Study of the Product QGC001 as a Single Dose and Multiple Doses Administered Orally to Healthy Adult Subjects

Phase 1

Completed

• Conditions: Essential Hypertension
• Interventions: Drug: QGC001 [(3S,3'S)-4,4'-dithiobis (3-aminobutane-1-sulfonic acid)]; Drug: Placebo

• Registration Number: NCT01900184
• Lead Sponsor: Quantum Genomics SA

Brief Summary

1QG2 is a Phase 1 study aiming to assess the safety and tolerability of ascending single/multiple oral doses (SAD \& MAD) in healthy young subjects, the preliminary food interaction and the effect of QGC001 on blood pressure and heart rate, but also to determine pharmacokinetic preliminary profiles of QGC001 and its metabolite EC33 and pharmacodynamic preliminary profiles of QGC001 and its metabolite EC33 especially effects on the renin-angiotensin-aldosterone and copeptin systems.

Detailed Description

Not available

Study Timeline

• Study Start: 2012-12
• Primary Completion: 2013-03
• Study Completion: 2013-03
• Study First Submitted: 2013-06-27
• Status Verified: 2013-07
• Study First Submitted QC: 2013-07-11
• Last Update Submitted: 2013-07-11
• Study First Posted: 2013-07-16
• Last Update Posted: 2013-07-16

Recruitment & Eligibility

• Status: COMPLETED
• Sex: Male
• Target Recruitment: 69

Inclusion Criteria

• Caucasian, male healthy subjects of 18 to 45 years of age (inclusive).
• Body weight ≥50 kg, with a body mass index calculated as weight in kg/(height in m2) from 18 to 27 kg/m2 at screening.
• Subjects will sign and date an informed consent form before any study-specific screening procedure is performed.
• Healthy, as determined by the investigator on the basis of medical history, physical examination findings, clinical laboratory test results, vital sign measurements, and digital 12 lead ECG readings.
• Non-smoker or smoker of fewer than 5 cigarettes per day as determined by history. Must be able to abstain from smoking during the inpatient stay.
• Have a high probability for compliance with and completion of the study.

Exclusion Criteria

• Any significant cardiovascular, hepatic, renal, respiratory, gastrointestinal, endocrine, immunologic, dermatological, haematological, neurologic, psychiatric disease or history of any clinically important drug allergy.
• Acute disease state within 7 days before study day 1.
• History of drug abuse within 1 year before study day 1.
• History of alcoholism within 1 year before day 1. Consumption of more than 50 g of ethanol per day.
• Positive serologic findings for human immunodeficiency virus antibodies, hepatitis B surface antigen, and/or hepatitis C virus antibodies.
• Positive findings of urine drug screen (e.g., amphetamines, barbiturates, benzodiazepines, cannabinoids, cocaine, methadone, opiates, MDMA)
• History of any clinically important drug allergy.
• Prohibited Treatments: use of any investigational drug within 90 days or prescription drug within 30 days before investigational medical product administration.
• Consumption of any caffeine-containing products in excess of 6 cups per day (or equivalent), of grapefruit, grapefruit-containing products, or alcoholic beverages within 24 hours before study day 1.
• Use of any over-the-counter drugs including herbal supplements (except for the occasional use of acetaminophen [paracetamol], aspirin and vitamins ≤100% recommended daily allowance) within 7 days before investigational medicinal product administration.
• Donation of blood (i.e. 450 ml) within 90 days before study day 1.

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
500 mg bid of QGC001	QGC001 [(3S,3'S)-4,4'-dithiobis (3-aminobutane-1-sulfonic acid)]	Each dose of QGC001 will be administered in solution with 200 mL of purified water.
750 mg bid of QGC001	QGC001 [(3S,3'S)-4,4'-dithiobis (3-aminobutane-1-sulfonic acid)]	Each dose of QGC001 will be administered in solution with 200 mL of purified water.
1,000 mg bid of QGC001	QGC001 [(3S,3'S)-4,4'-dithiobis (3-aminobutane-1-sulfonic acid)]	Each dose of QGC001 will be administered in solution with 200 mL of purified water.
Placebo	Placebo	The placebo will be administered in solution with 200 mL of purified water.

