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体内研究微纳米二氧化钛对小鼠 6 种器官的遗传毒性和细胞毒性。

Investigation of genotoxic and cytotoxic effects of micro- and nanosized titanium dioxide in six organs of mice in vivo.

机构信息

Russian Academy of Medical Sciences, Moscow, Russian Federation.

出版信息

Mutat Res. 2011 Nov 27;726(1):8-14. doi: 10.1016/j.mrgentox.2011.07.010. Epub 2011 Aug 17.

DOI:10.1016/j.mrgentox.2011.07.010
PMID:21871579
Abstract

Titanium dioxide is manufactured worldwide in large quantities for use in a wide range of applications including as food additives, in cosmetics and pigments for coloring ingested and externally applied drugs. Although TiO(2) is chemically inert it can cause negative health effects, such as lung cancer in rats. However, the mechanisms involved in TiO(2)-induced genotoxicity and carcinogenicity have not been clearly defined and are poorly studied in vivo. In the present research genotoxicity and carcinogenicity of titanium dioxide were studied in a mouse model. We treated CBAB6F1 mice by oral gavage with titanium dioxide particles (microsized, TDM, 160nm; nanosized, TDN, 33nm) in doses of 40, 200 and 1000mg/kg bw, daily for seven days. Genotoxic effects were analyzed in the cells of brain, liver and bone marrow by means of the Comet assay and in the cells of bone marrow, forestomach, colon and testis with a poly-organ karyological assay (analysis of micronuclei, nuclear protrusions, atypical nuclei, multinucleated cells, mitotic and/or apoptotic index). TDM induced DNA-damage and micronuclei in bone-marrow cells and TDN induced DNA-damage in the cells of bone marrow and liver. TDM and TDN increased the mitotic index in forestomach and colon epithelia, the frequency of spermatids with two and more nuclei, and apoptosis in forestomach (only TDN) and testis. This is one of the first poly-organ studies of TDM- and TDN-induced genotoxicity in vivo in mice. These effects are caused by a secondary genotoxic mechanism associated with inflammation and/or oxidative stress. Given the increasing use of TiO(2) nanoparticles, these findings indicate a potential health hazard associated with exposure to TiO(2) particles.

摘要

二氧化钛在全球范围内大量生产,用于广泛的应用,包括食品添加剂、化妆品和颜料,用于着色摄入和外部应用的药物。虽然 TiO(2) 是化学惰性的,但它会引起负面的健康影响,例如大鼠肺癌。然而,TiO(2) 诱导的遗传毒性和致癌性的机制尚未明确界定,在体内研究得也很少。本研究在小鼠模型中研究了二氧化钛的遗传毒性和致癌性。我们通过口服灌胃方式用二氧化钛颗粒(微尺度,TDM,160nm;纳米尺度,TDN,33nm)处理 CBAB6F1 小鼠,剂量分别为 40、200 和 1000mg/kg bw,每天一次,共七天。通过彗星试验分析大脑、肝脏和骨髓细胞的遗传毒性效应,通过多器官核型分析(分析微核、核突起、非典型核、多核细胞、有丝分裂和/或凋亡指数)分析骨髓、前胃、结肠和睾丸细胞的遗传毒性效应。TDM 诱导骨髓细胞的 DNA 损伤和微核,TDN 诱导骨髓和肝脏细胞的 DNA 损伤。TDM 和 TDN 增加了前胃和结肠上皮的有丝分裂指数、具有两个或更多核的精子细胞的频率以及前胃(仅 TDN)和睾丸的凋亡。这是首次在体内进行的微尺度 TDM 和 TDN 诱导遗传毒性的多器官研究之一。这些效应是由与炎症和/或氧化应激相关的二级遗传毒性机制引起的。鉴于 TiO(2) 纳米颗粒的使用越来越多,这些发现表明与暴露于 TiO(2) 颗粒相关的潜在健康危害。

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