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通过彗星试验和胞质分裂阻滞微核试验评估柠檬酸盐包被的银纳米颗粒对人角质形成细胞的遗传毒性。

Genotoxicity of citrate-coated silver nanoparticles to human keratinocytes assessed by the comet assay and cytokinesis blocked micronucleus assay.

作者信息

Bastos V, Duarte I F, Santos C, Oliveira H

机构信息

CESAM & Laboratory of Biotechnology and Cytomics, Department of Biology, University of Aveiro, 3810-193, Aveiro, Portugal.

CICECO, Aveiro Institute of Materials, Department of Chemistry, University of Aveiro, 3810-193, Aveiro, Portugal.

出版信息

Environ Sci Pollut Res Int. 2017 Feb;24(5):5039-5048. doi: 10.1007/s11356-016-8240-6. Epub 2016 Dec 20.

Abstract

Silver nanoparticles (AgNPs) are widely used in industrial, cosmetic, and biomedical products, and humans are frequently exposed to these products through the skin. It is widely recognized that the characteristics of AgNPs (e.g., size, coating) may influence their cytotoxic effects, but their correlation with DNA damage and mitotic disorders remains poorly explored. In this study, human keratinocytes (HaCaT cell line) were exposed to well-characterized 30 nm AgNPs coated with citrate, and their effects on viability, DNA fragmentation (assessed by the comet assay), and micronuclei (MNi) induction (assessed by the cytokinesis-block micronucleus cytome assays, CBMN) were investigated. The results showed that 10 and 40 μg/mL AgNPs decreased cell proliferation and viability, and induced a significant genetic damage. This was observed by an increase of DNA amount in comet tail, which linearly correlated with dose and time of exposure. Also, cytostaticity (increase of mononucleated cells) and MNi rates increased in treated cells. In contrast, no significant changes were observed in nucleoplasmatic bridges (NPBs) or nuclear buds (NBUDs), although NBUDs tended to increase in all conditions and periods. The cytostatic effects on HaCaT cells were also shown by the decrease of their nuclear division index. Thus, both comet and CBMN assays supported the observation that citrate-AgNPs induced genotoxic effects on HaCaT cells. Considering that AgNPs are present in a vast number of consumer products and also in multiple nanomedicine skin applications and formulations, more research is needed to determine the properties that confer less toxicity of AgNPs to different cell lines.

摘要

银纳米颗粒(AgNPs)广泛应用于工业、化妆品和生物医学产品中,人类经常通过皮肤接触这些产品。人们普遍认识到AgNPs的特性(如尺寸、涂层)可能会影响其细胞毒性作用,但其与DNA损伤和有丝分裂紊乱的相关性仍未得到充分研究。在本研究中,将人角质形成细胞(HaCaT细胞系)暴露于具有良好表征的30 nm柠檬酸盐包被的AgNPs中,研究其对细胞活力、DNA片段化(通过彗星试验评估)和微核(MNi)诱导(通过胞质分裂阻滞微核细胞试验,CBMN评估)的影响。结果表明,10和40 μg/mL的AgNPs降低了细胞增殖和活力,并诱导了显著的遗传损伤。这通过彗星尾中DNA量的增加得以观察到,其与暴露剂量和时间呈线性相关。此外,处理后的细胞中细胞静止性(单核细胞增加)和MNi率增加。相比之下,尽管在所有条件和时间段内核质桥(NPBs)或核芽(NBUDs)均有增加趋势,但未观察到显著变化。HaCaT细胞的核分裂指数降低也显示出其细胞静止作用。因此,彗星试验和CBMN试验均支持柠檬酸盐包被的AgNPs对HaCaT细胞具有遗传毒性作用这一观察结果。鉴于AgNPs存在于大量消费品以及多种纳米医学皮肤应用和制剂中,需要更多研究来确定赋予AgNPs对不同细胞系较低毒性的特性。

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