Tuesday, May 6, 2014
published on http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3387329/
Lucchini RG,1,5 Dorman DC,2 Elder A,3 and Veronesi B4
The effects of inhaled particles have focused heavily on the respiratory and cardiovascular systems. Most studies have focused on inhaled metals, whereas less information is available for other particle types regarding the effects on the brain and other extra-pulmonary organs. We review here the available literature on nanoparticle uptake and transport through the olfactory pathway, the experimental data from animal and in vitro studies, and human epidemiological observations. Nanoparticles (< 0.1 μm in one dimension) may easily reach the brain from the respiratory tract via sensory neurons and transport from the distal alveoli into the blood or lymph as free particles or inside phagocytic cells. These mechanisms and subsequent biologic responses may be influenced by the chemical composition of inhaled particles. Animal studies with ambient particulate matter and certain other particles show alterations in neuro-inflammatory markers of oxidative stress and central neurodegeneration. Human observations indicate motor, cognitive, and behavioral changes especially after particulate metal exposure in children. Exposure to co-pollutants and/or underlying disease states could also impact both the biokinetics and effects of airborne particles in the brain. Data are needed from the areas of inhalation, neurology, and metal toxicology in experimental and human studies after inhalation exposure. An increased understanding of the neurotoxicity associated with air pollution exposure is critical to protect susceptible individuals in the workplace and the general population.
Olfactory transport of inhaled particles and metals
The olfactory system originates with specialized olfactory neurons found within the olfactory epithelium that lines a portion of the nasal cavity. Projections from the olfactory neurons form the olfactory nerve (cranial nerve I), which ultimately terminates in the olfactory bulb after the nerve tracts pass through the skull. Transport of xenobiotics – including particles – along the olfactory nerve provides a route (nose-to-brain) for delivery to the central nervous system (CNS) that bypasses the protective blood brain barrier.
Evaluation of nose-to-brain transport of xenobiotics is fraught with several technical challenges (Dhuria et al., 2010). To date, most experimental studies examining nose-to-brain transport have focused on metals and often used radiolabeled isotopes. Postmortem tissue collection can involve microdissection of the nasal cavity and brain or cryosectioning techniques coupled with autoradiography. Liquid scintillation, gamma spectrometry, mass spectrometry, proton induced X-ray emission (PIXE), atomic emission or absorption spectroscopy, and other more specialized analytical methods are used to quantify metal concentrations in tissues. The movement of paramagnetic metals can also be followed using brain magnetic resonance imaging (MRI). Some of these techniques are only semi-quantitative. Many experiments rely on intranasal delivery, typically by direct instillation of metal–containing solutions into one nostril. An alternative approach used in inhalation studies involves occluding one nostril, thus restricting olfactory transport to the side of the brain ipsilateral to the patent nostril. The reader is directed to the studies cited in this manuscript for more details concerning these and other methodological approaches.
The association between manganese (Mn) inhalation and neurotoxicity (Guilarte, 2010) has prompted investigators to examine the role of olfactory transport in the delivery of Mn to the brain. Initial studies examining direct nose-to-brain transport of Mn relied on intranasal instillation of 54Mn (as the soluble chloride salt) and documented the presence of 54Mn in the olfactory bulb of rats, mice, and freshwater pike on the side ipsilateral to the instilled nostril (Tjälve and Henriksson, 1999). These studies documented that ionic Mn crossed synapses within the olfactory pathway and traveled along secondary and tertiary neurons to more distal sites within the brain. Brenneman and coworkers (2000) were amongst the first to examine this transport route following Mn inhalation. Brenneman used an occluded nostril model and showed that delivery along the olfactory route accounted for nearly all of the 54Mn found in the olfactory bulb and tract of the rat brain following acute inhalation exposure. Lewis and coworkers (2005) reported that the rat trigeminal nerve may also deliver Mn from the nasal cavity to the brain. Olfactory transport rapidly (within 8–48 hr) delivers Mn to the olfactory bulb and tract. However, it appears to be relatively inefficient in delivering inhaled Mn to more distant brain structures. Using brain MRI, Cross et al. (2004) showed that nasally instilled Mn does not undergo transport to the rat striatum or other more distal brain structures. Likewise, Dorman and colleagues (2006) used brain MRI to demonstrate presumed olfactory transport of inhaled Mn sulfate – which is readily soluble in vivo – in rhesus monkeys. Dorman did not demonstrate evidence for direct translocation of Mn from the olfactory bulb to the globus pallidus, a known target for Mn neurotoxicity.
