A 12-WEEK TITRATE STUDY TO EVALUATE SAFETY, TOLERABILITY AND PHARMACODYNAMICS OF PF-06882961 IN ADULTS WITH TYPE 2 DIABETES MELLITUS AND IN NON-DIABETIC ADULTS WITH OBESITY

Phase 2

Completed

• Conditions: Diabetes; Obesity
• Interventions: Other: Placebo; Drug: PF-06882961

• Registration Number: NCT04617275
• Lead Sponsor: Pfizer

Brief Summary

This study will assess tolerability, safety, and pharmacodynamics (PD) of twice daily (BID) administration of PF- 06882961 in adult participants with Type 2 Diabetes Mellitus (T2DM) who are treated with metformin and in non-diabetic adults with obesity

Detailed Description

Not available

Study Timeline

• Study First Submitted: 2020-10-30
• Study First Submitted QC: 2020-10-30
• Study First Posted: 2020-11-05
• Study Start: 2021-01-06
• Primary Completion: 2021-11-17
• Study Completion: 2021-11-17
• Status Verified: 2022-11
• Results First Submitted: 2022-11-08
• Results First Submitted QC: 2022-11-08
• Last Update Submitted: 2022-11-08
• Results First Posted: 2022-12-08
• Last Update Posted: 2022-12-08

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 151

Inclusion Criteria

• Male or female participants between the ages of 18 and 75 years, inclusive, at Visit 1 (screening).

Exclusion Criteria

• Diagnosis of type 1 diabetes mellitus or secondary forms of diabetes.
• History of myocardial infarction, unstable angina, arterial revascularization, stroke, New York Heart Association Functional Class II IV heart failure, or transient ischemic attack within 6 months of screening (Visit 1).
• Participants with a known medical history of active liver disease (other than non alcoholic hepatic steatosis), including chronic active hepatitis B or C, or primary biliary cirrhosis.
• History of major depressive disorder or history of other severe psychiatric disorders (eg, schizophrenia or bipolar disorder) within the last 2 years.
• Any lifetime history of a suicide attempt.

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Arm 5 - Placebo in subjects with T2DM and Obesity	Placebo	Matching Placebo tablets taken twice a day (BID)
Arm 2-PF-06882961 starting dose of 10 mg BID titrated to 100 mg in participants with T2DM	PF-06882961	The dose will be titrated over 12 weeks, starting with a dose of 10 mg BID to reach the target dose of 120 mg BID. Titration steps include: 10 mg BID, 20 mg BID, 40 mg BID, 60 mg BID, 80 mg BID, 100 mg BID and 120 mg BID
Arm 3-PF-06882961 starting dose of 5 mg BID titrated to 80 mg in participants with T2DM	PF-06882961	The dose will be titrated over 12 weeks, starting with a dose of 5 mg BID to reach the target dose of 80 mg BID. Titration steps include: 5 mg BID, 10 mg BID, 20 mg BID, 40 mg BID, 60 mg BID and 80 mg BID
Arm 6-PF-06882961 starting dose of 10 mg BID titrated to 200 mg in participants with T2DM	PF-06882961	The dose will be titrated over 12 weeks, starting with a dose of 10 mg BID to reach the target dose of 200 mg BID. Titration steps include: 10 mg BID, 20 mg BID, 40 mg BID, 60 mg BID, 80 mg BID, 100 mg BID and 120 mg BID,140 mg BID, 160 mg BID, 180 MG BID, 200 mg BID
Arm 1-PF-06882961 starting dose of 5 milligram (mg) BID titrated to 120 mg in participants with T2DM	PF-06882961	The dose will be titrated over 12 weeks, starting with a dose of 5 mg BID to reach the target dose of 120 mg BID. Titration steps include: 5 mg BID, 10 mg BID, 20 mg BID, 40 mg BID, 60 mg BID, 80 mg BID, 100 mg BID and 120 mg BID
Arm 4-PF-06882961 starting dose of 10 mg BID titrated to 80 mg in participants with T2DM	PF-06882961	The dose will be titrated over 12 weeks, starting with a dose of 10 mg BID to reach the target dose of 80 mg BID. Titration steps include: 10 mg BID, 20 mg BID, 40 mg BID, 60 mg BID and 80 mg BID
Arm 7-PF-06882961 starting dose of 10 mg BID titrated to 200 mg in participants with Obesity	PF-06882961	The dose will be titrated over 12 weeks, starting with a dose of 10 mg BID to reach the target dose of 200 mg BID. Titration steps include: 10 mg BID, 20 mg BID, 40 mg BID, 60 mg BID, 80 mg BID, 100 mg BID and 120 mg BID,140 mg BID, 160 mg BID, 180 MG BID, 200 mg BID

