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The effect of PEG functionalization on the in vivo behavior and toxicity of CdTe quantum dots

机译:PEG官能化对CDTE量子点体内行为和毒性的影响

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摘要

CdTe quantum dots (QDs) are considered a potential toxic substance because they contain metal ions. However, most toxicology data are derived from in vitro studies or limited in vivo analysis and may not reflect in vivo responses and biodistribution. Proper modification is one of the most widely used routes to reduce the toxicity of QDs. Herein, we demonstrated the role of polyethylene glycol (PEG) in decreasing the toxicity of QDs by studying the animal survival, clinical biochemistry, organ histology, biodistribution and oxidative stress in thioglycolic acid (TGA)- and mercapto-acetohydrazide (TGH)-stabilized CdTe QD (TGA/TGH-CdTe QD)-treated groups. Via the histology, transmission electron microscopy (TEM) and biodistribution results, it was found that the QDs mainly accumulated in the liver and kidney at 7 days post-injection, and obvious tissue damage was also observed in the bare TGA/TGH-CdTe QD group. Based on the evaluation of oxidative stress in the liver and kidney, the indicators exhibited an obvious variation with a high dose of TGA/TGH-CdTe QDs. In contrast, the QD aggregation decreased in the liver and kidney with no clear physiological index variation after PEG functionalization. Thus, PEG plays an important role in decreasing the toxicity of the CdTe QDs, and both the accumulation of cadmium and oxidative stress variation instead of an isolation factor are responsible for the in vivo toxicity of these QDs.
机译:CdTe量子点(QDS)被认为是潜在的有毒物质,因为它们含有金属离子。然而,大多数毒理学数据来自体外研究或体内分析有限,可能不反映体内反应和生物分布。适当的修改是降低QDS毒性最广泛使用的路线之一。在此,我们证明了聚乙二醇(PEG)通过研究动物存活,临床生物化学,器官组织学,生物分布和氧化胁迫在巯基乙酸(TGA) - 和丙酰酰肼(TGH)(TGH) - 氧化(TGH) - 氧化术中降低QDS毒性的作用CdTe QD(TGA / TGH-CDTE QD) - 治疗组。通过组织学,透射电子显微镜(TEM)和生物分布结果,发现QDS在注射后7天主要积累在肝肾和肾脏中,并且在裸机/ TGH-CDTE QD中也观察到明显的组织损伤团体。基于肝肾中氧化应激的评价,该指标表现出具有高剂量TGA / TGH-CDTE QD的明显变化。相反,肝脏和肾的QD聚集在PEG官能化后没有明确的生理指标变化。因此,PEG在降低CDTE QD的毒性方面发挥着重要作用,并且镉的积累和氧化应激变化而不是分离因子的累积对这些QD的体内毒性负责。

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  • 来源
    《RSC Advances 》 |2019年第22期| 共8页
  • 作者单位

    Xuzhou Med Univ Jiangsu Key Lab New Drug Res &

    Clin Pharm Xuzhou 221004 Jiangsu Peoples R China;

    Xuzhou Med Univ Jiangsu Key Lab New Drug Res &

    Clin Pharm Xuzhou 221004 Jiangsu Peoples R China;

    Xuzhou Med Univ Jiangsu Key Lab New Drug Res &

    Clin Pharm Xuzhou 221004 Jiangsu Peoples R China;

    Xuzhou Med Univ Jiangsu Key Lab New Drug Res &

    Clin Pharm Xuzhou 221004 Jiangsu Peoples R China;

    Xuzhou Air Force Coll Xuzhou 221000 Jiangsu Peoples R China;

    Xuzhou Canc Hosp Xuzhou 221000 Jiangsu Peoples R China;

    Xuzhou Med Univ Jiangsu Key Lab New Drug Res &

    Clin Pharm Xuzhou 221004 Jiangsu Peoples R China;

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  • 正文语种 eng
  • 中图分类 化学 ;
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