2001
DOI: 10.4269/ajtmh.2001.65.685
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Phase 2 trial of WR6026, an orally administered 8-aminoquinoline, in the treatment of visceral leishmaniasis caused by Leishmania chagasi.

Abstract: Abstract. There are no recognized orally administered treatments for any of the leishmaniases. The 8-aminoquinoline WR6026 is an orally administered analog of primaquine that cured 50% of patients with kala-azar in Kenya at a dose of 1 mg/kg/day for 28 days. A further phase 2, open-label, dose-escalating safety and efficacy study was performed for kala-azar in Brazil. Cure rates for Brazilian patients treated for 28 days were as follows: 1 mg/kg/day: 0 of 4 (0%); 1.5 mg/kg/day: 1 of 6 (17%); 2.0 mg/kg/day: 4 o… Show more

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Cited by 110 publications
(69 citation statements)
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“…In conclusion, concerns about severe side effects from drug toxicity in the treatment of leishmaniasis, such as nephrotoxicity (74), pancreatitis (75), and hepatotoxicity (76,77) along with the development of drug resistance (78), have led to a need for the development of combined therapies for the leishmaniases, and notably for VL and drug-resistant cutaneous leishmaniasis. Our data suggest that a short-duration preconditioning regimen using broad-spectrum RTKIs, if proven safe in patients with active leishmaniasis, NO production by adherent splenocytes from infected mice treated as indicated.…”
Section: Discussionmentioning
confidence: 99%
“…In conclusion, concerns about severe side effects from drug toxicity in the treatment of leishmaniasis, such as nephrotoxicity (74), pancreatitis (75), and hepatotoxicity (76,77) along with the development of drug resistance (78), have led to a need for the development of combined therapies for the leishmaniases, and notably for VL and drug-resistant cutaneous leishmaniasis. Our data suggest that a short-duration preconditioning regimen using broad-spectrum RTKIs, if proven safe in patients with active leishmaniasis, NO production by adherent splenocytes from infected mice treated as indicated.…”
Section: Discussionmentioning
confidence: 99%
“…The sitamaquine sample with the lowest concentration analyzed here, 5 ng/mL, is sufficient to quantitate clinically relevant levels of sitamaquine in blood. In phase II clinical trials, the lowest dose administered gave mean plasma trough concentrations (i.e., concentration immediately before administration of the next dose) of 21 ng/mL after 28 d of administration [13].…”
Section: Accuracy and Precisionmentioning
confidence: 99%
“…The relevant examples are those of two anti-malarial compounds, NPC 1161 [53] and, especially, sitamaquine that is already in an advanced phase of clinical trials (see Section 4.3) [54][55][56]. …”
Section: Against Leishmaniasismentioning
confidence: 99%