Primary Outcome Measures

Name	Time	Method
Number of Participants With Treatment Emergent Adverse Events (AEs) by Severity	Baseline through follow-up (Day 112)	An AE was any untoward medical occurrence in a patient or clinical study participant, temporally associated with the use of study treatment, whether or not considered related to the study treatment. TEAEs were events between first dose of study drug and up to follow-up visit that were absent before treatment or that worsened after treatment. AEs presented below were TEAEs. The investigator was required to use clinical judgment to assess the potential relationship between investigational product and each AE, to define an treatment-related AE. Assessments of AE intensity were defined as mild (easily tolerated, causing minimal discomfort and not interfering with daily activities), moderate (causing sufficient discomfort and interferes with normal daily activities) and severe (preventing normal daily activities).

Secondary Outcome Measures

Name	Time	Method
Number of Participants With Vital Signs Meeting the Pre-defined Categorical Summarization Criteria	Baseline through Visit 10 (Day 91)	Vital signs abnormality criteria: 1) supine systolic blood pressure (SBP) \<90 millimeters of mercury (mmHg); 2) supine diastolic blood pressure (DBP) \<50 mmHg; 3) supine pulse rate \<40 or \>120 beats per minute (bpm); 4) change from baseline (increase or decrease) in supine SBP \>=30 mmHg; 5) change from baseline (increase or decrease) in supine DBP \>=20 mmHg.
Number of Participants With Laboratory Abnormalities (Without Regard to Baseline Abnormality)	Baseline through Visit 10 (Day 91)	Safety laboratory assessments included clinical chemistry, hematology, urinalysis, and other tests. Abnormality was determined at the investigator's discretion.
CFB in Fasting Plasma Glucose at Week 6	Baseline, Week 6	Baseline was defined as the result closest prior to dosing at Day1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points.
CFB in Glycolated HbA1c at Week 10	Baseline, Week 10	Baseline was defined as the result closest prior to dosing at Day1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points.
Change From Baseline (CFB) in Fasting Plasma Glucose at Week 2	Baseline, Week 2	Baseline was defined as the result closest prior to dosing at Day1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points.
CFB in Glycolated HbA1c at Week 4	Baseline, Week 4	Baseline was defined as the result closest prior to dosing at Day1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points.
Number of Participants With Categorical Scores on the Columbia Suicide Severity Rating Scale (C-SSRS)	Week 0, 2, 4, 6, 8, 10, 12, 13-14	The C-SSRS is an interview-based rating scale to systematically assess suicidal ideation and suicidal behavior. Participants who responded "yes" to the questions will be counted. Data relevant to the assessment of suicidality were mapped to the Columbia-Classification Algorithm of Suicide Assessment (C-CASA) codes.
CFB in Fasting Plasma Glucose at Week 4	Baseline, Week 4	Baseline was defined as the result closest prior to dosing at Day1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points.
Number of Participants With Electrocardiogram (ECG) Data Meeting the Pre-defined Categorical Summarization Criteria	Baseline through Visit 10 (Day 91)	ECG assessments included pulse rate (PR), QT, heart rate, QTcF intervals and QRS complex. ECG abnormalities criteria included: PR interval value \>= 300 msec, or baseline (BL) \>200 msec and \>=25% increase from BL, or BL \<=200 msec and \>=50% increase from BL; QRS interval value \>= 140msec, or \>=50% increase from BL; QTcF value \>450 and \<=480 msec, or \>480 and \<=500 msec, or \>500 msec, or increase from BL\>30 and \<=60 msec, or \>60msec.
CFB in Fasting Plasma Glucose at Week 10	Baseline, Week 10	Baseline was defined as the result closest prior to dosing at Day1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points.
CFB in Glycolated HbA1c at Week 8	Baseline, Week 8	Baseline was defined as the result closest prior to dosing at Day1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points.
CFB in Body Weight at Week 4 (Participants With T2DM)	Baseline, Week 4	Baseline was defined as the average of a duplicate measurement closest prior to dosing at Day 1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points. Average of the duplicate measurements (where applicable) was used in analyses.
CFB in Body Weight at Week 6 (Participants With T2DM)	Baseline, Week 6	Baseline was defined as the average of a duplicate measurement closest prior to dosing at Day 1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points. Average of the duplicate measurements (where applicable) was used in analyses.
Number of Participants With Response to Patient Health Questionnaire-9 (PHQ-9)	Week 0, 2, 4, 6, 8, 10, 12, 13-14.	The PHQ-9 is a 9 item self-report scale for the assessment of depressive symptoms. The PHQ-9 were completed by participants and reviewed by site staff at the pre-defined time points.
CFB in Fasting Plasma Glucose at Week 8	Baseline, Week 8	Baseline was defined as the result closest prior to dosing at Day1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points.
CFB in Fasting Plasma Glucose at Week 12	Baseline, Week 12	Baseline was defined as the result closest prior to dosing at Day1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points.
CFB in Glycolated Hemoglobin A1c (HbA1c) at Week 2	Baseline, Week 2	Baseline was defined as the result closest prior to dosing at Day1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points.
CFB in Glycolated HbA1c at Week 12	Baseline, Week 12	Baseline was defined as the result closest prior to dosing at Day1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points.
CFB in Body Weight at Week 2 (Participants With T2DM)	Baseline, Week 2	Baseline was defined as the average of a duplicate measurement closest prior to dosing at Day 1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points. Average of the duplicate measurements (where applicable) was used in analyses.