Much of the experimental evidence in support of the olfactory transport of Mn has come from rodent studies. Unlike people, rodents are obligate nasal breathers and have distinct airway turbinate and epithelial anatomy. These differences may affect Mn delivery to the olfactory epithelium and subsequent brain delivery. Although direct evidence for olfactory transport of Mn in people is currently lacking, this pathway is functional in human beings. Shiga et al. (2010) assessed the transport of nasally-administered thallium (201Tl) to the human brain in healthy volunteers using a combination of single photon emission computed tomography (SPECT), X-ray computed tomography (CT), and MRI. These studies demonstrated appreciable movement of Tl to the human olfactory bulb with transport kinetic properties that were most consistent with delivery via the olfactory nerve. These observations are consistent with results from rodent studies demonstrating olfactory transport of Tl (Kanayama et al., 2005), suggesting that the mechanisms involved in olfactory transport of metals are conserved across different species.
Transport mechanisms and the toxicological significance of olfactory transport of Mn remain poorly understood. Henriksson and Tjälve (2000) found that intranasal instillation of Mn resulted in alterations in olfactory bulb expression of glial fibrillary acidic protein (GFAP) and S-100b in rats, both of which are markers of astrocyte activation. In contrast, Dorman et al., (2004) did not observe changes in rat olfactory bulb GFAP concentrations following subchronic inhalation to Mn sulfate, even though olfactory bulb Mn concentrations were increased approximately 3.5-fold versus air-exposed controls. More recently, Villalobos et al. (2009) showed that the mouse olfactory bulb develops neuron degeneration and myelin sheath disorganization following high dose intraperitoneal Mn injection. Recent studies have suggested a role for divalent metal transporter (DMT-1) in Mn olfactory transport with enhanced transport occurring in anemic animals (Thompson et al., 2007).
Although direct nose-to-brain transport has garnered increased attention from neurotoxicologists, it is also important to note that certain metals do not undergo appreciable olfactory transport. For example, inhaled tungsten (Radcliffe et al., 2009) and iron (as the sulfate salt) are poorly transported from the nasal cavity (Rao et al., 2003). Evaluation of this type of toxicokinetic data can be assisted by the use of physiologically based pharmacokinetic models (PBPK) that have been developed to describe olfactory transport of Mn, tungsten, and iron (Leavens et al., 2007).
Air pollution is a complex mixture of gas- and particulate-phase components that has input from natural and anthropogenic sources. The composition of the particulate phase depends on the source(s), aerosol age, and size fraction and can include carbonaceous soot, metals, crustal elements, organics, and biologicals (e.g. pollens). Particles in ambient air exist in four size classes, with the smallest being the ultrafine or nanosized particles (NPs). Nanoparticles are defined as being <0 -="" .1="" a="" air="" an="" and="" anthropogenic="" are="" aria-expanded="false" aria-haspopup="true" as="" at="" atmosphere="" but="" by="" class="bibr popnode jig-ncbipopper" contribute="" dimension="" engineered="" exposure="" far="" href="http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3387329/#R12" in="" include="" least="" little="" m="" mass="" materials.="" most="" natural="" non-agglomerated="" numerous="" one="" or="" particles="" present="" rid="R12" role="button" singlet="" style="color: #642a8f;" the="" these="" to="" urban="" very="" when="">Finlayson-Pitts and Pitts, 2000
Using laboratory-generated model aerosols, studies of the biodistribution of poorly soluble NPs (carbonaceous, metal) have been performed. These studies have consistently found minute, but statistically significant, accumulation of NPs in extrapulmonary tissues, including liver, heart, kidney, spleen, and brain (Kreyling et al., 2009; Oberdörster et al., 2002; Semmler-Behnke et al., 2008). The work of Kreyling and colleagues has, in addition, demonstrated that this response is size-dependent (greater accumulation for smaller particles), but particle type-independent (Kreyling et al., 2009;Semmler-Behnke et al., 2008). Because of the exposure route (intratracheal inhalation), these studies did not directly examine the route by which NPs or their constituents entered the brain or if they indeed passed the blood-brain barrier.
