Idiotypes Expressed Early in Experimental Schistosoma mansoni Infections Predict Clinical Outcomes of Chronic Disease

doi:10.1084/jem.20020329

Published online 29 April 2002 doi:10.1084/jem.20020329

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© Rockefeller University Press, 0022-1007/2002/5/1223/ $5.00
The Journal of Experimental Medicine, Volume 195, Number 9, May 6, 2002 1223-1228

Brief Definitive Report

Idiotypes Expressed Early in Experimental Schistosoma mansoni Infections Predict Clinical Outcomes of Chronic Disease

M. Angela Montesano, Daniel G. Colley, Margaret T. Willard, George L. Freeman, Jr. and W. Evan Secor

Division of Parasitic Diseases, National Center for Infectious Diseases, Centers for Disease Control and Prevention, Public Health Service, U.S. Department of Health and Human Services, Atlanta, GA 30341

Address correspondence to W. Evan Secor, Immunology Branch/Division of Parasitic Diseases, Centers for Disease Control and Prevention, 4770 Buford Hwy., N.E.; MS-F13, Atlanta, GA 30341-3724. Phone: 770-488-4115; Fax: 770-488-4108; E-mail: was4{at}cdc.gov

In murine Schistosoma mansoni infections, schistosome-specificcross-reactive idiotypes (CRI) are present in the sera of micewith moderate splenomegaly syndrome (MSS) at 20 wk after infection.In contrast, sera from animals that have the more severe hypersplenomegalysyndrome (HSS) at 20 wk of infection do not express these CRIin their sera. To examine when these regulatory CRI first appearin mice that eventually develop MSS, sera from infected animalswere monitored for CRI from 1.5 to 20 wk of infection. In micethat eventually developed MSS, CRI were detected by 5 to 6 wkafter infection, plateaued by 8 to 10 wk, and persisted through20 wk of infection. Animals that developed HSS pathology orthat died before 20 wk of infection never expressed CRI. Moreover,CRI levels present in the sera of mice at 6 wk of infectionwere inversely correlated with splenomegaly and hepatic fibrosis,but not with parasitologic measures, at 20 wk after infection.These results suggest that critical events occur very earlyin some schistosome infections that induce the production ofregulatory idiotypes and that the presence or absence of theseidiotypes predicts, and possibly determines, subsequent morbidity.

Key Words: schistosomiasis • idiotypes • splenomegaly • mice • fibrosis

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