Treatment failure of pentavalent antimonial therapy for human visceral leishmaniasis: a meta-analysis

Jones, Caitlin; Welburn, Susan C.; Jones, Joshua D.

doi:10.29392/joghr.3.e2019048

Journal of Global Health Reports

2019

DOI: 10.29392/joghr.3.e2019048

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Treatment failure of pentavalent antimonial therapy for human visceral leishmaniasis: a meta-analysis

Caitlin Jones¹,

Susan C. Welburn²,

Joshua D. Jones³

Abstract: Back Background ground Visceral leishmaniasis is found primarily in developing countries and is a neglected tropical disease that causes approximately 300,000 new cases and 20,000 deaths annually and is often fatal if untreated. Monotherapy with pentavalent antimonials (SSG or MA) is a second-line treatment option in many endemic areas. This meta-analysis provides regional and national analyses of the proportions of antimonial treatment failures at the end-of-treatment and at follow-up according to the drug us… Show more

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Cited by 2 publications

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Global Lipidomics Reveals the Lipid Composition Heterogeneity of Extracellular Vesicles from Drug-Resistant Leishmania

Kim,

Ibarra-Meneses,

Fernandez-Prada

et al. 2024

Metabolites

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Background: The rise of drug-resistant Leishmania strains presents a significant challenge in the treatment of Leishmaniasis, a neglected tropical disease. Extracellular vesicles (EVs) produced by these parasites have gained attention for their role in drug resistance and host–pathogen interactions. Methods: This study developed and applied a novel lipidomics workflow to explore the lipid profiles of EVs from three types of drug-resistant Leishmania infatum strains compared to a wild-type strain. EVs were isolated through ultracentrifugation, and their lipid content was extracted using a modified Matyash protocol. LC-MS analysis was performed, and data processing in MS-DIAL enabled lipid identification and quantification. Statistical analysis in MetaboAnalyst revealed strain-specific lipid alterations, highlighting potential links between lipid composition and drug resistance mechanisms. Results: Our results show distinct alterations in lipid composition associated with drug resistance. Specifically, drug-resistant strains exhibited reduced levels of phosphatidylcholine (PC) and phosphatidylglycerol (PG), particularly in the amphotericin B-resistant strain LiAmB1000.1. Sterol and glycerolipid species, including cholesteryl ester (CE) and triacylglycerol (TG) were also found to be diminished in LiAmB1000.1. These changes suggest significant lipid remodeling under drug pressure, potentially altering the biophysical properties of EV membranes and their capacity for molecule transfer. Furthermore, the lipidomic profiles of EVs from the other resistant strains, LiSb2000.1 and LiMF200.5, also displayed unique alterations, underscoring strain-specific adaptations to different drug resistance mechanisms. Conclusions: These significant alterations in lipid composition suggest potential lipid-based mechanisms underlying drug resistance in Leishmania, providing new avenues for therapeutic intervention.

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Global Lipidomics Reveals the Lipid Composition Heterogeneity of Extracellular Vesicles from Drug-Resistant Leishmania

Kim,

Ibarra-Meneses,

Fernandez-Prada

et al. 2024

Metabolites

View full text Add to dashboard Cite

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Efficacy and safety of pharmacotherapeutic interventions used in visceral leishmaniasis clinical trials

Tiwari¹,

Bashir²,

Sahu³

et al. 2022

Asian Pacific Journal of Tropical Medicine

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Objective: To compare the efficacy and safety outcomes of different antileishmanial agents used in visceral leishmaniasis clinical trials. Methods: A systematic literature search in PubMed/MEDLINE, EMBASE, Cochrane, and Google Scholar was done using keywords “randomized controlled trials”, “antileishmanial” and “visceral leishmaniasis”. The outcomes included were cure rate, overall withdrawals, relapse rate, and treatment-emergent adverse events. Effect estimates through the frequentist network meta-analysis approach were presented as OR with 95% CI. Rankogram plots were used for identifying the “best intervention” based on p-scores obtained using the surface under the cumulative ranking. The risk of bias was evaluated by using Pedro Scale. Results: Seventeen randomized controlled trials with 5 143 visceral leishmaniasis patients who received different antileishmanial agents (amphotericin B, miltefosine, paromomycin, meglumine antimoniate, sodium stibogluconate, sitamaquine, and pentavalent antimonials) and met the inclusion criteria were included. For efficacy outcomes of the treatments, the rankogram of the network meta-analysis revealed that paromomycin (p-score=0.814 8) has the highest probability of being best in the pool, followed by sodium stibogluconate (OR 0.82, 95% CI 0.24-2.79, p-score=0.758 0), amphotericin B+miltefosine (OR 0.66, 95% CI 0.02-19.04, p-score=0.732 9) as compared to the remaining treatments; however, the most of the treatment-emergent adverse events were reported with sitamaquine. Conclusions: Paromomycin reported the highest cure rates, while the maximum treatment-emergent adverse events were seen with sitamaquine.

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Treatment failure of pentavalent antimonial therapy for human visceral leishmaniasis: a meta-analysis

Cited by 2 publications

References 55 publications

Global Lipidomics Reveals the Lipid Composition Heterogeneity of Extracellular Vesicles from Drug-Resistant Leishmania

Global Lipidomics Reveals the Lipid Composition Heterogeneity of Extracellular Vesicles from Drug-Resistant Leishmania

Efficacy and safety of pharmacotherapeutic interventions used in visceral leishmaniasis clinical trials

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