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A more recent version of this article appeared on September 1, 2007

Published online before print August 9, 2007
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Copyright © 2007 American Society for Investigative Pathology
American Journal of Pathology, doi:10.2353/ajpath.2007.061043

Accepted for publication June 14, 2007.

Article

Neutrophil Elastase Converts Human Immature Dendritic Cells into Transforming Growth Factor-{beta}1-Secreting Cells and Reduces Allostimulatory Ability

Paulo César Maffia*, Sandra Elizabeth Zittermann*{dagger}, María Lucila Scimone*, Nancy Tateosian*, Nicolás Amiano*, Diego Guerrieri*, Viviana Lutzky*, Diego Rosso{ddagger}, Horacio Eduardo Romeo{sect}, Verónica E. Garcia*, Andrew C. Issekutz{ddagger}, and H. Eduardo Chuluyan*@

From the Lanais de la Facultad de Medicina,* and Sección Hematología y Oncología,{ddagger} Departamento de Pediatría, Hospital de Clínicas "José de San Martín," Facultad de Medicina, y Departamento de Farmacología, Facultad de Medicina, Universidad de Buenos Aires, Buenos Aires, Argentina; the Department of Pediatrics,{dagger} Dalhousie University, Halifax, Nova Scotia, Canada; and the Department of Neurobiology,{sect} David Geffen School of Medicine at University of California Los Angeles, Los Angeles, California

@ To whom correspondence should be addressed. E-mail: chulu{at}interar.com.ar;echuluyan@hospitaldeclinicas.uba.ar.


  Abstract

During microbial infection, neutrophils (polymorphonuclear leukocytes; PMNs) activate dendritic cells (DCs). However, early reports illustrated that neutrophil-derived mediators may suppress responses to mitogens. In the present study, we investigated the mechanism used by PMNs to modulate the immunostimulatory ability of DCs. Autologous syngeneic PMNs decreased T-cell proliferation induced by allogeneic DCs. Culture supernatant (CS) derived from PMNs also decreased allostimulation ability of immature DCs and increased the expression of transforming growth factor (TGF)-{beta}1 on DCs. A TGF-{beta}1 monoclonal antibody, a CD40 monoclonal antibody, or a serine protease inhibitor reversed the effect of PMN CS on DC allostimulatory ability. Furthermore, elastase reproduced the inhibitory effect of PMN CS on DC allostimulatory ability and the TGF-{beta}1 production. The role of elastase was confirmed by examining PMN CS from two patients with cyclic neutropenia, a disease due to mutations in the neutrophil elastase gene. These PMN CS samples had reduced elastase activity and were unable to increase DC TGF-{beta}1 production. Moreover, elastase and PMN CS induced I{kappa}B{alpha} degradation in DCs. We conclude that PMNs decrease DC allostimulatory ability via production of elastase leading to a switch of immature DCs into TGF-{beta}1-secreting cells.






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Copyright © 2007 by the American Society for Investigative Pathology.