In vivo uptake and cellular distribution of gold nanoshells in a preclinical model of xenografted human renal cancer

IF 2.2 4区 工程技术 Q2 Chemistry
Mariana Pannerec-Varna, Philippe Ratajczak, Guilhem Bousquet, Irmine Ferreira, Christophe Leboeuf, Raphaël Boisgard, Guillaume Gapihan, Jérôme Verine, Bruno Palpant, Emmanuel Bossy, Eric Doris, Joel Poupon, Emmanuel Fort, Anne Janin
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引用次数: 16

Abstract

Large-sized gold nanoparticles, promising imaging and therapeutic tools in human cancer, need long-term studies evaluating tissue bio-distribution in blood, organs and tumor. In a preclinical model of mouse xenografted with human renal cancer, we analysed the bio-distribution of a single dose (160?μg/kg) intravenously injected of poly-ethylene glycol (PEG)ylated gold nanoshells (~150?nm), in blood, normal and tumoral tissues. Using inductively coupled plasma mass spectrometry (ICP-MS), dark field and electron microscopy, we performed a sequential study of nanoshell uptake and distribution in the tumor. We also studied microscopically the organs most sensitive to efficient anticancer drugs to detect a possible long-term toxicity. Gold quantities significantly decreased in blood between early and late time points, whereas they significantly increased in liver and spleen. In addition, gold nanoshells did not induce any tissue damage, such as necrosis, inflammatory infiltrate or fibrosis in mouse liver, spleen, kidney or bone marrow after 6?months. In human renal cancer xenografts, ICP-MS showed an early decrease of gold, with 1-week stability before decrease at Day 15. Dark field microscopy showed gold particles within the vessel lumen 5 to 30?min after nanoshell injection, while 24?h later, gold particle distribution was mainly intracellular. Electron microscopy identified nanoshells within blood vessels at 5 and 30?min, within endothelial cells at 3 and 6?h and within cytoplasms of macrophages in the tumoral tissue after 24?h. In conclusion, no toxicity was observed in mice 6?months after administration of PEGylated gold nanoshells and the distribution kinetics progressed from intravascular flow at 30?min to intratumoral cells 24?h later.

Abstract Image

金纳米壳在异种移植人类肾癌临床前模型中的体内摄取和细胞分布
大尺寸的金纳米颗粒是人类癌症中有前景的成像和治疗工具,需要长期研究来评估血液、器官和肿瘤中的组织生物分布。在人类肾癌异种移植小鼠临床前模型中,我们分析了单剂量(160 μg/kg)静脉注射聚乙二醇(PEG)基化金纳米壳(~150 μ nm)在血液、正常组织和肿瘤组织中的生物分布。利用电感耦合等离子体质谱(ICP-MS)、暗场和电子显微镜,我们对肿瘤中纳米壳的摄取和分布进行了顺序研究。我们还从显微镜下研究了对有效抗癌药物最敏感的器官,以检测可能的长期毒性。早、晚期血中金含量显著降低,肝、脾中金含量显著升高。此外,金纳米壳在6个月后未引起小鼠肝脏、脾脏、肾脏或骨髓的任何组织损伤,如坏死、炎症浸润或纤维化。在人类肾癌异种移植物中,ICP-MS显示早期金含量下降,在第15天下降之前保持1周的稳定性。暗场显微镜显示血管腔内有金颗粒5 ~ 30?注射纳米壳后Min,而24?H后,金颗粒主要分布在细胞内。电子显微镜在5和30?内皮细胞在3和6?H和24 H后肿瘤组织内巨噬细胞胞质内。结论:对小鼠6?在给予聚乙二醇化金纳米壳几个月后,分布动力学从30?最小到瘤内细胞24?h。
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来源期刊
Gold Bulletin
Gold Bulletin 工程技术-材料科学:综合
CiteScore
3.30
自引率
4.50%
发文量
0
审稿时长
3 months
期刊介绍: Gold Bulletin is the premier international peer reviewed journal on the latest science, technology and applications of gold. It includes papers on the latest research advances, state-of-the-art reviews, conference reports, book reviews and highlights of patents and scientific literature. Gold Bulletin does not publish manuscripts covering the snthesis of Gold nanoparticles in the presence of plant extracts or other nature-derived extracts. Gold Bulletin has been published over 40 years as a multidisciplinary journal read by chemists, physicists, engineers, metallurgists, materials scientists, biotechnologists, surface scientists, and nanotechnologists amongst others, both within industry and academia. Gold Bulletin is published in Association with the World Gold Council.
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