Use of Medication to Improve Weight Loss in Suboptimal Early Responders to Behavioral Treatment

Overview

This is a two-phase study. Phase 1 will evaluate obesity-related behavioral and biological characteristics as potential predictors of response to behavioral treatment (BT) for weight loss. Phase 2 is a double-blind, placebo-controlled, RCT to test whether adding weight loss medication to BT improves 24-week weight loss, as compared to BT with placebo, in subjects identified as having suboptimal early weight loss after 4 weeks of individual behavioral weight control. All participants, regardless of their early weight loss, will receive the same BT program of diet, physical activity, and behavior therapy for weight loss for an additional 24 weeks (28 total weeks of treatment).

Full Title of Study: “Use of Pharmacotherapy to Improve Weight Loss in Early Non-responders to Behavioral Treatment”

Study Type

  • Study Type: Interventional
  • Study Design
    • Allocation: Randomized
    • Intervention Model: Parallel Assignment
    • Primary Purpose: Treatment
    • Masking: Quadruple (Participant, Care Provider, Investigator, Outcomes Assessor)
  • Study Primary Completion Date: May 25, 2022

Detailed Description

Subjects will be a total of 150 adults, aged 21-70 years, with a body mass index (BMI) of 31 kg/m2 or above (28 kg/m2 with an obesity-related comorbidity). In phase 1, eligible subjects will complete questionnaires and an in-person baseline assessment of obesity-related behavioral characteristics (satiety, hunger, the relative reinforcing value of food [RRVfood], and impulsivity [delay discounting]), neuropeptides, and gastric emptying. After this baseline assessment, participants will begin an initial 4-week behavioral treatment (BT) "run-in" delivered individually in 20-30 minute weekly sessions (delivered virtually). The primary goal of phase 1 will be to evaluate baseline satiety, postprandial change in GLP-1, and gastric emptying as predictors of percent weight loss after 4 weeks of BT. We will also examine whether these variables predict categorization as a suboptimal early responder to BT (e.g., <2.0% loss; co-primary outcome). Secondary endpoints of phase 1 are percent weight loss from the start of the BT run-in (week -4) to randomization (week 0) and categorization as a suboptimal early responder, as predicted by additional behavioral characteristics (hunger as measured by VAS ratings, RRVfood as measured using a computer task, and impulsivity as measured using a delay discounting computer task) and neuropeptides (higher fasting ghrelin, lower fasting leptin, and lower postprandial changes in insulin and PYY). In phase 2, suboptimal early responders (based on weight loss during the BT run-in) will be randomly assigned to 24 weeks of: 1) BT plus placebo (BT+P); or 2) BT plus medication (BT+M; phentermine 15.0 mg). Both treatment groups will continue to attend 20-30 minute individual BT sessions (delivered virtually), weekly for the first 12 weeks and every other week for the last 12 weeks (total of 18 visits). Both treatment groups will also take once daily study medication (placebo or phentermine 15.0 mg) for the duration of the intervention period. Early BT responders identified during the run-in will receive the same 24-week BT program, but will not receive study medication or be included in the randomized trial. The assessments administered at baseline – questionnaires, including behavioral testing, blood draws, and measurements of body weight – will be repeated at randomization (week 0) and at week 24. The primary endpoint of phase 2 is change in body weight (i.e., % reduction in initial weight), as measured from randomization to week 24, among suboptimal early responders assigned to BT+P vs. BT+M. A randomized sample size of 50 non-responders (25 per group), assuming a 20% attrition rate, will give us 81.5% power to detect between-treatment group differences at week 24 of 4.5% (effect size: d = 0.82). Secondary endpoints of phase 2 will include change in body weight in kg from randomization to week 24, as well as the portion of suboptimal early responders who achieve a post-randomization loss of ≥ 5% and ≥ 10% of initial body weight. We will also examine differences between suboptimal early responders treated with BT+M vs. BT+P in changes in hunger, satiety, the reinforcing efficacy of food, and impulsivity between randomization and week 24. A comparison will also be made in percent weight loss from randomization to week 24 between suboptimal early responders treated with BT+M and early responders treated with BT alone. If you are interested in participating in this study, information and a link to contact the research team can be found here: https://clinicalresearch.itmat.upenn.edu/3XOX/ or you can call us at the numbers listed below.

Interventions

  • Behavioral: Behavioral Treatment
    • Behavioral treatment (BT) for weight loss includes diet and physical activity recommendations and behavior therapy strategies. All participants will complete an initial 4-week BT run-in, delivered in individual, 20-30 minute weekly sessions. After the end of the run-in, participants will be offered an additional 24 weeks of 20-30 minute individual BT sessions, occurring weekly for the first 12 weeks and every other week for the last 12 weeks (total of 18 visits).
  • Drug: Placebo
    • The study medication (placebo or phentermine 15.0 mg) is a once-daily self-administered pill.
  • Drug: Phentermine 15 MG
    • The study medication (placebo or phentermine 15.0 mg) is a once-daily self-administered pill.

