ND0701, A Novel Formulation of Apomorphine for Subcutaneous Infusion, in Comparison to a Commercial Apomorphine Formulation: 28-Day Pharmacokinetic Study in Minipigs and a Phase I Study in Healthy Volunteers to Assess the Safety, Tolerability, Pharmacokinetics and Relative Bioavailability

ND0701, A Novel Formulation of Apomorphine for Subcutaneous Infusion, in Comparison to a Commercial Apomorphine Formulation: 28-Day Pharmacokinetic Study in Minipigs and a Phase I Study in Healthy Volunteers to Assess the Safety, Tolerability, Pharmacokinetics and Relative Bioavailability

Background Subcutaneous apomorphine is used for the treatment of Parkinson’s disease (PD); however, infusion site reactions are a common adverse event (AE), which can lead to treatment discontinuation. Apomorphine formulations that are more tolerable and convenient for use are needed. Objective Our...

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Veröffentlicht in:CNS drugs 2018-05, Vol.32 (5), p.443-454
Hauptverfasser: Ramot, Yuval, Nyska, Abraham, Adar, Liat, Durlach, Cecile, Fishelovitch, Danny, Sacco, Giuseppe, Manno, Rosa Anna, Oren, Sheila, Perlstein, Itay, Yacobi-Zeevi, Oron
Format: Artikel
Sprache:eng
Schlagworte:
Adult
Alzheimer's disease
Animals
Apomorphine
Apomorphine - adverse effects
Apomorphine - pharmacokinetics
Apomorphine - pharmacology
Bioavailability
Biological Availability
Cross-Over Studies
Dopamine Agonists - adverse effects
Dopamine Agonists - pharmacokinetics
Dopamine Agonists - pharmacology
Drug dosages
Female
Humans
Infusions, Subcutaneous
Laboratory animals
Male
Medicine
Medicine & Public Health
Middle Aged
Movement disorders
Neurodegenerative diseases
Neurology
Neurosciences
Neurotoxicity
Nodules
Original Research Article
Parkinson's disease
Pharmacokinetics
Pharmacotherapy
Pilot Projects
Psychiatry
Psychopharmacology
Random Allocation
Safety
Skin
Skin - drug effects
Skin - pathology
Studies
Swine
Swine, Miniature
Toxicology
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Zusammenfassung:Background Subcutaneous apomorphine is used for the treatment of Parkinson’s disease (PD); however, infusion site reactions are a common adverse event (AE), which can lead to treatment discontinuation. Apomorphine formulations that are more tolerable and convenient for use are needed. Objective Our aim was to compare the toxicity and bioavailability of ND0701, a new concentrated formulation of apomorphine free base, with one of the commercially available apomorphine HCl formulations (APO-go ® , Britannia Pharmaceuticals Ltd). Methods (1) Preclinical study: 16 minipigs were randomly assigned to placebo, APO-go ® , and ND0701 groups, and treated for 28 days. Pharmacokinetic, clinical, and pathological assessments were performed. (2) Phase I study: 18 healthy volunteers participated in an open-label, two-sequence, randomized, three single-dose, partial crossover study to compare the pharmacokinetics, safety, and tolerability of ND0701 with APO-go ® (1%). Results (1) Preclinical study: No systemic toxicity was observed in apomorphine-treated minipigs, but local skin reactions were observed at the infusion sites. These effects were less frequent and less severe and recovery was more rapid for ND0701 compared with APO-go ® . (2) Phase I study: Both formulations were safe and well tolerated under the conditions of the study and no severe or serious treatment-emergent AEs were reported. Infusion site nodules were reported more frequently, with higher severity, and recovered slower at APO-go ® -treated sites compared with ND0701-treated sites. Bioavailability of apomorphine was comparable between the two formulations. Conclusion Based on these pilot studies, ND0701 appears to be superior to APO-go ® in terms of tolerability and safety, while maintaining comparable bioavailability with APO-go ® , and shows promise as a future treatment for PD.
ISSN:1172-7047
1179-1934
DOI:10.1007/s40263-018-0512-x