Journal of Toxicology
Volume 2011 (2011), Article ID
487074, 9 pages
doi:10.1155/2011/487074Review
ArticleOxidative Stress and Air Pollution ExposureMaura Lodovici and Elisabetta
BigagliDepartment of Pharmacology and Toxicology, University of Florence, Viale
Pieraccini 6, 50139 Florence,
ItalyReceived 15 December 2010; Revised 10 May 2011; Accepted 30 June
2011Academic Editor: Susan Sumner Copyright © 2011 Maura Lodovici and
Elisabetta Bigagli. .AbstractAir pollution is associated with increased cardiovascular and
pulmonary morbidity and mortality.
The mechanisms of air
pollution-induced health effects involve oxidative stress and inflammation. As
a matter of fact, particulate matter (PM), especially fine (PM2.5, PM < 2.5 μm) and
ultrafine (PM0.1, PM < 0.1 μm) particles, ozone, nitrogen oxides,
and transition metals, are potent oxidants or able to generate reactive oxygen
species (ROS). Oxidative stress can trigger redox-sensitive pathways that lead
to different biological processes such as inflammation and cell death. However,
it does appear that the susceptibility of target organ to oxidative injury also
depends upon its ability to upregulate protective scavenging systems. As
vehicular traffic is known to importantly contribute to PM exposure, its
intensity and quality must be strongly relevant determinants of the qualitative
characteristics of PM spread in the atmosphere. Change in the composition of
this PM is likely to modify its health impact.1. IntroductionNumerous
epidemiological studies have shown an increased morbidity and mortality due to
environmental air pollution [1, 2]. Environmental air does contain a complex
mixture of toxics, including particulate matter (PM), irritant gases, and
benzene. The chemical composition of particles does vary greatly and depends on
numerous geographical, meteorological, and source-specific variables.
Generally, environmental particles include inorganic components (sulfates,
nitrates, ammonium, chloride, and trace metals), elemental and organic
carbon, biological components (bacteria,
spores, and pollens), and adsorbed volatile and semivolatile organic compounds
[3]. In addition, environmental particles, when mixed with atmospheric gases
(ozone, sulfur nitric oxides, and carbon monoxide) can generate environmental
aerosols. Particles are usually defined as PM10 and PM2.5 with diameter less
than 10 and 2.5 μm, respectively. Any fraction may have different effects; that is,
PM with aerodynamic diameter less than 10 to 2.5 μm does generate a bigger amount of hydroxyl radical due to the heavy metals
adsorbed on the pores and surfaces of the particles, whereas particles of
larger size (PM10) deposit mainly in the upper airways and can be
cleared by the mucociliary system [4, 5]. Recently, however, interest has also
focused on the ultrafine particles (UFPs) with a diameter less than 100 nm; UFPs are considered important with respect to health
effects because of their very high alveolar deposition fraction, large surface
area, chemical composition, and ability to enter into the circulation and
induce inflammation. Vehicle emissions, in particular related to diesel
engines, diesel exhaust particles (DEPs), are a major source of environmental
UFPs, which in the presence of poor ventilation may penetrate indoor, where
additional sources including environmental tobacco smoke, cooking, burning of
candles, and chemical reactions are present [6–10]. Long-term exposure to high
levels of such particles can increase risk of cancer, respiratory diseases, and
arteriosclerosis, whereas short-term exposure peaks can cause exacerbation of bronchitis, asthma,
and other respiratory diseases as well as changes in heart-rate variability [2,
11–13]. The general consensus does indicate that the mechanism of air
pollution-induced health effects involves an inflammation-related cascade and
oxidation stress both in lung, vascular, and heart tissue [14–19]. Inflammation
is initially a protective mechanism
which removes the injurious stimuli and
produces reactive oxygen species (ROS) able to induce cell killing. In the
early phase of inflammation, oxidant stress does not directly cause cell damage and can induce the transcription of stress
defense genes including antioxidant genes. This preconditioning effect of ROS
enhances the resistance against future inflammatory oxidant stress and promotes
the initiation of tissue repair processes. The additional release of cell
contents amplifies the inflammatory process and consequently can induce tissue
injury [20]. Oxidation damage has been implicated in many degenerative and
nondegenerative diseases, including cardiovascular and pulmonary diseases,
diabetes, and Alzheimer disease. Oxidation stress derived from an unbalance
between ROS formation and individual antioxidant activity potentially does lead
to damage of lipids, proteins, and macromolecules such as DNA and RNA [21].
This paper will focus on the mechanisms of oxidative stress induction and
cellular damage by air pollution exposure on pulmonary and cardiovascular
systems.2. Possible Mechanisms of Oxidative Stress Induced by Air Pollution
ExposureIn the last decades, great attention has been paid to air pollution exposure due to vehicular
traffic and other combustion processes. PM and gas pollutants are considered to
be the most important factors in urban areas, and several mechanisms have been
hypothesized to explain the adverse health effects in humans, especially in the
cardiopulmonary system [22]. Although each air pollutant can exert its own
specific toxicity in the respiratory and cardiovascular systems, ozone, oxides
of nitrogen, and suspended particulates all share a common property of being
potent oxidants, either through direct effects on lipids and proteins or
indirectly through the activation of intracellular oxidant pathways [23–25].ROS
can be generated from the surface of particles where polycyclic aromatic
hydrocarbons (PAH) and nitro-PAH are
adsorbed, other than transition metals (iron, copper, chromium, and vanadium)
that catalyzing Fenton’s reaction (Fe2+ + H2O2 + H+ → Fe3+ + OH• + H2O) generate the highly
reactive hydroxyl radical able to induce oxidative DNA damage [26, 27]. Several
studies have shown that iron and other transition metals leaching from
particles or by their presence on particle surfaces play a role in the
generation of ROS in biological systems [28]. Particles bound benzo(a)pyrene
has been shown to be bioavailable and can induce oxidative DNA damage in
systemic target organs, including lung and kidney [29, 30]. Moreover, it should
be noted that ozone and nitrogen dioxide are usually present together with
particles in environmental air. They are also oxidants with potential effects
in terms of oxidative DNA damage. Similarly, volatile compounds, such as
benzene, in urban air pollution can induce DNA oxidation [31, 32]. In addition,
photochemical oxidants (ozone and peroxyacetyl nitrate), secondary pollutants
formed by the action of sunlight on an atmosphere that does contain reactive
hydrocarbons and NOx, contribute to increase oxidation stress [33]. Then, in
the presence of high ROS formation,
mitochondrial damage with induction of
NADPH- oxidase isoform 4 (NOX4) does occur, together with an activation of inflammatory cells
(neutrophils, eosinophils, and
monocytes) and increased numbers of macrophages capable of ROS and reactive
nitrogen species generation [34–36]. Initially, when oxidative stress is
relatively low, various transcription factors, such as the nuclear factor
erythroid-2 (Nrf2), induce a series of antioxidant and detoxification enzymes
(e.g., catalase, superoxide dismutase, and glutathione S-transferase) that
counteract ROS formation protecting from adverse biological outcomes [37, 38].