Arms, Groups and Cohorts

  • Active Comparator: Behavioral Treatment + Placebo
    • All participants will complete an initial 4-week behavioral treatment (BT) run-in. Participants with suboptimal early weight loss in the BT run-in will then be randomly assigned to 24 additional weeks of: 1) BT plus placebo (BT+P); or 2) BT plus medication (BT+M; phentermine 15.0 mg) in a double-blinded fashion. Both treatment groups will continue to attend individual BT sessions and will take a once daily study medication (placebo or phentermine 15.0 mg) for the duration of the intervention period. Early BT responders identified during the run-in will receive the same 24-week BT program, but will not receive study medication or be included in the randomized trial.
  • Active Comparator: Behavioral Treatment + Medication
    • All participants will complete an initial 4-week behavioral treatment (BT) run-in. Participants with suboptimal early weight loss in the BT run-in will then be randomly assigned to 24 additional weeks of: 1) BT plus placebo (BT+P); or 2) BT plus medication (BT+M; phentermine 15.0 mg) in a double-blinded fashion. Both treatment groups will continue to attend individual BT sessions and will take a once daily study medication (placebo or phentermine 15.0 mg) for the duration of the intervention period. Early BT responders identified during the run-in will receive the same 24-week BT program, but will not receive study medication or be included in the randomized trial.

Clinical Trial Outcome Measures

Primary Measures

  • Phase 1: Percent weight loss
    • Time Frame: Week -4 (start of BT run-in) to week 0 (randomization)
    • Co-primary outcomes – phase 1
  • Phase 1: Number of participants who are categorized as early non-responders at randomization, based on percent weight loss
    • Time Frame: Week -4 (start of BT run-in) to week 0 (randomization)
    • Co-primary outcomes – phase 1
  • Phase 1: Baseline satiety, as measured by visual analogue scales (range 0-100 mm) during a test meal; satiety quotient = [(fasting rating before preload – 60 min post-preload rating)] / (energy content of preload) x 100.
    • Time Frame: Baseline (week -5)
    • Primary predictor variable – phase 1
  • Phase 1: Baseline postprandial change in GLP-1 during a test meal
    • Time Frame: Baseline
    • Primary predictor variable – phase 1
  • Phase 1: Baseline gastric emptying during a test meal (acetaminophen test)
    • Time Frame: Baseline
    • Primary predictor variable – phase 1
  • Phase 2: Percent weight loss
    • Time Frame: Week 0 (randomization) to week 24
    • Primary outcomes – phase 2

Secondary Measures

  • Phase 1: Baseline hunger, as measured by visual analogue scales (range 0-100 mm, higher = more hunger) during a test meal
    • Time Frame: Baseline
    • Secondary predictor variable – phase 1
  • Phase 1: Baseline relative reinforcing value of food (computer task), number of food reinforcer points earned
    • Time Frame: Baseline
    • Secondary predictor variable – phase 1
  • Phase 1: Baseline delay discounting (computer task), area under the curve representing the ratio of immediate reward size to time delay
    • Time Frame: Baseline
    • Secondary predictor variable – phase 1
  • Phase 1: Baseline implicit wanting of food, reaction time on Leeds Food Preference Questionnaire
    • Time Frame: Baseline
    • Secondary predictor variable – phase 1
  • Phase 1: Baseline fasting ghrelin
    • Time Frame: Baseline
    • Secondary predictor variable – phase 1
  • Phase 1: Baseline fasting leptin
    • Time Frame: Baseline
    • Secondary predictor variable – phase 1
  • Phase 1: Baseline postprandial change in insulin during a test meal
    • Time Frame: Baseline
    • Secondary predictor variable – phase 1
  • Phase 1: Baseline postprandial change in peptide YY during a test meal
    • Time Frame: Baseline
    • Secondary predictor variable – phase 1
  • Phase 2: Weight loss (kg)
    • Time Frame: Week 0 (randomization) to week 24
    • Secondary outcomes – phase 2
  • Phase 2: Number of participants with a weight loss of 5% or greater of randomization body weight at week 24
    • Time Frame: Week 0 (randomization) to week 24
    • Secondary outcomes – phase 2
  • Phase 2: Number of participants with a weight loss of 10% or greater of randomization body weight at week 24
    • Time Frame: Week 0 (randomization) to week 24
    • Secondary outcomes – phase 2
  • Phase 2: Change in satiety, as measured by visual analogue scales (range 0-100 mm) during a test meal; satiety quotient = [(fasting rating before preload – 60 min post-preload rating)] / (energy content of preload) x 100.
    • Time Frame: Week 0 (randomization) to week 24
    • Secondary outcomes – phase 2
  • Phase 2: Change in hunger, as measured by visual analogue scales (range 0-100 mm, higher=more hunger) during a test meal
    • Time Frame: Week 0 (randomization) to week 24
    • Secondary outcomes – phase 2
  • Phase 2: Change in relative reinforcing value of food (computer task), number of food reinforcer points earned
    • Time Frame: Week 0 (randomization) to week 24
    • Secondary outcomes – phase 2
  • Phase 2: Change in delay discounting (computer task), area under the curve representing the ratio of immediate reward size to time delay
    • Time Frame: Week 0 (randomization) to week 24
    • Secondary outcomes – phase 2