Work done with elemental carbon NPs (very poorly-soluble) that were delivered to rats by whole-body inhalation exposure demonstrated that the olfactory bulb was a site of NP accumulation (Oberdörster et al., 2002). Uptake and transport by the olfactory nerve or perineural transport could account for the observed uptake. Elder and coworkers (2006) also employed freshly-generated Mn oxide NP-containing aerosols (to simulate welding fume) to expose rats via whole-body inhalation, which led to increases in olfactory bulb, striatum, cortex, and cerebellum Mn content. Although the Mn oxide particles were very poorly soluble, the contribution to the increases in brain from absorption in the deep lung and gastrointestinal tract could not be ruled out. However, when short-term exposures were conducted with the right olfactory bulb occluded, Mn accumulated only in the left olfactory bulb. These data support the idea that at least the early Mn accumulation occurs via olfactory transport. This finding is consistent with other studies using more soluble forms of Mn (Brenneman et al., 2000).
Evidence for Air Pollution-Induced Neurotoxicity
Early evidence linking air pollution and neurotoxicity was provided by Calderón-Garcidueñas and coworkers (2003), who reported neuropathological lesions in feral dogs living in Mexico City. Inflammation of the olfactory bulb and deficits in olfaction have also been observed in Mexican children residing in highly polluted areas (Calderón-Garcidueñas et al., 2010). Alpha-synuclein neuronal aggregation, an early neuropathological hallmark of sporadic Parkinson's disease, and accumulation of 3 nitrotyrosine and 8-hydroxydeoxyguanosine (8-OHdG), evidence of oxidative stress, were also detected in these children's brainstem nuclei (Calderón-Garcidueñas et al., 2011).
As mentioned earlier, the association between inhalation of certain metals and neurotoxicity has also been established. One case in point is definitely Mn neurotoxicity. For example, motor, cognitive and behavioral functions were assessed in healthy children (11–14 years old) and elderly (65–75 years old) residents in Valcamonica, Italy. In this area, an increased prevalence of parkinsonism had been observed in relationship with the Mn levels in the deposited dust from ferroalloy airborne emissions (Lucchini et al., 2007). Individual exposure to airborne particles was assessed with 24 hour personal sampling and chemical analysis of metal concentration in the filters. Soil metal concentrations were also assessed as a proxy of cumulative exposure from airborne emissions. Several associations were observed between Mn exposure and abnormalities of motor and olfactory functions in both age groups. Regression models showed impairment of motor coordination (Luria-Nebraska test, p=0.0005), hand dexterity (Aiming Pursuit test, p= 0.0115) and odor identification (Sniffin' task, p=0.003) associated with soil Mn concentrations, and tremor intensity with hair (p=0.01) and blood Mn (p=0.005), among the adolescents of the impacted area (Lucchini et al., this issue). The elderly subjects residing in the same areas showed similar impairment of motor coordination, hand dexterity and odor identification as the adolescents (Rentschler et al., this issue). The influence of genetic polymorphism was assessed considering the ATP13A2 gene, also known as PARK9, for a protective role in both Parkinson's Diseases and Mn toxicity (Gitler, 2009). Polymorphisms rs4920608 and rs2871776 significantly modified the effects of Mn exposure on impaired motor coordination in elderly (p for interaction= 0.03, p= 0.04 respectively), also after adjustments for age and gender (Rentschler et al., this issue). In addition, the rs2871776 G allele that was associated with the worst effect of Mn on motor coordination was linked to alteration of a binding site for the transcription factor Insulinoma-associated 1 (INSM1). This gene plays an important role in the developing CNS, and especially of olfactory progenitors, as shown in mouse (Rosenbaum et al., 2011) and human embryos (Duggan et al., 2008).
While the accumulation of NPs in brain, whether in the CNS parenchyma or in the vasculature, has been clearly demonstrated, less information is available concerning potential health-related outcome(s) from this exposure. Elder and coworkers (2006) showed increases in pro-inflammatory mediators and markers of oxidative stress and immune cell activation (e.g. tumor necrosis factor -α (TNF-α), superoxide dismutase, and GFAP) in rat brain regions where Mn accumulated following Mn oxide NP exposure. These findings suggest that NP exposure resulted in CNS oxidative stress and inflammation.
