A Safety and Efficacy Study Comparing Naltrexone SR/Bupropion SR and Placebo in Obese Subjects With Type 2 Diabetes

Phase 3

Completed

Conditions: Obesity
Diabetes Mellitus, Type 2
Overweight

Interventions: Drug: Placebo
Drug: Naltrexone SR 32 mg/bupropion SR 360 mg/ day
Behavioral: Ancillary therapy

Registration Number: NCT00474630

Lead Sponsor: Orexigen Therapeutics, Inc

Brief Summary: The purpose of this study is determine whether the combination of naltrexone SR and bupropion SR is safe and effective in treating obesity in subjects with type 2 diabetes.

Detailed Description: Optimal care of patients with diabetes mellitus includes vigorous and persistent efforts to achieve physiologic control of blood glucose as well as other often associated conditions including hypertension, dyslipidemia and excess weight. Pharmacologic interventions for the treatment of obesity in type 2 diabetes have shown significant reductions in HbA1c. Two Phase II clinical trials demonstrated that a combination of bupropion SR and naltrexone is associated with greater weight loss than bupropion SR alone, naltrexone alone, or placebo in subjects with uncomplicated obesity. The current study investigated the safety and efficacy of the combination of naltrexone SR and bupropion SR compared to placebo in obese subjects with type 2 diabetes mellitus.

Recruitment & Eligibility

Status: COMPLETED

Sex: All

Target Recruitment: 505

Inclusion Criteria

Female or male subjects aged 18 to 70 years of age (inclusive)
Body mass index (BMI) ≥27 and ≤45 kg/m²
Diagnosed with type 2 diabetes mellitus and on no injectable antidiabetes medication or inhaled insulin for more than 3 months prior to randomization
Took stable doses of oral single or combination hypoglycemic medications (biguanides, thiazolidinediones, meglitinides, α-glucosidase inhibitors, sulfonylureas, DPP4 inhibitors) for at least 3 months prior to randomization or did not take medications for the treatment of type 2 diabetes mellitus
Normotensive (systolic ≤145 mm Hg and diastolic ≤95 mm Hg). Antihypertensive medications were allowed with the exception of alpha-adrenergic blockers, and clonidine. Antihypertensive treatment was stable for at least 4 weeks prior to randomization.
Medications for the treatment of dyslipidemia were allowed with the exception of cholestyramine and cholestypol as long as the medical regimen had been stable for at least 4 weeks prior to randomization.
Free of opioid medication for 7 days prior to randomization
HbA1c between 7% and 10%, fasting blood glucose <270 mg/dL, and fasting triglycerides <400 mg/dL
No clinically significant abnormality of serum albumin, blood urea nitrogen (BUN), bilirubin, calcium, and phosphorus
Creatinine levels were ≤1.4 mg/dL for female subjects and ≤1.5 mg/dL for male subjects
Alanine aminotransferase (ALT) and aspartate aminotransferase (AST) levels were within 2.5 × upper limit of laboratory normal range (ULN)
No clinically significant abnormality of hematocrit, white blood cell (WBC) count, WBC differential, or platelets
No clinically significant abnormality on urinalysis
TSH within normal limits or normal T3, if TSH is below normal limits
Female subjects of childbearing potential had a negative serum pregnancy test
Negative urine drug screen
An IDS-SR score <2 on individual items 5 (sadness), 6 (irritability), 7 (anxiety/tension), and 18 (suicidality) and an IDS-SR total score <30
Female subjects of childbearing potential were non-lactating and agreed to continue to use effective contraception throughout the study and 30 days after discontinuation of study drug
Able to comply with all required study procedures and schedule
Able to speak and read English
Provided written informed consent

