Hexachlorobenzene-induced Immunopathology in Brown Norway Rats is Partly Mediated by T Cells

doi:10.1093/toxsci/kfh034

ToxSci Advance Access originally published online on December 2, 2003

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Toxicological Sciences 78, 88-95 (2004)
Copyright © 2004 by the Society of Toxicology

REGULAR ARTICLE

Hexachlorobenzene-induced Immunopathology in Brown Norway Rats is Partly Mediated by T Cells

Janine Ezendam^*^,^,^,1, Ine Hassing^*, Rob Bleumink^*, Joseph G. Vos^, and Raymond Pieters^*

^* Institute for Risk Assessment Sciences (IRAS), Immunotoxicology, Utrecht University, P.O. Box 80.176, 3508 TD Utrecht, Netherlands; National Institute for Public Health and the Environment, Laboratory for Toxicology, Pathology and Genetics, Bilthoven, P.O. Box 1 3720 BA, Netherlands; and Faculty of Veterinary Medicine, Department of Pathobiology, Utrecht University, P.O. Box 80.150, 3508 TD Utrecht, Netherlands

¹ To whom correspondence should be addressed at IRAS, Immunotoxicology, Utrecht University, P.O. Box 80.176, 3508 TD Utrecht, Netherlands. Fax: +31302535077. E-mail: J.Ezendam{at}iras.uu.nl.

ABSTRACT

Hexachlorobenzene (HCB) is a persistent environmental pollutantwith (auto)immune effects in humans and rats. The Brown Norway(BN) rat is very susceptible to HCB-induced immunopathology,and oral exposure causes inflammatory skin and lung lesions,splenomegaly, lymph node (LN) enlargement, and increased serumlevels of IgE and anti-ssDNA IgM. The role of T cells in HCB-inducedimmunopathology is unclear and to elucidate this CyclosporinA (CsA) was used. BN rats were exposed to either a control dietor a diet supplemented with 450 mg/kg HCB for 21 days. CsA treatmentstarted 2 days prior to HCB exposure and rats were injecteddaily with 20 mg/kg body weight CsA. Treatment with CsA preventedthe HCB-induced immunopathology significantly. The onset ofskin lesions was delayed and the severity was also stronglydecreased. Furthermore, CsA prevented the HCB-induced increasein spleen weight partly and the increase in auricular LN weightcompletely. The increase in serum IgE and IgM against ssDNAlevels was prevented completely. Macrophage infiltrations intothe spleen and lung still occurred but infiltrations of eosinophilicgranulocytes into the lung were prevented. Restimulation ofspleen cells with the T-cell mitogen ConA and the macrophageactivator LPS clearly showed that CsA inhibited T-cell activation,but not macrophage activation. Together, our results show thatboth T cells and macrophages play a prominent role in HCB-inducedimmunopathology.

Key Words: hexachlorobenzene; T cells; macrophages; immunostimulation; Cyclosporin A; Brown Norway rat.

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This article has been cited by other articles:

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Effects of the T cell inhibitor, cyclosporin A (CsA), on hexachlorobenzene (HCB)-induced immunopathology in the Brown Norway (BN) rat.
Toxicol. Sci., September 1, 2004; 81(1): 253 - 253.
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J. Ezendam, J. G. Vos, and R. Pieters
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Toxicol. Sci., September 1, 2004; 81(1): 254 - 255.
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				J. Ezendam, J. G. Vos, and R. Pieters Letter to the Editor Toxicol. Sci., September 1, 2004; 81(1): 254 - 255. [Full Text] [PDF]