In the second phase, if the protective antioxidant response fails or is
inadequate to deal with increasing ROS production, the result is a
proinflammatory situation with various cytotoxic effects [39]. These effects
are mediated by the redox-sensitive mitogen-activated protein kinase (MAPK) and
NF-κB cascades that are responsible for the expression of cytokines,
chemokines, and adhesion molecules, which are involved in inflammatory
processes [39].3. Atmospheric GasesGaseous pollutants contribute to a great
extent in composition variations of the atmosphere and are mainly due to
combustion of fossil fuels and to emission of motor vehicles [40].Ozone is a
strong oxidizing agent formed in the troposphere through a complex series of reactions
involving the action of sunlight in nitrogen dioxide and hydrocarbons. Ozone
initiate intracellular oxidative stress through ozonide and hydroperoxide
formation. This mechanism of oxidative damage involves the activation of Nrf2,
heat shock protein 70, NF-κB, increased expression of a range of
proinflammatory cytokines (TNFα and interleukin 1β), chemokines (e.g.,
interleukin 8), and adhesion genes; ozone is also an activator of protein-1 fos
and c-jun onco genes [41, 42]. The major
source of anthropogenic emissions of nitrogen oxides into the atmosphere is the
combustion of fossil fuels deriving from stationary sources (heating, power
generation) and motor vehicles. In environmental conditions, nitric oxide is
rapidly transformed into nitrogen dioxide by atmospheric oxidants such as ozone
[43].Various antioxidants, like ascorbic acid, uric acid, and thiols, act as
powerful scavengers of O3 and NO2• radical in body fluids, likely protecting
lung lining fluids against inhaled oxidizing air pollutants [44]. When such
defense mechanisms are overwhelmed, O3 may injure the underlying cells by
inducing lipid peroxidation and activating inflammatory gene expression
[45]. In vitro and in vivo studies, both
in animals and human beings, confirm the capacity of nitrogen dioxide to
activate oxidant pathways although less potently than ozone [46]. Volatile
organic compounds are a class of compounds which includes chemical species of
organic nature such as benzene, but the majority of gaseous pollutants are
inhaled and, therefore. mainly affect the respiratory and cardiovascular
systems. Among gaseous pollutants, carbon monoxide (CO) has been described as
one of the main pollutants responsible for the development of cardiovascular
diseases [47], while benzene can also
induce haematological problems and cancer [48].
Benzene is a commonly used industrial chemical and a constituent of
gasoline [31]. Inhalation is the most important route of absorption during
occupation-related exposure. Benzene toxicity is attributed to its metabolism,
which does lead to the formation of reactive metabolites such as hydroquinone
and its oxidized form benzoquinone which
are highly reactive molecules and, by means of redox cycling, produce
ROS [49]. Furthermore, the addition of
antioxidant enzymes has been shown to block oxidative damage induced by the
above-mentioned metabolites confirming the role of ROS production and oxidative
stress in hydroquinone and benzoquinone cytotoxicity [50]. Uzma et al. [31]
demonstrated that occupation-related
exposure to benzene causes oxidative stress, immune suppression, and inducing
the expression of tumour-suppressing gene p53 in gasoline filling workers.
These authors hypothesized that the increase in the p53 expression may block
the cell cycle at G1 phase and go on to repair DNA damage, which is the initial
step in tumour suppression.4. Oxidative Stress from Organic FractionAmbient PM,
does consist of complex and various mixtures of particles suspended in the
breathing air [50]. Major sources of PM are factories, power plants, refuse
incinerators, motor vehicles, building activity, fires, and natural windblown
dust. The size of the particles vary, and there is strong evidence supporting
that ultrafine and fine particles are more hazardous than larger ones in terms
of mortality and cardiovascular and respiratory effects [51].Results from
various surveys have demonstrated that oxidative potential of fine and
ultrafine particles is the result of significant amounts of organic carbon
compounds, such as quinones and PAHs. In the organic fraction originating in
the air from incomplete combustion processes, the major reactive and toxic
compounds are substituted (e.g., methyl naphthalene) and unsubstituted PAH, nitro-PAH (1-nitropyrene and
3-nitro-fluoranthene), dinitro-PAH
(dinitro pyrene) and peroxyacetyl
nitrate [52, 53]. Moreover, reactive intermediates in the oxidation of mixtures
of volatile organic compounds (VOCs), oxides of nitrogen (NOx), hydroxy
radical, and ozone are shown to play a central role in the formation and fate
of airborne toxic chemicals, PAH, and fine particles [52]. The main pathways of
metabolic activation of PAHs are generation of diol epoxides catalyzed by
cytochrome P450 (CYP450), leading to DNA adduct formation, formation of radical
cations catalyzed by CYP450 peroxidases, and formation of redox-active quinones
[54]. Valavanidis et al. [55] demonstrated that redox-active transition metals,
redox cycling quinoids and PAH act synergically to produce ROS. J. Y. C. Ma and
J. K. H. Ma [56] reported that organic fraction of DEP, mainly constituent of
PAH and quinones, does undergo to metabolic activation in the lung and liver of exposed animals, is able to induce CYP4501A1 isoform
expression that generates ROS and reactive PAH-quinones. In addition, PM
initiates inflammatory damage upregulating proinflammatory cytokines and
chemokines; in vitro observations have shown that PM exposure may cause
expression of nuclear factor NF-κB-related genes and oxidant-dependent NF-κB
activation [57, 58]. To defend against oxidative damage, cells increase the
production of antioxidant enzymes through the activation of the Nrf2, [37]
and PM appears to inhibit protective
enzymes involved in oxidative stress
responses leading to the activation of additional intracellular signaling
cascades that regulate the expression of cytokine and chemokine genes [59].
Many recent observations have shown that DEPs, because of their fine and
ultrafine composition, play an important role on oxidative cellular damage through
ROS generation causing lipid
peroxidation and oxidative DNA damage. Some DEPs consist of a carbon core or
organic droplets with adsorbed organic
compounds, such as PAH, quinines, and redox-active metals. The capacity of DEPs
to induce oxidative stress is largely related to these adsorbed components [60,
61].5. Oxidative Stress Induced by Transition MetalsTransition metals such as
iron, lead, mercury, cadmium, silver, nickel, vanadium, chromium, manganese,
and copper are detectable in PM2.5 and UFPs adsorbed on their surface and are
capable of ROS formation by Fenton’s reaction [35]. As critical constituents of
PM, transition metals were postulated to be involved in a number of
pathological processes of the respiratory system through free radical-mediated
damage [62]. They are natural components of the earth's crust and enter into
the environment through a wide variety of sources, including combustion, waste
water discharges, and manufacturing facilities. Iron is a well-known soot
suppressant that might be emitted into the atmosphere in the form of ultrafine
particles [63]. Zinc is a major metal element detected in traffic derived
PM2.5, deriving from waste oil samples
[64]. Copper is a component of car brake pads, however, ceramic brake pads
contain 10%–20% copper by mass, while the metallic brake pads contained about
70% iron with very little copper. This metal in PM has also been linked to road
traffic sources associated to PM2.5 [64]. Soluble metals in inhaled particles,
such as Fe, Ni, V, Co, Cu, and Cr, were associated with increased ROS
production, followed by cellular oxidative stress in airway epithelial cells
[65].6. Air Pollution Induced-Oxidative Damage in Target Organs: Cardiovascular
and Pulmonary Systems6.1. Cardiovascular SystemDiesel and gasoline vehicle
emissions in the urban areas have dominant contributions to environmental
particles, especially those located in the ultrafine range. Because of their
small size and large surface area, UFPs have demonstrated unique biochemical
characteristics, such as enhanced ability to adsorb or absorb organic molecules
and to penetrate into cellular targets in the human pulmonary and
cardiovascular systems [66, 67]. UFPs may be directly transported to the
cardiac vasculature, where they can induce arrhythmias, reduce myocyte
contractility, and decrease coronary blood flow [10, 68]. Studies by Brook et
al. [69] demonstrated that fine particulate air pollution and ozone cause acute
arterial vasoconstriction in healthy humans, while Urch et al. [70] reported that
fine particles exposure pollution raise blood pressure and impair vascular
function. In addition, UFP exposure depresses myocardial contractile response
and coronary flow in both spontaneously hypertensive and wild-type rats [71],
the same observation was found by Simkhovich et al. [72] in young and old rat
hearts. Long-term exposure to low
concentrations of PM2.5 has been shown to alter vasomotor tone, lead to
vascular inflammation, and potentiate atherosclerosis induced by highly
fat-containing chow in susceptible mice [73]. In addition, Suwa et al. [74]
reported that exposure to PM10 cause progression of atherosclerotic lesions
towards a more advanced phenotype hyperlipidemic rabbits. Moreover,
atherosclerotic lesions of thoracic aorta were reported to be significantly
increased with pronounced macrophage infiltration and lipid deposition in
Apolipoprotein E (−/−) ApoE (−/−) mice exposed to PM2.5 through NADPH oxidase
dependent pathways [75]. ApoE (−/−) mice exposed to ozone showed increased
oxidative stress and mitochondrial DNA damage, decreased vascular endothelial
nitric oxide synthase, and significantly
increased atherogenesis compared to filtered air exposed controls [76]. Recently, Cherng et al. [77] reported that
DEP exposure enhances vasoconstriction and diminishes acetylcholine-induced
dilatation in coronary arteries of animals in a nitric oxide synthase-dependent
manner. Baccarelli et al. [78] showed that air pollution is associated with
changes in the global coagulation function, after short-term exposure to air
pollution in normal subjects resident in
Lombardia Region, Italy. Road traffic-related pollutants may increase a
heart-rate-corrected QT interval among people with diabetes, obesity and nonsmoking
elderly individuals and the number of genetic variants related to oxidative
stress does increase this effect [79]. On the contrary, Mordukhovich et al.
