A phase 1 trial of AP30663, a KCa2 channel inhibitor in development for conversion of atrial fibrillation

Christina Yfanti; Birgitte Vestbjerg; Juliette van't Westende; Nils Edvardsson; Laia Meseguer Monfort; Morten Salling Olesen; Bo Hjorth Bentzen; Morten Grunnet; Boukje C. Eveleens Maarse; Jonas Goldin Diness; Michiel J. B. Kemme; Ulrik Sørensen; Matthijs Moerland; Michiel J. van Esdonk; Erica S. Klaassen; Pim Gal; Anders G. Holst

doi:10.1111/bcp.15973

A phase 1 trial of AP30663, a KCa2 channel inhibitor in development for conversion of atrial fibrillation

Christina Yfanti
, Birgitte Vestbjerg
, Juliette van't Westende
, Nils Edvardsson
, Laia Meseguer Monfort
, Morten Salling Olesen
, Bo Hjorth Bentzen
, Morten Grunnet
, Boukje C. Eveleens Maarse
, Jonas Goldin Diness
, Michiel J. B. Kemme
, Ulrik Sørensen
, Matthijs Moerland^*
, Michiel J. van Esdonk
, Erica S. Klaassen
, Pim Gal
, Anders G. Holst

^*Corresponding author for this work

Centre for Human Drug Research
Acesion Pharma
Sahlgrenska Academy
University of Copenhagen
Leiden University

Research output: Contribution to journal › Article › Academic › peer-review

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Abstract

Aims: AP30663 is a novel compound under development for pharmacological conversion of atrial fibrillation by targeting the small conductance Ca2+ activated K+ (KCa2) channel. The aim of this extension phase 1 study was to test AP30663 at higher single doses compared to the first-in-human trial. Methods: Sixteen healthy male volunteers were randomized into 2 cohorts: 6- and 8-mg/kg intravenous single-dose administration of AP30663 vs. placebo. Safety, pharmacokinetic and pharmacodynamic data were collected. Results: AP30663 was associated with mild and transient infusion site reactions with no clustering of other adverse events but with an estimated maximum mean QTcF interval prolongation of 45.2 ms (95% confidence interval 31.5–58.9) in the 6 mg/kg dose level and 50.4 ms (95% confidence interval 36.7–64.0) with 8 mg/kg. Pharmacokinetics was dose proportional with terminal half-life of around 3 h. Conclusion: AP30663 in doses up to 8 mg/kg was associated with mild and transient infusion site reactions and an increase of the QTcF interval. Supporting Information support that the QTc effect may be explained by an off-target inhibition of the IKr channel.

Original language	English
Journal	British journal of clinical pharmacology
DOIs	https://doi.org/10.1111/bcp.15973
Publication status	E-pub ahead of print - 2023

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SDG 3 Good Health and Well-being

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Yfanti, C., Vestbjerg, B., van't Westende, J., Edvardsson, N., Monfort, L. M., Olesen, M. S., Bentzen, B. H., Grunnet, M., Eveleens Maarse, B. C., Diness, J. G., Kemme, M. J. B., Sørensen, U., Moerland, M., van Esdonk, M. J., Klaassen, E. S., Gal, P., & Holst, A. G. (2023). A phase 1 trial of AP30663, a KCa2 channel inhibitor in development for conversion of atrial fibrillation. British journal of clinical pharmacology. Advance online publication. https://doi.org/10.1111/bcp.15973

@article{9cf55b2c522d41909b900bb7c8a33b4b,

title = "A phase 1 trial of AP30663, a KCa2 channel inhibitor in development for conversion of atrial fibrillation",

abstract = "Aims: AP30663 is a novel compound under development for pharmacological conversion of atrial fibrillation by targeting the small conductance Ca2+ activated K+ (KCa2) channel. The aim of this extension phase 1 study was to test AP30663 at higher single doses compared to the first-in-human trial. Methods: Sixteen healthy male volunteers were randomized into 2 cohorts: 6- and 8-mg/kg intravenous single-dose administration of AP30663 vs. placebo. Safety, pharmacokinetic and pharmacodynamic data were collected. Results: AP30663 was associated with mild and transient infusion site reactions with no clustering of other adverse events but with an estimated maximum mean QTcF interval prolongation of 45.2 ms (95\% confidence interval 31.5–58.9) in the 6 mg/kg dose level and 50.4 ms (95\% confidence interval 36.7–64.0) with 8 mg/kg. Pharmacokinetics was dose proportional with terminal half-life of around 3 h. Conclusion: AP30663 in doses up to 8 mg/kg was associated with mild and transient infusion site reactions and an increase of the QTcF interval. Supporting Information support that the QTc effect may be explained by an off-target inhibition of the IKr channel.",

