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Titanium dioxide nanoparticles stimulate sea urchin immune cell phagocytic activity involving TLR/p38 MAPK-mediated signalling pathway

机译:二氧化钛纳米颗粒刺激涉及TLR / p38 MAPK介导的信号通路的海胆免疫细胞吞噬活性

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摘要

Titanium dioxide nanoparticles (TiO2NPs) are one of the most widespread-engineered particles in use for drug delivery, cosmetics, and electronics. However, TiO2NP safety is still an open issue, even for ethical reasons. In this work, we investigated the sea urchin Paracentrotus lividus immune cell model as a proxy to humans, to elucidate a potential pathway that can be involved in the persistent TiO2NP-immune cell interaction in vivo. Morphology, phagocytic ability, changes in activation/inactivation of a few mitogen-activated protein kinases (p38 MAPK, ERK), variations of other key proteins triggering immune response (Toll-like receptor 4-like, Heat shock protein 70, Interleukin-6) and modifications in the expression of related immune response genes were investigated. Our findings indicate that TiO2NPs influence the signal transduction downstream targets of p38 MAPK without eliciting an inflammatory response or other harmful effects on biological functions. We strongly recommend sea urchin immune cells as a new powerful model for nano-safetyano-toxicity investigations without the ethical normative issue.
机译:二氧化钛纳米颗粒(TiO2NPs)是用于药物输送,化妆品和电子产品的最广泛设计的颗粒之一。但是,即使出于道德原因,TiO2NP的安全性仍然是一个未解决的问题。在这项工作中,我们调查了海胆Paracentrotus lividus免疫细胞模型作为人类的代理,以阐明可能与体内持久的TiO2NP-免疫细胞相互作用有关的潜在途径。形态,吞噬能力,​​一些促分裂原活化蛋白激酶(p38 MAPK,ERK)的激活/失活变化,触发免疫应答的其他关键蛋白的变异(Toll样受体4样,热休克蛋白70,白介素6 )和相关免疫反应基因表达的修饰进行了研究。我们的发现表明,TiO2NPs可影响p38 MAPK下游信号转导靶标,而不会引起炎症反应或对生物学功能的其他有害作用。我们强烈建议将海胆免疫细胞作为纳米安全/纳米毒性研究的新功能强大模型,而无需遵循道德规范问题。

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