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Efficacy and Safety of Gemcabene in Patients With Homozygous Familial Hypercholesterolemia on Stable, Lipid-Lowering Therapy (COBALT-1)

Primary Purpose

Hypercholesteremia

Status
Completed
Phase
Phase 2
Locations
International
Study Type
Interventional
Intervention
Gemcabene
Sponsored by
NeuroBo Pharmaceuticals Inc.
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional treatment trial for Hypercholesteremia focused on measuring LDL-C, Lipid Regulator

Eligibility Criteria

17 Years - undefined (Child, Adult, Older Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

  • Provision of written and signed informed consent (by patient or legal guardian) prior to any study-specific procedure;
  • Male or female ≥17 years of age at time of consent;
  • Diagnosis of HoFH by genetic confirmation (including compound heterozygosity) or a clinical diagnosis based on either (1) a history of an untreated LDL-C concentration >500 mg/dL (12.92 mmol/L) together with either appearance of xanthoma before 10 years of age, or evidence of heterozygous familial hypercholesterolemia in both parents or, if history is unavailable, (2) LDL-C >300 mg/dL (7.76 mmol/L) on maximally tolerated lipid-lowering drug therapy;
  • Currently on a stable, low-fat, low-cholesterol diet in combination with a pre-existing, regulatory-approved, not excluded lipid-lowering therapy (i.e., statins, monoclonal antibodies to PCSK9, cholesterol absorption inhibitors, bile acid sequestrants, or nicotinic acid, or any combination thereof) at a stable dose for at least 4 weeks prior to the Screening Visit;
  • Fasting LDL-C value >130 mg/dL (3.36 mmol/L) at the Screening Visit;
  • Physical examination, including vital signs, that is within normal limits or clinically acceptable to the Investigator;
  • Weight ≥50 kg;
  • Female patients must not be pregnant or lactating. Women of child-bearing potential must have a negative serum pregnancy test at the Screening Visit and negative urine dipstick on Day 1 prior to dosing in order to qualify for the study. Women who are surgically sterile or are clinically confirmed to be post-menopausal (i.e., documented amenorrhea for ≥1 year in the absence of other biological or physiological causes) are not considered to be of child-bearing potential; and
  • Women of child-bearing potential must agree to use acceptable methods of contraception throughout the duration of the study and for 30 days after the last dose of study drug. For this study, double-barrier contraception is required.

Exclusion Criteria:

  • Other forms of primary hyperlipoproteinemia and secondary causes of hypercholesterolemia (e.g., nephrotic syndrome or hypothyroidism);
  • Abnormal liver function test at the Screening Visit (aspartate aminotransferase or alanine aminotransferase >2 × the upper limit of normal [ULN]; total bilirubin >1.5 × ULN; or alkaline phosphatase >2 × ULN based on appropriate age and gender normal values). Patients with bilirubin >1.5 × ULN and history of Gilbert's syndrome may be included; reflexive direct bilirubin testing will be used to confirm Gilbert's syndrome;
  • Moderate (Grade B) or severe (Grade C) chronic hepatic impairment according to the Child Pugh classification;
  • Active liver disease (e.g., cirrhosis, alcoholic liver disease, hepatitis B virus [HBV], hepatitis C virus [HCV], autoimmune hepatitis, liver failure, liver cancer), history of liver transplant, or known diagnosis of human immunodeficiency virus (HIV);
  • Triglycerides value >400 mg/dL (4.52 mmol/L) at the Screening Visit;
  • Moderate to severe renal insufficiency defined as an estimated GFR <30 mL/min/1.73m2 (calculated using The Chronic Kidney Disease Epidemiology Collaboration equation) at the Screening Visit;
  • Abnormal urinalysis (proteinuria greater than trace or any male or non-menstruating female with greater than trace hematuria), confirmed by reflexive urine protein:creatinine ratio testing;
  • Uncontrolled thyroid disease: hyperthyroidism or hypothyroidism as defined by thyroid stimulating hormone (TSH) below the lower limit of normal or >1.5 × ULN, respectively, at the Screening Visit. If controlled, treatment should be stable for at least 3 months prior to the Screening Visit;
  • Type 1 diabetes mellitus or uncontrolled type 2 diabetes mellitus (hemoglobin A1c [HbA1c] value >8%), or any diabetic patient taking insulin and/or thiazolidinediones;
  • New York Heart Association Class III or IV heart failure;
  • Myocardial infarction, severe or unstable angina pectoris, coronary angioplasty, coronary artery bypass graft, or other major cardiovascular events resulting in hospitalization within 3 months of the Screening Visit. Patients with adequately treated stable angina, per Investigator assessment, may be included;
  • Uncontrolled cardiac arrhythmia or prolonged QT on the Screening Visit or Day 1 prior to dosing ECG (QTcF >450 msec for men and >470 msec for women) or known family history of prolonged QT or unexplained sudden cardiac death;
  • Uncontrolled hypertension, defined as sitting systolic blood pressure >180 mmHg or diastolic blood pressure >110 mmHg, and confirmed by repeat measurement;
  • Currently receiving cancer treatments or, in the Investigator's opinion, at risk of relapse for recent cancer;
  • Use of fibrate lipid-lowering agent 6 weeks prior to the Screening Visit;
  • Hypersensitivity to or a history of significant adverse reactions to any fibrate lipid lowering agent;
  • Use of apheresis (LDL or plasma) 8 weeks prior to the Screening Visit;
  • Use of lomitapide 2 months prior to the Screening Visit;
  • Use of mipomersen 5 months prior to the Screening Visit;
  • Use of any excluded medications or supplements (e.g., potent cytochrome P450 [CYP] 3A4 inhibitors);
  • History of drug or alcohol abuse within the past year or inability to comply with protocol requirements, including subject restrictions;
  • Previously treated with gemcabene;
  • Participation in another clinical study of an investigational agent or device concurrently or within 1 month prior to the Screening Visit, or use of an investigational agent within 1 month or 5 half-lives (if known), whichever is longer, prior to the Screening Visit; or
  • Any other finding which, in the opinion of the Investigator, would compromise the patient's safety or participation in the study.

