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首页> 外文期刊>Journal of pharmacological sciences. >Contrasting dose-effects of multi-glycoside of Tripterygium wilfordii HOOK. f. on glomerular inflammation and hepatic damage in two types of anti-Thy1.1 glomerulonephritis.
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Contrasting dose-effects of multi-glycoside of Tripterygium wilfordii HOOK. f. on glomerular inflammation and hepatic damage in two types of anti-Thy1.1 glomerulonephritis.

机译:雷公藤多甙甙的对比剂量效应F。对肾小球炎症和肝损害有两种抗Thy1.1肾小球肾炎的作用。

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摘要

Multi-glycoside, one of the extracted compounds from Tripterygium wilfordii HOOK. f. (GTW), has been shown to be clinically effective in suppressing glomerular inflammation in chronic kidney disease. However, its clinical application is often limited by its cytotoxic actions on the liver. This study was performed to contrast the dose-effects of GTW on glomerular inflammation and hepatic damage in two types of anti-Thy1.1 glomerulonephritis (GN). Rats with acute or chronic anti-Thy1.1 GN were either left untreated (the Vehicle group) or treated with a high or low dose of GTW and sacrificed on day 7 or day 45. GTW was administrated 3 days before or at the same time as the antibody injection and lasted until sacrifice. GTW at high dose ameliorated glomerular macrophage accumulation, mesangial proliferation, proteinuria, and interleukin-2 expression in the acute anti-Thy1.1 GN model, but caused structural and functional lesions in the liver. In contrast, GTW at low dose improved activated macrophage and T lymphocyte infiltration, mesangial injury, proteinuria, and interleukin-2 and interferon-γ expressions without hepatic toxicity in the chronic model of GN induced by anti-Thy1.1 antibody. In conclusion, GTW at low dose not only effectively inhibits glomerular inflammation but also avoids severe injuries to the liver.
机译:多糖苷,雷公藤提取物之一。 F。 (GTW)已被证明可有效抑制慢性肾脏疾病中的肾小球炎症。但是,其临床应用通常受到其对肝脏的细胞毒性作用的限制。进行这项研究的目的是为了对比GTW对两种类型的抗Thy1.1肾小球肾炎(GN)的肾小球炎症和肝损伤的剂量效应。患有急性或慢性抗Thy1.1 GN的大鼠(未经治疗)(媒介物组)或接受高剂量或低剂量的GTW治疗,并在第7天或第45天处死。将GTW于3天前或同时给药作为抗体注射,并持续至牺牲。高剂量的GTW在急性抗Thy1.1 GN模型中改善了肾小球巨噬细胞的积累,肾小球膜增生,蛋白尿和白介素2的表达,但在肝脏引起结构和功能性损害。相反,在抗Thy1.1抗体诱导的GN慢性模型中,低剂量的GTW改善了活化的巨噬细胞和T淋巴细胞浸润,肾小球膜损害,蛋白尿以及白介素2和干扰素γ的表达而无肝毒性。总之,低剂量的GTW不仅可以有效抑制肾小球炎症,而且还可以避免对肝脏的严重伤害。

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