Pharmacokinetics comparison of two pegylated interferon alfa formulations in healthy volunteers

Detalhes bibliográficos
Autor(a) principal: Costa, Marisa Boff da
Data de Publicação: 2018
Outros Autores: Picon, Paulo Dornelles, Sander, Guilherme Becker, Nodarse Cuni, Hugo, Valenzuela Silva, Carmen M, Páez Meireles, Rolando, Góes, Ana Carolina Magalhães Andrade, Batoreu, Nadia Maria, Maia, Maria de Lourdes de Sousa, Albuquerque, Elizabeth Maciel, Matos, Denise Cristina de Souza, López Saura, Pedro Antonio
Tipo de documento: Artigo
Idioma: eng
Título da fonte: Repositório Institucional da UFRGS
Texto Completo: http://hdl.handle.net/10183/196689
Resumo: Background: Several countries have used pegylation technology to improve the pharmacokinetic properties of essential drugs. Recently, a novel interferon alfa-2b protein conjugated to four-branched 12 kDa polyethylene glycol molecules was developed jointly between Cuba and Brazil. The aim of this study was to compare the pharmacokinetic properties of BIP48 (pegylated interferon alfa-2b from Bio-Manguinhos/Fiocruz, Brazil) to those of PEGASYS® (commercially available pegylated interferon alfa-2a from Roche Pharmaceutical). Methods: This phase I, single-centre, randomized, double-blind crossover trial enrolled 31 healthy male volunteers aged 19 to 35 who were allocated to two stages, either side of a 5-week wash-out period, with each arm lasting 14 consecutive days after subcutaneous administration of 180 μg of one formulation or the other (study or comparator). The main outcome variable was serum pegylated interferon concentrations in 15 samples collected during the course of the study and tested using an enzyme immunoassay. Results: There were no differences between formulations in terms of magnitude or absorption parameters. Analysis of time parameters revealed that BIP48 remained in the body significantly longer than PEGASYS® (Tmax: 73 vs. 54 h [p = 0.0010]; MRT: 133 vs. 115 h [p = 0.0324]; ke: 0.011 vs. 0.013 h(−1) [p = 0.0153]; t1/2: 192 vs. 108 h [p = 0.0218]). Conclusion: BIP48 showed the expected pharmacokinetic profile for a pegylated product with a branched molecular structure. Compared to PEGASYS®, the magnitude absorption was similar, but time parameters were consistent with slower elimination. Further studies should be conducted to evaluate the clinical implications of these findings. A phase II-III repeated-dose clinical trial is ongoing to study these findings in patients with chronic hepatitis C virus infection.
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spelling Costa, Marisa Boff daPicon, Paulo DornellesSander, Guilherme BeckerNodarse Cuni, HugoValenzuela Silva, Carmen MPáez Meireles, RolandoGóes, Ana Carolina Magalhães AndradeBatoreu, Nadia MariaMaia, Maria de Lourdes de SousaAlbuquerque, Elizabeth MacielMatos, Denise Cristina de SouzaLópez Saura, Pedro Antonio2019-07-09T02:38:41Z20182050-6511http://hdl.handle.net/10183/196689001096129Background: Several countries have used pegylation technology to improve the pharmacokinetic properties of essential drugs. Recently, a novel interferon alfa-2b protein conjugated to four-branched 12 kDa polyethylene glycol molecules was developed jointly between Cuba and Brazil. The aim of this study was to compare the pharmacokinetic properties of BIP48 (pegylated interferon alfa-2b from Bio-Manguinhos/Fiocruz, Brazil) to those of PEGASYS® (commercially available pegylated interferon alfa-2a from Roche Pharmaceutical). Methods: This phase I, single-centre, randomized, double-blind crossover trial enrolled 31 healthy male volunteers aged 19 to 35 who were allocated to two stages, either side of a 5-week wash-out period, with each arm lasting 14 consecutive days