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Immunosuppressive effects of hydroxychloroquine and artemisinin combination therapy via the nuclear factor-kappa B signaling pathway in lupus nephritis mice

机译:羟基氯喹和青蒿素组合治疗通过核因子-Kappa发信息途径狼疮性肾炎小鼠的免疫抑制作用

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摘要

Lupus nephritis (LN) is one of the most common and severe manifestations of systemic lupus erythematosus, leading to permanent renal damage and chronic kidney disease. Hydroxychloroquine (HCQ) serves a protective role against lupus-associated clinical manifestations and medical complications; however, it results in numerous adverse reactions, limiting its long-term use. The aim of the present study was to investigate the combined effect of HCQ and artemisinin (ART) on LN, and to elucidate the underlying mechanisms. An in vivo LN mouse model was prepared, and the animals were administered prednisone (PDS; serving as a positive control), high-dose HCQ (H-HCQ) or low-dose HCQ combined with ART (L-HCQ + ART) once daily for 8 weeks. The body weight, serum biochemical parameters, immune and inflammatory indicators, renal and spleen histological alterations, and mRNA expression levels of Kruppel-like factor 15 (KLF15) and nuclear factor-kappa B (NF-kappa B) were analyzed. It was observed that L-HCQ + ART and H-HCQ ameliorated the LN-induced body weight decrease, and significantly decreased the levels of anti-double stranded DNA, antinuclear antibodies, immunoglobulin G, interferon gamma , tumor necrosis factor-alpha and transforming growth factor-beta 1, as well as improved the kidney and spleen pathology, when compared with the model group. In addition, L-HCQ + ART and H-HCQ treatments induced KLF15 upregulation and NF-kappa B downregulation. These results indicated that treatment with L-HCQ + ART exerted renoprotective effects by regulating the expression levels of cytokines, KLF15 and NF-kappa B. This combination treatment may have a similar immunosuppressive effect as PDS and H-HCQ, and may be a promising alternative for LN treatment.
机译:狼疮肾炎(LN)是全身狼疮红斑狼疮最常见和严重的表现之一,导致肾脏损伤永久性肾病和慢性肾病。羟氯喹(HCQ)对狼疮相关的临床表现和医疗并发症提供保护作用;然而,它导致许多不良反应,限制了长期使用。本研究的目的是探讨HCQ和青蒿素(ART)对LN的综合作用,并阐明潜在机制。制备了体内LN小鼠模型,并将动物施用泼尼松(PDS;用作阳性对照),高剂量HCQ(H-HCQ)或低剂量HCQ与ART(L-HCQ + ART)结合一次每天8周。分析了体重,血清生化参数,免疫和炎症指示剂,肾病和脾脏组织学改变,以及Kruppel样因子15(KLF15)和核因子-Kappab(NF-Kappa B)的mRNA表达水平。已经观察到L-HCQ + ART和H-HCQ改善了LN诱导的体重减轻,并且显着降低了抗双链DNA,抗核抗体,免疫球蛋白G,干扰素γ,肿瘤坏死因子-α和转化水平与模型组相比,生长因子-β1,以及改善肾脏和脾脏病理学。此外,L-HCQ +技术和H-HCQ治疗诱导KLF15上调和NF-Kappa B下调。这些结果表明,通过调节细胞因子,KLF15和NF-Kappa B的表达水平,用L-HCQ +艺术治疗施加了一次保护作用。这种组合治疗可能具有与PDS和H-HCQ相似的免疫抑制作用,并且可能是有希望的替代方法治疗。

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    Guangzhou Univ Chinese Med Dept Pharmacol Coll Chinese Mat Med 232 East Ring Rd Guangzhou;

    Guangzhou Univ Chinese Med Dept Pharmacol Coll Chinese Mat Med 232 East Ring Rd Guangzhou;

    Guangzhou Univ Chinese Med Dept Pharmacol Coll Chinese Mat Med 232 East Ring Rd Guangzhou;

    Guangzhou Univ Chinese Med Dept Pharmacol Coll Chinese Mat Med 232 East Ring Rd Guangzhou;

    Guangzhou Univ Chinese Med Dept Pharmacol Coll Chinese Mat Med 232 East Ring Rd Guangzhou;

    Guangzhou Univ Chinese Med Sci &

    Technol Ind Pk 436 Chen Tai Rd Guangzhou 510445 Guangdong;

    Artepharm Co Ltd Guangzhou 510032 Guangdong Peoples R China;

    Guangzhou Univ Chinese Med Dept Pharmacol Coll Chinese Mat Med 232 East Ring Rd Guangzhou;

    Guangzhou Univ Chinese Med Dept Pharmacol Coll Chinese Mat Med 232 East Ring Rd Guangzhou;

    Guangzhou Univ Chinese Med Dept Pharmacol Coll Chinese Mat Med 232 East Ring Rd Guangzhou;

    Guangzhou Univ Chinese Med Sci &

    Technol Ind Pk 436 Chen Tai Rd Guangzhou 510445 Guangdong;

    Guangzhou Univ Chinese Med Dept Pharmacol Coll Chinese Mat Med 232 East Ring Rd Guangzhou;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 治疗学;
  • 关键词

    immunosuppressive effect; artemisinin; hydroxychloroquine; lupus nephritis;

    机译:免疫抑制作用;青蒿素;羟基氯喹;狼疮肾炎;

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