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Miltefosine enhances the fitness of a non-virulent drug-resistant Leishmania infantum strain.

J Antimicrob Chemother. 2019; 
Eberhardt E, Bulté D, Van Bockstal L, Van den Kerkhof M, Cos P, Delputte P, Hendrickx S, Maes L, Caljon G.
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Codon Optimization 12 The WT and MIL-R strain were transfected with the red-shifted firefly luciferase gene variant PpyRE927 that was codon optimized for expression in Leishmania (GenScript).... For integration in the pLEXSY-hyg2 vector (Jena Bioscience), NcoI and NotI restriction sites were added to the 50 and 30 end respectively (GenScript). Get A Quote

摘要

Miltefosine is currently the only oral drug for visceral leishmaniasis, and although deficiency in an aminophospholipid/miltefosine transporter (MT) is sufficient to elicit drug resistance, very few naturally miltefosine-resistant (MIL-R) strains have yet been isolated. This study aimed to make a detailed analysis of the impact of acquired miltefosine resistance and miltefosine treatment on in vivo infection.,Bioluminescent versions of a MIL-R strain and its syngeneic parental line were generated by integration of the red-shifted firefly luciferase PpyRE9. The fitness of both lines was compared in vitro (growth rate, metacyclogenesis and macrophage infectivity) and in BALB/c mice through non-invasive biolumines... More

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