Novo Nordisk is developing a new study medicine, Etavopivat, to treat individuals with sickle cell disease (SCD). The purpose of the study is to determine the effect of Etavopivat on the electrical activity of the heart in healthy participants. The study comprises two parts: Part A and Part B. Part A investigates the safety of a high dose of Etavopivat. In this phase, participants will receive either a single dose of Etavopivat or a placebo. Which treatment the participant gets is decided by chance. In Part B, participants will get four different treatments on four different occasions: Etavopivat in 2 different doses (the new medicine that cannot be prescribed), a dummy medicine (placebo), and an already approved medicine (moxifloxacin). The order of the 4 study medicines is decided by chance. There will be a break of 7 days between each treatment. For Part A, the study duration will be from 10 to 36 days, and for Part B, the study duration will be from 27 to 53 days.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
QUADRUPLE
Enrollment
33
Etavopivat will be administered orally.
Moxifloxacin will be administered orally.
Placebo matching Etavopivat will be administered orally.
PAREXEL Intl - EPCU-Baltimore
Baltimore, Maryland, United States
Part A: Number of treatment-emergent adverse events (AEs)
Measured as count of events.
Time frame: From dosing (Day 1) until end of study (Day 8)
Part B: Change from baseline in Fridericia heart rate corrected QT interval (ΔQTcF) for etavopivat
Measured as milliseconds.
Time frame: From pre-dose to post etavopivat/ etavopivat placebo dose on day 1 to day 23
Part A: Number of treatment-emergent clinically significant abnormal findings in electrocardiogram (ECGs)
Measured as count of treatment-emergent clinically significant abnormal findings in ECGs.
Time frame: From dosing (Day 1) until end of study (Day 8)
Parts A and B: Cmax,etavopivat- Maximum observed etavopivat plasma concentration after a single dose
Measured as nanograms per milliliter (ng/mL).
Time frame: Day 1 (Part B)/ From day 1 to day 5 (Part A) after investigational medicinal product (IMP) administration
Parts A and B: AUC0-last,etavopivat- Area under the etavopivat plasma concentration-time curve from 0 hours to the time of last quantifiable concentration
Measured as hours\*nanograms per milliliter (h\*ng/mL).
Time frame: Day 1 (Part B)/ From day 1 to day 5 (Part A) after IMP administration
Parts A and B: AUC0-inf,etavopivat- Area under the etavopivat plasma concentration-time curve from 0 hours and extrapolated to infinity after a single dose
Measured as h\*ng/mL.
Time frame: Day 1 (Part B)/ From day 1 to day 5 (Part A) after IMP administration
Parts A and B: tmax,etavopivat- Time to maximum observed etavopivat plasma concentration after a single dose
Measured as hours.
Time frame: Day 1 (Part B)/ From day 1 to day 5 (Part A) after IMP administration
Parts A and B: t½ etavopivat- Terminal half-life for etavopivat after a single dose
Measured as hours.
Time frame: Day 1 (Part B)/ From day 1 to day 5 (Part A) after IMP administration
Parts A and B: CL/F etavopivat- Apparent plasma clearance of etavopivat after a single dose
Measured as liters per hour (L/h).
Time frame: Day 1 (Part B)/ From day 1 to day 5 (Part A) after IMP administration
Parts A and B: Vz/F etavopivat- Apparent volume of distribution of etavopivat after a single dose based on plasma concentration values
Measured as liters (L).
Time frame: Day 1 (Part B)/ From day 1 to day 5 (Part A) after IMP administration
Part B: ΔQTcF for moxifloxacin
Measured as milliseconds.
Time frame: From pre-dose to post moxifloxacin dose on day 1 to day 23
Part B: Change from baseline in heart rate (ΔHR). Categorical outliers for HR
Measured as milliseconds.
Time frame: From pre-dose to post etavopivat/ etavopivat placebo dose on day 1 to day 23
Part B: Change from baseline in PR interval (ΔPR). Categorical outliers for PR
Measured as milliseconds.
Time frame: From pre-dose to post etavopivat/ etavopivat placebo dose on day 1 to day 23
Part B: Change from baseline in QRS complex duration (ΔQRS). Categorical outliers for QRS
Measured as milliseconds.
Time frame: From pre-dose to post etavopivat/ etavopivat placebo dose on day 1 to day 23
Part B: Frequency of treatment emergent changes of ECG morphology
Measured as count of treatment emergent changes of ECG morphology.
Time frame: From pre-dose to post etavopivat/ etavopivat placebo dose on day 1 to day 23
Part B: Change from baseline in ΔHR. Categorical outliers for HR
Measured as milliseconds.
Time frame: From pre-dose to post moxifloxacin dose on day 1 to day 23
Part B: Change from baseline in ΔPR. Categorical outliers for PR
Measured as milliseconds.
Time frame: From pre-dose to post moxifloxacin dose on day 1 to day 23
Part B: Change from baseline in ΔQRS. Categorical outliers for QRS
Measured as milliseconds.
Time frame: From pre-dose to post moxifloxacin dose on day 1 to day 23
Part B: Frequency of treatment emergent changes of ECG morphology
Measured as count of treatment emergent changes of ECG morphology.
Time frame: From pre-dose to post moxifloxacin dose on day 1 to day 23
Part B: ΔQTcF for etavopivat
Measured as milliseconds.
Time frame: From pre-dose to post etavopivat/etavopivat placebo dose on day 1 to day 23
This platform is for informational purposes only and does not constitute medical advice. Always consult a qualified healthcare professional.