[80], despite the positive associations between blood pressure and black
carbon, found no effects on gene variants related to antioxidative defense.
Increases in black carbon and PM2.5 were associated with increases in blood
pressure, heart-rate, endothelin-1, vascular endothelial growth factor, and
oxidative stress markers and with a decrease in brachial artery diameter in
nonsmoking seniors [81]. More recently, Kooter et al. [82] showed that
diesel engine exhaust exposure induces a pulmonary antioxidant response, with
an increased activity of the anti-oxidant enzymes glutathione peroxidase,
superoxide dismutase, heme oxygenase-1 protein, heme oxygenase activity, and
uric acid which precedes the
inflammatory response (an increase in IL-6 and TNF-α) in rats. In addition,
since the authors found that increased plasma thrombogenicity and antioxidant
defense gene expression in aorta tissue shortly after the exposure does occur,
they hypothesized a direct translocation of diesel engine exhaust components to
the vasculature even if the mediation by other pathways cannot be excluded
[82]. 6.2. PulmonaryA strong correlation
has been found between PM concentration of redox-active compounds and damage in
macrophages and bronchial epithelial cells [83–85]. Moreover, in human airway
epithelial cells, organic compounds adsorbed on particle surfaces does promote
inflammation through CYP1A1-mediated ROS generation and release of cytokines
after activation of transduction pathways involving MAPK and the transcription
factor NF-kappaB [86]. Recently, Andersson et al. [26] reported that
1-nitropyrene, one of the most abundant nitro-PAHs in diesel exhausts, induces
DNA damage by ROS formation in human
endothelial cells, and this effect was mainly mediated by metabolites mainly
generating by reduction of nitro group, as it has been previously reported by
Topinka et al. [87] in rat hepatocytes. Increased production of ROS after PM
exposure is suggested by the finding that many of the proinflammatory genes
(TNF-α and IL-8, among others) induced upon exposure to PM are regulated by
redox sensitive transcription factors such as NF-κB, activator protein 1 (AP-1)
and CAATT/enhancer binding protein (C/EBP). Activation of these transcription
factors and increased transcription of downstream genes has been reported in
human alveolar and bronchial epithelial cells in response to PM exposure
[88–92]. Several studies have demonstrated that air pollution particles induce
inflammatory mediator release and oxidative stress in lung epithelial cells and
alveolar macrophages. When reaching the bone marrow [93], cytokines and
chemokines released from the lung stimulate migration of neutrophils and their
precursors into the circulation. In the short-term, there is acute tissue
damage with activation of the epidermal-growth-factor receptor pathway, and
evidence for organ-repair responses [94]. Vanadium pentoxide (V2O5) is a
component of PM derived from fuel combustion as well as a source of
occupation-related exposure in humans [95]. Sørensen et al. [95] indicate that
vanadium and chromium (VI) detectable in PM(2.5) have an effect on oxidative
DNA damage in human lymphocytes, after
reduction to chromium (III) in the
cells. Since, outdoor PM and urinary 1-hydroxypyrene (PAH exposure marker) were
synergistically associated with urinary MDA levels of schoolchildren, Bae et
al. [96] concluded that exposure to PM air pollution and PAH can induce
oxidative stress in schoolchildren. In addition, these authors found that
urinary MDA levels are also associated with some metals bound to PM10 and PM2.5
suggesting that metals bound to PM are
responsible, at least in part, for the oxidative stress [96]. The oxidized
species arising from the reaction between ozone and lining fluid are involved
in the signaling cascade of inflammatory cells into the lung and contribute to
the acute bronchoconstrictor response and hyperresponsiveness observed in asthma
on exposure to this pollutant [97, 98]. Furthermore, has been reported that
ozone is able to induce apoptosis, DNA damage, and cytotoxicity on human
alveolar epithelial type I-like cells and in mice exposed to ozone for 6 weeks
[99, 100]. While, Ferecatu et al. [84] reported an antiapoptotic effect of PAH
adsorbed on PM2.5 that in addition to the well-documented inflammatory response
may explain the persistence of a prolonged inflammation state induced after
pollution exposure and might delay repair processes of injured tissues in
primary cultures of human bronchial epithelial cells. Chirino et al. [101]
found ROS generation and decreased glutathione and the activity of the
antioxidant enzymes, such as superoxide
dismutase and glutathione reductase, in a human lung epithelial cell line
exposed to PM10. Recently, it has been found that bus drivers exposed to PAH
and volatile compounds displayed a
higher level of DNA instability and oxidative damage than the controls and the
incidence of oxidized lesions in lymphocyte DNA correlated with exposure to
benzene. Moreover, those of the drivers with at least one variant of
8-oxoguanine glycosylate 1 (hOGG1) (Cys/Cys or Ser/Cys) allele tended to have
higher oxidative DNA damage in lymphocyte than those with the wild genotype
[102]. In addition, in the same year Delfino et al. [103] reported that PM
(ranged from 0.25 to 2.5 μm) and O3
were positively associated with exhaled
nitrogen monoxide and that PM0.25, CO, and NO were positively associated
with IL-6, while ROS were
associated with both outcomes in elderly
subjects enrolled.7. Defense Mechanisms against ROS FormationAntioxidants in
the lung are the first line of defense against ROS [104]. The composition and
quantity of antioxidants in respiratory tract lining fluids may represent an
important determinant of individual responsiveness to air pollutants, but it
should be thought of as a dynamic equilibrium with the antioxidant defenses
within the epithelium and a more remote plasma pool [105]. Interestingly, the results obtained by Osburn
and Kensler [106] demonstrated that the
activation of transcriptional factor Nrf2 determines an upregulation of
antioxidant enzymes that represents an adaptive response to face the exposure
to oxidant pollutants providing a pivotal defense mechanism against
environmental hazards, including various air pollutants. Successively, Rubio et
al. [107] observed that Nrf2 does protect against benzene metabolites in human
lung cells, and knockdown of Nrf2 greatly does enhance cytotoxicity and cell
death associated with reduced glutathione levels and loss of inducibility of
antioxidant response elements (ARE-driven) genes.Although the interrelation
among antioxidant levels in the respiratory tract, cellular and plasma levels
are not well understood, it appears that the susceptibility of the lung to
oxidative injury depends largely on its ability to upregulate protective
scavenging systems. A recent review by Rubio et al. [108] indicates that air
pollutants are Nrf2 pathway inductors which regulate the expression of
cytoprotective and detoxifying enzymes as well as antioxidants having an
important role in the defense against atmospheric pollutant-induced toxicity.8.
