Multiparametric in vitro genotoxicity assessment of different variants of amorphous silica nanomaterials in rat alveolar epithelial cells.

IF 3.6 3区 医学 Q3 NANOSCIENCE & NANOTECHNOLOGY
Nanotoxicology Pub Date : 2023-08-01 Epub Date: 2023-12-01 DOI:10.1080/17435390.2023.2265481
Fátima Brandão, Carla Costa, Maria João Bessa, Vanessa Valdiglesias, Bryan Hellack, Andrea Haase, Sónia Fraga, João Paulo Teixeira
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引用次数: 0

Abstract

The hazard posed to human health by inhaled amorphous silica nanomaterials (aSiO2 NM) remains uncertain. Herein, we assessed the cyto- and genotoxicity of aSiO2 NM variants covering different sizes (7, 15, and 40 nm) and surface modifications (unmodified, phosphonate-, amino- and trimethylsilyl-modified) on rat alveolar epithelial (RLE-6TN) cells. Cytotoxicity was evaluated at 24 h after exposure to the aSiO2 NM variants by the lactate dehydrogenase (LDH) release and WST-1 reduction assays, while genotoxicity was assessed using different endpoints: DNA damage (single- and double-strand breaks [SSB and DSB]) by the comet assay for all aSiO2 NM variants; cell cycle progression and γ-H2AX levels (DSB) by flow cytometry for those variants that presented higher cytotoxic and DNA damaging potential. The variants with higher surface area demonstrated a higher cytotoxic potential (SiO2_7, SiO2_15_Unmod, SiO2_15_Amino, and SiO2_15_Phospho). SiO2_40 was the only variant that induced significant DNA damage on RLE-6TN cells. On the other hand, all tested variants (SiO2_7, SiO2_15_Unmod, SiO2_15_Amino, and SiO2_40) significantly increased total γ-H2AX levels. At high concentrations (28 µg/cm2), a decrease in G0/G1 subpopulation was accompanied by a significant increase in S and G2/M sub-populations after exposure to all tested materials except for SiO2_40 which did not affect cell cycle progression. Based on the obtained data, the tested variants can be ranked for its genotoxic DNA damage potential as follows: SiO2_7 = SiO2_40 = SiO2_15_Unmod > SiO2_15_Amino. Our study supports the usefulness of multiparametric approaches to improve the understanding on NM mechanisms of action and hazard prediction.

无定形二氧化硅纳米材料在大鼠肺泡上皮细胞中不同变体的多参数体外遗传毒性评估。
吸入的无定形二氧化硅纳米材料(aSiO2-NM)对人类健康造成的危害仍不确定。在此,我们评估了覆盖不同大小(7、15和40)的aSiO2-NM变体的细胞和遗传毒性 nm)和对大鼠肺泡上皮(RLE-6TN)细胞的表面修饰(未修饰的、膦酸、氨基和三甲基甲硅烷基修饰的)。24时评估细胞毒性 通过乳酸脱氢酶(LDH)释放和WST-1还原试验暴露于aSiO2-NM变体后h,同时使用不同的终点评估遗传毒性:通过彗星试验评估所有aSiO2-NM变体的DNA损伤(单链和双链断裂[SSB和DSB]);细胞周期进展和γ-H2AX水平(DSB)。具有较高表面积的变体表现出较高的细胞毒性潜力(SiO2_7、SiO2_15_Unmod、SiO2_15-Amino和SiO2_15_Phospho)。SiO2_ 40是唯一能诱导RLE-6TN细胞DNA损伤的变体。另一方面,所有测试的变体(SiO2_7、SiO2_15_Unmod、SiO2_15-Amino和SiO2_40)都显著增加了总γ-H2AX水平。在高浓度(28µg/cm2)下,暴露于除SiO2_40外的所有测试材料后,G0/G1亚群的减少伴随着S和G2/M亚群的显著增加,SiO2_40不影响细胞周期进展。根据获得的数据,测试的变体可以根据其基因毒性DNA损伤潜力进行如下排序:SiO2_7 = SiO2_40 = SiO2_15_Unmod > SiO2_ 15_氨基。我们的研究支持多参数方法的有用性,以提高对NM作用机制和危害预测的理解。
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来源期刊
Nanotoxicology
Nanotoxicology 医学-毒理学
CiteScore
10.10
自引率
4.00%
发文量
45
审稿时长
3.5 months
期刊介绍: Nanotoxicology invites contributions addressing research relating to the potential for human and environmental exposure, hazard and risk associated with the use and development of nano-structured materials. In this context, the term nano-structured materials has a broad definition, including ‘materials with at least one dimension in the nanometer size range’. These nanomaterials range from nanoparticles and nanomedicines, to nano-surfaces of larger materials and composite materials. The range of nanomaterials in use and under development is extremely diverse, so this journal includes a range of materials generated for purposeful delivery into the body (food, medicines, diagnostics and prosthetics), to consumer products (e.g. paints, cosmetics, electronics and clothing), and particles designed for environmental applications (e.g. remediation). It is the nano-size range if these materials which unifies them and defines the scope of Nanotoxicology . While the term ‘toxicology’ indicates risk, the journal Nanotoxicology also aims to encompass studies that enhance safety during the production, use and disposal of nanomaterials. Well-controlled studies demonstrating a lack of exposure, hazard or risk associated with nanomaterials, or studies aiming to improve biocompatibility are welcomed and encouraged, as such studies will lead to an advancement of nanotechnology. Furthermore, many nanoparticles are developed with the intention to improve human health (e.g. antimicrobial agents), and again, such articles are encouraged. In order to promote quality, Nanotoxicology will prioritise publications that have demonstrated characterisation of the nanomaterials investigated.
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