Exclusion Criteria

Type I diabetes mellitus
"Brittle-diabetes" or any hospitalization or emergency room visit due to poor diabetic control within 6 months prior to screening, history of diabetes-related dehydration leading to hospitalization, or history or evidence of ketoacidosis
Obesity of known endocrine origin other than diabetes mellitus (e.g., untreated hypothyroidism, Cushing's syndrome, established polycystic ovary syndrome)
Diabetes mellitus secondary to pancreatitis or pancreatectomy
Serious medical condition including but not limited to renal or hepatic insufficiency and Class III or IV congestive heart failure; history of myocardial infarction, angina pectoris, claudication, or acute limb ischemia within 6 months prior to screening; lifetime history of stroke
History of malignancy with exception of non-melanoma skin cancer or surgically cured cervical cancer within 5 years prior to screening
Loss or gain of more than 5.0 kg within the 3 months prior to screening
Severe microvascular or macrovascular complications of diabetes, including but not limited to proliferative retinopathy, active limb ulcerations, amputation of metatarsals or above
Serious psychiatric illness, including lifetime history of bipolar disorder, schizophrenia or other psychosis, bulimia, and anorexia nervosa; current serious personality disorder (e.g., borderline or antisocial); current severe major depressive disorder; recent (6 months prior to screening) suicide attempt or current active suicidal ideation; or recent hospitalization due to psychiatric illness
Response to the bipolar disorder questions that indicated the presence of bipolar disorder
Required medications for the treatment of a psychiatric disorder (with the exception of short term insomnia) within 6 months prior to screening
History of drug or alcohol abuse or dependence within 1 year prior to screening
Baseline ECG with a QTc interval (Bazett's formula) >450 msec (men) and >470 msec (women) or the presence of any clinically significant cardiac abnormalities, including but not limited to patterns consistent with recent myocardial ischemia, electrolyte abnormalities, or atrial or ventricular dysrhythmia or significant conduction abnormalities
Received the following excluded concomitant medications: any psychotropic agents (including antipsychotic, antidepressant, anxiolytic, mood stabilizer, anticonvulsant agents, and agents for the treatment of attention deficit disorder) with the exception of low-dose benzodiazepine or hypnotic agents for the treatment of insomnia (up to 2 mg lorazepam/day or equivalent dose of a benzodiazepine or hypnotic agent); any anorectic or weight loss agents; any over-the-counter dietary supplements or herbs with psychoactive, appetite, or weight effects; alpha-adrenergic blockers; dopamine agonists; clonidine; coumadin; theophylline; cimetidine; oral corticosteroids; cholestyramine, cholestypol, Depo Provera®; smoking cessation agents; use of opioid or opioid-like medications, including analgesics and antitussives
History of surgical or device intervention for obesity (e.g., gastric banding)
History of seizures of any etiology, or of predisposition to seizures (e.g., history of cerebrovascular accident, head trauma with ≥5 minutes loss of consciousness, concussion symptoms lasting ≥15 minutes, brain surgery, skull fracture, subdural hematoma, or febrile seizures)
Treatment with bupropion or naltrexone within 12 months prior to screening
History of hypersensitivity or intolerance to bupropion or naltrexone
Changes in smoking status or in tobacco or nicotine use within 3 months prior to screening or planned during study participation
Participated in a weight loss management program within one month prior to randomization
Females who were pregnant or breast-feeding or planned to become pregnant during the study period or within 30 days of discontinuing study drug
Planned surgical procedure that could impact the conduct of the study
Received any investigational drug or used an experimental device or procedure within the previous 30 days
Participated in any previous clinical trial conducted by Orexigen
Had any condition that in the opinion of the investigator made the subject unsuitable for inclusion into the study

Study & Design

Study Type: INTERVENTIONAL

Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Placebo	Placebo	Placebo with ancillary therapy
NB32	Naltrexone SR 32 mg/bupropion SR 360 mg/ day	Naltrexone SR 32 mg/bupropion SR 360 mg/ day with ancillary therapy
Placebo	Ancillary therapy	Placebo with ancillary therapy
NB32	Ancillary therapy	Naltrexone SR 32 mg/bupropion SR 360 mg/ day with ancillary therapy

Primary Outcome Measures

Name	Time	Method
Co-primary: Body Weight- Mean Percent Change	Baseline, 56 weeks
Co-primary: Body Weight- Proportion of Subjects With ≥5% Decrease	Baseline, 56 weeks