ConclusionsIn conclusion, several experimental and epidemiological studies have
proved exposure to air pollution to be
an important determinant of overall pulmonary and cardiovascular risk damage
and possibly have an influence on
traditional risk factors. Although each environmental pollutant has its own
mechanism of toxicity, most pollutants, like UFP, PM2.5, ozone, nitrogen
oxides, and transition metals, are
potent oxidants or capable of ROS production. Consequently, the promotion of
oxidative stress has been identified as one of the most important mechanisms
responsible for toxic air pollutant effects. Oxidative stress can trigger
redox-sensitive pathways that lead to different biological processes like
inflammation and cell death. Recently, Environmental Pollution Agency (EPA)
revised the level of the 24-h PM2.5 standard to 35 μg/m3,
moved the 24-h PM10 standard from 75 at
150 μg/m3, and revoked the annual standard, because available evidence
generally did not suggest a link between
long-term exposure to current ambient levels of coarse particles and health
or welfare effects [109]. However, a vast number of data indicate that
in general, smaller size fraction, containing higher concentration of PAH,
transition metal, and semiquinones, has a higher ROS capacity and consequently
should be capable to induce severe toxicological effects. Thus, change in the
composition of this PM are likely to modify its health impact. Road traffic is
known to vastly contribute to PM exposure. Traffic intensity and quality should
then be important determinants of the qualitative characteristics of PM spread
in the atmosphere. In addition, although the interrelation between antioxidant
levels in respiratory and cardiovascular systems, cellular and plasma levels is
not yet well understood; it appears that the susceptibility of target organs to
oxidative injury largely depends on cell ability to upregulate protective
scavenging systems such as Nrf2. This transcription factor does regulate the
expression of numerous cytoprotective genes that detoxify reactive species
playing an important role in the defense
against atmospheric pollutant-induced toxicity.However, many questions remain
unanswered, but in the future, rapid developments in molecular biology,
proteomics, and genomics will help to completely clarify the biological mechanisms involved in pulmonary and cardiovascular injuries caused by air
pollution.AcknowledgmentThis work is supported by a fund of University of
Florence.References
J. Schwartz, “Air pollution and
daily mortality: a review and meta analysis,” Environmental Research, vol. 64,
no. 1, pp. 36–52, 1994. View at Publisher · View at Google Scholar · View at
PubMed · View at ScopusD. W. Dockery, A. C. Pope III, X. Xu et al., “An
association between air pollution and mortality in six U.S. cities,” New
England Journal of Medicine, vol. 329, no. 94, pp. 1753–1759, 1993. View at
Publisher · View at Google Scholar · View at PubMed · View at ScopusR. M.
Harrison and J. Yin, “Particulate matter in the atmosphere: which particle
properties are important for its effects on health?” Science of the Total
Environment, vol. 249, no. 1–3, pp. 85–101, 2000. View at Publisher · View at
Google Scholar · View at Scopus Environmental Protection Agency, Air Quality
Criteria for Particulate Matter, vol. III of EPA/600/P-95/001CF, National
Center for Environmental Assessment, Research Triangle Park, NC, USA, 1996. J.
Ferin, G. Oberdörster, and D. P. Penney, “Pulmonary retention of ultrafine and
fine particles in rats,” American Journal of Respiratory Cell and Molecular
Biology, vol. 6, no. 5, pp. 535–542, 1992. View at ScopusJ. Ferin, “Pulmonary
retention and clearance of particles,” Toxicology Letters, vol. 72, no. 1–3,
pp. 121–125, 1994. View at Publisher · View at Google Scholar · View at
ScopusL. Kliucininkas, D. Martuzevicius, E. Krugly et al., “Indoor and outdoor
concentrations of fine particles, particle-bound PAHs and volatile organic
compounds in Kaunas, Lithuania,” Journal of Environmental Monitoring, vol. 13,
no. 1, pp. 182–191, 2011. View at Publisher · View at Google Scholar · View at
PubMedM. Dennekamp, S. Howarth, C. A. J. Dick, J. W. Cherrie, K. Donaldson, and
A. Seaton, “Ultrafine particles and nitrogen oxides generated by gas and
electric cooking,” Occupational and Environmental Medicine, vol. 58, no. 8, pp.
511–516, 2001. View at Publisher · View at Google Scholar · View at ScopusJ. I.
Levy, T. Dumyahn, and J. D. Spengler, “Particulate matter and polycyclic
aromatic hydrocarbon concentrations in indoor and outdoor microenvironments in
Boston, Massachusetts,” Journal of Exposure Analysis and Environmental
Epidemiology, vol. 12, no. 2, pp. 104–114, 2002. View at Publisher · View at
Google Scholar · View at ScopusU. Franck, O. Herbarth, B. Wehner, A.
Wiedensohler, and M. Manjarrez, “How do the indoor size distributions of
airborne submicron and ultrafine particles in the absence of significant indoor
sources depend on outdoor distributions?” Indoor Air, vol. 13, no. 2, pp.
174–181, 2003. View at Publisher · View at Google Scholar · View at ScopusB.
Brunekreef and S. T. Holgate, “Air pollution and health,” The Lancet, vol. 360,
no. 9341, pp. 1233–1242, 2002. View at Publisher · View at Google Scholar ·
View at PubMed · View at ScopusA. Peters, D. W. Dockery, J. E. Muller, and M.
A. Mittleman, “Increased particulate air pollution and the triggering of
myocardial infarction,” Circulation, vol. 103, no. 23, pp. 2810–2815, 2001.
View at ScopusY. J. Li, H. Takizawa, and T. Kawada, “Role of oxidative stresses
induced by diesel exhaust particles in airway inflammation, allergy and asthma:
their potential as a target of chemoprevention,” Inflammation and Allergy, vol.
9, no. 4, pp. 300–305, 2010. A. J. Ghio, C. Kim, and R. B. Devlin,
“Concentrated ambient air particles induce mild pulmonary inflammation in
healthy human volunteers,” American Journal of Respiratory and Critical Care
Medicine, vol. 162, no. 3 I, pp. 981–988, 2001. View at ScopusK. Donaldson and
V. Stone, “Current hypotheses on the mechanisms of toxicity of ultrafine
particles,” Annali dell'Istituto Superiore di Sanita, vol. 39, no. 3, pp. 405–410,
2003. View at ScopusX. Y. Li, D. Brown, S. Smith, W. MacNee, and K. Donaldson,
“Short-term inflammatory responses following intratracheal instillation of fine
and ultrafine carbon black in rats,” Inhalation Toxicology, vol. 11, no. 8, pp.
