Gene expression profiles and protein-protein interaction networks in THP-1 cells exposed to metal-based nanomaterials.

Šíma Michal, Líbalová Helena, Závodná Táňa, Vrbová Kristýna, Kléma Jiří, Rössner Pavel
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Abstract

We analyzed gene expression in THP-1 cells exposed to metal-based nanomaterials (NMs) [TiO2 (NM-100), ZnO (NM-110), SiO2 (NM-200), Ag (NM-300 K)]. A functional enrichment analysis of the significant differentially expressed genes (DEGs) identified the key modulated biological processes and pathways. DEGs were used to construct protein-protein interaction networks. NM-110 and NM-300 K induced changes in the expression of genes involved in oxidative and genotoxic stress, immune response, alterations of cell cycle, detoxification of metal ions and regulation of redox-sensitive pathways. Both NMs shared a number of highly connected protein nodes (hubs) including CXCL8, ATF3, HMOX1, and IL1B. NM-200 induced limited transcriptional changes, mostly related to the immune response; however, several hubs (CXCL8, ATF3) were identical with NM-110 and NM-300 K. No effects of NM-100 were observed. Overall, soluble nanomaterials NM-110 and NM-300 K exerted a wide variety of toxic effects, while insoluble NM-200 induced immunotoxicity; NM-100 caused no detectable changes on the gene expression level.

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暴露于金属基纳米材料的 THP-1 细胞的基因表达谱和蛋白质相互作用网络。
我们分析了暴露于金属基纳米材料(NMs)[TiO2(NM-100)、ZnO(NM-110)、SiO2(NM-200)、Ag(NM-300 K)]的 THP-1 细胞的基因表达。对显著差异表达基因(DEGs)的功能富集分析确定了关键的调节生物过程和途径。DEGs 被用于构建蛋白质-蛋白质相互作用网络。NM-110 和 NM-300 K 诱导了涉及氧化和基因毒性应激、免疫反应、细胞周期改变、金属离子解毒和氧化还原敏感通路调控的基因表达变化。两种 NMs 都共享一些高度连接的蛋白质节点(枢纽),包括 CXCL8、ATF3、HMOX1 和 IL1B。NM-200 诱导了有限的转录变化,主要与免疫反应有关;然而,几个枢纽(CXCL8、ATF3)与 NM-110 和 NM-300 K 相同。总之,可溶性纳米材料 NM-110 和 NM-300 K 产生了多种毒性效应,而不溶性纳米材料 NM-200 引发了免疫毒性;NM-100 在基因表达水平上没有引起可检测到的变化。
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