Biodiesel exhaust particle airway toxicity and the role of polycyclic aromatic hydrocarbons

Christopher Chinedu Ogbunuzor(University College London), Leonie Francina Hendrina Fransen(UK Health Security Agency), Midhat Talibi(University College London), Zuhaib Ali Khan(University College London), Abigail Dalzell(UK Health Security Agency), Adam Laycock(UK Health Security Agency), Daniel Southern(University College London), Aaron Eveleigh(University College London), Nicos Ladommatos(University College London), Paul Hellier(University College London), Martin O. Leonard(Environment Agency)
Ecotoxicology and Environmental Safety
May 12, 2023
Cited by 9Open Access
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Abstract

Renewable alternatives to fossil diesel (FD) including fatty acid methyl ester (FAME) biodiesel have become more prevalent. However, toxicity of exhaust material from their combustion, relative to the fuels they are displacing has not been fully characterised. This study was carried out to examine particle toxicity within the lung epithelium and the role for polycyclic aromatic hydrocarbons (PAHs). Exhaust particles from a 20% (v/v) blend of FAME biodiesel had little impact on primary airway epithelial toxicity compared to FD derived particles but did result in an altered profile of PAHs, including an increase in particle bound carcinogenic B[a]P. Higher blends of biodiesel had significantly increased levels of more carcinogenic PAHs, which was associated with a higher level of stress response gene expression including CYP1A1, NQO1 and IL1B. Removal of semi-volatile material from particulates abolished effects on airway cells. Particle size difference and toxic metals were discounted as causative for biological effects. Finally, combustion of a single component fuel (Methyl decanoate) containing the methyl ester molecular structure found in FAME mixtures, also produced more carcinogenic PAHs at the higher fuel blend levels. These results indicate the use of FAME biodiesel at higher blends may be associated with an increased particle associated carcinogenic and toxicity risk.


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