A study to assess the safety, tolerability, pharmacokinetics and pharmacodynamics of multiple ascending doses of AZD9567.
This is a phase 1, randomised, single-blind, multiple ascending dose, double-dummy sequential group study in healthy subjects . The study is planned to have 6 cohorts with the option to include up to two additional cohorts if deemed necessary. Nine subjects participated in the first cohort (7 subjects randomised to receive AZD9567 and 2 subjects randomised to receive prednisolone 20 mg)and eleven subjects will participate in subsequent 3 cohorts (7 subjects will be randomised to receive AZD9567 and 4 subjects randomised to receive prednisolone 20 mg). A cohort 5 was included in the study in version 4.0 of the CSP. In this cohort two doses of prednisolone was tested, 5 mg and 20 mg. Up to six dose levels of AZD9567 are planned to be tested in the study and an additional cohort will be used in case any previous dose needs to be repeated or a new lower dose explored (ref CSP 5.0). Therefore a maximum of 95 individuals could be included in the study (as stated in version 5.0 of this protocol). Subjects will be dosed for 5 consecutive days and a follow-up visit will occur 10-14 days after the last dose.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
SINGLE
Enrollment
64
Oral suspension Multiple doses 5 days of treatment Once daily
Oral suspension Multiple doses 5 days of treatment Once daily
Oral suspension Multiple doses 5 days of treatment Once daily
Research Site
Berlin, Germany
Research Site
Harrow, United Kingdom
Safety and tolerability: Adverse events (AEs)
Adverse events will be summarized by each dose of AZD9567, pooled prednisolone 20 mg and pooled AZD9567 doses. Tabulations will include causality and severity (mild, moderate and severe), where applicable, and be presented by System Organ Class (SOC) and Preferred Term (PT) where applicable.
Time frame: Up to 5 days
Safety and tolerability: Vital signs (blood pressure [BP], pulse rate, weight and oral body temperature)
Descriptive statistics will be presented by treatment and time point for both observed values and changes from baseline, based on the safety analysis sets. The incidence of clinically notable vital sign abnormalities (vital signs outside the predefined criteria) will be summarized.
Time frame: Up to 5 days
Safety and tolerability: Clinical laboratory safety evaluations (hematology, serum biochemistry [including S-cortisol and basal S-DHEAS], coagulation and urinalysis)
Summary tabulations will be presented by treatment including observed values and changes from baseline. Shift tables will be presented to show the shifts from baseline to the minimum and maximum post-baseline measurements, respectively, by treatment, based on the safety analysis set.
Time frame: Up to 5 days
Safety and tolerability: Electrocardiograms (12-lead dECGs, safety ECG's, and telemetry)
Results of the safety ECGs, including normal/abnormal and specific findings will be listed for each subject.
Time frame: Up to 5 days
Safety and tolerability: Physical examinations
The results of the physical examination will be listed by body system for each subject.
Time frame: Up to 5 days
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Oral suspension Multiple doses 5 days of treatment Once daily
Oral Multiple doses 5 days of treatment Once daily
Oral Multiple doses 5 days of treatment Once daily
Oral Multiple doses 5 days of treatment Once daily
Oral Multiple doses 5 days of treatment Once daily
Oral Multiple doses 5 days of treatment Once daily
Pharmacokinetic parameter: Observed maximum concentration (Cmax)
Plasma concentrations, and plasma PK parameters will be summarized by dose level of AZD9567 using descriptive statistics (n, geometric mean, geometric coefficient of variation \[CV%\], arithmetic mean, arithmetic Standard Deviation (SD), minimum, median and maximum) based on the respective PK analysis sets.
Time frame: Up to 5 days
Pharmacokinetic parameter: Area Under the curve from 0 to last quantifiable (AUC (0-last))
Plasma concentrations, and plasma PK parameters will be summarized by dose level of AZD9567 using descriptive statistics (n, geometric mean, geometric coefficient of variation \[CV%\], arithmetic mean, arithmetic Standard Deviation (SD), minimum, median and maximum) based on the respective PK analysis sets.
Time frame: Up to 5 days
Pharmacokinetic parameter: Area Under the curve from 0 to 24h (AUC (0-24))
Plasma concentrations, and plasma PK parameters will be summarized by dose level of AZD9567 using descriptive statistics (n, geometric mean, geometric coefficient of variation \[CV%\], arithmetic mean, arithmetic Standard Deviation (SD), minimum, median and maximum) based on the respective PK analysis sets.
Time frame: Up to 5 days
Pharmacokinetic parameter: Area Under the curve from 0 to infinity (AUC(0-inf))
Plasma concentrations, and plasma PK parameters will be summarized by dose level of AZD9567 using descriptive statistics (n, geometric mean, geometric coefficient of variation \[CV%\], arithmetic mean, arithmetic Standard Deviation (SD), minimum, median and maximum) based on the respective PK analysis sets.
Time frame: Up to 5 days
Pharmacokinetic parameter: Area Under the curve from 0 to last quantifiable divided by the dose (AUC(0-last)/D)
Plasma concentrations, and plasma PK parameters will be summarized by dose level of AZD9567 using descriptive statistics (n, geometric mean, geometric coefficient of variation \[CV%\], arithmetic mean, arithmetic Standard Deviation (SD), minimum, median and maximum) based on the respective PK analysis sets.
