Investigation of the effect of the dual orexin receptor antagonist almorexant on ophthalmological, spermatogenic, and hormonal variables in healthy male subjects

•The dual orexin receptor antagonist almorexant was administered once daily to healthy male subjects for 4 weeks.•A battery of ophthalmological, spermatogenetic, and hormone variables was assessed.•No clinically relevant effects were detected in spite of some findings in toxicology studies in rats a...

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Published inBiomedicine & pharmacotherapy Vol. 133; p. 110955
Main Authors Dingemanse, Jasper, Charef, Pascal, Black, Jed, Gouws, Chris
Format Journal Article
LanguageEnglish
Published France Elsevier Masson SAS 01.01.2021
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ISSN0753-3322
1950-6007
1950-6007
DOI10.1016/j.biopha.2020.110955

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Abstract •The dual orexin receptor antagonist almorexant was administered once daily to healthy male subjects for 4 weeks.•A battery of ophthalmological, spermatogenetic, and hormone variables was assessed.•No clinically relevant effects were detected in spite of some findings in toxicology studies in rats and dogs. The aim of this single-center, double-blind study was to investigate the effect of a 4-week once daily administration of 200 mg almorexant on tear film break-up time, spermatogenesis, hormone levels, and pancreatic elastase in stool in healthy male subjects. Almorexant 200 mg or matching placebo was administered in the evening for 4 weeks once daily to 56 healthy male subjects. Changes in ophthalmological variables, sperm composition, hormone levels, and pancreatic elastase levels in stool were evaluated periodically up to 8 weeks after discontinuation of drug administration. Blood samples for pharmacokinetic measurements were taken after 4 weeks to confirm compliance to study drug intake. The results of this study revealed no treatment effects of almorexant, neither on tear film break-up time nor on other ophthalmological variables investigated during this study. Furthermore, spermatogenesis, hormones of the hypothalamic-pituitary-adrenal and –gonadal axes, and endocrine pancreatic secretion were shown to be not affected by a 4-week once daily administration of almorexant. Almorexant was well tolerated and had no effect on the spectrum of pharmacodynamic variables assessed. Ophthalmology and testicular findings detected in preclinical studies were not observed in this clinical study. Therefore, these preclinical findings appear not to be relevant for humans and do not prevent from conducting larger clinical trials with either healthy subjects or patients.
AbstractList The aim of this single-center, double-blind study was to investigate the effect of a 4-week once daily administration of 200 mg almorexant on tear film break-up time, spermatogenesis, hormone levels, and pancreatic elastase in stool in healthy male subjects. Almorexant 200 mg or matching placebo was administered in the evening for 4 weeks once daily to 56 healthy male subjects. Changes in ophthalmological variables, sperm composition, hormone levels, and pancreatic elastase levels in stool were evaluated periodically up to 8 weeks after discontinuation of drug administration. Blood samples for pharmacokinetic measurements were taken after 4 weeks to confirm compliance to study drug intake. The results of this study revealed no treatment effects of almorexant, neither on tear film break-up time nor on other ophthalmological variables investigated during this study. Furthermore, spermatogenesis, hormones of the hypothalamic-pituitary-adrenal and -gonadal axes, and endocrine pancreatic secretion were shown to be not affected by a 4-week once daily administration of almorexant. Almorexant was well tolerated and had no effect on the spectrum of pharmacodynamic variables assessed. Ophthalmology and testicular findings detected in preclinical studies were not observed in this clinical study. Therefore, these preclinical findings appear not to be relevant for humans and do not prevent from conducting larger clinical trials with either healthy subjects or patients.
The aim of this single-center, double-blind study was to investigate the effect of a 4-week once daily administration of 200 mg almorexant on tear film break-up time, spermatogenesis, hormone levels, and pancreatic elastase in stool in healthy male subjects.BACKGROUND/AIMSThe aim of this single-center, double-blind study was to investigate the effect of a 4-week once daily administration of 200 mg almorexant on tear film break-up time, spermatogenesis, hormone levels, and pancreatic elastase in stool in healthy male subjects.Almorexant 200 mg or matching placebo was administered in the evening for 4 weeks once daily to 56 healthy male subjects. Changes in ophthalmological variables, sperm composition, hormone levels, and pancreatic elastase levels in stool were evaluated periodically up to 8 weeks after discontinuation of drug administration. Blood samples for pharmacokinetic measurements were taken after 4 weeks to confirm compliance to study drug intake.METHODSAlmorexant 200 mg or matching placebo was administered in the evening for 4 weeks once daily to 56 healthy male subjects. Changes in ophthalmological variables, sperm composition, hormone levels, and pancreatic elastase levels in stool were evaluated periodically up to 8 weeks after discontinuation of drug administration. Blood samples for pharmacokinetic measurements