Article
Increased Plasmodium falciparum Parasitemia in Non-splenectomized Saimiri sciureus Monkeys Treated with Clodronate Liposomes
Registro en:
CUNHA, Janaiara A. et al. Increased Plasmodium falciparum Parasitemia in Non-splenectomized Saimiri sciureus Monkeys Treated with Clodronate Liposomes. Frontiers in Cellular and Infection Microbiology, v.7, Article 408, 14p, Sept. 2017.
2235-2988
10.3389/fcimb.2017.00408
Autor
Cunha, Janaiara A.
Carvalho, Leonardo J. M.
Bianco Junior, Cesare
Andrade, Márcia C. R.
Riccio, Lilian R. Pratt
Riccio, Evelyn K. P.
Machado, Marcelo Pelajo
Silva, Igor J. da
Druilhe, Pierre
Daniel-Ribeiro, Cláudio Tadeu
Resumen
A major constraint in the study ofPlasmodium falciparummalaria, including vaccine development, lies on the parasite's strict human host specificity and therefore the shortage of animal experimental models able to harbor human plasmodia. The best experimental models are neo-tropical primates of the genus Saimiri and Aotus, but they require splenectomy to reduce innate defenses for achieving high and consistent parasitemias, an important limitation. Clodronate-liposomes (CL) have been successfully used to deplete monocytes/macrophages in several experimental models. We investigated whether a reduction in the numbers of phagocytic cells by CL would improve the development ofP. falciparumparasitemia in non-splenectomizedSaimiri sciureusmonkeys. Depletion ofS. sciureussplenocytes afterin vitroincubation with CL was quantified using anti-CD14 antibodies and flow cytometry. Non-infected andP. falciparum-infectedS. sciureuswere injected intravenously twice a week with either CL at either 0.5 or 1 mL (5 mg/mL) or phosphate buffered saline (PBS). Animals were monitored during infection and treated with mefloquine. After treatment and euthanasia, spleen and liver were collected for histological analysis.In vitroCL depletedS. sciureussplenic monocyte/macrophage population in a dose- and time-dependent manner.In vivo, half ofP. falciparum-infectedS. sciureustreated with CL 0.5 mL, and two-thirds of those treated with CL 1 mL developed high parasitemias requiring mefloquine treatment, whereas all control animals were able to self-control parasitemia without the need for antimalarial treatment. CL-treated infectedS. sciureusshowed a marked decrease in the degree of splenomegaly despite higher parasitemias, compared to PBS-treated animals. Histological evidence of partial monocyte/macrophage depletion, decreased hemozoin phagocytosis and decreased iron recycling was observed in both the spleen and liver of CL-treated infectedS. sciureus. CL is capable of promoting higher parasitemia inP. falciparum-infectedS. sciureus, associated with evidence of partial macrophage depletion in the spleen and liver. Macrophage depletion by CL is therefore a practical and viable alternative to surgical splenectomy in this experimental model.