709–731, 1999. View at ScopusY. Bai, A. K. Suzuki, and M. Sagai, “The cytotoxic
effects of diesel exhaust particles on human pulmonary artery endothelial cells
in vitro: role of active oxygen species,” Free Radical Biology and Medicine,
vol. 30, no. 5, pp. 555–562, 2001. View at Publisher · View at Google Scholar ·
View at ScopusS. Hirano, A. Furuyama, E. Koike, and T. Kobayashi,
“Oxidative-stress potency of organic extracts of diesel exhaust and urban fine
particles in rat heart microvessel endothelial cells,” Toxicology, vol. 187,
no. 2-3, pp. 161–170, 2003. View at Publisher · View at Google Scholar · View
at ScopusL. E. Wold, B. Z. Simkhovich, M. T. Kleinman et al., “In vivo and in
vitro models to test the hypothesis of particle-induced effects on cardiac function
and arrhythmias,” Cardiovascular Toxicology, vol. 6, no. 1, pp. 69–78, 2006.
View at Publisher · View at Google Scholar · View at ScopusH. Jaeschke,
“Reactive oxygen and mechanisms of inflammatory liver injury: present
concepts,” Journal of Gastroenterology and Hepatology, vol. 26, no. 1, pp.
173–179, 2011. View at Publisher · View at Google Scholar · View at PubMed ·
View at ScopusL. Risom, P. Møller, and S. Loft, “Oxidative stress-induced DNA
damage by particulate air pollution,” Mutation Research, vol. 592, no. 1-2, pp.
119–137, 2005. View at Publisher · View at Google Scholar · View at PubMed ·
View at ScopusJ. Schnelle-Kreis, U. Küpper, M. Sklorz et al., “Daily
measurement of organic compounds in ambient particulate matter in Augsburg,
Germany: new aspects on aerosol sources and aerosol related health effects,”
Biomarkers, vol. 14, no. 1, pp. 39–44, 2009. View at Publisher · View at Google
Scholar · View at PubMed · View at ScopusP. MØller and S. Loft, “Oxidative
damage to DNA and lipids as biomarkers of exposure to air pollution,”
Environmental Health Perspectives, vol. 118, no. 8, pp. 1126–1136, 2010. View
at Publisher · View at Google Scholar · View at PubMed · View at ScopusA.
Valavanidis, K. Fiotakis, and T. Vlachogianni, “Airborne particulate matter and
human health: toxicological assessment and importance of size and composition
of particles for oxidative damage and carcinogenic mechanisms,” Journal of
Environmental Science and Health C, vol. 26, no. 4, pp. 339–362, 2008. View at
Publisher · View at Google Scholar · View at PubMed · View at ScopusH. A. Jeng,
“Chemical composition of ambient particulate matter and redox activity,”
American Journal of Physiology Lung Cell Molecular Physiology,
vol. 293, pp. 170–181, 2007. H. Andersson, E. Piras, J. Demma, and B. Hellman,
“Low levels of the air pollutant 1-nitropyrene induce DNA damage, increased
levels of reactive oxygen species and endoplasmic reticulum stress in human
endothelial cells,” Toxicology, vol. 262, no. 1, pp. 57–64, 2009. View at Publisher
· View at Google Scholar · View at PubMed · View at ScopusJ. H. Park, A. B.
Troxel, R. G. Harvey, and T. M. Penning, “Polycyclic aromatic hydrocarbon (PAH)
o-quinones produced by the Aldo-Keto-Reductases (AKRs) generate abasic sites,
oxidized pyrimidines, and 8-Oxo-dGuo via reactive oxygen species,” Chemical
Research in Toxicology, vol. 19, no. 5, pp. 719–728, 2006. View at Publisher ·
View at Google Scholar · View at PubMed · View at ScopusA. J. Ghio, J. H.
Richards, J. D. Carter, and M. C. Madden, “Accumulation of iron in the rat lung
after tracheal instillation of diesel particles,” Toxicologic Pathology, vol.
28, no. 4, pp. 619–627, 2000. View at ScopusP. Gerde, B. A. Muggenburg, M.
Lundborg, Y. Tesfaigzi, and A. R. Dahl, “Respiratory epithelial penetration and
clearance of particle-borne benzo[a]pyrene,” Research Report, vol. 101, pp.
5–27, 2001. View at ScopusK. B. Kim and B. M. Lee, “Oxidative stress to DNA,
protein, and antioxidant enzymes (superoxide dismutase and catalase) in rats
treated with benzo(a)pyrene,” Cancer Letters, vol. 113, no. 1-2, pp. 205–212,
1997. View at Publisher · View at Google Scholar · View at ScopusN. Uzma, S. S.
Kumar, and M. A. H. Hazari, “Exposure to benzene induces oxidative stress,
alters the immune response and expression of p53 in gasoline filling workers,”
American Journal of Industrial Medicine, vol. 53, no. 12, pp. 1264–1270, 2010.
View at Publisher · View at Google Scholar · View at PubMed · View at ScopusM.
Sørensen, H. Skov, H. Autrup, O. Hertel, and S. Loft, “Urban benzene exposure
and oxidative DNA damage,” Science of the Total Environment, vol. 309, no. 1–3,
pp. 69–80, 2003. View at Publisher · View at Google Scholar · View at PubMed ·
View at ScopusH. H. Liu, Y. C. Wu, and H. L. Chen, “Production of ozone and
reactive oxygen species after welding,” Archives of Environmental Contamination
and Toxicology, vol. 53, no. 4, pp. 513–518, 2007. View at Publisher · View at
Google Scholar · View at PubMed · View at ScopusA. Baulig, M. Garlatti, V.
Bonvallot et al., “Involvement of reactive oxygen species in the metabolic
pathways triggered by diesel exhaust particles in human airway epithelial
cells,” American Journal of Physiology, vol. 285, no. 3, pp. L671–L679, 2003.
View at ScopusN. Li, C. Sioutas, A. Cho et al., “Ultrafine particulate
pollutants induce oxidative stress and mitochondrial damage,” Environmental
Health Perspectives, vol. 111, no. 4, pp. 455–460, 2003. View at ScopusN.
Amara, R. Bachoual, M. Desmard et al., “Diesel exhaust particles induce matrix
metalloprotease-1 in human lung epithelial cells via a NADP(H) oxidase/NOX4
redox-dependent mechanism,” American Journal of Physiology, vol. 293, no. 1,
pp. L170–L181, 2007. View at Publisher · View at Google Scholar · View at
PubMed · View at ScopusK. W. Kang, S. J. Lee, and S. G. Kim, “Molecular
mechanism of Nrf2 activation by oxidative stress,” Antioxidants and Redox
Signaling, vol. 7, no. 11-12, pp. 1664–1673, 2005. View at Publisher · View at
Google Scholar · View at PubMed · View at ScopusJ. D. Hayes and M. McMahon,
“NRF2 and KEAP1 mutations: permanent activation of an adaptive response in
cancer,” Trends in Biochemical Sciences, vol. 34, no. 4, pp. 176–188, 2009.
View at Publisher · View at Google Scholar · View at PubMed · View at ScopusA.
H. Sprague and R. A. Khalil, “Inflammatory cytokines in vascular dysfunction
and vascular disease,” Biochemical Pharmacology, vol. 78, no. 6, pp. 539–552,
2009. View at Publisher · View at Google Scholar · View at PubMed · View at
ScopusK. Katsouyanni, “Ambient air pollution and health,” British Medical
Bulletin, vol. 68, pp. 143–156, 2003. View at Publisher · View at Google
Scholar · View at ScopusB. G. Nichols, J. S. Woods, D. L. Luchtel, J. Corral,
and J. Q. Koenig, “Effects of ozone exposure on nuclear factor-κB activation
and tumor necrosis factro-α expression in human nasal epithelial cells,”
Toxicological Sciences, vol. 60, no. 2, pp. 356–362, 2001. View at Publisher ·
View at Google Scholar · View at ScopusD. Bassett, C. Elbon-Copp, S. Otterbein,
H. Barraclough-Mitchell, M. DeLorme, and H. Yang, “Inflammatory cell
availability affects ozone-induced lung damage,” Journal of Toxicology and
Environmental Health A, vol. 64, no. 7, pp. 547–565, 2001. View at Publisher ·
View at Google Scholar · View at PubMed · View at Scopus WHO, “Air quality
guidelines: for Europe,” World Health Organization Regional Publications, no.