CFB in Body Weight at Week 10 (Non-diabetic Participants With Obesity)	Baseline, Week 10	Body weight were measured in duplicate as indicated. The second weight measurement were obtained at least 1-2 minutes apart from the first weight measurement. Weight were recorded using a calibrated scale (with the same scale used if possible for the duration of the study) reporting weight in kilograms (kg), and accuracy to the nearest 0.1 kg; ie, the device distinguished a difference between 68.4 kg vs 68.3 kg. The scale was placed on a stable, flat surface. Weight measurement was taken under the following conditions: participant is in a fasted state; after void of urine; after removal of shoes, bulky layers of clothing and jackets so that only light clothing remained; while remaining was during the measurement.
CFB in Glycolated HbA1c at Week 6	Baseline, Week 6	Baseline was defined as the result closest prior to dosing at Day1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points.
CFB in Body Weight at Week 8 (Participants With T2DM)	Baseline, Week 8	Baseline was defined as the average of a duplicate measurement closest prior to dosing at Day 1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points. Average of the duplicate measurements (where applicable) was used in analyses.
CFB in Body Weight at Week 6 (Non-diabetic Participants With Obesity)	Baseline, Week 6	Body weight were measured in duplicate as indicated. The second weight measurement were obtained at least 1-2 minutes apart from the first weight measurement. Weight were recorded using a calibrated scale (with the same scale used if possible for the duration of the study) reporting weight in kilograms (kg), and accuracy to the nearest 0.1 kg; ie, the device distinguished a difference between 68.4 kg vs 68.3 kg. The scale was placed on a stable, flat surface. Weight measurement was taken under the following conditions: participant is in a fasted state; after void of urine; after removal of shoes, bulky layers of clothing and jackets so that only light clothing remained; while remaining was during the measurement.
CFB in Body Weight at Week 8 (Non-diabetic Participants With Obesity)	Baseline, Week 8	Body weight were measured in duplicate as indicated. The second weight measurement were obtained at least 1-2 minutes apart from the first weight measurement. Weight were recorded using a calibrated scale (with the same scale used if possible for the duration of the study) reporting weight in kilograms (kg), and accuracy to the nearest 0.1 kg; ie, the device distinguished a difference between 68.4 kg vs 68.3 kg. The scale was placed on a stable, flat surface. Weight measurement was taken under the following conditions: participant is in a fasted state; after void of urine; after removal of shoes, bulky layers of clothing and jackets so that only light clothing remained; while remaining was during the measurement.
CFB in Body Weight at Week 12 (Non-diabetic Participants With Obesity)	Baseline, Week 12	Body weight were measured in duplicate as indicated. The second weight measurement were obtained at least 1-2 minutes apart from the first weight measurement. Weight were recorded using a calibrated scale (with the same scale used if possible for the duration of the study) reporting weight in kilograms (kg), and accuracy to the nearest 0.1 kg; ie, the device distinguished a difference between 68.4 kg vs 68.3 kg. The scale was placed on a stable, flat surface. Weight measurement was taken under the following conditions: participant is in a fasted state; after void of urine; after removal of shoes, bulky layers of clothing and jackets so that only light clothing remained; while remaining was during the measurement.
CFB in Body Weight at Week 10 (Participants With T2DM)	Baseline, Week 10	Baseline was defined as the average of a duplicate measurement closest prior to dosing at Day 1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points. Average of the duplicate measurements (where applicable) was used in analyses.
CFB in Body Weight at Week 2 (Non-diabetic Participants With Obesity)	Baseline, Week 2	Body weight were measured in duplicate as indicated. The second weight measurement were obtained at least 1-2 minutes apart from the first weight measurement. Weight were recorded using a calibrated scale (with the same scale used if possible for the duration of the study) reporting weight in kilograms (kg), and accuracy to the nearest 0.1 kg; ie, the device distinguished a difference between 68.4 kg vs 68.3 kg. The scale was placed on a stable, flat surface. Weight measurement was taken under the following conditions: participant is in a fasted state; after void of urine; after removal of shoes, bulky layers of clothing and jackets so that only light clothing remained; while remaining was during the measurement.
CFB in Body Weight at Week 4 (Non-diabetic Participants With Obesity)	Baseline, Week 4	Body weight were measured in duplicate as indicated. The second weight measurement were obtained at least 1-2 minutes apart from the first weight measurement. Weight were recorded using a calibrated scale (with the same scale used if possible for the duration of the study) reporting weight in kilograms (kg), and accuracy to the nearest 0.1 kg; ie, the device distinguished a difference between 68.4 kg vs 68.3 kg. The scale was placed on a stable, flat surface. Weight measurement was taken under the following conditions: participant is in a fasted state; after void of urine; after removal of shoes, bulky layers of clothing and jackets so that only light clothing remained; while remaining was during the measurement.
CFB in Body Weight at Week 12 (Participants With T2DM)	Baseline, Week 12	Baseline was defined as the average of a duplicate measurement closest prior to dosing at Day 1. The MMRM model included treatment, time, strata (male versus female) and treatment-by-time interaction as fixed effects, baseline as a covariate and the baseline-by-time interaction with time fitted as a repeated effect and participant as a random effect. An unstructured covariance matrix was used to estimate the variances and covariance within participant across time points. Average of the duplicate measurements (where applicable) was used in analyses.

