Antileishmanial Aminopyrazoles: Studies into Mechanisms and Stability of Experimental Drug Resistance

Kerkhof, Magali Van den; Mabille, Dorien; Hendrickx, Sarah; Leprohon, Philippe; Mowbray, Charles E.; Braillard, Stéphanie; Ouellette, Marc; Maes, Louis; Caljon, Guy

doi:10.1128/aac.00152-20

Cited by 9 publications

(9 citation statements)

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“…Although successful for other compounds, in vitro and in vivo resistance selection procedures were unable to generate Leishmania clones resistant to our oxaborole compounds. Additionally, the role of efflux pumps as a potential mechanism of resistance to these compounds was evaluated using inhibitors of ABC-transporters such as verapamil, cyclosporine A and probenecid [ 51 , 55 , 56 , 57 , 58 ]. These studies suggest that antileishmanial oxaboroles are not substrates of the evaluated transporters, unlike several other antileishmanials shown to be prone to efflux through these pumps [ 39 , 42 , 43 , 44 , 45 , 46 , 47 , 48 , 49 ].…”

Section: Discussionmentioning

confidence: 99%

“…The medium was replaced 2 h later with fresh RPMI-1640 medium containing oxaborole and one of the ABC-transporter inhibitors, namely, verapamil (MDR and MRP inhibitor), cyclosporine A (broad specificity efflux inhibitor), or probenecid (MRP inhibitor). The ABC-transporter inhibitor was added at a single concentration below its EC 50 which was previously determined [ 51 ]; verapamil was added at 8 µM, probenecid at 700 µM, and cyclosporine A at 1.5 µM for L. infantum and 2 µM for L. donovani . A 4-fold dilution series was prepared for the oxaboroles with the highest in-test concentration of 10 µM.…”

Section: Methodsmentioning

confidence: 99%

“…L. infantum and L. donovani log-phase promastigotes were diluted to a concentration of 10 6 promastigotes/well in a 96-well plate, whereafter dilutions of Sb III and oxaborole were added either with or without the ABC-transporter inhibitor. Pump inhibitor concentrations were previously determined and were identical to those in the intracellular assay [ 51 ]. EC 50 -values with and without ABC-transporter inhibitor were determined as described above in the extracellular susceptibility assay and the different conditions were compared.…”

Section: Methodsmentioning

confidence: 99%

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Identification of Resistance Determinants for a Promising Antileishmanial Oxaborole Series

et al. 2021

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Current treatment options for visceral leishmaniasis have several drawbacks, and clinicians are confronted with an increasing number of treatment failures. To overcome this, the Drugs for Neglected Diseases initiative (DNDi) has invested in the development of novel antileishmanial leads, including a very promising class of oxaboroles. The mode of action/resistance of this series to Leishmania is still unknown and may be important for its further development and implementation. Repeated in vivo drug exposure and an in vitro selection procedure on both extracellular promastigote and intracellular amastigote stages were both unable to select for resistance. The use of specific inhibitors for ABC-transporters could not demonstrate the putative involvement of efflux pumps. Selection experiments and inhibitor studies, therefore, suggest that resistance to oxaboroles may not emerge readily in the field. The selection of a genome-wide cosmid library coupled to next-generation sequencing (Cos-seq) was used to identify resistance determinants and putative targets. This resulted in the identification of a highly enriched cosmid, harboring genes of chromosome 2 that confer a subtly increased resistance to the oxaboroles tested. Moderately enriched cosmids encompassing a region of chromosome 34 contained the cleavage and polyadenylation specificity factor (cpsf) gene, encoding the molecular target of several related benzoxaboroles in other organisms.

