Association of water extract of green propolis and liposomal meglumine antimoniate in the treatment of experimental visceral leishmaniasis.
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2014
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This work investigated the use of water extract of
green propolis (WEP) and its association with free or liposomal
meglumine antimoniate (MA) for the treatment of murine
visceral leishmaniasis. Mice infected with Leishmania
infantum were treated with oral doses of WEP associated or
not with a single dose of liposomal MA by intraperitoneal
route. Parasite burden was assessed in the liver and spleen by
limiting dilution assay, and alterations in the spleen cellular
phenotype were evaluated by flow cytometry. Tissue damage
was assessed by determination of biochemical markers of the
liver, heart, and kidney function and histopathological analysis
of the liver and spleen. Our data showed that treatmentwith
WEP was able to reduce parasite load in the liver but not in the
spleen. On the other hand, liposomal MA reduced parasite
load in both organs. Unexpectedly, there was no synergism
with the combination of WEP and liposomal MA in reducing
the parasite load. The histopathological analysis showed that
administration of WEP, liposomal MA, or their association
was able to protect the liver and spleen fromlesions caused by
infection. No alteration in the profile of spleen cells by flow
cytometry or in the liver, heart, and kidney functions by
biochemical markers due to any of the treatments was observed.
These results demonstrate that althoughWEP was able
to significantly reduce the liver parasite load, its association
with liposomalMA did not lead to significant improvement in
reducing parasite load. On the other hand, treatment with
WEP and/or liposomal MA protected the liver and spleen
from lesions caused by the infection.
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FERREIRA, F. M. et al. Association of water extract of green propolis and liposomal meglumine antimoniate in the treatment of experimental visceral leishmaniasis. Parasitology Research, v. 113, p. 533-543, 2014. Disponível em: <http://link.springer.com/article/10.1007%2Fs00436-013-3685-8>. Acesso em: 20 jan. 2017.