91, pp. 1–287, 2001. View at ScopusW. Yang and S. T. Omaye, “Air pollutants,
oxidative stress and human health,” Mutation Research, vol. 674, no. 1-2, pp.
45–54, 2009. View at Publisher · View at Google Scholar · View at PubMed · View
at ScopusB. Kosmider, J. E. Loader, R. C. Murphy, and R. J. Mason, “Apoptosis
induced by ozone and oxysterols in human alveolar epithelial cells,” Free
Radical Biology and Medicine, vol. 48, no. 11, pp. 1513–1524, 2010. View at
Publisher · View at Google Scholar · View at PubMed · View at ScopusH. Bayram,
R. J. Sapsford, M. M. Abdelaziz, and O. A. Khair, “Effect of ozone and nitrogen
dioxide on the release of proinflammatory mediators from bronchial epithelial
cells of nonatopic nonasthmatic subjects and atopic asthmatic patients in
vitro,” Journal of Allergy and Clinical Immunology, vol. 107, no. 2, pp.
287–294, 2001. View at Publisher · View at Google Scholar · View at PubMed ·
View at ScopusM. L. Bell, R. D. Peng, F. Dominici, and J. M. Samet, “Emergency
hospital admissions for cardiovascular diseases and ambient levels of carbon
monoxide results for 126 united states urban counties,” Circulation, vol. 120,
no. 11, pp. 949–955, 2009. View at Publisher · View at Google Scholar · View at
PubMed · View at ScopusG. Barreto, D. Madureira, F. Capani, L. Aon-Bertolino,
E. Saraceno, and L. D. Alvarez-Giraldez, “The role of catechols and free
radicals in benzene toxicity: an oxidative DNA damage pathway,” Environmental
and Molecular Mutagenesis, vol. 50, no. 9, pp. 771–780, 2009. View at Publisher
· View at Google Scholar · View at PubMed · View at ScopusJ. L. Bolton, M. A.
Trush, T. M. Penning, G. Dryhurst, and T. J. Monks, “Role of quinones in
toxicology,” Chemical Research in Toxicology, vol. 13, no. 3, pp. 135–160,
2000. View at Publisher · View at Google Scholar · View at ScopusU. Pöschl,
“Atmospheric aerosols: composition, transformation, climate and health
effects,” Angewandte Chemie, vol. 44, no. 46, pp. 7520–7540, 2005. View at
Publisher · View at Google Scholar · View at PubMed · View at ScopusE. Boldo,
C. Linares, J. Lumbreras et al., “Health impact assessment of a reduction in
ambient PM(2.5) levels in Spain,” Environment International, vol. 37, no. 2,
pp. 342–348, 2011. View at Publisher · View at Google Scholar · View at PubMed
· View at ScopusG. L. Squadrito, R. Cueto, B. Dellinger, and W. A. Pryor,
“Quinoid redox cycling as a mechanism for sustained free radical generation by
inhaled airborne particulate matter,” Free Radical Biology and Medicine, vol.
31, no. 9, pp. 1132–1138, 2001. View at Publisher · View at Google Scholar ·
View at ScopusB. J. Finlayson-Pitts Jr. and J. N. Pitts, “Tropospheric air
pollution: ozone, airborne toxics, polycyclic aromatic hydrocarbons, and
particles,” Science, vol. 276, no. 5315, pp. 1045–1052, 1997. View at Publisher
· View at Google Scholar · View at ScopusV. Bonvallot, A. Baeza-Squiban, A.
Baulig et al., “Organic compounds from diesel exhaust particles elicit a
proinflammatory response in human airway epithelial cells and induce cytochrome
p450 1A1 expression,” American Journal of Respiratory Cell and Molecular
Biology, vol. 25, no. 4, pp. 515–521, 2001. View at ScopusA. Valavanidis, K. Fiotakis,
E. Bakeas, and T. Vlahogianni, “Electron paramagnetic resonance study of the
generation of reactive oxygen species catalysed by transition metals and
quinoid redox cycling by inhalable ambient particulate matter,” Redox Report,
vol. 10, no. 1, pp. 37–51, 2005. View at Publisher · View at Google Scholar ·
View at PubMed · View at ScopusJ. Y. C. Ma and J. K. H. Ma, “The dual effect of
the particulate and organic components of diesel exhaust particles on the
alteration of pulmonary immune/inflammatory responses and metabolic enzymes,”
Journal of Environmental Science and Health C, vol. 20, no. 2, pp. 117–147,
2002. View at Publisher · View at Google Scholar · View at PubMed · View at
ScopusA. Shukla, C. Timblin, K. BeruBe et al., “Inhaled particulate matter
causes expression of nuclear factor (NF)-κB-related genes and oxidant-dependent
NF-κB activation in vitro,” American Journal of Respiratory Cell and Molecular
Biology, vol. 23, no. 2, pp. 182–187, 2000. View at ScopusR. Li, Z. Ning, R.
Majumdar et al., “Ultrafine particles from diesel vehicle emissions at
different driving cycles induce differential vascular pro-inflammatory
responses: implication of chemical components and NF-κB signaling,” Particle
and Fibre Toxicology, vol. 7, no. 1, pp. 6–18, 2010. View at Publisher · View
at Google Scholar · View at PubMed · View at ScopusR. Li, Z. Ning, J. Cui et
al., “Ultrafine particles from diesel engines induce vascular oxidative stress
via JNK activation,” Free Radical Biology and Medicine, vol. 15, no. 46, pp.
775–782, 2009. View at Publisher · View at Google Scholar · View at PubMed ·
View at ScopusK. S. Kouassi, S. Billet, G. Garçon et al., “Oxidative damage
induced in A549 cells by physically and chemically characterized air
particulate matter (PM2.5) collected in Abidjan, Côte d'Ivoire,” Journal of
Applied Toxicology, vol. 30, no. 4, pp. 310–320, 2010. View at Publisher · View
at Google Scholar · View at PubMed · View at ScopusA. Saxon and D.
Diaz-Sanchez, “Air pollution and allergy: you are what you breathe,” Nature
Immunology, vol. 6, no. 3, pp. 223–226, 2005. View at Publisher · View at
Google Scholar · View at PubMed · View at ScopusE. Vidrio, H. Jung, and C.
Anastasio, “Generation of hydroxyl radicals from dissolved transition metals in
surrogate lung fluid solutions,” Atmospheric Environment, vol. 42, no. 18, pp.
4369–4379, 2008. View at Publisher · View at Google Scholar · View at PubMed ·
View at ScopusP. J. Schaumann, J. Borm, A. Herbrich et al., “Metal-rich ambient
particles (particulate matter2.5) cause airway inflammation in healthy
subjects,” American Journal of Respiratory and Critical Care Medicine, vol.
170, no. 8, pp. 898–903, 2004. View at Publisher · View at Google Scholar ·
View at PubMed · View at ScopusM. E. Gerlofs-Nijland, J. A. M. A. Dormans, H.
J. T. Bloemen et al., “Toxicity of coarse and fine particulate matter from
sites with contrasting traffic profiles,” Inhalation Toxicology, vol. 19, no.
