交通来源的颗粒物在人细支气管上皮细胞引发的促炎反应中不同机制的作用。

IF 7.2 1区 医学 Q1 TOXICOLOGY
Magne Refsnes, Tonje Skuland, Rikke Jørgensen, Vegard Sæter-Grytting, Brynhild Snilsberg, Johan Øvrevik, Jørn A Holme, Marit Låg
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引用次数: 0

摘要

背景:交通产生的颗粒物是造成环境颗粒物(PM)对健康不利影响的重要因素。在北欧国家,来自道路路面的矿物颗粒和柴油废气颗粒(DEP)是交通来源的PM的重要组成部分。在本研究中,我们比较了两条公路隧道中矿物颗粒和DEP对PM的促炎反应,并研究了其中的机制。方法:在两种不同石料铺砌的公路隧道中取样100µg/mL粗颗粒物(PM10-2.5)、细颗粒物(PM2.5-0.18)和超细颗粒物(PM0.18),评估其在人支气管上皮细胞(HBEC3-KT)中的促炎潜能,并与DEP和不同石料颗粒进行比较。ELISA法检测促炎因子(CXCL8、IL-1α、IL-1β)的释放,qPCR法检测炎症相关基因(COX2、CXCL8、IL-1α、IL-1β、TNF-α)、氧化还原反应(HO-1)和代谢(CYP1A1、CYP1B1、PAI-2)的表达。研究了芳烃受体(AhR)抑制剂CH223191和抗氧化剂n -乙酰半胱氨酸(NAC)对芳烃受体(AhR)和活性氧(ROS)的作用。结果:公路隧道PM可引起CXCL8、COX2、IL-1α、IL-1β、TNF-α、COX2、PAI-2、CYP1A1、CYP1B1和HO-1表达的时间依赖性增加,且在早期时间点,细PM的作用强于粗PM。石颗粒样品和DEP诱导的细胞因子释放在一个隧道中低于所有大小分级PM样品,在另一个隧道中低于细PM样品。CH223191部分降低IL-1α和CXCL8的释放和表达,以及COX2在细粒和粗粒PM中的表达,这取决于通道、响应和时间点。而CYP1A1的表达被CH223191显著降低,HO-1的表达不受影响。NAC降低了IL-1α和CXCL8的释放和表达,降低了COX2的表达,增强了CYP1A1和HO-1的表达。结论:研究结果表明,公路隧道PM在HBEC3-KT细胞中的促炎反应并非仅归因于矿物颗粒或DEP。促炎反应似乎涉及ahr依赖机制,提示有机成分的作用。ros介导的机制也参与其中,可能通过不依赖ahr的途径。DEP可能是ahr依赖性反应的一个贡献者,尽管其他来源可能很重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Role of different mechanisms in pro-inflammatory responses triggered by traffic-derived particulate matter in human bronchiolar epithelial cells.

Role of different mechanisms in pro-inflammatory responses triggered by traffic-derived particulate matter in human bronchiolar epithelial cells.

Role of different mechanisms in pro-inflammatory responses triggered by traffic-derived particulate matter in human bronchiolar epithelial cells.

Role of different mechanisms in pro-inflammatory responses triggered by traffic-derived particulate matter in human bronchiolar epithelial cells.

Background: Traffic-derived particles are important contributors to the adverse health effects of ambient particulate matter (PM). In Nordic countries, mineral particles from road pavement and diesel exhaust particles (DEP) are important constituents of traffic-derived PM. In the present study we compared the pro-inflammatory responses of mineral particles and DEP to PM from two road tunnels, and examined the mechanisms involved.

Methods: The pro-inflammatory potential of 100 µg/mL coarse (PM10-2.5), fine (PM2.5-0.18) and ultrafine PM (PM0.18) sampled in two road tunnels paved with different stone materials was assessed in human bronchial epithelial cells (HBEC3-KT), and compared to DEP and particles derived from the respective stone materials. Release of pro-inflammatory cytokines (CXCL8, IL-1α, IL-1β) was measured by ELISA, while the expression of genes related to inflammation (COX2, CXCL8, IL-1α, IL-1β, TNF-α), redox responses (HO-1) and metabolism (CYP1A1, CYP1B1, PAI-2) was determined by qPCR. The roles of the aryl hydrocarbon receptor (AhR) and reactive oxygen species (ROS) were examined by treatment with the AhR-inhibitor CH223191 and the anti-oxidant N-acetyl cysteine (NAC).

Results: Road tunnel PM caused time-dependent increases in expression of CXCL8, COX2, IL-1α, IL-1β, TNF-α, COX2, PAI-2, CYP1A1, CYP1B1 and HO-1, with fine PM as more potent than coarse PM at early time-points. The stone particle samples and DEP induced lower cytokine release than all size-fractionated PM samples for one tunnel, and versus fine PM for the other tunnel. CH223191 partially reduced release and expression of IL-1α and CXCL8, and expression of COX2, for fine and coarse PM, depending on tunnel, response and time-point. Whereas expression of CYP1A1 was markedly reduced by CH223191, HO-1 expression was not affected. NAC reduced the release and expression of IL-1α and CXCL8, and COX2 expression, but augmented expression of CYP1A1 and HO-1.

Conclusions: The results indicate that the pro-inflammatory responses of road tunnel PM in HBEC3-KT cells are not attributed to the mineral particles or DEP alone. The pro-inflammatory responses seem to involve AhR-dependent mechanisms, suggesting a role for organic constituents. ROS-mediated mechanisms were also involved, probably through AhR-independent pathways. DEP may be a contributor to the AhR-dependent responses, although other sources may be of importance.

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来源期刊
CiteScore
15.90
自引率
4.00%
发文量
69
审稿时长
6 months
期刊介绍: Particle and Fibre Toxicology is an online journal that is open access and peer-reviewed. It covers a range of disciplines such as material science, biomaterials, and nanomedicine, focusing on the toxicological effects of particles and fibres. The journal serves as a platform for scientific debate and communication among toxicologists and scientists from different fields who work with particle and fibre materials. The main objective of the journal is to deepen our understanding of the physico-chemical properties of particles, their potential for human exposure, and the resulting biological effects. It also addresses regulatory issues related to particle exposure in workplaces and the general environment. Moreover, the journal recognizes that there are various situations where particles can pose a toxicological threat, such as the use of old materials in new applications or the introduction of new materials altogether. By encompassing all these disciplines, Particle and Fibre Toxicology provides a comprehensive source for research in this field.
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