Particle Exposure, Oxidative Stress, and Neurotoxicity
When reports began emerging in the epidemiological literature suggesting that inhaled ambient particulate-containing air pollution could induce adverse cardiovascular health outcomes (Peters et al., 2000; Pope et al., 1999; Schwartz et al., 1999), the underlying mechanisms that might explain the observations were unclear. Two plausible mechanisms that were pursued were 1) the release of soluble mediators (inflammatory and/or hormonal) from respiratory tract target cells and 2) the translocation of air pollution constituents out of the lungs to secondary target tissues. Similar mechanisms may serve as plausible explanations for responses of the CNS following pollutant exposure.
The association between oxidative stress, inflammatory processes, and neurodegenerative disease is being currently investigated. For example, a two-fold faster rate of decline in Alzheimer's disease (AD) patients is associated with acute systemic inflammation as determined via increases in serum TNF-α (Holmes et al., 2009). Furthermore, McAlpine and colleagues (2009) showed that the inhibition of TNF signaling significantly reduced amyloid beta protein deposition in brain in a mouse model of AD.
Subsequent studies with an oxidative stress-compromised (i.e., ApoE −/−) mouse model and their normal C57BL/6 background strain have shed additional light on the role of oxidative stress in particulate matter (PM)-induced neurotoxicity (Veronesi et al., 2005). Veronesi exposed these mice to concentrated ambient particulate matter (CAPs) collected from a state park in Tuxedo, NY. After the 6–7 month exposure, the mice were killed and formalin-perfused. The brains were serially sectioned and immunohistologically stained for tyrosine hydroxylase (TH), a marker for dopaminergic neurons and for GFAP, a marker of astrocytic proliferation. TH-neuronal loss in the substantia nigra was analyzed morphometrically. No significant differences in air or CAPs-exposed wild-type mice were seen. However, a 29% reduction in TH-neuronal loss was shown in the CAPs exposed brains of Apo E −/− mice relative to air-exposed Apo E −/− mice. This established oxidative stress as a predisposing condition for the brain damage associated with particulate matter air pollution (Veronesi et al., 2005).
Since microglia (brain macrophages) are critical to oxidative stress-mediated neurodegeneration (Block et al., 2007), the BV2 cells (immortalized mouse (C57/BL6) microglial cell line) were exposed to samples of CAPs and their cellular and genomic response examined. Exposure of the BV2 microglia to CAPs reduced intracellular levels of ATP and stimulated pro-inflammatory cytokines TNF-α and interleukin-6 after 6 hr of exposures. Microarrays on the CAPs exposed BV2 microglia indicated that exposure stimulated genes associated with innate immune pathways (e.g., Toll Like Receptor signaling), oxidative stress-mediated inflammation (e.g., Notch activating pathway for nuclear factor-kB signaling), and multiple pro-apoptotic pathways (Sama et al., 2007). The mechanism(s) underlying PM-CNS toxicity are still unresolved but these and other studies suggest that neurotoxicity in the PM-exposed animals is related to oxidative stress and innate immune pathways.
The “nose-brain” interaction as a route of entry for air pollutants is a topic of emerging interest that deserves further research, especially considering the possibility that NP can be transported to target brain areas. The transport of other toxic components of air pollution, such as gases (ozone, carbon monoxide, sulfur oxides, nitrogen oxides), organic compounds (polycyclic aromatic hydrocarbons and endotoxins) and metals (vanadium, nickel, manganese) also need to be considered. In vivo and in vitro evidence supports the epidemiological evidence of neurotoxicity following exposure to air pollution, with an important role played by the olfactory tract. Although mechanisms driving air pollution-induced CNS pathology are poorly understood, new evidence suggests that microglial activation may be a key component, with an important contribution of conditions that predispose the individual to oxidative stress. In summary, although the transport of airborne particles and NP is demonstrated through the olfactory tract, further research must be addressed to explain the mechanisms of toxicity, focusing on the inflammatory changes that are induced by this type of exposure. Early data also suggests that children may be at particular risk from air pollution exposure since childhood and adolescence are crucial periods of brain development associated with dynamic behavioral, cognitive and emotional changes.