Secondary Outcome Measures

Name	Time	Method
Change in Fasting Triglycerides Levels, Using Log-transformed Data	Baseline, 56 weeks
Change in Fasting Blood Glucose Levels	Baseline, 56 weeks
Change in Waist Circumference	Baseline, 56 weeks
HbA1c- Proportion of Subjects With HbA1c <7% at Endpoint	Baseline, 56 weeks
Percent of Subjects Requiring Rescue Medications for Diabetes	Baseline, 56 weeks
Change in HbA1c Levels	Baseline, 56 weeks
Change in Fasting HDL Cholesterol Levels	Baseline, 56 weeks
Percent of Subjects With Dose Reduction in Oral Antidiabetes Medications	Baseline, 56 weeks
HbA1c- Proportion of Subjects With HbA1c <6.5% at Endpoint	Baseline, 56 weeks
Change in Fasting LDL Cholesterol Levels	Baseline, 56 weeks
Change in Diastolic Blood Pressure	Baseline, 56 weeks
Percent of Subjects With Dose Increase in Oral Antidiabetes Medications	Baseline, 56 weeks
Change in HOMA-IR Levels, Using Log-transformed Data	Baseline, 56 weeks	HOMA-IR= Homeostasis Model Assessment-Insulin Resistance
Change in IWQOL-Lite Total Scores	Baseline, 56 weeks	IWQOL-Lite= Impact of Weight on Quality of Life-Lite Questionnaire Total score is based on a scale from 0 to 100, with 0 representing the poorest and 100 the best quality of life and where a score of 71-79 indicates moderate impairment
Percent of Subjects Discontinuing Due to Poor Glycemic Control	Baseline, 56 weeks	Due to pre-specified hypothesis testing design, no formal statistical inference testing was performed. Odds ratio not calculated as there were no subjects in the NB32 group that discontinued due to poor glycemic control.
Change in Question 19 From 21-Item COE (Control of Eating) Questionnaire	Baseline, 56 weeks	Question 19: Generally, how difficult has it been to control your eating? Scoring: 0=not at all difficult; 100=extremely difficult
Body Weight- Proportion of Subjects With ≥10% Decrease	Baseline, 56 weeks
Change in Fasting Insulin Levels, Using Log-transformed Data	Baseline, 56 weeks
Change in Systolic Blood Pressure	Baseline, 56 weeks
Change in High-sensitivity C Reactive Protein (Hs-CRP) Levels, Using Log-transformed Data	Baseline, 56 weeks
Change in IDS-SR Total Scores	Baseline, 56 weeks	IDS-SR= Inventory of Depressive Symptoms-Subject Rated IDS-SR total score is based on 30 items. The total score can range from 0-84, with 0 being no depressive symptoms and 84 being very severe depressive symptoms. A total score ≤ 13 indicates no depression.
Change in Food Craving Inventory Sweets Subscale Score	Baseline, 56 weeks	The Food Craving Inventory is a 33-item self-report measure designed to assess specific food cravings and is organized into 4 subscales (high fats, sweets, carbohydrates/starches, and fast-food fats). A craving was defined as an intense desire to consume a particular food (or food type) that was difficult to resist over the past month. Subjects rated their frequency of cravings for each of the 33 items using a 5-point scale, where 1=never, 2=rarely, 3=sometimes, 4=often, and 5=always. The sweets subscale consisted of 8 items and the score ranges from 8 (better outcome) to 40 (worse outcome).
Change in Food Craving Inventory Carbohydrates Subscale Score	Baseline, 56 weeks	The Food Craving Inventory is a 33-item self-report measure designed to assess specific food cravings and is organized into 4 subscales (high fats, sweets, carbohydrates/starches, and fast-food fats). A craving was defined as an intense desire to consume a particular food (or food type) that was difficult to resist over the past month. Subjects rated their frequency of cravings for each of the 33 items using a 5-point scale, where 1=never, 2=rarely, 3=sometimes, 4=often, and 5=always. The carbohydrates subscale consisted of 8 items and the score ranges from 8 (better outcome) to 40 (worse outcome).

