Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
| Name | Class |
|---|---|
| CTC Clinical Trial Consultants AB | INDUSTRY |
Not provided
Not provided
Not provided
Not provided
This study is a proof of concept study to demonstrate that EMP16-02, a fixed dose combination (FDC) of orlistat and acarbose in an oral multiple-unit modified release (MR) formulation leads to a clinically relevant decrease in body weight. The study aims to evaluate the efficacy, safety and tolerability of treatment with two different doses of EMP16 02 (120 mg orlistat/40 mg acarbose and 150 mg orlistat/50 mg acarbose) for 26 weeks on reducing body weight in obese patients.
This study is a proof of concept study to demonstrate that EMP16-02, a fixed dose combination (FDC) of orlistat and acarbose in an oral multiple-unit modified release (MR) formulation leads to a clinically relevant decrease in body weight. The study aims to evaluate the efficacy, safety and tolerability of treatment with two different doses of EMP16 02 (120 mg orlistat/40 mg acarbose and 150 mg orlistat/50 mg acarbose) for 26 weeks on reducing body weight in obese patients.
EMP16-02 will be given to obese patients with an initial BMI ≥ 30 kg/m² or ≥ 28 kg/m² in the presence of other risk factors (e.g., hypertension, glucose dysregulation such as impaired glucose tolerance and type 2 diabetes mellitus (T2DM) and/or dyslipidaemia.
The study consists of 6 visits to the research clinic, including screening and follow-up. There will be no overnight stays at the clinic.
Visit 1: Screening (Visit 1) will take place from Day -28 to Day -1. Visit 2: Eligible and consenting patients will arrive at the research clinic in the morning of the first dosing day (Day 1, Visit 2) after at least 8 hours overnight fasting.
A re-check of eligibility including a brief physical examination, vital signs and assessment of body weight will be conducted. The patients will be randomised to either of two doses of EMP16-02 or placebo:
Between visit 2 and 3: Patients randomised to EMP16-02 will start with a run-in period of 6 weeks during which the dose is sequentially increased. From week 7, all patients will have reached their final intended dose and a 20 week treatment and observation period will start. The run-in phase will start at a dose of 60 mg O and 20 mg A TID, which will sequentially be increased with 30 mg O/10 mg A every two weeks until the target doses of 120 mg O/40 mg A TID (for the lower dose group) and 150 mg O/50 mg A TID (for the higher dose group) are reached. Placebo treatment consists of matching oral capsules. Placebo and EMP16-02 capsules need to be taken TID together with three daily meals.
Visit 3-5: Patients will come to the clinic at Visit 3 (week 7), Visit 4 (week 14) and Visit 5 (week 26) for safety assessments and assessments of weight and anthropometric measurements. Patients will arrive in the morning after at least 8 hours overnight fasting. All visits will start with a brief physical examination followed by blood sampling (fasting) and assessment of body weight and body composition. A standardised breakfast will be served during which the patient will take the IMP. All or a selection of the questionnaires, including the satiety and craving questionnaire, will be filled in in a similar way as during Visit 2.
New IMP will be handed out to the patients at Visit 2, 3 and 4. At Visit 5 (week 26), the patients will take the last dose during breakfast at the clinic.
After 18 and 22 weeks of treatment (Day 123 ± 3 days and Day 151 ± 3 days, respectively), patients will be asked to answer questions about IMP compliance, occurrence of adverse events (AEs) and use of concomitant medication using an electronic diary.
Visit 6: A follow up safety visit.