Participating in This Clinical Trial

Inclusion Criteria

1. BMI ≥ 31 kg/m² (or 28 kg/m2 with obesity-related comorbidity) 2. Age ≥ 21 years and ≤ 70 years 3. Eligible female patients will be:

  • non-pregnant, evidenced by a negative urine pregnancy test – non-lactating – surgically sterile or postmenopausal, or they will agree to continue to use an accepted method of birth control during the study. Acceptable methods of birth control are: hormonal contraceptives; double barrier method (condom with spermicide or diaphragm with spermicide); intrauterine device; surgical sterility; abstinence; and/or postmenopausal status (defined as at least 2 years without menses). 4. Subjects must: – have a primary care provider (PCP) who is responsible for providing routine care – understand and be willing to comply with all study-related procedures and agree to participate in the study by giving written informed consent – plan to remain in the Philadelphia area for the next 9 months or more Exclusion Criteria:

1. Pregnant or nursing, or plans to become pregnant in the next 9 months. 2. Uncontrolled hypertension (systolic blood pressure ≥ 140 mm Hg or diastolic blood pressure ≥ 90 mm Hg) 3. Type 1 diabetes 4. Type 2 diabetes 5. A fasting blood glucose > 126 mg/dL (on second assessment after first elevated value) 6. History of cardiovascular disease (e.g., coronary artery disease, stroke, arrhythmias, congestive heart failure, or heart block greater than first degree 7. Clinically significant hepatic or renal disease 8. Hyperthyroidism 9. Other thyroid disease, not controlled 10. History of malignancy (except for non-melanoma skin cancer) in past 5 years 11. Narrow angle glaucoma 12. Presence or history of marked agitation 13. Current severe major depressive episode (BDI-II score ≥ 29), current active suicidal ideation, or history of suicide attempts within the past 5 years. 14. Any severity of thought or bipolar disorder, or bulimia nervosa. 15. Psychiatric hospitalization within the past 6 months 16. Self-reported alcohol or substance abuse within the past 6 months, including at-risk drinking (current consumption of ≥ 14 alcoholic drinks per week) 17. Past year history of drug abuse 18. Use in the past 2 weeks of monoamine oxidase inhibitors 19. Current use of serotonin-norepinephrine reuptake inhibitors (SNRIs; e.g. venlafaxine, duloxetine, desvenlafaxine, milnacipran, levomilnacipran). 20. Use in past 6 months of medications known to induce significant weight loss (i.e., prescription weight loss medications) or weight gain (e.g., chronic use of oral steroids, second generation antipsychotics) 21. Loss of ≥ 5% of initial body weight within the past 6 months 22. History of (or plans for) bariatric surgery (e.g., roux en y gastric bypass, sleeve gastrectomy, gastric banding), endoscopic intragastric balloon, or aspire assist. 23. Inability to walk 5 blocks comfortably or engage in some other form of aerobic activity (e.g., swimming) 24. Known or suspected allergy to sympathomimetic amines or related products 25. The receipt of any investigational drug within 6 months prior to this trial 26. Previous participation in this trial (e.g., randomized and failed to participate) 27. Changes to any chronic medication (type or dosage) within the past 3 months. 28. Any serious or unstable medical or psychological condition that, in the opinion of the investigator, would compromise the patient's safety or successful participation in the study Other Therapy: Subjects will be expected to use medications (prescribed by their PCP) to control traditional cardiometabolic risk factors (e.g., hypertension, hypercholesterolemia, etc) and other co-morbid conditions, with the exception of medications listed above under "exclusions." In all cases, the subjects' PCP will be asked at the study's outset to keep medication does constant throughout the study, whenever possible. Subjects will be expected to have been on their medication regimen (including the dose) for 3 months prior to beginning the BT program. To be eligible to participate in the randomized phase of the trial, subjects must also: 1. Complete at least 3 out of 4 treatment sessions during the 4-week BT run-in and attend a randomization visit. Attending an in-person makeup session within one week of a missed visit will count as having attended the run-in visit. 2. Lose < 2.0% of initial weight during the 4-week BT run-in. Early BT responders who lose>=2% during the BT run-in will be offered the same 24-week BT program, but will not receive study medication or be included in the randomized trial.

Gender Eligibility: All

Minimum Age: 21 Years

Maximum Age: 70 Years

Are Healthy Volunteers Accepted: No

Investigator Details

  • Lead Sponsor
    • University of Pennsylvania
  • Collaborator
    • National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
  • Provider of Information About this Clinical Study
    • Sponsor
  • Overall Official(s)
    • Jena S Tronieri, PhD, Principal Investigator, Perelman School of Medicine at the University of Pennsylvania

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