Time frame: Up to 5 days
Pharmacokinetic parameter: Area Under the curve from 0 to 24h divided by the dose (AUC(0-24)/D)
Plasma concentrations, and plasma PK parameters will be summarized by dose level of AZD9567 using descriptive statistics (n, geometric mean, geometric coefficient of variation \[CV%\], arithmetic mean, arithmetic Standard Deviation (SD), minimum, median and maximum) based on the respective PK analysis sets.
Time frame: Up to 5 days
Pharmacokinetic parameter: Area Under the curve from 0 to infinity divided by the dose (AUC/D)
Plasma concentrations, and plasma PK parameters will be summarized by dose level of AZD9567 using descriptive statistics (n, geometric mean, geometric coefficient of variation \[CV%\], arithmetic mean, arithmetic Standard Deviation (SD), minimum, median and maximum) based on the respective PK analysis sets.
Time frame: Up to 5 days
Pharmacokinetic parameter: Observed maximum concentration divided by the dose (Cmax/D)
Plasma concentrations, and plasma PK parameters will be summarized by dose level of AZD9567 using descriptive statistics (n, geometric mean, geometric coefficient of variation \[CV%\], arithmetic mean, arithmetic Standard Deviation (SD), minimum, median and maximum) based on the respective PK analysis sets.
Time frame: Up to 5 days
Pharmacokinetic parameter: Time to reach maximum concentration (tmax)
Plasma concentrations, and plasma PK parameters will be summarized by dose level of AZD9567 using descriptive statistics (n, geometric mean, geometric coefficient of variation \[CV%\], arithmetic mean, arithmetic Standard Deviation (SD), minimum, median and maximum) based on the respective PK analysis sets.
Time frame: Up to 5 days
Pharmacokinetic parameter: Terminal rate constant (λz)
Plasma concentrations, and plasma PK parameters will be summarized by dose level of AZD9567 using descriptive statistics (n, geometric mean, geometric coefficient of variation \[CV%\], arithmetic mean, arithmetic Standard Deviation (SD), minimum, median and maximum) based on the respective PK analysis sets.
Time frame: Up to 5 days
Pharmacokinetic parameter: Terminal half-life (t1/2)
Plasma concentrations, and plasma PK parameters will be summarized by dose level of AZD9567 using descriptive statistics (n, geometric mean, geometric coefficient of variation \[CV%\], arithmetic mean, arithmetic Standard Deviation (SD), minimum, median and maximum) based on the respective PK analysis sets.
Time frame: Up to 5 days
Pharmacokinetic parameter: Apparent clearance divided by AUC (CL/F)
Plasma concentrations, and plasma PK parameters will be summarized by dose level of AZD9567 using descriptive statistics (n, geometric mean, geometric coefficient of variation \[CV%\], arithmetic mean, arithmetic Standard Deviation (SD), minimum, median and maximum) based on the respective PK analysis sets.
Time frame: Up to 5 days
Pharmacokinetic parameter: Aparent volume of distribution estimated by dividing de apparent clearance (Vz/F)
Plasma concentrations, and plasma PK parameters will be summarized by dose level of AZD9567 using descriptive statistics (n, geometric mean, geometric coefficient of variation \[CV%\], arithmetic mean, arithmetic Standard Deviation (SD), minimum, median and maximum) based on the respective PK analysis sets.
Time frame: Up to 5 days
Pharmacokinetic parameter: Average plasma concentration (Cav)
Plasma concentrations, and plasma PK parameters will be summarized by dose level of AZD9567 using descriptive statistics (n, geometric mean, geometric coefficient of variation \[CV%\], arithmetic mean, arithmetic Standard Deviation (SD), minimum, median and maximum) based on the respective PK analysis sets.
Time frame: Up to 5 days
Pharmacokinetic parameter: fluctuation index
Plasma concentrations, and plasma PK parameters will be summarized by dose level of AZD9567 using descriptive statistics (n, geometric mean, geometric coefficient of variation \[CV%\], arithmetic mean, arithmetic Standard Deviation (SD), minimum, median and maximum) based on the respective PK analysis sets.
Time frame: Up to 5 days
Pharmacodynamic parameter: Plasma glucose measured by Oral Glucose Tolerance Test (OGTT)
Concentration data for the OGTT (plasma glucose) will be listed and summarized by treatment, visit and time point. Each of the plasma glucose AUC (total net and incremental) parameters (0 to 2 hours and 0 to 4 hours) will be listed and summarized (including changes from baseline for the AUC values, where the baseline is the AUC values measured on Day -1) by visit and treatment for the final clinical study report. In addition, the glucose ratio values by time point and their corresponding AUCs will also be summarized.
Time frame: Up to 5 days
Pharmacodynamic parameter: Serum insulin measured by Oral Glucose Tolerance Test (OGTT)
Concentration data for the OGTT (serum insulin) will be listed and summarized by treatment, visit and time point. Each of the serum insulin AUC (total net and incremental) parameters (0 to 2 hours and 0 to 4 hours) will be listed and summarized (including changes from baseline for the AUC values, where the baseline is the AUC values measured on Day -1) by visit and treatment for the final clinical study report. In addition, the serum insulin ratio values by time point and their corresponding AUCs will also be summarized.
Time frame: Up to 5 days
Pharmacodynamic parameter: Serum C-peptide measured by Oral Glucose Tolerance Test (OGTT)
Concentration data for the OGTT (serum C-peptide) will be listed and summarized by treatment, visit and time point. Each of the serum C-peptide AUC (total net and incremental) parameters (0 to 2 hours and 0 to 4 hours) will be listed and summarized (including changes from baseline for the AUC values, where the baseline is the AUC values measured on Day -1) by visit and treatment for the final clinical study report.
Time frame: Up to 5 days