Not provided
Not provided
Not provided
Not provided
| Label | Type | Description | Intervention Names |
|---|---|---|---|
| EMP16-02 120 mg orlistat/40 mg acarbose | Experimental | Dosage form: Oral, modified-release (MR) fixed dose combination (FDC) of orlistat and acarbose formulated in capsules. Dosage: 120 mg O/40 mg A (given as 2 capsules EMP16-02-60/20). Frequency: Three times daily (TID) together with the three main daily meals .Taken halfway through each meal, together with approximately 100-200 mL water (or other drink). Duration: 26 weeks. |
|
| EMP16-02 150 mg orlistat/50 mg acarbose | Experimental | Dosage form: Oral, modified-release (MR) fixed dose combination (FDC) of orlistat and acarbose formulated in capsules. Dosage: 150 mg O/50 mg A (given as 1 capsule EMP16-02-90/30 and 1 capsule EMP16-02-60/20). Frequency: Three times daily (TID) together with the three main daily meals .Taken halfway through each meal, together with approximately 100-200 mL water (or other drink). Duration: 26 weeks. |
|
| Placebo | Placebo Comparator | Dosage form: Matching, oral capsule. Identical in appearance but contain only cellulose. Dosage: Placebo (given as 2 placebo capsules) Frequency: Three times daily (TID) together with the three main daily meals .Taken halfway through each meal, together with approximately 100-200 mL water (or other drink). Duration: 26 weeks. |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| EMP16-02 120 mg orlistat/40 mg acarbose | Drug | EMP16-02 capsules are composed of three pharmaceutical fractions (granules denoted G1, G2 and G3). G1= Prolonged release of acarbose, G2= Enteric-coated granule fraction containing orlistat and acarbose, G3= Orlistat with a delayed on-set release mechanism. |
| Measure | Description | Time Frame |
|---|---|---|
| Body weight, relative (%) change from baseline for EMP16-02 (120 mg O/40 mg A) | Relative (%) change from baseline in body weight after 26 weeks of treatment with EMP16-02 (120 mg O/40 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Measure | Description | Time Frame |
|---|---|---|
| Body weight, absolute change from baseline for EMP16-02 (120 mg O/40 mg A) | Absolute change from baseline in body weight after 14 and 26 weeks of treatment with EMP16-02 (120 mg O/40 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 14 and week 26. |
| Body weight, relative (%) and absolute change from baseline for EMP16-02 (150 mg O/50 mg A) |
Not provided
Inclusion Criteria:
Women of non-childbearing potential are defined as pre-menopausal females who are sterilised (tubal ligation or permanent bilateral occlusion of fallopian tubes); or post menopausal defined as 12 months of amenorrhea (in questionable cases a blood sample with simultaneous detection of follicle stimulating hormone [FSH] 25 140 IE/L).
Exclusion Criteria:
Not provided
Not provided
Not provided
Not provided
Not provided
| Name | Affiliation | Role |
|---|---|---|
| Helena Litorp, MD, PhD | CTC Clinical Trial Consultants AB | Principal Investigator |
| Daniel Wilhelms, MD, PhD | CTC Clinical Trial Consultants AB | Principal Investigator |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Clinical Trial Consultants AB | Linköping | 58758 | Sweden | |||
| Clinical Trial Consultants AB |
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
This is an exploratory, randomised, double-blind and placebo-controlled study.
Not provided
Not provided
This is a double-blind study and the allocation of treatments will not be disclosed until clean file has been declared and the database has been locked.
Active treatment and placebo capsules are identical in appearance.
|
|
| EMP16-02 150 mg orlistat/50 mg acarbose | Drug | EMP16-02 capsules are composed of three pharmaceutical fractions (granules denoted G1, G2 and G3). G1= Prolonged release of acarbose, G2= Enteric-coated granule fraction containing orlistat and acarbose, G3= Orlistat with a delayed on-set release mechanism. |
|
|
| Placebo | Drug | Matching oral placebo capsules |
|
Relative (%) and absolute change from baseline in body weight after 14 and 26 weeks of treatment with EMP16-02 (150 mg O/50 mg A) as compared to placebo. |
| From first dose to last dose (week 26). Measured at baseline, week 14 and week 26. |
| Proportion of patients with ≥5% and ≥10% decrease in body weight for EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Proportion of patients with ≥5% and ≥10% decrease in body weight compared to baseline after 14 and 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 14 and week 26. |
| BMI, relative (%) and absolute change from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Relative (%) and absolute change from baseline in BMI after 14 and 26 weeks of treatment with EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 14 and week 26. |
| Waist circumference, absolute change from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Absolute change from baseline in waist circumference after 14 and 26 weeks of treatment with EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 14 and week 26. |
| Sagittal diameter, absolute change from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Absolute change from baseline in sagittal diameter after 14 and 26 weeks of treatment with EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 14 and week 26. |
| Percentage body fat, relative (%) and absolute change from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Relative (%) and absolute change from baseline in percentage body fat after 14 and 26 weeks of treatment with EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 14 and week 26. |
| Questionnaire Satiety and craving, after 14 and 26 weeks for EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Questionnaire Satiety and craving (generated by Empros Pharma AB) after 14 and 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo, corrected for satiety and craving after standardised breakfast at baseline. The questionnaire is generated by Empros Pharma and consists of 7 questions about sense of hunger, sense of satiety and cravings for certain types of food that needs to be answered on a scale from 0 (not at all) to 9 (extremely much). | From first dose to last dose (week 26). Measured at baseline, week 7, week 14, and week 26. |
