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与交通相关的纳米/超细颗粒中的多环芳烃、多环芳烃诱导的致癌潜力以及颗粒提取物诱导的细胞毒性。

PAHs, PAH-induced carcinogenic potency, and particle-extract-Induced cytotoxicity of traffic-related nano/ultrafine particles.

作者信息

Lin Chih-Chung, Chen Shui-Jen, Huang Kuo-Lin, Lee Wen-Jhy, Lin Wen-Yinn, Tsai Jen-Hsiung, Chaung Hso-Chi

机构信息

Department of Environmental Engineering and Science, National Pingtung University of Science and Technology, Nei Pu, PingTung 91201, Taiwan.

出版信息

Environ Sci Technol. 2008 Jun 1;42(11):4229-35. doi: 10.1021/es703107w.

Abstract

Polycyclic aromatic hydrocarbons (PAHs) bound in nano/ ultrafine particles from vehicle emissions may cause adverse health effects. However, little is known about the characteristics of the nanoparticle-bound PAHs and the PAH-associated carcinogenic potency/cytotoxicity; therefore, traffic-related nano/ultrafine particles were collected in this study using a microorifice uniform deposition impactor(MOUDI) and a nano-MOUDI. For PM0.056--18, the difference in size-distribution of particulate total-PAHs between non-after-rain and after-rain samples was statistically significant at alpha = 0.05; however, this difference was not significant for PM0.01--0.056. The PAH correlation between PM0.01--0.1 and PM0.1--1.8 was lower for the after-rain samples than forthe non-after-rain samples. The average particulate total-PAHs in five samplings displayed a trimodal distribution with a major peak in the Aitken mode (0.032--0.056 microm). About half of the particulate total-PAHs were in the ultrafine size range. The BaPeq sums of BaP, IND, and DBA (with toxic equivalence factors > or = 0.1) accounted for approximately 90% of the total-BaPeq in the nano/ultrafine particles, although these three compounds contributed little to the mass of the sampled particles. The mean content of the particle-bound total-PAHs/-BaPeqs and the PAH/BaPeq-derived carcinogenic potency followed the order nano > ultrafine > fine > coarse. For a sunny day sample, the cytotoxicity of particle extracts (using 1:1 (v/v) n-hexane/dichloromethane) was significantly higher (p < 0.05) for the nano (particularly the 10-18 nm)/ultrafine particles than for the coarser particles and bleomycin. Therefore, traffic-related nano and ultrafine particles are possibly cytotoxic.

摘要

车辆排放的纳米/超细颗粒中结合的多环芳烃(PAHs)可能会对健康产生不利影响。然而,对于与纳米颗粒结合的PAHs的特性以及与PAH相关的致癌潜能/细胞毒性知之甚少;因此,本研究使用微孔均匀沉积冲击器(MOUDI)和纳米MOUDI收集了与交通相关的纳米/超细颗粒。对于PM0.056-18,雨后和雨后样品之间颗粒总PAHs的粒径分布差异在α=0.05时具有统计学意义;然而,对于PM0.01-0.056,这种差异并不显著。雨后样品中PM0.01-0.1与PM0.1-1.8之间的PAH相关性低于雨后样品。五次采样中的平均颗粒总PAHs呈现出三峰分布,在艾肯模态(0.032-0.056微米)中有一个主峰。约一半的颗粒总PAHs处于超细粒径范围内。BaP、IND和DBA(毒性当量因子≥0.1)的BaPeq总和约占纳米/超细颗粒中总BaPeq的90%,尽管这三种化合物对采样颗粒的质量贡献很小。颗粒结合的总PAHs/-BaPeqs的平均含量以及PAH/BaPeq衍生的致癌潜能遵循纳米>超细>细>粗的顺序。对于一个晴天的样品,颗粒提取物(使用1:1(v/v)正己烷/二氯甲烷)对纳米(特别是10-18纳米)/超细颗粒的细胞毒性显著高于粗颗粒和博来霉素(p<0.05)。因此,与交通相关的纳米和超细颗粒可能具有细胞毒性。

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