细胞因子参与了纤维化。尤其是,巨噬细胞中与NF-?BIZ相关的细胞因子水平的增加显着上调了TGF-β诱导的肾成纤维细胞活化。此外,用NF-?BIZ敲低巨噬细胞进行的实验表明,TGF-β-诱导的肾成纤维细胞活化降低。本研究的发现提供了有关NF-?BIZ与年龄相关的进行性肾纤维化的证据,并为其预防提供了潜在的靶标。

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