首页> 外文期刊>Acta Radiologica >Effects of gadolinium contrast agents in naive and nephrectomized rats: relevance to nephrogenic systemic fibrosis.
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Effects of gadolinium contrast agents in naive and nephrectomized rats: relevance to nephrogenic systemic fibrosis.

机译:contrast对比剂在未治疗和肾切除的大鼠中的作用:与肾源性系统性纤维化的相关性。

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BACKGROUND: Human nephrogenic systemic fibrosis (NSF) is a rare condition reported in patients with severe renal insufficiency exposed to a gadolinium (Gd)-based contrast agent. An animal model of NSF could help to investigate its mechanisms and lead to prevention and treatment. PURPOSE: To evaluate a possible animal model of NSF using naive and partially nephrectomized rats to induce conditions similar to those in patients at risk of NSF. MATERIAL AND METHODS: Naive rats received intravenous doses of 5 or 10 mmol/kg Omniscan; 5 mmol/kg Magnevist; 1 mmol/kg caldiamide; 1, 2.5, or 5 mmol/kg gadodiamide; 25 micromol/kg GdCl(3); or 25 micromol/kg Gd citrate. Partially nephrectomized rats received 5 mmol/kg Omniscan; 5 mmol/kg Magnevist; 1 mmol/kg caldiamide; 1 mmol/kg gadodiamide; 25 micromol/kg GdCl(3); or 25 micromol/kg Gd citrate. There were three or four animals per group. Clinical signs were recorded during treatment. At termination, clinical biochemistry, histopathology, and tissue Gd and Zn concentrations were investigated. RESULTS: Similar responses to treatment were seen in naive and nephrectomized rats. High doses of gadodiamide were toxic, necessitating early termination of the affected animals. Skin lesions appeared in naive and nephrectomized groups treated with gadodiamide or Omniscan, coinciding with the onset of signs of pruritus, i.e., intensive scratching. The histomorphological features of the skin lesions were also consistent with superficial physical trauma. Dermal fibrosis was not a feature of these skin lesions in any of the groups, i.e., no increased collagen density, CD34+ cells, or increased fibroblasts. This was supported by skinfold measurements that demonstrated no increased skin thickness. Treatment with the gadolinium-based contrast agents and Gd salts resulted in increased Gd content of several tissues. The Gd salts were mainly taken up by the liver and spleen, possibly reflecting formation of insoluble particles and macrophage uptake. Zn tissue concentrations were normal or increased. Other major treatment-related changes included increased serum rat C-reactive protein and histamine; mineralization affecting the dermis, stomach, and blood vessels; and renal proximal tubule vacuolation. CONCLUSION: The visible skin lesions seen in this study appeared to be caused by excessive scratching in response to pruritus. As there was no evidence of dermal fibrosis, the cardinal feature of human NSF, this did not appear to be a model of human NSF.
机译:背景:人类肾源性系统性纤维化(NSF)是一种严重的肾功能不全患者,使用to(Gd)造影剂暴露后的罕见病。 NSF的动物模型可以帮助研究其机制并导致预防和治疗。目的:使用未成熟的和部分经肾切除的大鼠诱发与患有NSF风险的患者相似的疾病,以评估可能的NSF动物模型。材料与方法:幼稚大鼠接受5或10 mmol / kg Omniscan的静脉内剂量。 5 mmol / kg Magnevist; 1 mmol / kg乙二酰胺; 1、2.5或5 mmol / kg加多二酰胺; 25 micromol / kg GdCl(3);或25 micromol / kg柠檬酸Gd。部分肾切除的大鼠接受5 mmol / kg Omniscan; 5 mmol / kg Magnevist; 1 mmol / kg乙二酰胺; 1 mmol / kg加二酰胺; 25 micromol / kg GdCl(3);或25 micromol / kg柠檬酸Gd。每组有三到四只动物。治疗期间记​​录临床症状。终止时,研究了临床生物化学,组织病理学和组织中Gd和Zn的浓度。结果:在幼稚和肾切除的大鼠中也观察到类似的治疗反应。高剂量的gadodiamide有毒,必须尽早终止患病动物。皮肤病变出现在接受过加多巴胺或Omniscan治疗的幼稚和肾切除组中,与瘙痒的迹象即剧烈抓挠相吻合。皮肤病变的组织形态学特征也与浅表身体创伤一致。在任何一组中,皮肤纤维化都不是这些皮肤损伤的特征,即胶原密度,CD34 +细胞或成纤维细胞没有增加。这通过皮褶测量得到支持,该皮褶测量没有显示出皮肤厚度增加。用based基造影剂和Gd盐进行治疗会导致一些组织的Gd含量增加。 Gd盐主要被肝脏和脾脏吸收,可能反映了不溶性颗粒的形成和巨噬细胞的摄取。锌组织浓度正常或升高。其他与治疗有关的主要变化包括血清大鼠C反应蛋白和组胺的增加。矿化影响真皮,胃和血管;和肾近端小管空泡化。结论:本研究中可见的皮肤损伤似乎是由于瘙痒引起的过度抓挠引起的。由于没有证据表明真皮纤维化是人类NSF的主要特征,因此这似乎不是人类NSF的模型。

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