after subcutaneous administration of 180 μg of one formulation or the other (study or comparator). The main outcome variable was serum pegylated interferon concentrations in 15 samples collected during the course of the study and tested using an enzyme immunoassay. Results: There were no differences between formulations in terms of magnitude or absorption parameters. Analysis of time parameters revealed that BIP48 remained in the body significantly longer than PEGASYS® (Tmax: 73 vs. 54 h [p = 0.0010]; MRT: 133 vs. 115 h [p = 0.0324]; ke: 0.011 vs. 0.013 h(−1) [p = 0.0153]; t1/2: 192 vs. 108 h [p = 0.0218]). Conclusion: BIP48 showed the expected pharmacokinetic profile for a pegylated product with a branched molecular structure. Compared to PEGASYS®, the magnitude absorption was similar, but time parameters were consistent with slower elimination. Further studies should be conducted to evaluate the clinical implications of these findings. A phase II-III repeated-dose clinical trial is ongoing to study these findings in patients with chronic hepatitis C virus infection.application/pdfengBMC pharmacology and toxicology. London. Vol. 19, no. 1 (2018), 8 p.FarmacocinéticaInterferon alfaAntiviraisPharmacokineticsPegylated interferon-alfaPhase IPharmacokinetics comparison of two pegylated interferon alfa formulations in healthy volunteersEstrangeiroinfo:eu-repo/semantics/articleinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/openAccessreponame:Repositório Institucional da UFRGSinstname:Universidade Federal do Rio Grande do Sul (UFRGS)instacron:UFRGSTEXT001096129.pdf.txt001096129.pdf.txtExtracted Texttext/plain38667http://www.lume.ufrgs.br/bitstream/10183/196689/2/001096129.pdf.txt38b45bef1b81abda1781e84b4e874223MD52ORIGINAL001096129.pdfTexto completo (inglês)application/pdf602092http://www.lume.ufrgs.br/bitstream/10183/196689/1/001096129.pdffffa5d9a393984922af123c83a788c9aMD5110183/1966892019-07-10 02:34:46.368303oai:www.lume.ufrgs.br:10183/196689Repositório de PublicaçõesPUBhttps://lume.ufrgs.br/oai/requestopendoar:2019-07-10T05:34:46Repositório Institucional da UFRGS - Universidade Federal do Rio Grande do Sul (UFRGS)false
dc.title.pt_BR.fl_str_mv Pharmacokinetics comparison of two pegylated interferon alfa formulations in healthy volunteers
title Pharmacokinetics comparison of two pegylated interferon alfa formulations in healthy volunteers
spellingShingle Pharmacokinetics comparison of two pegylated interferon alfa formulations in healthy volunteers
Costa, Marisa Boff da
Farmacocinética
Interferon alfa
Antivirais
Pharmacokinetics
Pegylated interferon-alfa
Phase I
title_short Pharmacokinetics comparison of two pegylated interferon alfa formulations in healthy volunteers
title_full Pharmacokinetics comparison of two pegylated interferon alfa formulations in healthy volunteers
title_fullStr Pharmacokinetics comparison of two pegylated interferon alfa formulations in healthy volunteers
title_full_unstemmed Pharmacokinetics comparison of two pegylated interferon alfa formulations in healthy volunteers
title_sort Pharmacokinetics comparison of two pegylated interferon alfa formulations in healthy volunteers
author Costa, Marisa Boff da
author_facet Costa, Marisa Boff da
Picon, Paulo Dornelles
Sander, Guilherme Becker
Nodarse Cuni, Hugo
Valenzuela Silva, Carmen M
Páez Meireles, Rolando
Góes, Ana Carolina Magalhães Andrade
Batoreu, Nadia Maria
Maia, Maria de Lourdes de Sousa
Albuquerque, Elizabeth Maciel
Matos, Denise Cristina de Souza
López Saura, Pedro Antonio
author_role author
author2 Picon, Paulo Dornelles
Sander, Guilherme Becker
Nodarse Cuni, Hugo
Valenzuela Silva, Carmen M
Páez Meireles, Rolando
Góes, Ana Carolina Magalhães Andrade
Batoreu, Nadia Maria
