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基于镉/硒/碲的量子点705在生物系统中的化学归宿:毒性影响。

The chemical fate of the Cd/Se/Te-based quantum dot 705 in the biological system: toxicity implications.

作者信息

Lin Chia-Hua, Chang Louis W, Chang Han, Yang Mo-Hsiung, Yang Chung-Shi, Lai Wan-Hau, Chang Wan-Hsuan, Lin Pinpin

机构信息

Division of Environmental Health and Occupational Medicine, National Health Research Institutes, Zhunan, Taiwan.

出版信息

Nanotechnology. 2009 May 27;20(21):215101. doi: 10.1088/0957-4484/20/21/215101. Epub 2009 May 5.

Abstract

QD705 is a cadmium/selenium/tellurium (Cd/Se/Te)-based quantum dot with good potential for biomedical applications. Although the biological fate of QD705 is established, its chemical fate in the biological system is still unknown. Since the chemical nature of Cd in QD705 (either stays as bounded Cd or becomes free Cd) is closely related to the toxicity of this nanocrystal, information on its chemical fate is critically needed. In this study we investigated the chemical fate of QD705 in the kidneys of mice. We used the molar ratio of Cd and Te (increased Cd/Te ratio signifies increased Cd release from QD705) and the induction of tissue metallothionein (MT) as markers for elevated free Cd in tissues. Our study indicated that 100% of QD705 (measured as Cd) was still retained in the body 16 weeks after exposure, with significant time redistribution to the kidneys. Furthermore, there were an elevation in both the molar Cd/Te ratio and MT-1 expression in the kidneys, suggesting that free Cd was released from QD705. Thus QD705 is not as stable or biologically inert as many may have once believed. Our study demonstrated that free Cd indeed can be released from QD705 in the kidneys and increases the risk of renal toxicity.

摘要

QD705是一种基于镉/硒/碲(Cd/Se/Te)的量子点,在生物医学应用方面具有良好的潜力。尽管QD705的生物归宿已明确,但其在生物系统中的化学归宿仍不清楚。由于QD705中镉的化学性质(要么以结合态镉存在,要么变成游离镉)与这种纳米晶体的毒性密切相关,因此迫切需要有关其化学归宿的信息。在本研究中,我们调查了QD705在小鼠肾脏中的化学归宿。我们使用镉与碲的摩尔比(镉/碲比值增加表明从QD705释放的镉增加)以及组织金属硫蛋白(MT)的诱导作为组织中游离镉升高的标志物。我们的研究表明,暴露16周后,100%的QD705(以镉计)仍保留在体内,且有明显的时间依赖性重新分布至肾脏。此外,肾脏中的镉/碲摩尔比和MT-1表达均升高,表明有游离镉从QD705释放出来。因此,QD705并不像许多人曾经认为的那样稳定或具有生物惰性。我们的研究表明,游离镉确实可以从肾脏中的QD705释放出来,并增加肾毒性风险。

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