cris.boxmetadata.label.title
Experimental infection of immunomodulated NOD/LtSz-SCID mice as a new model for Plasmodium falciparum erythrocytic stages
cris.boxmetadata.label.dateissued
01 browse.startsWith.months.january 2005
cris.boxmetadata.label.accesslevel
metadata only access
cris.boxmetadata.label.resourcetype
journal article
cris.boxmetadata.label.authors
Instituto de Salud Carlos III
cris.boxmetadata.label.abstract
The main objective of this study was to determine whether a chemical immunomodulation protocol could reduce the resistance of NOD/LtSz-SCID mice to Plasmodium falciparum infection and provide an improved mouse model for screening the antimalarial activity of new compounds. This model was compared with the presently used immunodeficient Beige/Nude/ Xid (BNX) mouse model, using the same protocol, in terms of percentage of infected mice, parasite development, leukocyte response and phagocytosis of P. falciparum infected cells in various organs. Our results show that the combination of the chemical immune modulation protocol with the genetic background of NOD/ LtSz-SCID mice results in the development of long-lasting P. falciparum infection in a high percentage of mice. A comparison of the results obtained in the histological study for both mouse models suggests that the higher rate of success in NOD/LtSz-SCID mice could be related to the reduced macrophage recruitment developed in different tissues to remove the parasite from blood. © Springer-Verlag 2004.
cris.boxmetadata.label.citationstartpage
97
cris.boxmetadata.label.citationendpage
105
cris.boxmetadata.label.volume
95
cris.boxmetadata.label.issue
2
cris.boxmetadata.label.language
English
cris.boxmetadata.label.ocdeknowledgeArea
Parasitología
cris.boxmetadata.label.doi
cris.boxmetadata.label.scopusidentifier
2-s2.0-13644269362
cris.boxmetadata.label.pubmedidentifier
cris.boxmetadata.label.source
Parasitology Research
cris.boxmetadata.label.containerissn
09320113
cris.boxmetadata.label.sponsor
Acknowledgements We thank Ana Maria Aransay, Dario Cabanes, Elizabeth Ferrer, Edurne Laurin and Maria Jesus Perteguer for their contributions. We also thank the Retrovirus Diagnosis Unit of the Instituto de Salud Carlos III for blood supplies. This work has been supported by the Research Network of Tropical Disease Centres in Spain (RICET), by the Intramural Programme from the Instituto de Salud Carlos III (Expedient 03/11) and by a grant from the Seneca Foundation from the Autonomous Community of Murcia. The experiments comply with the current laws of the country in which they were performed.
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