The Distribution of Nifurtimox Across the Healthy and Trypanosome-Infected Murine Blood-Brain and Blood-Cerebrospinal Fluid Barriers

Jeganathan, S; Sanderson, Lisa; Dogruel, Murat; Rodgers, Jean; Croft, Simon L.; Thomas, Sarah

doi:10.1124/jpet.110.172981

Cited by 24 publications

(36 citation statements)

References 35 publications

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“…This was consistent with an earlier study in rats, which found that 35 S-nifurtimox is rapidly distributed throughout the host, and that both the blood-brain or placental barriers were permeable to the drug [175]. This could be the result of its lipophilicity (octanol-saline partition coefficient = 5.46 [173]), which might allow a simple diffusion across membranes. Certainly, no transporter for nifurtimox uptake has, to date, been identified, either in the host or in trypanosomes, including with RNAi library screens [171].…”

Section: Nifurtimoxsupporting

confidence: 91%

“…The accumulation of nifurtimox across the BBB was investigated by Sarah Thomas using both a murine perfusion system and an in vitro model based on immortalised human BBB cells [173,174]. Nifurtimox readily crossed the BBB and blood-CSF barriers and this was not significantly different in healthy mice or infected mice where the barrier integrity had been compromised [173]. This almost certainly means that the uptake of nifurtimox at the BBB is trans-cellular rather than paracellular (i.e., between cells).…”

Section: Nifurtimoxmentioning

confidence: 99%

“…Yet, nifurtimox, bearing a polar nitro group, is not very lipophilic, the trans-cellular uptake at the BBB is consistent with a transporter, and it has been argued that almost all drugs require a transport mechanism [176] and that absence of proof for the involvement of a transporter simply means we haven't looked well enough [177]. Moreover, Jeganathan et al reported a higher concentration of 3 H-nifurtimox in the CNS compared with plasma [173], which would be hard to explain without active import, especially since there is also a component of extrusion across the barrier (see below). Of potential importance for NECT, eflornithine reduced CNS accumulation of 3 H-nifurtimox by > 50%, presumably by interfering at the level of a transporter at the barrier [173], although that result could not be reproduced in the later study with cultured human BBB cells [174].…”

Section: Nifurtimoxmentioning

confidence: 99%

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The Drugs of Sleeping Sickness: Their Mechanisms of Action and Resistance, and a Brief History

Koning

2020

TropicalMed

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With the incidence of sleeping sickness in decline and genuine progress being made towards the WHO goal of eliminating sleeping sickness as a major public health concern, this is a good moment to evaluate the drugs that ‘got the job done’: their development, their limitations and the resistance that the parasites developed against them. This retrospective looks back on the remarkable story of chemotherapy against trypanosomiasis, a story that goes back to the very origins and conception of chemotherapy in the first years of the 20 century and is still not finished today.

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Section: Nifurtimoxsupporting

confidence: 91%

Section: Nifurtimoxmentioning

confidence: 99%

Section: Nifurtimoxmentioning

confidence: 99%

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The Drugs of Sleeping Sickness: Their Mechanisms of Action and Resistance, and a Brief History

Koning

2020

TropicalMed

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“…1) and the known ability of nifurtimox to penetrate the blood brain barrier2425, we pursued further studies of nifurtimox in neural tumor cell lines. In order to determine the mechanism of decreased neural tumor cell viability after treatment with nifurtimox, we performed assays for DNA ladder formation and for cleavage of PARP to establish whether nifurtimox treatment induced apoptosis.…”

Section: Resultsmentioning

confidence: 99%

“…Nifurtimox has been previously shown to penetrate the BBB in preclinical models2425, and nifurtimox has demonstrated efficacy in late stage African trypanosomiasis (African sleeping sickness), defined by the presence of active CNS infection3536. It is unclear whether the penetrability of the BBB is similar in patients with infection compared to those with malignancies.…”

Section: Discussionmentioning

confidence: 99%

Nifurtimox Is Effective Against Neural Tumor Cells and Is Synergistic with Buthionine Sulfoximine

Zhang

Scorsone

et al. 2016

Sci Rep

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Children with aggressive neural tumors have poor survival rates and novel therapies are needed. Previous studies have identified nifurtimox and buthionine sulfoximine (BSO) as effective agents in children with neuroblastoma and medulloblastoma. We hypothesized that nifurtimox would be effective against other neural tumor cells and would be synergistic with BSO. We determined neural tumor cell viability before and after treatment with nifurtimox using MTT assays. Assays for DNA ladder formation and poly-ADP ribose polymerase (PARP) cleavage were performed to measure the induction of apoptosis after nifurtimox treatment. Inhibition of intracellular signaling was measured by Western blot analysis of treated and untreated cells. Tumor cells were then treated with combinations of nifurtimox and BSO and evaluated for viability using MTT assays. All neural tumor cell lines were sensitive to nifurtimox, and IC50 values ranged from approximately 20 to 210 μM. Nifurtimox treatment inhibited ERK phosphorylation and induced apoptosis in tumor cells. Furthermore, the combination of nifurtimox and BSO demonstrated significant synergistic efficacy in all tested cell lines. Additional preclinical and clinical studies of the combination of nifurtimox and BSO in patients with neural tumors are warranted.

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Synthesis, in vitro Antileishmanial Efficacy and Hit/Lead Identification of Nitrofurantoin‐Triazole Hybrids

et al. 2022

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Leishmaniasis is a vector-borne neglected parasitic infection affecting thousands of individuals, mostly among populations in low-to moderate-income developing countries. In the absence of protective vaccines, the management of the disease banks solely on chemotherapy. However, the clinical usefulness of current antileishmanial drugs is threatened by their toxicity and the emergence of multidrug-resistant strains of the causative pathogens. This emphasizes the imperative for the development of new and effective antileishmanial agents. In this regard, we synthesized and evaluated in vitro the antileishmanial activity and cytotoxicity profile of a series of nitrofurantoin-triazole hybrids. The nitrofurantoin derivative 1 featuring propargyl moiety was distinctively the most active of all, was nontoxic to human cells and possessed submicromolar cellular activity selectively directed towards the pathogens of the life threatening visceral leishmaniasis. Hence it was identified as potential antileishmanial lead for further investigation into its prospective to act as alternative to therapies.

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The Distribution of Nifurtimox Across the Healthy and Trypanosome-Infected Murine Blood-Brain and Blood-Cerebrospinal Fluid Barriers

Cited by 24 publications

References 35 publications

The Drugs of Sleeping Sickness: Their Mechanisms of Action and Resistance, and a Brief History

The Drugs of Sleeping Sickness: Their Mechanisms of Action and Resistance, and a Brief History

Nifurtimox Is Effective Against Neural Tumor Cells and Is Synergistic with Buthionine Sulfoximine

Synthesis, in vitro Antileishmanial Efficacy and Hit/Lead Identification of Nitrofurantoin‐Triazole Hybrids

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