Trial Locations

Locations (37)

Emerson Clinical Research Institute; 🇺🇸 Washington, District of Columbia, United States

Clinical Neuroscience Solutions, Inc.; 🇺🇸 Memphis, Tennessee, United States

Solaris Clinical Research; 🇺🇸 Meridian, Idaho, United States

Wade Family Medicine; 🇺🇸 Bountiful, Utah, United States

Bountiful Internal Medicine; 🇺🇸 Bountiful, Utah, United States

PMG Research of Charlotte, LLC; 🇺🇸 Charlotte, North Carolina, United States

PMG Research of Rocky Mount, LLC - Investigational Product and Mail delivery; 🇺🇸 Rocky Mount, North Carolina, United States

Arizona Research Center; 🇺🇸 Phoenix, Arizona, United States

California Research Foundation; 🇺🇸 San Diego, California, United States

University Clinical Investigators, Inc.; 🇺🇸 Tustin, California, United States

Innovative Research of West Florida, Inc.; 🇺🇸 Clearwater, Florida, United States

Acevedo Clinical Research Associates; 🇺🇸 Miami, Florida, United States

Pines Care Research Center, LLC; 🇺🇸 Pembroke Pines, Florida, United States

Clinical Research Professionals; 🇺🇸 Chesterfield, Missouri, United States

PMG Research of Raleigh, LLC d/b/a PMG Research of Cary; 🇺🇸 Cary, North Carolina, United States

Sterling Research Group, Ltd.; 🇺🇸 Cincinnati, Ohio, United States

Dallas Diabetes Research Center; 🇺🇸 Dallas, Texas, United States

Juno Research, LLC; 🇺🇸 Houston, Texas, United States

Unity Health - Searcy Medical Center; 🇺🇸 Searcy, Arkansas, United States

Desert Oasis Healthcare Medical Group; 🇺🇸 Palm Springs, California, United States

Catalina Research Institute, LLC; 🇺🇸 Montclair, California, United States

Rancho Cucamonga Clinical Research; 🇺🇸 Rancho Cucamonga, California, United States

Diablo Clinical Research, Inc.; 🇺🇸 Walnut Creek, California, United States

Meridian Clinical Research, LLC; 🇺🇸 Sioux City, Iowa, United States

Nola Care LLC; 🇺🇸 Metairie, Louisiana, United States

Research Integrity, LLC; 🇺🇸 Owensboro, Kentucky, United States

Meridian Clinical Research, LLC DBA Regional Clinical Research; 🇺🇸 Endwell, New York, United States

PMG Research of Hickory, LLC; 🇺🇸 Hickory, North Carolina, United States

PMG Research of Winston-Salem, LLC; 🇺🇸 Winston-Salem, North Carolina, United States

PMG Research of Rocky Mount, LLC - Patient Visits; 🇺🇸 Rocky Mount, North Carolina, United States

Carolina Research Center, Inc.; 🇺🇸 Shelby, North Carolina, United States

Palmetto Primary Care Physicians (physicals only); 🇺🇸 Summerville, South Carolina, United States

Heritage Valley Medical Group, Inc.; 🇺🇸 Beaver, Pennsylvania, United States

Consano Clinical Research, LLC; 🇺🇸 Shavano Park, Texas, United States

Manassas Clinical Research Center; 🇺🇸 Manassas, Virginia, United States

Palmetto Clinical Research; 🇺🇸 Summerville, South Carolina, United States

Progressive Clinical Research; 🇺🇸 Bountiful, Utah, United States