| Haemoglobin A1C (HbA1c): Relative (%) and absolute change from baseline for EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Relative (%) and absolute change from baseline in fasting haemoglobin A1C (HbA1c) after 7, 14 and 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 7, week 14, and week 26. |
| Glucose: Relative (%) and absolute change from baseline for EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Relative (%) and absolute change from baseline in fasting glucose after 7, 14 and 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 7, week 14, and week 26. |
| Insulin: Relative (%) and absolute change from baseline for EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Relative (%) and absolute change from baseline in fasting insulin after 7, 14 and 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 7, week 14, and week 26. |
| Total cholesterol: Relative (%) and absolute change from baseline for EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Relative (%) and absolute change from baseline in fasting total cholesterol after 7, 14 and 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 7, week 14, and week 26. |
| High-density lipoprotein (HDL): Relative (%) and absolute change from baseline for EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Relative (%) and absolute change from baseline in fasting high-density lipoprotein (HDL) after 7, 14 and 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 7, week 14, and week 26. |
| Low-density lipoprotein (LDL): Relative (%) and absolute change from baseline for EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Relative (%) and absolute change from baseline in fasting low-density lipoprotein (LDL) after 7, 14 and 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 7, week 14, and week 26. |
| Triglycerides: Relative (%) and absolute change from baseline for EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Relative (%) and absolute change from baseline in fasting triglycerides after 7, 14 and 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 7, week 14, and week 26. |
| Albumin: Relative (%) and absolute change from baseline for EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Relative (%) and absolute change from baseline in fasting albumin after 7, 14 and 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 7, week 14, and week 26. |
| High-sensitivity C-reactive protein (hs CRP): Relative (%) and absolute change from baseline for EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Relative (%) and absolute change from baseline in fasting high-sensitivity C-reactive protein (hs CRP) after 7, 14 and 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 7, week 14, and week 26. |
| Alanine aminotransferase (ALT): Relative (%) and absolute change from baseline for EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Relative (%) and absolute change from baseline in fasting alanine aminotransferase (ALT) after 7, 14 and 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 7, week 14, and week 26. |
| Aspartate aminotransferase (AST): Relative (%) and absolute change from baseline for EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Relative (%) and absolute change from baseline in fasting aspartate aminotransferase (AST) after 7, 14 and 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 7, week 14, and week 26. |
| Alkaline phosphatase (ALP): Relative (%) and absolute change from baseline for EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Relative (%) and absolute change from baseline in fasting alkaline phosphatase (ALP) after 7, 14 and 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 7, week 14, and week 26. |
| Gamma-glutamyl transferase (GGT): Relative (%) and absolute change from baseline for EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Relative (%) and absolute change from baseline in fasting gamma-glutamyl transferase (GGT) after 7, 14 and 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 7, week 14, and week 26. |
| Proportion of diabetic (fasting glucose ≥ 7.0 mmol/L) and prediabetic patients (fasting glucose ≥ 6.1 mmol/L and < 7.0 mmol/L) for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Change from baseline in the proportion of diabetic (fasting glucose ≥ 7.0 mmol/L) and prediabetic patients (fasting glucose ≥ 6.1 mmol/L and < 7.0 mmol/L) after 14 and 26 weeks of treatment with EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 14 and week 26. |
| Blood pressure, relative (%) and absolute change from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Relative (%) and absolute change from baseline in blood pressure after 14 and 26 weeks of treatment with EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 14 and week 26. |
| Health and life quality questionnaire (RAND-36), change from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Change from baseline in quality of life after 26 weeks of treatment with EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. The questionnaire is owned by RAND Corporation USA and translated to swedish by Registercentrum SydOst (RCSO). The health and quality of life questionnaire consists of 36 questions about how the patient experiences his/her own physical and mental health. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Activity and sleep questionnaire, change from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Change from baseline in activity and sleep after 26 weeks of treatment with EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. The questionnaire is generated by Empros Pharma. The activity and sleep questionnaire consists of 2 questions about physical activity and sleep during the previous day/night. | From first dose to last dose (week 26). Measured at baseline, week 7, week 14 and week 26. |
| Drop-out rate (overall and GI-related), for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Dropout rate (overall and GI-related) following treatment with EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose until the date of drop-out, assessed up to 26 weeks. |