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Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

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Identification of Resistance Determinants for a Promising Antileishmanial Oxaborole Series

et al. 2021

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“…In a recent study, the EC 50 and EC 90 values of the four different drugs (AmB, miltefosine, paramomycin and SSG) under different conditions of media flow like static, low flow and high flow were evaluated. Besides, IC 50 values of three different drugs DNDi‐1044, DNDi‐8012 and DNDi‐5561 were also evaluated using intracellular and extracellular promastigote assays (Van den Kerkhof et al, 2020). The involvement of efflux pump inhibitors like MDR and MRP were evaluated.…”

Section: Pharmacology Of Antileishmanial Drugsmentioning

confidence: 99%

“…AmB, miltefosine, paramomycin and SSG) under different conditions of media flow like static, low flow and high flow were evaluated.Besides, IC 50 values of three different drugs DNDi-1044, DNDi-8012 and DNDi-5561 were also evaluated using intracellular and extracellular promastigote assays (Van denKerkhof et al, 2020). The involvement of efflux pump inhibitors like MDR and MRP were evaluated.The ABC transport inhibitors were evaluated for their cytotoxic effects on MRC5 cells and their inhibitors effect on both amastigote and promastigote forms (Van denKerkhof et al, 2020). To determine the drug susceptibility of clinical Leishmania isolates in laboratory conditions, different cell-based drug susceptibility assays were evaluated.…”

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confidence: 99%

Road‐map of pre‐clinical treatment for Visceral Leishmaniasis

Mazire

Agarwal

Roy

2021

Drug Development Research

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Visceral leishmaniasis (VL) or Kala‐azar, is the most lethal form of leishmaniasis, is still prevalent in many countries where it is endemic. It is a threat to human life caused by protozoan parasite Leishmania donovani. The severity of the disease is further increased as the treated individuals might have a chance of developing Post Kala‐azar Dermal Leishmaniasis (PKDL) in the long run. Moreover, several countries have reported high number of HIV‐VL co‐infected patients. Therefore, there is a dire need for the development of efficient diagnostic methods and drugs in order to combat the disease and to control the spread of disease. At present, the treatment for VL entirely relies on therapeutic drugs as no vaccine is available yet. Ever since 1900s a series of drugs have been invented and used for treatment of VL; but the need for one such cost‐effective treatment that would completely cure the disease with minimal side‐effects, low relapse rate with high efficacy and less toxicity remains yet to be fulfilled. Therefore, identifying novel compounds is very crucial to develop potent antileishmanial agents. Thus, this review enlists several instances of drug development, including the pharmacokinetic and pharmacodynamic properties of antileishmanial drugs, different experimental animal models used to investigate the disease progression and to analyze treatment dosage and pharmacological aspect of drugs. Furthermore, the existing gap in drug development and future measures to improve the process are also discussed in this review.

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In Vivo Bioluminescence Imaging Reveals Differences in Leishmania infantum Parasite Killing Kinetics by Antileishmanial Reference Drugs

Hendrickx,

Feijens,

Escudié

et al. 2024

ACS Infect. Dis.

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The bioluminescent Leishmania infantum BALB/c mouse model was used to evaluate the parasiticidal drug action kinetics of the reference drugs miltefosine, paromomycin, sodium stibogluconate, and liposomal amphotericin B. Infected mice were treated for 5 days starting from 7 days post-infection, and parasite burdens were monitored over time via bioluminescence imaging (BLI). Using nonlinear regression analyses of the BLI signal, the parasite elimination half-life (t 1/2) in the liver, bone marrow, and whole body was determined and compared for the different treatment regimens. Significant differences in parasiticidal kinetics were recorded. A single intravenous dose of 0.5 mg/kg liposomal amphotericin B was the fastest acting with a t 1/2 of less than 1 day. Intraperitoneal injection of paromomycin at 320 mg/kg for 5 days proved to be the slowest with a t 1/2 of about 5 days in the liver and 16 days in the bone marrow. To conclude, evaluation of the cidal kinetics of the different antileishmanial reference drugs revealed striking differences in their parasite elimination half-lives. This BLI approach also enables an in-depth pharmacodynamic comparison between novel drug leads and may constitute an essential tool for the design of potential drug combinations.

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Antileishmanial Aminopyrazoles: Studies into Mechanisms and Stability of Experimental Drug Resistance

Cited by 9 publications

References 80 publications

Identification of Resistance Determinants for a Promising Antileishmanial Oxaborole Series

Identification of Resistance Determinants for a Promising Antileishmanial Oxaborole Series

Road‐map of pre‐clinical treatment for Visceral Leishmaniasis

In Vivo Bioluminescence Imaging Reveals Differences in Leishmania infantum Parasite Killing Kinetics by Antileishmanial Reference Drugs

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