In Vitro Exposure of Jurkat T-Cells to Industrially Important Organic Solvents in Binary Combination: Interaction Analysis

doi:10.1093/toxsci/kfm274

ToxSci Advance Access originally published online on November 2, 2007
Toxicological Sciences 2008 101(2):263-274; doi:10.1093/toxsci/kfm274

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In Vitro Exposure of Jurkat T-Cells to Industrially Important Organic Solvents in Binary Combination: Interaction Analysis

Catherine McDermott^*^,, Ashley Allshire^*^,, Frank van Pelt^*^, and James J. A. Heffron^*^,^,1

^* Environmental Research Institute Department of Biochemistry Department of Pharmacology and Therapeutics Department of Biochemistry, University College Cork, Lee Maltings, Cork 1, Ireland

¹ To whom correspondence should be addressed at Department of Biochemistry, University College Cork, Lee Maltings, Prospect Row, Cork, Ireland. Fax: +35-32-14-90-42-15. E-mail: j.heffron{at}ucc.ie.

Received August 15, 2007; accepted October 30, 2007

Abstract

Humans are frequently exposed to mixtures of environmental pollutantsat low levels over prolonged periods of time yet most toxicitystudies deal with acute exposure to high concentrations of singlechemicals. Investigation of the biological effects and possibletoxic interactions during long-term exposure to such mixturesis warranted. Here Jurkat T-cells were exposed to toluene, n-hexaneand methyl ethyl ketone in binary combination. Concentrationranges were centered on thresholds at which the individual agentscaused cell toxicity under otherwise similar conditions, andconcentrations were confirmed by headspace gas chromatography.After 5 days cells were harvested and toxicity measured in termsof membrane damage (lactate dehydrogenase [LDH] leakage), perturbationsin [Ca²⁺]_i and changes in glutathione redox status. Data forall three endpoints were subjected to isobolographic analysisto test for interaction between components of the solvent mixture.Almost all combinations of toluene and n-hexane elicited greaterthan additive toxicity in terms of each of the three endpoints,as did methyl ethyl ketone (MEK)/n-hexane and MEK/toluene combinationsfor the LDH and glutathione endpoints. The main exceptions werethe two combinations involving MEK, which caused less than additiveeffects on perturbations of [Ca²⁺]_i. It is concluded that toxicityin immune-derived T cells may exhibit greater than additiveeffects when there is coexposure to organic solvents. This mayhave implications for risk assessment of environmental exposureto these agents.

Key Words: mixture toxicity; in vitro; organic solvent; isobolographic analysis.

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