RL research is supported by funding from the European Union through its Sixth Framework Program for RTD (contract no FOOD-CT-2006- 016253), and by Award Number R01ES019222 from the National Institute of Environmental Health Sciences (NIEHS). AE is supported by funding from the National Institutes of Health (R01CA134218, RC2ES018741). The content is solely the responsibility of the authors and does not necessarily represent the official views of the EU, the US Environmental Protection Agency, or the National Institutes of Health. DD acknowledges that Afton Chemical Corporation provided him with a travel grant that allowed his participation at the Xian International Meeting. .
Publisher's Disclaimer: This is a PDF file of an unedited manuscript that has been accepted for publication. As a service to our customers we are providing this early version of the manuscript. The manuscript will undergo copyediting, typesetting, and review of the resulting proof before it is published in its final citable form. Please note that during the production process errors may be discovered which could affect the content, and all legal disclaimers that apply to the journal pertain.
- Block ML, Zecca L, Hong JS. Microglia-mediated neurotoxicity: uncovering the molecular mechanisms. Nat Rev Neurosci. 2007 Jan;8(1):57–69. [PubMed]
- Brenneman KA, Wong BA, Buccellato MA, Costa ER, Gross EA, Dorman DC. Direct olfactory transport of inhaled manganese (54MnCl2) to the rat brain: toxicokinetic investigations in a unilateral nasal occlusion model. Toxicol. Appl. Pharmacol. 2000;169(3):238–48. [PubMed]
- Calderón-Garcidueñas L, Maronpot RR, Torres-Jardon R, Henríquez-Roldán C, Schoonhoven R, Acuña-Ayala H, Villarreal-Calderón A, Nakamura J, Fernando R, Reed W, Azzarelli B, Swenberg JA. DNA damage in nasal and brain tissues of canines exposed to air pollutants is associated with evidence of chronic brain inflammation and neurodegeneration. Toxicol Pathol.2003 Sep-Oct;31(5):524–38. [PubMed]
- Calderón-Garcidueñas L, D'Angiulli A, Kulesza RJ, Torres-Jardón R, Osnaya N, Romero L, Keefe S, Herritt L, Brooks DM, Avila-Ramirez J, Delgado-Chávez R, Medina-Cortina H, González-González LO. Air pollution is associated with brainstem auditory nuclei pathology and delayed brainstem auditory evoked potentials. Int J Dev Neurosci. 2011 Jun;29(4):365–75.[PMC free article] [PubMed]
- Calderón-Garcidueñas L, Franco-Lira M, Henríquez-Roldán C, Osnaya N, González-Maciel A, Reynoso-Robles R, Villarreal-Calderon R, Herritt L, Brooks D, Keefe S, Palacios-Moreno J, Villarreal-Calderon R, Torres-Jardón R, Medina-Cortina H, Delgado-Chávez R, Aiello-Mora M, Maronpot RR, Doty RL. Urban air pollution: influences on olfactory function and pathology in exposed children and young adults. Exp Toxicol Pathol. 2010 Jan;62(1):91–102.[PMC free article] [PubMed]
- Cross DJ, Minoshima S, Anzai Y, Flexman JA, Keogh BP, Kim Y, Maravilla KR. Statistical mapping of functional olfactory connections of the rat brain in vivo. Neuroimage.2004;23:1326–35. [PubMed]
- Dhuria SV, Hanson LR, Frey WH., 2nd Intranasal delivery to the central nervous system: Mechanisms and experimental considerations. J Pharm Sci. 2010;99(4):1654–73. [PubMed]
- Dorman DC, McManus BE, Parkinson CU, Manuel CA, McElveen AM, Everitt JI. Nasal toxicity of manganese sulfate and manganese phosphate in young male rats following subchronic (13-week) inhalation exposure. Inhal Toxicol. 2004;16(6–7):481–8. 2004. [PubMed]
- Dorman DC, Struve MF, Wong BA, Dye JA, Robertson ID. Correlation of brain magnetic resonance imaging changes with pallidal manganese concentrations in rhesus monkeys following subchronic manganese inhalation. Toxicol Sci. 2006;92(1):219–27. [PubMed]
- Duggan A, Madathany T, de Castro SC, Gerrelli D, Guddati K, Garcia-Anoveros J. Transient expression of the conserved zinc finger gene INSM1 in progenitors and nascent neurons throughout embryonic and adult neurogenesis. J Comp Neurol. 2008;507(4):1497–1520.[PubMed]
- Elder A, Gelein R, Silva V, Feikert T, Opanashuk L, Carter J, Potter R, Maynard A, Ito Y, Finkelstein J, Oberdörster G. Translocation of inhaled ultrafine manganese oxide particles to the central nervous system. Environ Health Perspect. 2006;114:1172–1178. [PMC free article][PubMed]
- Finlayson-Pitts BJ, Pitts JN. Chemistry of the Upper and Lower Atmosphere: Theory, Experiments, and Applications. Academic Press; San Diego, CA: 2000.
