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首页> 外文期刊>Journal of Pharmacological and Toxicological Methods >Nanoparticle contrast-enhanced micro-CT: A preclinical tool for the 3D imaging of liver and spleen in longitudinal mouse studies
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Nanoparticle contrast-enhanced micro-CT: A preclinical tool for the 3D imaging of liver and spleen in longitudinal mouse studies

机译:纳米粒子对比增强微型CT:纵向小鼠研究中肝脏和脾脏3D成像的临床前工具

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In drug discovery and development, X-ray micro-computed tomography (micro-CT) has gained increasing importance over the past decades. In recent years, micro-CT imaging of soft tissues has become popular due to the introduction of a variety of radiopaque contrast agents. More recently, nanoparticle-based ExiTron nano 12,000 has become commercially available for the nonclinical micro-CT imaging of soft tissues in rodents. Phagocytosis and accumulation of the contrast agent by Kupffer cells in the liver, as well as macrophages in the spleen, increase the soft tissue X-ray attenuation for up to 6 months. Therefore, it is essential to understand the potential toxicity of this nanomaterial in micro-CT imaging prior to its application in pharmacology and/or toxicology studies. Herein, we describe the time-course and distribution of the contrast in the liver, spleen and blood after a single intravenous injection (IV) of this nanoparticle contrast agent at 0.1 ml/mouse. Thoracic images of male adult C57BL/6 mice were acquired using a Bruker SkyScan 1276 micro-CT over a period of 29 days. The stability of X-ray attenuation enhancement in the above tissues was also tested after a single dose of Kupffer cell toxicant gadolinium chloride (GdCl3) at 15 mg/kg on day 2. The liver, spleen and kidney were examined microscopically on days 15 and 29 post treatment. Serum and liver cytokines (IL-1 beta, IL-2, IL-6, IL-10, IL-12p70, IFN-., IP-10, MIP1-alpha, MIP1-beta and TNF-alpha) were quantified on days 15 and 29 as indicators of a pro-inflammatory response to treatment. This study determined that there was an accumulation of amphophilic granular material in the cells of the mononuclear phagocyte system in the liver and spleen following a single dose of ExiTron nano 12,000 and a second dose of GdCl3 or its vehicle. However, ExiTron nano12000 contrast administration did not cause any hepatotoxicity in the liver, nor did pro-inflammatory cytokines release in the liver or serum. Similarly, there were no adverse pathologies in the spleen or kidneys. In summary, ExiTron nano12000 contrast agent-enhanced micro-CT could be used as a safe method in up to 29-day longitudinal efficacy and toxicology mouse studies for the non-invasive assessment of the liver and spleen.
机译:在药物发现和发展中,X射线微计算机断层扫描(Micro-CT)在过去几十年中获得了越来越重要的。近年来,由于引入各种无线电话造影剂,软组织的微型CT成像变得很受欢迎。最近,基于纳米粒子的抗剥离纳米12,000已商购获得啮齿动物软组织的非临床微型CT成像。在肝脏中Kupffer细胞的吞噬和积聚造影剂,以及脾脏中的巨噬细胞,增加了长达6个月的软组织X射线衰减。因此,在其在药理学和/或毒理学研究中应用之前,必须了解该纳米材料中该纳米材料的潜在毒性。在此,我们描述了在该纳米颗粒造影剂的单个静脉注射剂(IV)下在0.1ml /小鼠的静脉内注射剂(iv)之后的肝脏,脾和血液中的对比度的时间过程和分布。使用Bruker Skyscan 1276 Micro-CT在29天内获得雄性成年C57BL / 6小鼠的胸部图像。在第2天在15mg / kg的单一剂量Kupffer细胞毒物氯化钆(Gdcl3)之后还测试了上述组织中X射线衰减增强的稳定性。在第15天和第15天和治疗后29个。血清和肝细胞因子(IL-1β,IL-2,IL-6,IL-10,IL-12P70,IFN-,IP-10,MIP1-α,MIP1-Beta和TNF-alpha)在几天内量化15和29作为对治疗的促炎症反应的指标。该研究确定,在单一剂量的抗硝酸纳米12,000和第二剂量的GdCl3或其载体中,在肝脏和脾脏中,在肝脏和脾脏中,在单核吞噬细胞系统的细胞中积累了含有的含累含累的细胞和脾脏。然而,Exitron NaNO12000对比度给药在肝脏中没有引起任何肝毒性,也不是肝脏或血清中的促炎细胞因子释放。同样,脾脏或肾脏中没有不利的病理学。总之,Exitron Nano12000造影剂增强的微型CT可用作最多29天的纵向疗效和毒理学小鼠研究的安全方法,用于肝脏和脾脏的非侵入性评估。

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