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Surface coatings of ZnO nanoparticles mitigate differentially a host of transcriptional,protein and signalling responses in primary human olfactory cells
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نویسنده
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osmond-mcleod m.j. ,osmond r.i.w. ,oytam y. ,mccall m.j. ,feltis b. ,mackay-sim a. ,wood s.a. ,cook a.l.
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منبع
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particle and fibre toxicology - 2013 - دوره : 10 - شماره : 1
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چکیده
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Background: inhaled nanoparticles have been reported in some instances to translocate from the nostril to the olfactory bulb in exposed rats. in close proximity to the olfactory bulb is the olfactory mucosa,within which resides a niche of multipotent cells. cells isolated from this area may provide a relevant in vitro system to investigate potential effects of workplace exposure to inhaled zinc oxide nanoparticles.methods: four types of commercially-available zinc oxide (zno) nanoparticles,two coated and two uncoated,were examined for their effects on primary human cells cultured from the olfactory mucosa. human olfactory neurosphere-derived (hons) cells from healthy adult donors were analyzed for modulation of cytokine levels,activation of intracellular signalling pathways,changes in gene-expression patterns across the whole genome,and compromised cellular function over a 24 h period following exposure to the nanoparticles suspended in cell culture medium.results: zno nanoparticle toxicity in hons cells was mediated through a battery of mechanisms largely related to cell stress,inflammatory response and apoptosis,but not activation of mechanisms that repair damaged dna. surface coatings on the zno nanoparticles mitigated these cellular responses to varying degrees.conclusions: the results indicate that care should be taken in the workplace to minimize generation of,and exposure to,aerosols of uncoated zno nanoparticles,given the adverse responses reported here using multipotent cells derived from the olfactory mucosa. © 2013 osmond-mcleod et al.; licensee biomed central ltd.
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کلیدواژه
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Cell-signalling; DNA-damage; Gene expression; Nanoparticle; Olfactory; Zinc oxide
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آدرس
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csiro advanced materials tcp (nanosafety),csiro animal,food and health sciences,po box 52,north ryde,nsw 1670, Australia, tgr biosciences,thebarton,sa 5031, Australia, csiro advanced materials tcp (nanosafety),csiro animal,food and health sciences,po box 52,north ryde,nsw 1670, Australia, csiro advanced materials tcp (nanosafety),csiro animal,food and health sciences,po box 52,north ryde,nsw 1670, Australia, school of medical sciences,rmit university,bundoora,vic 3083,australia,centre for green chemistry,monash university,clayton,vic 3800, Australia, national centre for adult stem cell research,eskitis institute for cell and molecular therapies,griffith university,brisbane,qld 4111, Australia, national centre for adult stem cell research,eskitis institute for cell and molecular therapies,griffith university,brisbane,qld 4111, Australia, national centre for adult stem cell research,eskitis institute for cell and molecular therapies,griffith university,brisbane,qld 4111,australia,school of human life sciences,university of tasmania,launceston,tas 7250, Australia
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Authors
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