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Published online before print June 18, 2007

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(Journal of Leukocyte Biology. 2007;82:630-637.)
© 2007 by Society for Leukocyte Biology

ABCC transporter inhibition reduces zymosan-induced peritonitis

Daniela F. P. Leite^*,,, Juliana Echevarria-Lima, Samira Cardoso Ferreira^||, João B. Calixto and Vivian M. Rumjanek^*,1

^* Institutos de Bioquímica Médica and
Biofísica Carlos Chagas Filho and
Departamento de Imunologia, Instituto de Microbiologia Paulo Góes, Universidade Federal do Rio de Janeiro (UFRJ), Rio de Janeiro, Brazil; and
Departamento de Farmacologia and
^|| Hospital Universitário, Universidade Federal de Santa Catarina (UFSC), Florianópolis, Brazil

¹ Correspondence: Laboratório de Imunologia Tumoral, sala H2003, Instituto de Bioquímica Médica, Centro de Ciências da Saúde, Universidade Federal do Rio de Janeiro, Cidade Universitária, Rio de Janeiro, Brazil. E-mail: vivian{at}bioqmed.ufrj.br

Inflammatory mediators are released from injured tissues being responsible for the first steps of inflammatory processes. Multidrug efflux transporters, members of the ATP-binding cassette (ABC) family, are ubiquitously expressed. ABCC molecules transport several endogenous substances, including leukotriene C₄ (LTC₄) and PGE₂, which are involved in zymosan-induced inflammation. The present study investigated the role played by ABCC transporters on zymosan-induced peritonitis in mice. Most of the resident peritoneal cells were macrophages, based on their morphology and membrane-activated complex 3 expression. RT-PCR demonstrated that these cells expressed ABCC, and ABCC activity was analyzed in vivo via the s.c. injection of ABCC inhibitors [probenecid (PROB) 200 mg/kg or MK571 20 mg/kg], followed by an i.v. injection of carboxyfluorescein diacetate (CFDA), an ABCC fluorescent substrate. Both inhibitors increased CFDA accumulation, suggesting ABCC impairment. Moreover, ABCC reversors decreased zymosan-induced plasma exudation by 86.6 ± 7.4 and 97.6 ± 2.3%, a feature related to a diminished secretion of LTC₄ (65.1±11 and 47.8±9.9%) and PGE₂ (under basal levels). Cell migration was inhibited similarly. Furthermore, PROB and MK571 inhibited IL-1ß by 83.4 ± 13 and 71.2 ± 13.4% and TNF- content by 47 ± 4.5 and 28.9 ± 0.8%, respectively. NO metabolites and reactive oxygen species production were also reduced. The present results suggest that ABCC molecules have a relevant role in the acute inflammatory response produced by zymosan in mice.

Key Words: LTC₄ • NOx • ROS • macrophages • MK571 • probenecid • PGE₂ • TNF- • IL-1ß