又小又危险?常见接触颗粒和纳米颗粒的潜在毒性机制

IF 4.6
Rachel E. Hewitt , Helen F. Chappell , Jonathan J. Powell
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引用次数: 20

摘要

我们通过皮肤、口腔和吸入途径不断接触到大量的非生物性、持久性微粒。在细胞相互作用的完美尺寸下,这种现代颗粒暴露要么是有意的(例如添加剂/赋形剂),要么是无意的(例如污染)。口服或皮肤接触普通颗粒是否有显著的不良影响尚不清楚。然而,发病率或死亡率增加与空气中颗粒暴露之间的关系已得到充分证实。大的纳米颗粒和微粒吸附环境分子,包括抗原和过敏原,并将它们输送到细胞中,可能具有辅助作用。较小的纳米颗粒可能具有增强的氧化还原活性,因为增加的表面积或带隙效应。在某些情况下,超小纳米颗粒可以连接细胞受体或与其他细胞机制相互作用并驱动不同的细胞信号传导。这些,以及潜在的炎性体激活,被认为是理解或揭穿颗粒毒性的可行途径。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Small and dangerous? Potential toxicity mechanisms of common exposure particles and nanoparticles

We are continuously exposed to large numbers of nonbiological, persistent particulates through dermal, oral and inhalation routes. At sizes perfect for cell interactions, such modern particle exposures are derived from human engineering either purposefully (e.g. additives/excipients) or inadvertently (e.g. pollution). Whether oral or dermal exposure to common particles has significant adverse effects is not yet known. However, relationships between increased morbidity or mortality and airborne particle exposure are well established. Large nanoparticles and microparticles adsorb environmental molecules, including antigens and allergens, and deliver them to cells potentially with an adjuvant effect. Smaller nanoparticles may have enhanced redox activity because of increased surface areas or band gap effects. Under some circumstances, ultrasmall nanoparticles can ligate cellular receptors or interact with other cell machinery and drive distinct cell signalling. These, as well as the potential for inflammasome activation, are discussed as feasible pathways to understanding or debunking particle toxicity.

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来源期刊
Current opinion in toxicology
Current opinion in toxicology Toxicology, Biochemistry
CiteScore
8.50
自引率
0.00%
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审稿时长
64 days
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