Somatostatin Negatively Regulates Parasite Burden and Granulomatous Responses in Cysticercosis

Abstract

Cysticercosis is an infection of tissues with the larval cysts of the cestode,Taenia  solium. While live parasites elicit little or no inflammation, dying parasites initiate a granulomatous reaction presenting as painful muscle nodules or seizures when cysts are located in the brain. We previously showed in theT. crassicepsmurine model of cysticercosis that substance P (SP), a neuropeptide, was detected in early granulomas and was responsible for promoting granuloma formation, while somatostatin (SOM), another neuropeptide and immunomodulatory hormone, was detected in late granulomas; SOM’s contribution to granuloma formation was not examined. In the current studies, we used somatostatin knockout (SOM−/−) mice to examine the hypothesis that SOM downmodulates granulomatous inflammation in cysticercosis, thereby promoting parasite growth. Our results demonstrated that parasite burden was reduced 5.9-fold in SOM−/−mice compared to WT mice (P<0.05). This reduction in parasite burden in SOM−/−mice was accompanied by a 95% increase in size of their granulomas (P<0.05), which contained a 1.5-fold increase in levels of IFN-γand a 26-fold decrease in levels of IL-1β(P<0.05for both) compared to granulomas from WT mice. Thus, SOM regulates both parasite burden and granulomatous inflammation perhaps through modulating granuloma production of IFN-γand IL-1β.Corrigendum to “Somatostatin Negatively Regulates Parasite Burden and Granulomatous Responses in Cysticercosis”