13, pp. 1055–1069, 2007. View at Publisher · View at Google Scholar · View at
PubMed · View at ScopusA. M. Knaapen, T. Shi, P. J. A. Borm, and R. P. F.
Schins, “Soluble metals as well as the insoluble particle fraction are involved
in cellular DNA damage induced by particulate matter,” Molecular and Cellular
Biochemistry, vol. 234-235, pp. 317–326, 2002. View at Publisher · View at
Google Scholar · View at ScopusA. Peters, H. E. Wichmann, T. Tuch, J. Heinrich,
and J. Heyder, “Respiratory effects are associated with the number of ultrafine
particles,” American Journal of Respiratory and Critical Care Medicine, vol.
155, no. 4, pp. 1376–1383, 1997. View at ScopusC. A. Pope, J. B. Muhlestein, H.
T. May, D. G. Renlund, J. L. Anderson, and B. D. Horne, “Ischemic heart disease
events triggered by short-term exposure to fine particulate air pollution,” Circulation,
vol. 114, no. 23, pp. 2443–2448, 2006. View at Publisher · View at Google
Scholar · View at PubMed · View at ScopusR. J. Delfino, C. Sioutas, and S.
Malik, “Potential role of ultrafine particles in associations between airborne
particle mass and cardiovascular health,” Environmental Health Perspectives,
vol. 113, no. 8, pp. 934–946, 2005. View at Publisher · View at Google Scholar
· View at ScopusR. D. Brook, J. R. Brook, B. Urch, R. Vincent, S. Rajagopalan,
and F. Silverman, “Inhalation of fine particulate air pollution and ozone
causes acute arterial vasoconstriction in healthy adults,” Circulation, vol.
105, no. 13, pp. 1534–1536, 2002. View at Publisher · View at Google Scholar ·
View at ScopusB. Urch, F. Silverman, P. Corey et al., “Acute blood pressure
responses in healthy adults during controlled air pollution exposures,”
Environmental Health Perspectives, vol. 113, no. 8, pp. 1052–1055, 2005. View
at Publisher · View at Google Scholar · View at ScopusH. Hwang, R. A. Kloner,
M. T. Kleinman, and B. Z. Simkhovich, “Direct and acute cardiotoxic effects of
ultrafine air pollutants in spontaneously hypertensive rats and Wistar-Kyoto
rats,” Journal of Cardiovascular Pharmacology and Therapeutics, vol. 13, no. 3,
pp. 189–198, 2008. View at Publisher · View at Google Scholar · View at PubMed
· View at ScopusB. Z. Simkhovich, P. Marjoram, M. T. Kleinman, and R. A.
Kloner, “Direct and acute cardiotoxicity of ultrafine particles in young adult
and old rat hearts,” Basic Research in Cardiology, vol. 102, no. 6, pp.
467–475, 2006. View at Publisher · View at Google Scholar · View at PubMed ·
View at ScopusQ. Sun, A. Wang, X. Jin et al., “Long-term air pollution exposure
and acceleration of atherosclerosis and vascular inflammation in an animal
model,” Journal of the American Medical Association, vol. 294, no. 23, pp.
3003–3010, 2005. View at Publisher · View at Google Scholar · View at PubMed ·
View at ScopusT. Suwa, J. C. Hogg, K. B. Quinlan, A. Ohgami, R. Vincent, and S.
F. Van Eeden, “Particulate air pollution induces progression of
atherosclerosis,” Journal of the American College of Cardiology, vol. 39, no.
6, pp. 935–942, 2002. View at Publisher · View at Google Scholar · View at
ScopusG. C. Chuang, Z. Yang, D. G. Westbrook et al., “Pulmonary ozone exposure
induces vascular dysfunction, mitochondrial damage, and atherogenesis,”
American Journal of Physiology, vol. 297, no. 2, pp. L209–L216, 2009. View at
Publisher · View at Google Scholar · View at PubMed · View at ScopusM. J.
Campen, A. K. Lund, T. L. Knuckles et al., “Inhaled diesel emissions alter
atherosclerotic plaque composition in ApoE(-/-) mice,” Toxicology and Applied
Pharmacology, vol. 242, no. 3, pp. 310–317, 2010. View at Publisher · View at
Google Scholar · View at PubMed · View at ScopusT. W. Cherng, M. L. Paffett, O.
Jackson-Weaver, M. J. Campen, B. R. Walker, and N. L. Kanagy, “Mechanisms of
diesel-induced endothelial nitric oxide synthase dysfunction in coronary
arterioles,” Environmental Health Perspectives, vol. 119, no. 1, pp. 98–103, 2011.
View at Publisher · View at Google Scholar · View at PubMedA. Baccarelli, A.
Zanobetti, I. Martinelli et al., “Effects of exposure to air pollution on blood
coagulation,” Journal of Thrombosis and Haemostasis, vol. 5, no. 2, pp.
252–260, 2007. View at Publisher · View at Google Scholar · View at PubMed ·
View at ScopusE. S. Baja, J. D. Schwartz, G. A. Wellenius et al.,
“Traffic-related air pollution and QT interval: modification by diabetes,
obesity, and oxidative stress gene polymorphisms in the normative aging study,”
Environmental Health Perspectives, vol. 118, no. 6, pp. 840–846, 2010. View at
Publisher · View at Google Scholar · View at PubMed · View at ScopusI.
Mordukhovich, E. Wilker, H. Suh et al., “Black carbon exposure, oxidative
stress genes, and blood pressure in a repeated-measures study,” Environmental
Health Perspectives, vol. 117, no. 11, pp. 1767–1772, 2009. View at Publisher ·
View at Google Scholar · View at PubMed · View at ScopusL. Liu, T. Ruddy, M.
Dalipaj et al., “Effects of indoor, outdoor, and personal exposure to
particulate air pollution on cardiovascular physiology and systemic mediators
in seniors,” Journal of Occupational and Environmental Medicine, vol. 51, no.
9, pp. 1088–1098, 2009. View at Publisher · View at Google Scholar · View at
PubMed · View at ScopusI. M. Kooter, M. E. Gerlofs-Nijland, A. J. Boere, et
al., “Diesel engine exhaust initiates a sequence of pulmonary and
cardiovascular effects in rats,” Environmental Health Perspectives, vol. 118,
no. 8, pp. 1126–1136, 2010. L. J. den Hartigh, M. W. Lamé, W. Ham, M. J.
Kleeman, F. Tablin, and D. W. Wilson, “Endotoxin and polycyclic aromatic
hydrocarbons in ambient fine particulate matter from Fresno, California
initiate human monocyte inflammatory responses mediated by reactive oxygen
species,” Toxicology in Vitro, vol. 24, no. 7, pp. 1993–2002, 2010. View at
Publisher · View at Google Scholar · View at PubMed · View at ScopusI.
Ferecatu, M. C. Borot, C. Bossard et al., “Polycyclic aromatic hydrocarbon
components contribute to the mitochondria-antiapoptotic effect of fine
particulate matter on human bronchial epithelial cells via the aryl hydrocarbon
receptor,” Particle and Fibre Toxicology, vol. 7, no. 1, pp. 18–32, 2010. View
at Publisher · View at Google Scholar · View at PubMed · View at ScopusA.
Baulig, M. Garlatti, V. Bonvallot et al., “Involvement of reactive oxygen
species in the metabolic pathways triggered by diesel exhaust particles in
human airway epithelial cells,” American Journal of Physiology, vol. 285, no. 3,
pp. L671–L679, 2003. View at ScopusA. Churg, C. Xie, X. Wang, R. Vincent, and
R. D. Wang, “Air pollution particles activate NF-κB on contact with airway
epithelial cell surfaces,” Toxicology and Applied Pharmacology, vol. 208, no.