Sites / Locations

  • Westside Medical Associates of Los Angeles
  • Robarts Research Institute
  • Ecogene-21
  • Montreal Heart Institute
  • Wolfson Medical Center Internal Medicine Dept.
  • Center for Research, Prevention and Treatment of Atherosclerosis - Cardiology Department of Medicine Kiryat Hadassah
  • Ziv Medical Center Internal Medicine Department

Arms of the Study

Arm 1

Arm Type

Experimental

Arm Label

Gemcabene

Arm Description

Participants with homozygous familial hypercholesterolemia (HoFH) on stable lipid lowering therapy received 300 milligram (mg) of Gemcabene, orally once daily from day 1 to 28 followed by 600 mg of Gemcabene, orally once daily from day 29 to 56 followed by 900 mg of Gemcabene, orally once daily from day 57 to 84. Participants were followed until Day 112.

Outcomes

Primary Outcome Measures

Percent Change From Baseline in LDL-C at Day 28
Percent Change From Baseline in LDL-C at Day 56
Percent Change From Baseline in LDL-C at Day 84

Secondary Outcome Measures

Change From Baseline in Fasting LDL-C
Percent Change From Baseline in Fasting Non-HDL-C
Change From Baseline in Fasting Non-HDL-C
Percent Change From Baseline in Fasting Total Cholesterol (TC)
Change From Baseline in Fasting Total Cholesterol (TC)
Percent Change From Baseline in Fasting Triglycerides (TG)
Change From Baseline in Fasting Triglycerides (TG)
Percent Change From Baseline in Fasting HDL-C
Change From Baseline in Fasting HDL-C
Percent Change From Baseline in Fasting VLDL-C
Change From Baseline in Fasting VLDL-C
Percent Change From Baseline in Fasting LDL-C as Per Receptor Mutation Status
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Change From Baseline in Fasting LDL-C as Per Receptor Mutation Status
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Percent Change From Baseline in Fasting Non-HDL-C as Per Receptor Mutation Status
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Change From Baseline in Fasting Non-HDL-C as Per Receptor Mutation Status
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Percent Change From Baseline in Fasting VLDL-C as Per Receptor Mutation Status
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Change From Baseline in Fasting VLDL-C as Per Receptor Mutation Status
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Percent Change From Baseline in Fasting HDL-C as Per Receptor Mutation Status
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Change From Baseline in Fasting HDL-C as Per Receptor Mutation Status
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Percent Change From Baseline in Fasting TC as Per Receptor Mutation Status
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Change From Baseline in Fasting TC as Per Receptor Mutation Status
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Percent Change From Baseline in Fasting TG as Per Receptor Mutation Status
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Change From Baseline in Fasting TG as Per Receptor Mutation Status
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Number of Participants Achieving LDL-C Reduction of ≥15%
Number of Participants Achieving LDL-C Reduction of ≥20%
Number of Participants Achieving LDL-C Reduction of ≥25%
Number of Participants Achieving LDL-C Reduction of ≥30%
Number of Participants Achieving an LDL-C Value <100 mg/dL (2.59 mmol/L)
Percent Change From Baseline in High-sensitivity C-reactive Protein (hsCRP)
Change From Baseline in High-sensitivity C-reactive Protein (hsCRP)
Percent Change From Baseline in Fibrinogen
Change From Baseline in Fibrinogen
Percent Change From Baseline in Fasting Lipoprotein(a)
Change From Baseline in Fasting Lipoprotein(a)
Percent Change From Baseline in Fasting Apolipoprotein B
Change From Baseline in Fasting Apolipoprotein B
Percent Change From Baseline in Fasting Apolipoprotein A-I
Change From Baseline in Fasting Apolipoprotein A-I
Percent Change From Baseline in Fasting Apolipoprotein A-II
Change From Baseline in Fasting Apolipoprotein A-II
Percent Change From Baseline in Fasting Apolipoprotein C-II
Change From Baseline in Fasting Apolipoprotein C-II
Percent Change From Baseline in Fasting Apolipoprotein C-III
Change From Baseline in Fasting Apolipoprotein C-III
Percent Change From Baseline in Fasting Apolipoprotein E
Change From Baseline in Fasting Apolipoprotein E