Trial Locations

Locations (53): Center for Nutrition and Metabolic Diseases, Univ. of Nevada
🇺🇸
Reno, Nevada, United States
ClinSearch
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Chattanooga, Tennessee, United States
Central Ohio Nutrition Center, Inc.
🇺🇸
Columbus, Ohio, United States
SelfCenter, PC
🇺🇸
Fairhope, Alabama, United States
Impact Clinical Trials
🇺🇸
Beverly Hills, California, United States
HealthStar Research
🇺🇸
Hot Springs, Arkansas, United States
Northern California Research
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Carmichael, California, United States
Sierra Medical Research
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Fresno, California, United States
Advance Clinical Research Institute
🇺🇸
Orange, California, United States
Apex Research Institue
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Santa Ana, California, United States
LCFP Inc.
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Fort Myers, Florida, United States
Suncoast Clinical Research
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Palm Harbor, Florida, United States
Miami Research Associates
🇺🇸
Miami, Florida, United States
University Clinical Research
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Pembroke Pines, Florida, United States
CSRA Partners in Health, Inc
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Augusta, Georgia, United States
Central Kentucky Research Associates, Inc.
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Lexington, Kentucky, United States
Deaconess Clinic
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Evansville, Indiana, United States
Northwest Indiana Center for Clinical Research
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Valparaiso, Indiana, United States
L-Marc
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Louisville, Kentucky, United States
Trover Center for Clinical Studies
🇺🇸
Madisonville, Kentucky, United States
Health Trends Research, LLC
🇺🇸
Baltimore, Maryland, United States
FutureCare Studies
🇺🇸
Springfield, Massachusetts, United States
The Center for Pharmaceutical Research
🇺🇸
Kansas City, Missouri, United States
Twin Cities Clinical Research
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Brooklyn Center, Minnesota, United States
Mercy Health Research
🇺🇸
St. Louis, Missouri, United States
Radiant Research, Inc.
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St. Louis, Missouri, United States
Central New York Clinical Research
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Manlius, New York, United States
Lovelace Scientific Resources
🇺🇸
Albuquerque, New Mexico, United States
Rochester Clinical Research, Inc
🇺🇸
Rochester, New York, United States
Diabetes care and Information Center
🇺🇸
Flushing, New York, United States
Metrolina Medical Research
🇺🇸
Charlotte, North Carolina, United States
Your Diabetes Endocrine and Nutrition Group
🇺🇸
Mentor, Ohio, United States
Rapid Medical Research, Inc.
🇺🇸
Cleveland, Ohio, United States
Palmetto Medical Research
🇺🇸
Mt. Pleasant, South Carolina, United States
Baylor Endocrine Center
🇺🇸
Dallas, Texas, United States
The Cooper Institute
🇺🇸
Dallas, Texas, United States
Diabetes Center of the Southwest
🇺🇸
Midland, Texas, United States
Summit Research Network, Inc.
🇺🇸
Seattle, Washington, United States
Northside Internal Medicine
🇺🇸
Spokane, Washington, United States
East-West Medical Research Institute
🇺🇸
Honolulu, Hawaii, United States
Affiliated Research Institute
🇺🇸
San Diego, California, United States
VA San Diego Healthcare System
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San Diego, California, United States
Clinical Research Associates, Inc.
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Nashville, Tennessee, United States
InVisions Consultants, LLC
🇺🇸
San Antonio, Texas, United States
Diabetes & Glandular Disease Research Associates, Inc.
🇺🇸
San Antonio, Texas, United States
Wells Institute for Health Awareness
🇺🇸
Kettering, Ohio, United States
HOPE Research Institute
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Phoenix, Arizona, United States
Chase Medical Research, LLC
🇺🇸
Waterbury, Connecticut, United States
Medical Research Institute
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Slidell, Louisiana, United States
Pennington Biomedical Research Center
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Baton Rouge, Louisiana, United States
Pivotal Research Centers
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Peoria, Arizona, United States
Endocrinology & Diabetes Consultants
🇺🇸
Dover, New Hampshire, United States
Mountain View Clinical Research
🇺🇸
Greer, South Carolina, United States