In vitro and in vivo toxicity and histopathological evaluation of Gd(III)anionic Linear globular dendrimer second-generation G2-C595 nanoprobe

Mehdi Mirzaei; Mohammad Esmaeil Akbari; Mohammad Ali Mohagheghi; Seyed Mohammad Tavangar; Bita Mehravi; Mehdi Shafiee Ardestani

摘要

Objective(s): Toxico-histopathological studies are used to assess the toxic impacts of nanoparticles in organism exposure. The present study aimed to evaluate the prospective nano-cytotoxicity impacts of Gd(III)-anionic linear globular dendrimer second-generation G2-C595 (Gd[III] dendrimer G2-C595) contrast nanoprobe in terms of the exposure of many nude mice organs and organisms. In addition, we assessed the potential of the Gd(III)-dendrimer G2-C595 nanoprobe as a novel magnetic resonance imaging (MRI) nano-contrast agent for the human breast cancer cell line (MCF-7) and human embryonic kidney cell line (HEK-293).Materials and Methods: Gadolinium (Gd[III]) was loaded with dendrimer G2 and conjugated with the C595 monoclonal antibody to generate the Gd(III)-dendrimer G2-C595 to determine the impact on MUC1 beneficial cancer tumors. The cytotoxic effects of the Gd(III)-dendrimer G2-C595 nanoprobe on the HEK-293 cells were also investigated in-vitro and in-vivo. In addition, the Gd(III)-dendrimer G2-C595 nanoprobe was used on nude mice bearing the MCF-7 tumors to explore its specific activity against the in-vivo model of cancer.Results: The Gd(III)-dendrimer G2-C595 contrast nanoprobes affected the cytotoxicity of MCF-7, and no in-vivo toxicity was induced in the HEK-293 cells, kidneys, heart, lungs, brain, liver tissues, and other organs.Conclusion: According to the results, the Gd(III)-dendrimer G2 and Gd(III)-dendrimer G2-C595 induced no toxicity in the HEK-293 cells and heart, liver, and brain tissues of mice. In addition, the Gd(III)-dendrimer G2-C595 showed specific anti-action against the in-vivo tumor model. Therefore, the Gd(III)-dendrimer G2-C595 nanoprobe is highly recommended as a novel and effective MR contrast agent and antitumor carrier agent. Furthermore, the Gd(III)-dendrimer G2-C595 nano-sized probes demonstrated excellent biocompatibility and safety with no impact on normal organ functioning.

机译：目的：毒性组织病理学研究用于评估纳米颗粒在生物体暴露中的毒性冲击。本研究旨在评估GD（III）的前瞻性纳米细胞毒性影响 - 在许多裸鼠器官的暴露方面，对比纳米骨（GD [III]树枝状细胞G2-C595）对比纳米孔的前瞻性纳米细胞毒性影响和生物。此外，我们评估了GD（III）-Dendrimer G2-C595纳米骨孔的电位作为人乳腺癌细胞系（MCF-7）和人胚胎肾细胞系的新型磁共振成像（MRI）纳米造影剂（HEK-293）。材料和方法：用树枝状聚合物G2加载钆（GD [III]）并与C595单克隆抗体缀合，以产生GD（III）-Dendrimer G2-C595，以确定对MUC1有益癌症肿瘤的影响。还在体外和体内研究了GD（III）-Dendrimer G2-C595纳米骨孔对HEK-293细胞的细胞毒性作用。此外，Gd（III）-dendrimer G2-C595纳米骨瓣用于携带MCF-7肿瘤的裸鼠，以探讨其针对体内癌症模型的特异性活动。结果：GD（III）-Dendimer G2- C595对比度纳米素影响MCF-7的细胞毒性，在HEK-293细胞，肾脏，心脏，肺，脑，肝组织和其他器官中没有诱导体内毒性。结论：根据结果，GD （iii） - 丁二烯来G2和Gd（III）-dendrimer G2-C595在HEK-293细胞和心脏，肝脏和小鼠的脑组织中诱导毒性。此外，GD（III）-Dendrimer G2-C595对体内肿瘤模型表现出特异性的抗动作。因此，强烈建议使用GD（III）-DendRimer G2-C595纳米骨虫作为新颖的和有效的MR造影剂和抗肿瘤载体剂。此外，GD（III）-Dendrimer G2-C595纳米大小探针展示了出色的生物相容性和安全性，对正常器官功能没有影响。

In vitro and in vivo toxicity and histopathological evaluation of Gd(III)anionic Linear globular dendrimer second-generation G2-C595 nanoprobe

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