Targeting liver stage malaria with metformin
Iset Medina Vera, … , Maria M. Mota, Liliana Mancio-Silva
Iset Medina Vera, … , Maria M. Mota, Liliana Mancio-Silva
Published December 19, 2019
Citation Information: JCI Insight. 2019;4(24):e127441. https://doi.org/10.1172/jci.insight.127441.
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Research Article Infectious disease Microbiology

Targeting liver stage malaria with metformin

Abstract

Despite an unprecedented 2 decades of success, the combat against malaria — the mosquito-transmitted disease caused by Plasmodium parasites — is no longer progressing. Efforts toward eradication are threatened by the lack of an effective vaccine and a rise in antiparasite drug resistance. Alternative approaches are urgently needed. Repurposing of available, approved drugs with distinct modes of action are being considered as viable and immediate adjuncts to standard antimicrobial treatment. Such strategies may be well suited to the obligatory and clinically silent first phase of Plasmodium infection, where massive parasite replication occurs within hepatocytes in the liver. Here, we report that the widely used antidiabetic drug, metformin, impairs parasite liver stage development of both rodent-infecting Plasmodium berghei and human-infecting P. falciparum parasites. Prophylactic treatment with metformin curtails parasite intracellular growth in vitro. An additional effect was observed in mice with a decrease in the numbers of infected hepatocytes. Moreover, metformin provided in combination with conventional liver- or blood-acting antimalarial drugs further reduced the total burden of P. berghei infection and substantially lessened disease severity in mice. Together, our findings indicate that repurposing of metformin in a prophylactic regimen could be considered for malaria chemoprevention.

Authors

Iset Medina Vera, Margarida T. Grilo Ruivo, Leonardo F. Lemos Rocha, Sofia Marques, Sangeeta N. Bhatia, Maria M. Mota, Liliana Mancio-Silva

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Figure 2

Metformin treatment reduces P. falciparum development in human hepatocytes.

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Metformin treatment reduces P. falciparum development in human hepatocyt...
(A) Timeline of metformin treatment, infection, and sample collection. Primary human hepatocytes were infected with 60,000 P. falciparum sporozoites. Prophylactic dosing of metformin (50 and 200 μM) started at 3 hours after infection and repeated daily. Cultures were fixed at day 4 after infection. (B) Representative immunofluorescence images of P. falciparum parasites stained with anti-PfHSP70 antibodies (shown in red) for nontreated control and 200 μM metformin treatment. Nuclei were stained with Hoechst (shown in blue). Scale bar: 5 μm. (C and D) Quantification of P. falciparum size distribution (C) and density (D) at day 4 after infection. The total number of parasites analyzed in 2 independent experiments is 190, CTL; 143, MET 50 μM; 140, MET 200 μM. The outliers in the box plots represent 5% of data points. The box plots depict the minimum and maximum values (whiskers), the upper and lower quartiles, and the median. The length of the box represents the interquartile range. The dots in the scatter plot represent 1 well, and the horizontal bars show the mean, in 1 of the 2 experiments. Ordinary 1-way ANOVA test, ****P < 0.0001.