Primary Outcome Measures

Name	Time	Method
Adverse events	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Red blood cell count	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Haemoglobin	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Haematocrit	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
White blood cell count with differential	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Platelet count	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Plasma sodium	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Plasma potassium	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Plasma calcium	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Plasma total bilirubin	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Plasma conjugated bilirubin	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Plasma Aspartate Amino Transferase (ASAT)	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Plasma Alanine Amino Transferase (ALAT)	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Plasma Gamma Glutamyl Transferase (GGT)	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Plasma alkaline phosphatases	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Plasma total protein	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Plasma Creatine PhosphoKinase (CPK)	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Plasma creatinine	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Plasma glucose	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Plasma cholesterol	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Plasma triglycerides	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Urinary pH	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Urinary protein	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Urinary glucose	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Urinary leukocytes	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Urinary nitrites	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Urinary ketones	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Urinary blood	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Weight assessment (kg)	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Body temperature (°C)	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Supine and orthostatic (systolic and diastolic) blood pressure	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
Heart rate	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD
12-lead ECG	up to 4 weeks for SAD, 5 weeks for FI and 6 weeks for MAD

Secondary Outcome Measures

Name	Time	Method
Maximum observed plasma concentration (Cmax) of QGC001	up to 3 days for SAD and FI, up to 9 days for MAD	Cohorts SAD 1 to 4 and MAD 1 to 3.
Time at which Cmax is observed (tmax) of QGC001	up to 3 days for SAD and FI, up to 9 days for MAD	Cohorts SAD 1 to 4 and MAD 1 to 3.
Elimination rate constant (λz) of QGC001	up to 3 days for SAD and FI, up to 9 days for MAD	Cohorts SAD 1 to 4 and MAD 1 to 3.
Terminal half-life (t1/2,z) of QGC001	up to 3 days for SAD and FI, up to 9 days for MAD	Cohorts SAD 1 to 4 and MAD 1 to 3.
Area Under the Concentration-time curve (AUClast and AUC0-∞) of QGC001	up to 3 days for SAD and FI, up to 9 days for MAD	Cohorts SAD 1 to 4 and MAD 1 to 3.
Maximum observed plasma concentration (MRCmax) of metabolic ratios	up to 3 days for SAD and FI, up to 9 days for MAD	Cohorts SAD 1 to 4 and MAD 1 to 3.
Area Under the Concentration-time curve (MRAUC) of metabolic ratios	up to 3 days for SAD and FI, up to 9 days for MAD	Cohorts SAD 1 to 4 and MAD 1 to 3.
Cumulative amount eliminated (Ae)	up to 2 days for SAD and FI, up to 8 days for MAD	Cohorts SAD 1 to 4 and MAD 1 to 3.
Fraction recovered (Fe)	up to 2 days for SAD and FI, up to 8 days for MAD	Cohorts SAD 1 to 4 and MAD 1 to 3.
Renal clearance (CLR)	up to 2 days for SAD and FI, up to 8 days for MAD	Cohorts SAD 1 to 4 and MAD 1 to 3.
Plasma renin	up to 2 days for SAD and FI, up to 8 days for MAD	Determination of renin in blood samples. Cohorts SAD 1 to 3 and MAD 1 to 3.
Plasma aldosterone	up to 2 days for SAD and FI, up to 8 days for MAD	Determination of aldosterone in blood samples. Cohorts SAD 1 to 3 and MAD 1 to 3.
Plasma cortisol	up to 2 days for SAD and FI, up to 8 days for MAD	Determination of cortisol in blood samples. Cohorts SAD 1 to 3 and MAD 1 to 3.
Plasma copeptin	up to 2 days for SAD and FI, up to 8 days for MAD	Determination of copeptin in blood samples. Cohorts SAD 1 to 3 and MAD 1 to 3.
Urinary aldosterone	up to 2 days for SAD and FI, up to 8 days for MAD	Aldosterone analysis in urine samples. Cohorts SAD 1 to 3 and MAD 1 to 3.
Urinary cortisol	up to 2 days for SAD and FI, up to 8 days for MAD	Cortisol analysis in urine samples. Cohorts SAD 1 to 3 and MAD 1 to 3.
Urinary sodium	up to 2 days for SAD and FI, up to 8 days for MAD	Sodium analysis in urine samples. Cohorts SAD 1 to 3 and MAD 1 to 3.
Urinary potassium	up to 2 days for SAD and FI, up to 8 days for MAD	Potassium analysis in urine samples. Cohorts SAD 1 to 3 and MAD 1 to 3.
Urinary creatinine	up to 2 days for SAD and FI, up to 8 days for MAD	Creatinine analysis in urine samples. Cohorts SAD 1 to 3 and MAD 1 to 3.
Systolic and Diastolic Blood Pressure	up to 8 days for MAD	Cohorts MAD 1 to 3.
Heart Rate	up to 8 days for MAD	Cohorts MAD 1 to 3.

Trial Locations

Locations (1)

Biotrial PARIS; 🇫🇷 Rueil-Malmaison, France