were taken after 4 weeks to confirm compliance to study drug intake.The results of this study revealed no treatment effects of almorexant, neither on tear film break-up time nor on other ophthalmological variables investigated during this study. Furthermore, spermatogenesis, hormones of the hypothalamic-pituitary-adrenal and -gonadal axes, and endocrine pancreatic secretion were shown to be not affected by a 4-week once daily administration of almorexant.RESULTSThe results of this study revealed no treatment effects of almorexant, neither on tear film break-up time nor on other ophthalmological variables investigated during this study. Furthermore, spermatogenesis, hormones of the hypothalamic-pituitary-adrenal and -gonadal axes, and endocrine pancreatic secretion were shown to be not affected by a 4-week once daily administration of almorexant.Almorexant was well tolerated and had no effect on the spectrum of pharmacodynamic variables assessed. Ophthalmology and testicular findings detected in preclinical studies were not observed in this clinical study. Therefore, these preclinical findings appear not to be relevant for humans and do not prevent from conducting larger clinical trials with either healthy subjects or patients.CONCLUSIONAlmorexant was well tolerated and had no effect on the spectrum of pharmacodynamic variables assessed. Ophthalmology and testicular findings detected in preclinical studies were not observed in this clinical study. Therefore, these preclinical findings appear not to be relevant for humans and do not prevent from conducting larger clinical trials with either healthy subjects or patients.
•The dual orexin receptor antagonist almorexant was administered once daily to healthy male subjects for 4 weeks.•A battery of ophthalmological, spermatogenetic, and hormone variables was assessed.•No clinically relevant effects were detected in spite of some findings in toxicology studies in rats and dogs. The aim of this single-center, double-blind study was to investigate the effect of a 4-week once daily administration of 200 mg almorexant on tear film break-up time, spermatogenesis, hormone levels, and pancreatic elastase in stool in healthy male subjects. Almorexant 200 mg or matching placebo was administered in the evening for 4 weeks once daily to 56 healthy male subjects. Changes in ophthalmological variables, sperm composition, hormone levels, and pancreatic elastase levels in stool were evaluated periodically up to 8 weeks after discontinuation of drug administration. Blood samples for pharmacokinetic measurements were taken after 4 weeks to confirm compliance to study drug intake. The results of this study revealed no treatment effects of almorexant, neither on tear film break-up time nor on other ophthalmological variables investigated during this study. Furthermore, spermatogenesis, hormones of the hypothalamic-pituitary-adrenal and –gonadal axes, and endocrine pancreatic secretion were shown to be not affected by a 4-week once daily administration of almorexant. Almorexant was well tolerated and had no effect on the spectrum of pharmacodynamic variables assessed. Ophthalmology and testicular findings detected in preclinical studies were not observed in this clinical study. Therefore, these preclinical findings appear not to be relevant for humans and do not prevent from conducting larger clinical trials with either healthy subjects or patients.
ArticleNumber 110955
Author Charef, Pascal
Black, Jed
Dingemanse, Jasper
Gouws, Chris
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Keywords Hormones
Ophthalmology
Spermatogenesis
Meibomian gland
Orexin
Almorexant
Language English
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Snippet •The dual orexin receptor antagonist almorexant was administered once daily to healthy male subjects for 4 weeks.•A battery of ophthalmological,...
The aim of this single-center, double-blind study was to investigate the effect of a 4-week once daily administration of 200 mg almorexant on tear film...
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StartPage 110955
SubjectTerms Acetamides - administration & dosage
Acetamides - adverse effects
Acetamides - blood
Acetamides - pharmacokinetics
Administration, Oral
Adult
Almorexant
Biomarkers - blood
Double-Blind Method
Drug Administration Schedule
Healthy Volunteers
Hormones
Hormones - blood
Humans
Isoquinolines - administration & dosage
Isoquinolines - adverse effects
Isoquinolines - blood
Isoquinolines - pharmacokinetics
Lacrimal Apparatus - drug effects
Lacrimal Apparatus - physiology
Male
Meibomian gland
Ophthalmology
Orexin
Orexin Receptor Antagonists - administration & dosage
Orexin Receptor Antagonists - adverse effects
Orexin Receptor Antagonists - blood
Orexin Receptor Antagonists - pharmacokinetics
Patient Safety
Prospective Studies
Risk Assessment
Sleep Aids, Pharmaceutical - administration & dosage
Sleep Aids, Pharmaceutical - adverse effects
Sleep Aids, Pharmaceutical - blood
Sleep Aids, Pharmaceutical - pharmacokinetics
South Africa
Spermatogenesis
Spermatogenesis - drug effects
Tears
Time Factors
Young Adult
Title Investigation of the effect of the dual orexin receptor antagonist almorexant on ophthalmological, spermatogenic, and hormonal variables in healthy male subjects
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https://dx.doi.org/10.1016/j.biopha.2020.110955
https://www.ncbi.nlm.nih.gov/pubmed/33190032
https://www.proquest.com/docview/2461001774
Volume 133
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