Nanoliposomal Buparvaquone Immunomodulates Leishmania infantum-Infected Macrophages and Is Highly Effective in a Murine Model

Costa-Silva, Thaís A.; Galisteo, Andrés Jimenez; Lindoso, José Ângelo Lauletta; Barbosa, Leandro R.S.; Tempone, André G.

doi:10.1128/aac.02297-16

Cited by 28 publications

(21 citation statements)

References 52 publications

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“…Anti-leishmanial activity was evaluated in vitro for L. donovani, Leishmania aethiopica, L. major, Leishmania amazonensis, Leishmania mexicana, Leishmania panamensis, L. infantum, Leishmania chagasi, L. braziliensis , and L. tropica promastigotes and amastigotes resulting in IC 50 -values of 0.001–5.495 μM (Mäntylä et al, 2004a , b ; Reimão et al, 2012 ; Jamal et al, 2015 ). Animal models showed that the in vivo efficiency was higher when prodrugs of buparvaquone were applied (Croft et al, 1992 ; Garnier et al, 2007 ) or when a nanoliposomal drug preparation was used (da Costa-Silva et al, 2017 ).…”

Section: Targeting Transport Processes Of Parasites At Different Levementioning

confidence: 99%

Targeting Channels and Transporters in Protozoan Parasite Infections

2018

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Infectious diseases caused by pathogenic protozoa are among the most significant causes of death in humans. Therapeutic options are scarce and massively challenged by the emergence of resistant parasite strains. Many of the current anti-parasite drugs target soluble enzymes, generate unspecific oxidative stress, or act by an unresolved mechanism within the parasite. In recent years, collections of drug-like compounds derived from large-scale phenotypic screenings, such as the malaria or pathogen box, have been made available to researchers free of charge boosting the identification of novel promising targets. Remarkably, several of the compound hits have been found to inhibit membrane proteins at the periphery of the parasites, i.e., channels and transporters for ions and metabolites. In this review, we will focus on the progress made on targeting channels and transporters at different levels and the potential for use against infections with apicomplexan parasites mainly Plasmodium spp. (malaria) and Toxoplasma gondii (toxoplasmosis), with kinetoplastids Trypanosoma brucei (sleeping sickness), Trypanosoma cruzi (Chagas disease), and Leishmania ssp. (leishmaniasis), and the amoeba Entamoeba histolytica (amoebiasis).

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Section: Targeting Transport Processes Of Parasites At Different Levementioning

confidence: 99%

Targeting Channels and Transporters in Protozoan Parasite Infections

2018

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“…where k B is the Boltzmann constant, T is the absolute temperature, η is the viscosity of the solvent, and D h and D app are the hydrodynamic diameter and the apparent diffusion coefficient, respectively (Costa-Silva et al, 2017).…”

Section: Methodsmentioning

confidence: 99%

“…The measurement for each sample was repeated for at least three times. In order to avoid multiple scattering, the samples were diluted 20-fold in the appropriate buffer before the measurements (Lamy et al, 1966; Costa-Silva et al, 2017). LP-SERT treatment was analyzed by culture microtitration as previously reported (Park and Lee, 2008).…”

Section: Methodsmentioning

confidence: 99%

“…Finding new uses for FDA-approved drugs is known as drug repositioning, and has been considered an excellent approach for neglected diseases to reduce the costs and time of the research (Andrews et al, 2014; Huang et al, 2015; Costa-Silva et al, 2017). Currently, all available drugs for the clinical treatment of leishmaniases were introduced by the repositioning approach.…”

Section: Introductionmentioning

confidence: 99%

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Sertraline Delivered in Phosphatidylserine Liposomes Is Effective in an Experimental Model of Visceral Leishmaniasis

Romanelli

Costa-Silva

Cunha-Júnior

et al. 2019

Front. Cell. Infect. Microbiol.

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Liposomes containing phosphatidylserine (PS) has been used for the delivery of drugs into the intramacrophage milieu. Leishmania (L.) infantum parasites live inside macrophages and cause a fatal and neglected viscerotropic disease, with a toxic treatment. Sertraline was studied as a free formulation (SERT) and also entrapped into phosphatidylserine liposomes (LP-SERT) against intracellular amastigotes and in a murine model of visceral leishmaniasis. LP-SERT showed a potent activity against intracellular amastigotes with an EC50 value of 2.5 μM. The in vivo efficacy of SERT demonstrated a therapeutic failure. However, when entrapped into negatively charged liposomes (−58 mV) of 125 nm, it significantly reduced the parasite burden in the mice liver by 89% at 1 mg/kg, reducing the serum levels of the cytokine IL-6 and upregulating the levels of the chemokine MCP-1. Histopathological studies demonstrated the presence of an inflammatory infiltrate with the development of granulomas in the liver, suggesting the resolution of the infection in the treated group. Delivery studies showed fluorescent-labeled LP-SERT in the liver and spleen of mice even after 48 h of administration. This study demonstrates the efficacy of PS liposomes containing sertraline in experimental VL. Considering the urgent need for VL treatments, the repurposing approach of SERT could be a promising alternative.

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“…Another drug under test for liposome delivery is buparvaquone, an extensively studied drug for the treatment of visceral leishmaniosis. da Costa-Silva et al reported that buparvaquone, which has an immunomodulatory effect in host cells, when entrapped in phosphatidylserine (PS) exposing-liposomes, as a delivery approach to macrophage, is highly effective at low doses at eliminating Leishmania infantum parasites in a hamster model ( 52 ).…”

Section: Liposomes As Carrier For Drugsmentioning

confidence: 99%

The Multirole of Liposomes in Therapy and Prevention of Infectious Diseases

et al. 2018

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Liposomes are closed bilayer structures spontaneously formed by hydrated phospholipids that are widely used as efficient delivery systems for drugs or antigens, due to their capability to encapsulate bioactive hydrophilic, amphipathic, and lipophilic molecules into inner water phase or within lipid leaflets. The efficacy of liposomes as drug or antigen carriers has been improved in the last years to ameliorate pharmacokinetics and capacity to release their cargo in selected target organs or cells. Moreover, different formulations and variations in liposome composition have been often proposed to include immunostimulatory molecules, ligands for specific receptors, or stimuli responsive compounds. Intriguingly, independent research has unveiled the capacity of several phospholipids to play critical roles as intracellular messengers in modulating both innate and adaptive immune responses through various mechanisms, including (i) activation of different antimicrobial enzymatic pathways, (ii) driving the fusion–fission events between endosomes with direct consequences to phagosome maturation and/or to antigen presentation pathway, and (iii) modulation of the inflammatory response. These features can be exploited by including selected bioactive phospholipids in the bilayer scaffold of liposomes. This would represent an important step forward since drug or antigen carrying liposomes could be engineered to simultaneously activate different signal transduction pathways and target specific cells or tissues to induce antigen-specific T and/or B cell response. This lipid-based host-directed strategy can provide a focused antimicrobial innate and adaptive immune response against specific pathogens and offer a novel prophylactic or therapeutic option against chronic, recurrent, or drug-resistant infections.

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Nanoliposomal Buparvaquone Immunomodulates Leishmania infantum-Infected Macrophages and Is Highly Effective in a Murine Model

Cited by 28 publications

References 52 publications

Targeting Channels and Transporters in Protozoan Parasite Infections

Targeting Channels and Transporters in Protozoan Parasite Infections

Sertraline Delivered in Phosphatidylserine Liposomes Is Effective in an Experimental Model of Visceral Leishmaniasis

The Multirole of Liposomes in Therapy and Prevention of Infectious Diseases

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