首页> 美国卫生研究院文献>International Journal of Molecular Sciences >The Differential Effect of Carbon Dots on Gene Expression and DNA Methylation of Human Embryonic Lung Fibroblasts as a Function of Surface Charge and Dose
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The Differential Effect of Carbon Dots on Gene Expression and DNA Methylation of Human Embryonic Lung Fibroblasts as a Function of Surface Charge and Dose

机译:碳点对人胚肺成纤维细胞基因表达和DNA甲基化的差异作用与表面电荷和剂量的关系

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摘要

This study presents a toxicological evaluation of two types of carbon dots (CD), similar in size (<10 nm) but differing in surface charge. Whole-genome mRNA and miRNA expression (RNAseq), as well as gene-specific DNA methylation changes, were analyzed in human embryonic lung fibroblasts (HEL 12469) after 4 h and 24 h exposure to concentrations of 10 and 50 µg/mL (for positive charged CD; pCD) or 10 and 100 µg/mL (for negative charged CD, nCD). The results showed a distinct response for the tested nanomaterials (NMs). The exposure to pCD induced the expression of a substantially lower number of mRNAs than those to nCD, with few commonly differentially expressed genes between the two CDs. For both CDs, the number of deregulated mRNAs increased with the dose and exposure time. The pathway analysis revealed a deregulation of processes associated with immune response, tumorigenesis and cell cycle regulation, after exposure to pCD. For nCD treatment, pathways relating to cell proliferation, apoptosis, oxidative stress, gene expression, and cycle regulation were detected. The expression of miRNAs followed a similar pattern: more pronounced changes after nCD exposure and few commonly differentially expressed miRNAs between the two CDs. For both CDs the pathway analysis based on miRNA-mRNA interactions, showed a deregulation of cancer-related pathways, immune processes and processes involved in extracellular matrix interactions. DNA methylation was not affected by exposure to any of the two CDs. In summary, although the tested CDs induced distinct responses on the level of mRNA and miRNA expression, pathway analyses revealed a potential common biological impact of both NMs independent of their surface charge.
机译:这项研究对两种类型的碳点(CD)进行了毒理学评估,其大小相似(<10 nm),但表面电荷不同。在暴露于10和50 µg / mL浓度的人胚胎肺成纤维细胞(HEL 12469)中4小时和24小时后,分析了全基因组mRNA和miRNA表达(RNAseq)以及基因特异性DNA甲基化变化。带正电荷的CD; pCD)或10和100 µg / mL(带负电荷的CD,nCD)。结果显示出对测试的纳米材料(NMs)有明显的响应。暴露于pCD所诱导的mRNA表达要比nCD所表达的mRNA少得多,而在两个CD之间几乎没有差异表达的基因。对于两种CD,失控的mRNA的数量均随剂量和暴露时间的增加而增加。通路分析显示,暴露于pCD后,与免疫反应,肿瘤发生和细胞周期调控相关的过程的调控解除。对于nCD治疗,检测到与细胞增殖,凋亡,氧化应激,基因表达和周期调节有关的途径。 miRNA的表达遵循相似的模式:nCD暴露后变化更为明显,而两张CD之间很少有差异表达的miRNA。对于两种CD,基于miRNA-mRNA相互作用的途径分析均显示出与癌症相关的途径,免疫过程和细胞外基质相互作用所涉及的过程的失控。 DNA甲基化不受暴露于两个CD中的任何一个的影响。总之,尽管测试的CD诱导了mRNA和miRNA表达水平的不同反应,但通路分析显示了这两种NM的潜在共同生物学影响,而与它们的表面电荷无关。

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