1, pp. 37–45, 2005. View at Publisher · View at Google Scholar · View at PubMed
· View at ScopusJ. Topinka, L. R. Schwarz, F. Kiefer et al., “DNA adduct
formation in mammalian cell cultures by polycyclic aromatic hydrocarbons (PAH)
and nitro-PAH in coke oven emission extract,” Mutation Research, vol. 419, no.
1–3, pp. 91–105, 1998. View at Publisher · View at Google Scholar · View at
ScopusL. A. Jimenez, J. Thompson, D. A. Brown et al., “Activation of NF-κB by
PM10 occurs via an iron-mediated mechanism in the absence of IκB degradation,”
Toxicology and Applied Pharmacology, vol. 15, no. 166, pp. 101–110, 2000. View
at Publisher · View at Google Scholar · View at PubMed · View at ScopusS.
Becker, L. A. Dailey, J. M. Soukup, S. C. Grambow, R. B. Devlin, and Y. C. T.
Huang, “Seasonal variations in air pollution particle-induced inflammatory
mediator release and oxidative stress,” Environmental Health Perspectives, vol.
113, no. 8, pp. 1032–1038, 2005. View at Publisher · View at Google Scholar ·
View at ScopusS. Becker, S. Mundandhara, R. B. Devlin, and M. Madden,
“Regulation of cytokine production in human alveolar macrophages and airway
epithelial cells in response to ambient air pollution particles: further
mechanistic studies,” Toxicology and Applied Pharmacology, vol. 207, no. 2, supplement,
pp. S269–S275, 2005. View at Publisher · View at Google Scholar · View at
PubMed · View at ScopusS. S. Salvi, C. Nordenhall, A. Blomberg et al., “Acute
exposure to diesel exhaust increases IL-8 and GRO-α production in healthy human
airways,” American Journal of Respiratory and Critical Care Medicine, vol. 161,
no. 2 I, pp. 550–557, 2000. View at ScopusE. D. Karoly, Z. Li, X. Hyseni, and
Y. C. T. Huang, “Up-regulation of tissue factor in human pulmonary artery
endothelial cells after ultrafine particle exposure,” Environmental Health
Perspectives, vol. 115, no. 4, pp. 535–540, 2007. View at Publisher · View at
Google Scholar · View at PubMed · View at ScopusH. Ishii, S. Hayashi, J. C.
Hogg et al., “Alveolar macrophage-epithelial cell interaction following
exposure to atmospheric particles induces the release of mediators involved in
monocyte mobilization and recruitment,” Respiratory Research, vol. 6, pp.
87–99, 2005. View at Publisher · View at Google Scholar · View at PubMed · View
at ScopusG. Oberdörster, “Significance of particle parameters in the evaluation
of exposure-dose-response relationships of inhaled particles,” Inhalation
Toxicology, vol. 8, pp. 73–89, 1996. View at ScopusM. Sørensen, R. P. F.
Schins, O. Hertel, and S. Loft, “Transition metals in personal samples of PM2.5
and oxidative stress in human volunteers,” Cancer Epidemiology Biomarkers and
Prevention, vol. 14, no. 5, pp. 1340–1343, 2005. View at Publisher · View at
Google Scholar · View at PubMed · View at ScopusS. Bae, X. C. Pan, S. Y. Kim et
al., “Exposures to particulate matter and polycyclic aromatic hydrocarbons and
oxidative stress in schoolchildren,” Environmental Health Perspectives, vol.
118, no. 4, pp. 579–583, 2010. View at Publisher · View at Google Scholar ·
View at PubMed · View at ScopusH. Song, W. Tan, and X. Zhang, “Ozone induces
inflammation in bronchial epithelial cells,” Journal of Asthma, vol. 48, no. 1,
pp. 79–83, 2011. View at Publisher · View at Google Scholar · View at PubMedI.
S. Mudway and F. J. Kelly, “Ozone and the lung: a sensitive issue,” Molecular
Aspects of Medicine, vol. 21, no. 1–2, pp. 1–48, 2000. View at Publisher · View
at Google Scholar · View at ScopusB. Kosmider, J. E. Loader, R. C. Murphy, and
R. J. Mason, “Apoptosis induced by ozone and oxysterols in human alveolar
epithelial cells,” Free Radical Biology and Medicine, vol. 48, no. 11, pp.
1513–1524, 2010. View at Publisher · View at Google Scholar · View at PubMed ·
View at ScopusK. Triantaphyllopoulos, F. Hussain, M. Pinart et al., “A model of
chronic inflammation and pulmonary emphysema after multiple ozone exposures in
mice,” American Journal of Physiology, vol. 300, no. 5, pp. L691–L700, 2011.
View at Publisher · View at Google Scholar · View at PubMedY. I. Chirino, Y.
Sánchez-Pérez, Á. R. Osornio-Vargas et al., “PM10 impairs the antioxidant
defense system and exacerbates oxidative stress driven cell death,” Toxicology
Letters, vol. 193, no. 3, pp. 209–216, 2010. View at Publisher · View at Google
Scholar · View at PubMed · View at ScopusY. Bagryantseva, B. Novotna, P.
Rossner et al., “Oxidative damage to biological macromolecules in Prague bus
drivers and garagemen: impact of air pollution and genetic polymorphisms,”
Toxicology Letters, vol. 199, no. 1, pp. 60–68, 2010. View at Publisher · View
at Google Scholar · View at PubMed · View at ScopusR. J. Delfino, N. Staimer,
T. Tjoa et al., “Associations of primary and secondary organic aerosols with
airway and systemic inflammation in an elderly panel cohort,” Epidemiology,
vol. 21, no. 6, pp. 892–902, 2010. View at Publisher · View at Google Scholar ·
View at PubMed · View at ScopusF. J. Kelly and T. D. Tetley, “Nitrogen dioxide
depletes uric acid and ascorbic acid but not glutathione from lung lining
fluid,” Biochemical Journal, vol. 325, no. 1, pp. 95–99, 1997. View at ScopusA.
F. Behndig, I. S. Mudway, J. L. Brown et al., “Airway antioxidant and
inflammatory responses to diesel exhaust exposure in healthy humans,” European
Respiratory Journal, vol. 27, no. 2, pp. 359–365, 2006. View at Publisher ·
View at Google Scholar · View at PubMed · View at ScopusW. O. Osburn and T. W.
Kensler, “Nrf2 signaling: an adaptive response pathway for protection against
environmental toxic insults,” Mutation Research, vol. 659, no. 1-2, pp. 31–39,
2008. View at Publisher · View at Google Scholar · View at PubMed · View at
ScopusV. Rubio, J. Zhang, M. Valverde, E. Rojas, and Z. Z. Shi, “Essential role
of Nrf2 in protection against hydroquinone- and benzoquinone-induced
cytotoxicity,” Toxicology in Vitro, vol. 25, no. 2, pp. 521–529, 2010. View at
Publisher · View at Google Scholar · View at PubMed · View at ScopusV. Rubio,
M. Valverde, and E. Rojas, “Effects of atmospheric pollutants on the Nrf2
survival pathway,” Environmental Science and Pollution Research, vol. 17, no.
2, pp. 369–382, 2010. View at Publisher · View at Google Scholar · View at
PubMed · View at Scopus EPA, “Integrated science assessment for particulate
matter,” Provisional Draft (Personal communication), 2008.
No comments:
Post a Comment