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Pyrogenic and Precipitated Amorphous Silica Nanoparticles Differentially Affect Cell Responses to LPS in Human Macrophages

机译:热源和沉淀的无定形二氧化硅纳米粒子差异地影响人巨噬细胞中对LPS的细胞反应

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摘要

Previous work has demonstrated that precipitated (NM-200) and pyrogenic (NM-203) Amorphous Silica Nanoparticles (ASNPs) elicit the inflammatory activation of murine macrophages, with more pronounced effects observed with NM-203. Here, we compare the effects of low doses of NM-200 and NM-203 on human macrophage-like THP-1 cells, assessing how the pre-exposure to these nanomaterials affects the cell response to lipopolysaccharide (LPS). Cell viability was affected by NM-203, but not by NM-200, and only in the presence of LPS. While NM-203 stimulated mTORC1, neither ASNPs activated NFκB or the transcription of its target genes and NM-200 and NM-203 caused a block of the autophagic flux and inhibited the LPS-dependent increase of Glutamine Synthetase (GS) expression. Both ASNPs suppressed the activation of caspase-1, delaying the LPS-dependent secretion of IL-1β. Thus, ASNPs modulate several important pathways in human macrophages, altering their response to LPS. NM-203 had larger effects on autophagy, mTORC1 activity and GS expression than NM-200, confirming the higher biological activity of pyrogenic ASNPs when compared with precipitated ASNPs.
机译:以前的工作证明,沉淀(NM-200)和热原(NM-203)非晶二氧化硅纳米颗粒(ASNPS)引发了鼠巨噬细胞的炎症活化,用NM-203观察到更明显的效果。在此,我们将低剂量NM-200和NM-203对人巨噬细胞样THP-1细胞的影响进行比较,评估对这些纳米材料的预接触程度如何影响对脂多糖(LPS)的细胞应答。细胞活力受NM-203的影响,但不是NM-200,并且仅在LPS存在下。虽然NM-203刺激MTORC1,但既不是ASNPS活化的NFκB或其靶基因的转录和NM-200和NM-203导致自噬透气块并抑制谷氨酰胺合成酶(GS)表达的LPS依赖性增加。 ASNPS均抑制了Caspase-1的活化,延迟了IL-1β的LPS依赖性分泌。因此,ASNP调节人巨噬细胞中的几种重要途径,改变它们对LPS的响应。 NM-203对自噬,MTORC1活性和GS表达的效果大于NM-200,与沉淀的AsNP相比,确认热原叶片的较高生物活性。

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