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两种锐钛矿 TiO2 纳米材料对人肠道和肝脏细胞系的慢性影响。

Chronic effects of two rutile TiO nanomaterials in human intestinal and hepatic cell lines.

机构信息

Toxicology of Contaminants Unit, Fougères Laboratory, ANSES, French Agency for Food, Environmental and Occupational Health & Safety, 10 B rue Claude Bourgelat - Javené, 35306, Fougères, France.

German Federal Institute for Risk Assessment, Max-Dohrn-Straße 8-10, 10589, Berlin, Germany.

出版信息

Part Fibre Toxicol. 2022 May 17;19(1):37. doi: 10.1186/s12989-022-00470-1.

Abstract

BACKGROUND

TiO nanomaterials (NMs) are present in a variety of food and personal hygiene products, and consumers are exposed daily to these NMs through oral exposition. While the bulk of ingested TiO NMs are eliminated rapidly in stool, a fraction is able to cross the intestinal epithelial barrier and enter systemic circulation from where NMs can be distributed to tissues, primarily liver and spleen. Daily exposure to TiO NMs, in combination with a slow rate of elimination from tissues, results in their accumulation within different tissues. Considerable evidence suggests that following oral exposure to TiO NMs, the presence of NMs in tissues is associated with a number of adverse effects, both in intestine and liver. Although numerous studies have been performed in vitro investigating the acute effects of TiO NMs in intestinal and hepatic cell models, considerably less is known about the effect of repeated exposure on these models. In this study, we investigated the cytotoxic effects of repeated exposure of relevant models of intestine and liver to two TiO NMs differing in hydrophobicity for 24 h, 1 week and 2 weeks at concentrations ranging from 0.3 to 80 µg/cm. To study the persistence of these two NMs in cells, we included a 1-week recovery period following 24 h and 1-week treatments. Cellular uptake by TEM and ToF-SIMS analyses, as well as the viability and pro-inflammatory response were evaluated. Changes in the membrane composition in Caco-2 and HepaRG cells treated with TiO NMs for up to 2 weeks were also studied.

RESULTS

Despite the uptake of NM-103 and NM-104 in cells, no significant cytotoxic effects were observed in either Caco-2 or HepaRG cells treated for up to 2 weeks at NM concentrations up to 80 µg/cm In addition, no significant effects on IL-8 secretion were observed. However, significant changes in membrane composition were observed in both cell lines. Interestingly, while most of these phospholipid modifications were reversed following a 1-week recovery, others were not affected by the recovery period.

CONCLUSION

These findings indicate that although no clear effects on cytotoxicity were observed following repeated exposure of differentiated Caco-2 and HepaRG cells to TiO NMs, subtle effects on membrane composition could induce potential adverse effects in the long-term.

摘要

背景

TiO 纳米材料(NMs)存在于各种食品和个人卫生产品中,消费者每天通过口服暴露于这些 NMs。虽然摄入的 TiO NMs 大部分在粪便中迅速消除,但有一部分能够穿过肠上皮屏障并进入全身循环,从那里 NMs 可以分布到组织中,主要是肝脏和脾脏。每天暴露于 TiO NMs,加上从组织中缓慢消除,导致它们在不同组织中积累。大量证据表明,口服暴露于 TiO NMs 后,组织中 NMs 的存在与肠道和肝脏中的许多不良反应有关。尽管已经进行了大量的体外研究,以调查 TiO NMs 在肠和肝细胞模型中的急性影响,但对这些模型的重复暴露的影响知之甚少。在这项研究中,我们研究了两种亲水性不同的 TiO NMs 对相关肠和肝模型的重复暴露 24 小时、1 周和 2 周对细胞的细胞毒性作用,浓度范围为 0.3 至 80µg/cm。为了研究这两种 NMs 在细胞中的持久性,我们在 24 小时和 1 周处理后包括了 1 周的恢复期。通过 TEM 和 ToF-SIMS 分析评估了细胞摄取以及细胞活力和促炎反应。还研究了用 TiO NMs 处理最多 2 周的 Caco-2 和 HepaRG 细胞的膜组成变化。

结果

尽管 NM-103 和 NM-104 被细胞摄取,但在浓度高达 80µg/cm 的情况下,用 NM 处理最多 2 周的 Caco-2 和 HepaRG 细胞均未观察到明显的细胞毒性作用。此外,未观察到对 IL-8 分泌的显著影响。然而,在两种细胞系中都观察到膜组成的显著变化。有趣的是,虽然大多数这些磷脂修饰在 1 周恢复期后得到逆转,但其他修饰不受恢复期的影响。

结论

这些发现表明,尽管分化的 Caco-2 和 HepaRG 细胞反复暴露于 TiO NMs 后未观察到明显的细胞毒性作用,但对膜组成的细微影响可能会在长期内引起潜在的不良反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bcba/9112549/41310e591011/12989_2022_470_Fig2_HTML.jpg

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