| Frequency and severity of AEs, for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Frequency and severity of AEs during 26 weeks of treatment with EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose until date of resolution of last AE registered or to End of study visit (week 28), whichever comes first. |
| Bilirubin (total), clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in bilirubin (total) after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Bilirubin (conjugated), clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in bilirubin (conjugated) after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Calcium, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in calcium after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Creatinine, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in creatinine after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Phosphate, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in phosphate after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Potassium, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in potassium after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Sodium, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in sodium after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Urea, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in urea after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Haematocrit, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in haematocrit after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Haemoglobin (Hb), clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in haemoglobin (Hb) after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Platelet count, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in platelet count after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Red blood cell (RBC) count, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in Red blood cell (RBC) count after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| White blood cell (WBC) count, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in White blood cell (WBC) count after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Activated Partial Thromboplastin Time (APTT), clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in Activated Partial Thromboplastin Time (APTT) after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Prothrombin Complex International Normalised Ratio (PK[INR]), clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in Prothrombin Complex International Normalised Ratio (PK[INR]) after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Erythrocytes in urine, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in erythrocytes in urine after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Glucose in urine, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in glucose in urine after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Ketones in urine, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in ketones in urine after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Leucocytes in urine, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in leucocytes in urine after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Nitrites in urine, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in nitrites in urine after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| pH in urine, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in pH in urine after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Protein in urine, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in protein in urine after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Specific gravity in urine, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in specific gravity in urine after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Urobilinogen in urine, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in urobilinogen in urine after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| ECG HR interval, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in ECG HR interval after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| ECG PR interval, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in ECG PR interval after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| ECG QRS interval, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in ECG QRS interval after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| ECG QT interval, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in ECG QT interval after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| ECG QTcF interval, clinically significant relative (%) and absolute changes from baseline for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Clinically significant relative (%) and absolute changes from baseline in ECG QTcF interval after 26 weeks of treatment with EMP16 02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline and week 26. |
| Gastrointestinal symptom rating scale (GSRS), for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | GI tolerability after 2, 4, 6, 8, 14 and 26 weeks of treatment with EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo.The questionnaire is owned by AstraZeneca. The GSRS consists of 15 questions about gastrointestinal symptoms combined into 5 symtom clusters; reflux, abdominal discomfort, indigestion, constipation and diarrhoea. The GSRS has a seven-point graded Likert-type scale where 1 represents absence of troublesome symptoms and 7 represents very troublesome symptoms. | From first dose to last dose (week 26). Measured at baseline, after 2, 4, 6, 8, 14 and 26 weeks. |
| IMP compliance, for EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) | Compliance after 7, 14 and 26 weeks of treatment with EMP16-02 (120 mg O/40 mg A and 150 mg O/50 mg A) as compared to placebo. | From first dose to last dose (week 26). Measured at baseline, week 7, week 14, and week 26. |
| Uppsala |
| 75237 |
| Sweden |
| ID | Term |
|---|---|
| D050177 | Overweight |
| D009765 | Obesity |
| ID | Term |
|---|---|
| D044343 | Overnutrition |
| D009748 | Nutrition Disorders |
| D009750 | Nutritional and Metabolic Diseases |
| D001835 | Body Weight |
| D012816 | Signs and Symptoms |
| D013568 | Pathological Conditions, Signs and Symptoms |
Not provided
Not provided