Maia, Maria de Lourdes de Sousa
Albuquerque, Elizabeth Maciel
Matos, Denise Cristina de Souza
López Saura, Pedro Antonio
author2_role author
author
author
author
author
author
author
author
author
author
author
dc.contributor.author.fl_str_mv Costa, Marisa Boff da
Picon, Paulo Dornelles
Sander, Guilherme Becker
Nodarse Cuni, Hugo
Valenzuela Silva, Carmen M
Páez Meireles, Rolando
Góes, Ana Carolina Magalhães Andrade
Batoreu, Nadia Maria
Maia, Maria de Lourdes de Sousa
Albuquerque, Elizabeth Maciel
Matos, Denise Cristina de Souza
López Saura, Pedro Antonio
dc.subject.por.fl_str_mv Farmacocinética
Interferon alfa
Antivirais
topic Farmacocinética
Interferon alfa
Antivirais
Pharmacokinetics
Pegylated interferon-alfa
Phase I
dc.subject.eng.fl_str_mv Pharmacokinetics
Pegylated interferon-alfa
Phase I
description Background: Several countries have used pegylation technology to improve the pharmacokinetic properties of essential drugs. Recently, a novel interferon alfa-2b protein conjugated to four-branched 12 kDa polyethylene glycol molecules was developed jointly between Cuba and Brazil. The aim of this study was to compare the pharmacokinetic properties of BIP48 (pegylated interferon alfa-2b from Bio-Manguinhos/Fiocruz, Brazil) to those of PEGASYS® (commercially available pegylated interferon alfa-2a from Roche Pharmaceutical). Methods: This phase I, single-centre, randomized, double-blind crossover trial enrolled 31 healthy male volunteers aged 19 to 35 who were allocated to two stages, either side of a 5-week wash-out period, with each arm lasting 14 consecutive days after subcutaneous administration of 180 μg of one formulation or the other (study or comparator). The main outcome variable was serum pegylated interferon concentrations in 15 samples collected during the course of the study and tested using an enzyme immunoassay. Results: There were no differences between formulations in terms of magnitude or absorption parameters. Analysis of time parameters revealed that BIP48 remained in the body significantly longer than PEGASYS® (Tmax: 73 vs. 54 h [p = 0.0010]; MRT: 133 vs. 115 h [p = 0.0324]; ke: 0.011 vs. 0.013 h(−1) [p = 0.0153]; t1/2: 192 vs. 108 h [p = 0.0218]). Conclusion: BIP48 showed the expected pharmacokinetic profile for a pegylated product with a branched molecular structure. Compared to PEGASYS®, the magnitude absorption was similar, but time parameters were consistent with slower elimination. Further studies should be conducted to evaluate the clinical implications of these findings. A phase II-III repeated-dose clinical trial is ongoing to study these findings in patients with chronic hepatitis C virus infection.
publishDate 2018
dc.date.issued.fl_str_mv 2018
dc.date.accessioned.fl_str_mv 2019-07-09T02:38:41Z
dc.type.driver.fl_str_mv Estrangeiro
info:eu-repo/semantics/article
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
format article
status_str publishedVersion
dc.identifier.uri.fl_str_mv http://hdl.handle.net/10183/196689
dc.identifier.issn.pt_BR.fl_str_mv 2050-6511
dc.identifier.nrb.pt_BR.fl_str_mv 001096129
identifier_str_mv 2050-6511
001096129
url http://hdl.handle.net/10183/196689
dc.language.iso.fl_str_mv eng
language eng
dc.relation.ispartof.pt_BR.fl_str_mv BMC pharmacology and toxicology. London. Vol. 19, no. 1 (2018), 8 p.
dc.rights.driver.fl_str_mv info:eu-repo/semantics/openAccess
eu_rights_str_mv openAccess
dc.format.none.fl_str_mv application/pdf
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instname_str Universidade Federal do Rio Grande do Sul (UFRGS)
instacron_str UFRGS
institution UFRGS
reponame_str Repositório Institucional da UFRGS
collection Repositório Institucional da UFRGS
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