- Gitler AD, Chesi A, Geddie ML, Strathearn KE, Hamamichi S, Hill KJ, et al. α-Synuclein is part of a diverse and highly conserved interaction network that includes PARK9 and manganese toxicity. Nat Genet. 2009;41:308–315. [PMC free article] [PubMed]
- Guilarte TR. Manganese and Parkinson's disease: a critical review and new findings. Environ Health Perspect. 2010;118(8):1071–80. [PMC free article] [PubMed]
- Henriksson J, Tjälve H. Manganese taken up into the CNS via the olfactory pathway in rats affects astrocytes. Toxicol. Sci. 2000;55(2):392–8. [PubMed]
- Holmes C, Cunningham C, Zotova E, Woolford J, Dean C, Kerr S, Culliford D, Perry VH. Systemic inflammation and disease progression in Alzheimer disease. Neurology. 2009;73:768–774. [PMC free article] [PubMed]
- International Committee on Radiological Protection . Human Respiratory Tract Model for Radiological Protection. A Report of Committee 2 of the ICRP. Pergamon Press; Oxford: 1994.
- Kanayama Y, Enomoto S, Irie T, Amano R. Axonal transport of rubidium and thallium in the olfactory nerve of mice. Nucl Med Biol. 2005;32(5):505–12. [PubMed]
- Kreyling WG, Semmler-Behnke M, Seitz J, Scymczak W, Wenk A, Mayer P, Takenaka S, Oberdörster G. Size dependence of the translocation of inhaled iridium and carbon nanoparticle aggregates from the lung of rats to the blood and secondary target organs. Inhal Toxicol.2009;21:55–60. [PubMed]
- Leavens TL, Rao D, Andersen ME, Dorman DC. Evaluating transport of manganese from olfactory mucosa to striatum by pharmacokinetic modeling. Toxicol Sci. 2007;97(2):265–78.[PubMed]
- Lewis J, Bench G, Myers O, Tinner B, Staines W, Barr E, Divine KK, Barrington W, Karlsson J. Trigeminal uptake and clearance of inhaled manganese chloride in rats and mice.Neurotoxicology. 2005;6:113–23. [PubMed]
- Lucchini R, Albini E, Benedetti L, Borghesi S, Coccaglio R, Malara E, Parrinello G, Garattini S, Resola S, Alessio L. High Prevalence Of Parkinsonian Disorders Associated To Manganese Exposure In The Vicinities Of Ferroalloy Industries. Am J Ind Med. 2007;50(11):788–800.[PubMed]
- Lucchini RG, Guazzetti S, Zoni S, Donna F, Peter S, Zacco A, Bontempi E, Zimmerman NJ, Smith DR. Tremor, olfactory and motor changes in Italian adolescents exposed to historical ferro-manganse emission. Neurotoxicology. this issue. [PMC free article] [PubMed]
- McAlpine FE, Lee JK, Harms AS, Ruhn KA, Blurton-Jones M, Hong J, Das P, Golde TE, LaFerla FM, Oddo S, Blesch A, Tansey MG. Inhibition of soluble TNF signaling in a mouse model of Alzheimer's disease prevents pre-plaque amyloid-associated neuropathology.Neurobiol.Dis. 2009;34:163–177. [PMC free article] [PubMed]
- Oberdörster G, Sharp Z, Atudorei V, Elder A, Gelein R, Lunts A, Kreyling W, Cox C. Extrapulmonary translocation of ultrafine carbon particles following whole-body inhalation exposure of rats. J Toxicol Environ Health. 2002;65:1531–1543. [PubMed]
- Pekkanen J, Timonen KL, Ruuskanen J, Reponen A, Mirme A. Effects of ultrafine and fine particles in urban air on peak expiratory flow among children with asthmatic symptoms.Environ Res. 1997;74:24–33. [PubMed]