author = "Christina Yfanti and Birgitte Vestbjerg and \{van't Westende\}, Juliette and Nils Edvardsson and Monfort, \{Laia Meseguer\} and Olesen, \{Morten Salling\} and Bentzen, \{Bo Hjorth\} and Morten Grunnet and \{Eveleens Maarse\}, \{Boukje C.\} and Diness, \{Jonas Goldin\} and Kemme, \{Michiel J. B.\} and Ulrik S{\o}rensen and Matthijs Moerland and \{van Esdonk\}, \{Michiel J.\} and Klaassen, \{Erica S.\} and Pim Gal and Holst, \{Anders G.\}",

year = "2023",

doi = "10.1111/bcp.15973",

language = "English",

journal = "British journal of clinical pharmacology",

issn = "0306-5251",

publisher = "Wiley Blackwell",

}

Yfanti, C, Vestbjerg, B, van't Westende, J, Edvardsson, N, Monfort, LM, Olesen, MS, Bentzen, BH, Grunnet, M, Eveleens Maarse, BC, Diness, JG, Kemme, MJB, Sørensen, U, Moerland, M, van Esdonk, MJ, Klaassen, ES, Gal, P & Holst, AG 2023, 'A phase 1 trial of AP30663, a KCa2 channel inhibitor in development for conversion of atrial fibrillation', British journal of clinical pharmacology. https://doi.org/10.1111/bcp.15973

TY - JOUR

T1 - A phase 1 trial of AP30663, a KCa2 channel inhibitor in development for conversion of atrial fibrillation

AU - Yfanti, Christina

AU - Vestbjerg, Birgitte

AU - van't Westende, Juliette

AU - Edvardsson, Nils

AU - Monfort, Laia Meseguer

AU - Olesen, Morten Salling

AU - Bentzen, Bo Hjorth

AU - Grunnet, Morten

AU - Eveleens Maarse, Boukje C.

AU - Diness, Jonas Goldin

AU - Kemme, Michiel J. B.

AU - Sørensen, Ulrik

AU - Moerland, Matthijs

AU - van Esdonk, Michiel J.

AU - Klaassen, Erica S.

AU - Gal, Pim

AU - Holst, Anders G.

PY - 2023

Y1 - 2023

N2 - Aims: AP30663 is a novel compound under development for pharmacological conversion of atrial fibrillation by targeting the small conductance Ca2+ activated K+ (KCa2) channel. The aim of this extension phase 1 study was to test AP30663 at higher single doses compared to the first-in-human trial. Methods: Sixteen healthy male volunteers were randomized into 2 cohorts: 6- and 8-mg/kg intravenous single-dose administration of AP30663 vs. placebo. Safety, pharmacokinetic and pharmacodynamic data were collected. Results: AP30663 was associated with mild and transient infusion site reactions with no clustering of other adverse events but with an estimated maximum mean QTcF interval prolongation of 45.2 ms (95% confidence interval 31.5–58.9) in the 6 mg/kg dose level and 50.4 ms (95% confidence interval 36.7–64.0) with 8 mg/kg. Pharmacokinetics was dose proportional with terminal half-life of around 3 h. Conclusion: AP30663 in doses up to 8 mg/kg was associated with mild and transient infusion site reactions and an increase of the QTcF interval. Supporting Information support that the QTc effect may be explained by an off-target inhibition of the IKr channel.

AB - Aims: AP30663 is a novel compound under development for pharmacological conversion of atrial fibrillation by targeting the small conductance Ca2+ activated K+ (KCa2) channel. The aim of this extension phase 1 study was to test AP30663 at higher single doses compared to the first-in-human trial. Methods: Sixteen healthy male volunteers were randomized into 2 cohorts: 6- and 8-mg/kg intravenous single-dose administration of AP30663 vs. placebo. Safety, pharmacokinetic and pharmacodynamic data were collected. Results: AP30663 was associated with mild and transient infusion site reactions with no clustering of other adverse events but with an estimated maximum mean QTcF interval prolongation of 45.2 ms (95% confidence interval 31.5–58.9) in the 6 mg/kg dose level and 50.4 ms (95% confidence interval 36.7–64.0) with 8 mg/kg. Pharmacokinetics was dose proportional with terminal half-life of around 3 h. Conclusion: AP30663 in doses up to 8 mg/kg was associated with mild and transient infusion site reactions and an increase of the QTcF interval. Supporting Information support that the QTc effect may be explained by an off-target inhibition of the IKr channel.

UR - https://www.scopus.com/pages/publications/85181680564

UR - https://www.ncbi.nlm.nih.gov/pubmed/37990600

U2 - 10.1111/bcp.15973

DO - 10.1111/bcp.15973

M3 - Article

C2 - 37990600

SN - 0306-5251

JO - British journal of clinical pharmacology

JF - British journal of clinical pharmacology

ER -

A phase 1 trial of AP30663, a KCa2 channel inhibitor in development for conversion of atrial fibrillation

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