Safety and pharmacokinetic profile of fixed-dose ivermectin with an innovative 18mg tablet in healthy adult volunteers

Ivermectin is a pivotal drug for the control of onchocerciasis and lymphatic filariasis, which is increasingly identified as a useful drug for the control of other Neglected Tropical Diseases. Its role in the treatment of soil transmitted helminthiasis through improved efficacy against Trichuris tri...

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Autores principales: Muñoz, Jose, Ballester, Maria Rosa, Antonijoan, Rosa Maria, Gich, Ignasi, Rodríguez, Montse, Colli, Enrico, Gold, Silvia, Krolewiecki, Alejandro J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2018
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5773004/
https://www.ncbi.nlm.nih.gov/pubmed/29346388
http://dx.doi.org/10.1371/journal.pntd.0006020
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author Muñoz, Jose
Ballester, Maria Rosa
Antonijoan, Rosa Maria
Gich, Ignasi
Rodríguez, Montse
Colli, Enrico
Gold, Silvia
Krolewiecki, Alejandro J.
author_facet Muñoz, Jose
Ballester, Maria Rosa
Antonijoan, Rosa Maria
Gich, Ignasi
Rodríguez, Montse
Colli, Enrico
Gold, Silvia
Krolewiecki, Alejandro J.
author_sort Muñoz, Jose
collection PubMed
description Ivermectin is a pivotal drug for the control of onchocerciasis and lymphatic filariasis, which is increasingly identified as a useful drug for the control of other Neglected Tropical Diseases. Its role in the treatment of soil transmitted helminthiasis through improved efficacy against Trichuris trichiura in combination with other anthelmintics might accelerate the progress towards breaking transmission. Ivermectin is a derivative of Avermectin B1, and consists of an 80:20 mixture of the equipotent homologous 22,23 dehydro B1a and B1b. Pharmacokinetic characteristics and safety profile of ivermectin allow to explore innovative uses to further expand its utilization through mass drug administration campaigns to improve coverage rates. We conducted a phase I clinical trial with 54 healthy adult volunteers who sequentially received 2 experimental treatments using a new 18 mg ivermectin tablet in a fixed-dose strategy of 18 and 36 mg single dose regimens, compared to the standard, weight based 150–200 μg/kg, regimen. Volunteers were recruited in 3 groups based on body weight. Plasma concentrations of ivermectin were measured through HPLC up to 168 hours post treatment. Safety data showed no significant differences between groups and no serious adverse events: headache was the most frequent adverse event in all treatment groups, none of them severe. Pharmacokinetic parameters showed a half-life between 81 and 91 h in the different treatment groups. When comparing the systemic bioavailability (AUC(0)(t) and C(max)) of the reference product (WA-ref) with the other two study groups using fixed doses, we observed an overall increase in AUC(0)(t) and C(max) for the two experimental treatments of 18 mg and 36 mg. Body mass index (BMI) and weight were associated with t(1/2) and V/F, probably reflecting the high liposolubility of IVM with longer retention times proportional to the presence of more adipose tissue. Systemic exposure to ivermectin (AUC(0)(t) or C(max)) was not associated with BMI or weight in our study. These findings contribute to further understand the pharmacokinetic characteristics of ivermectin, highlighting its safety across different dosing regimens. They also correlate with known pharmacokinetic parameters showing stable levels of AUC and C(max) across a wide range of body weights, which justifies the strategy of fix dosing from a pharmacokinetic perspective. TRIAL REGISTRATION: ClinicalTrials.gov NCT03173742.
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spelling pubmed-57730042018-01-26 Safety and pharmacokinetic profile of fixed-dose ivermectin with an innovative 18mg tablet in healthy adult volunteers Muñoz, Jose Ballester, Maria Rosa Antonijoan, Rosa Maria Gich, Ignasi Rodríguez, Montse Colli, Enrico Gold, Silvia Krolewiecki, Alejandro J. PLoS Negl Trop Dis Research Article Ivermectin is a pivotal drug for the control of onchocerciasis and lymphatic filariasis, which is increasingly identified as a useful drug for the control of other Neglected Tropical Diseases. Its role in the treatment of soil transmitted helminthiasis through improved efficacy against Trichuris trichiura in combination with other anthelmintics might accelerate the progress towards breaking transmission. Ivermectin is a derivative of Avermectin B1, and consists of an 80:20 mixture of the equipotent homologous 22,23 dehydro B1a and B1b. Pharmacokinetic characteristics and safety profile of ivermectin allow to explore innovative uses to further expand its utilization through mass drug administration campaigns to improve coverage rates. We conducted a phase I clinical trial with 54 healthy adult volunteers who sequentially received 2 experimental treatments using a new 18 mg ivermectin tablet in a fixed-dose strategy of 18 and 36 mg single dose regimens, compared to the standard, weight based 150–200 μg/kg, regimen. Volunteers were recruited in 3 groups based on body weight. Plasma concentrations of ivermectin were measured through HPLC up to 168 hours post treatment. Safety data showed no significant differences between groups and no serious adverse events: headache was the most frequent adverse event in all treatment groups, none of them severe. Pharmacokinetic parameters showed a half-life between 81 and 91 h in the different treatment groups. When comparing the systemic bioavailability (AUC(0)(t) and C(max)) of the reference product (WA-ref) with the other two study groups using fixed doses, we observed an overall increase in AUC(0)(t) and C(max) for the two experimental treatments of 18 mg and 36 mg. Body mass index (BMI) and weight were associated with t(1/2) and V/F, probably reflecting the high liposolubility of IVM with longer retention times proportional to the presence of more adipose tissue. Systemic exposure to ivermectin (AUC(0)(t) or C(max)) was not associated with BMI or weight in our study. These findings contribute to further understand the pharmacokinetic characteristics of ivermectin, highlighting its safety across different dosing regimens. They also correlate with known pharmacokinetic parameters showing stable levels of AUC and C(max) across a wide range of body weights, which justifies the strategy of fix dosing from a pharmacokinetic perspective. TRIAL REGISTRATION: ClinicalTrials.gov NCT03173742. Public Library of Science 2018-01-18 /pmc/articles/PMC5773004/ /pubmed/29346388 http://dx.doi.org/10.1371/journal.pntd.0006020 Text en © 2018 Muñoz et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Muñoz, Jose
Ballester, Maria Rosa
Antonijoan, Rosa Maria
Gich, Ignasi
Rodríguez, Montse
Colli, Enrico
Gold, Silvia
Krolewiecki, Alejandro J.
Safety and pharmacokinetic profile of fixed-dose ivermectin with an innovative 18mg tablet in healthy adult volunteers
title Safety and pharmacokinetic profile of fixed-dose ivermectin with an innovative 18mg tablet in healthy adult volunteers
title_full Safety and pharmacokinetic profile of fixed-dose ivermectin with an innovative 18mg tablet in healthy adult volunteers
title_fullStr Safety and pharmacokinetic profile of fixed-dose ivermectin with an innovative 18mg tablet in healthy adult volunteers
title_full_unstemmed Safety and pharmacokinetic profile of fixed-dose ivermectin with an innovative 18mg tablet in healthy adult volunteers
title_short Safety and pharmacokinetic profile of fixed-dose ivermectin with an innovative 18mg tablet in healthy adult volunteers
title_sort safety and pharmacokinetic profile of fixed-dose ivermectin with an innovative 18mg tablet in healthy adult volunteers
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5773004/
https://www.ncbi.nlm.nih.gov/pubmed/29346388
http://dx.doi.org/10.1371/journal.pntd.0006020
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