- Peters A, Liu E, Verrier RL, Schwartz J, Gold DR, Mittleman M, Baliff J, Oh JA, Allen G, Monahan K, Dockery DW. Air pollution and incidence of cardiac arrhythmia. Epidemiol.2000;11:11–17. [PubMed]
- Pope CA, III, Verrier RL, Lovett EG, Larson AC, Raizenne ME, Kanner RE, Schwartz J, Villegas GM, Gold DR, Dockery DW. Heart rate variability associated with particulate air pollution. Am.Heart J. 1999;138:890–899. [PubMed]
- Radcliffe PM, Olabisi AO, Wagner DJ, Leavens T, Wong BA, Struve MF, Chapman GD, Wilfong ER, Dorman DC. Acute sodium tungstate inhalation is associated with minimal olfactory transport of tungsten (188W) to the rat brain. Neurotoxicology. 2009;30(3):445–50. [PubMed]
- Rao DB, Wong BA, McManus BE, McElveen AM, James AR, Dorman DC. Inhaled iron, unlike manganese, is not transported to the rat brain via the olfactory pathway. Toxicol Appl Pharmacol. 2003;193(1):116–26. [PubMed]
- Rentschler G, Covolo L, Ahmadi Haddad A, Lucchini RG, Zoni S, Broberg K. ATP13A2 (PARK9)polymorphisms influences the neurotoxic effects of manganese. Neurotoxicology. this issue.[PMC free article] [PubMed]
- Rosenbaum JN, Duggan A, Garcia-Anoveros J. Insm1 promotes the transition of olfactory progenitors from apical and proliferative to basal, terminally dividing and neuronogenic. Neural Dev. 2011;6:6. [PMC free article] [PubMed]
- Sama P, Long TC, Hester S, Tajuba J, Parker J, Chen LC, Veronesi B. The Cellular and Genomic Response of an Immortalized Microglia Cell Line (BV2) to Concentrated Ambient Particulate Matter. Inhalation Toxicology. 2007;19(13):1079–87. [PubMed]
- Schwartz J. Air Pollution and Admissions for Heart Disease in Eight U.S. Cities. Epidemiol.1999;10:17–22. [PubMed]
- Semmler-Behnke M, Kreyling WG, Lipka J, Fertsch S, Wenk A, Takenaka S, Schmid G, Brandau W. Biodistribution of 1.4- and 18-nm gold particles in rats. Small. 2008;4:2108–2111.[PubMed]
- Shiga H, Taki J, Yamada M, Washiyama K, Amano R, Matsuura Y, Matsui O, Tatsutomi S, Yagi S, Tsuchida A, Yoshizaki T, Furukawa M, Kinuya S, Miwa T. Evaluation of the olfactory nerve transport function by SPECT-MRI fusion image with nasal thallium-201 administration.Mol Imaging Biol. 2010 Epub ahead of print. [PubMed]
- Thompson K, Molina RM, Donaghey T, Schwob JE, Brain JD, Wessling-Resnick M. Olfactory uptake of manganese requires DMT1 and is enhanced by anemia. FASEB J. 2007;21:223–230.[PMC free article] [PubMed]
- Tjälve H, Henriksson J. Uptake of metals in the brain via olfactory pathways. Neurotoxicology.1999;20(2–3):181–95. [PubMed]
- Veronesi B, Makwana O, Pooler M, Chen L. Effects of subchronic exposure to concentrated air pollution in Apo E −/− mice: VII. Degeneration of dopaminergic neurons. Inhal Toxicol.2005;17(4–5):235–241. [PubMed]
- Villalobos V, Bonilla E, Castellano A, Novo E, Caspersen R, Giraldoth D, Medina-Leendertz S. Ultrastructural changes of the olfactory bulb in manganese-treated mice. Biocell.2009;33(3):187–97. [PubMed]
To our health !!!
Health Essentials LLC.