Full Information

First Posted
March 12, 2016
Last Updated
June 3, 2020
Sponsor
NeuroBo Pharmaceuticals Inc.
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1. Study Identification

Unique Protocol Identification Number
NCT02722408
Brief Title
Efficacy and Safety of Gemcabene in Patients With Homozygous Familial Hypercholesterolemia on Stable, Lipid-Lowering Therapy (COBALT-1)
Official Title
A Phase 2 Open-Label, Dose-Finding Study to Assess the Efficacy, Safety, and Tolerability of Gemcabene in Patients With Homozygous Familial Hypercholesterolemia on Stable, Lipid Lowering Therapy (COBALT-1)
Study Type
Interventional

2. Study Status

Record Verification Date
June 2020
Overall Recruitment Status
Completed
Study Start Date
June 2016 (Actual)
Primary Completion Date
April 2017 (Actual)
Study Completion Date
July 2017 (Actual)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Sponsor
Name of the Sponsor
NeuroBo Pharmaceuticals Inc.

4. Oversight

Data Monitoring Committee
No

5. Study Description

Brief Summary
The purpose of this study was to assess the efficacy, safety, and tolerability of multiple doses of Gemcabene in patients with HoFH on stable, lipid-lowering therapy.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Hypercholesteremia
Keywords
LDL-C, Lipid Regulator

7. Study Design

Primary Purpose
Treatment
Study Phase
Phase 2
Interventional Study Model
Single Group Assignment
Masking
None (Open Label)
Allocation
N/A
Enrollment
8 (Actual)

8. Arms, Groups, and Interventions

Arm Title
Gemcabene
Arm Type
Experimental
Arm Description
Participants with homozygous familial hypercholesterolemia (HoFH) on stable lipid lowering therapy received 300 milligram (mg) of Gemcabene, orally once daily from day 1 to 28 followed by 600 mg of Gemcabene, orally once daily from day 29 to 56 followed by 900 mg of Gemcabene, orally once daily from day 57 to 84. Participants were followed until Day 112.
Intervention Type
Drug
Intervention Name(s)
Gemcabene
Intervention Description
300 mg tablet orally once daily for four weeks followed by 600 mg tablet orally once daily for four weeks followed by 900 mg tablet orally once daily for four weeks.
Primary Outcome Measure Information:
Title
Percent Change From Baseline in LDL-C at Day 28
Time Frame
Baseline, day 28
Title
Percent Change From Baseline in LDL-C at Day 56
Time Frame
Baseline, day 56
Title
Percent Change From Baseline in LDL-C at Day 84
Time Frame
Baseline, day 84
Secondary Outcome Measure Information:
Title
Change From Baseline in Fasting LDL-C
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting Non-HDL-C
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting Non-HDL-C
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting Total Cholesterol (TC)
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting Total Cholesterol (TC)
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting Triglycerides (TG)
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting Triglycerides (TG)
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting HDL-C
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting HDL-C
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting VLDL-C
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting VLDL-C
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting LDL-C as Per Receptor Mutation Status
Description
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting LDL-C as Per Receptor Mutation Status
Description
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting Non-HDL-C as Per Receptor Mutation Status
Description
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting Non-HDL-C as Per Receptor Mutation Status
Description
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting VLDL-C as Per Receptor Mutation Status
Description
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting VLDL-C as Per Receptor Mutation Status
Description
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting HDL-C as Per Receptor Mutation Status
Description
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting HDL-C as Per Receptor Mutation Status
Description
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting TC as Per Receptor Mutation Status
Description
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting TC as Per Receptor Mutation Status
Description
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting TG as Per Receptor Mutation Status
Description
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting TG as Per Receptor Mutation Status
Description
Receptor mutation status was categorized as LDLr status and EAS clinical diagnosis of HoFH which was reported in this outcome measure.
Time Frame
Baseline, days 28, 56 and 84
Title
Number of Participants Achieving LDL-C Reduction of ≥15%
Time Frame
Days 28, 56 and 84
Title
Number of Participants Achieving LDL-C Reduction of ≥20%
Time Frame
Days 28, 56 and 84
Title
Number of Participants Achieving LDL-C Reduction of ≥25%
Time Frame
Days 28, 56 and 84
Title
Number of Participants Achieving LDL-C Reduction of ≥30%
Time Frame
Days 28, 56 and 84
Title
Number of Participants Achieving an LDL-C Value <100 mg/dL (2.59 mmol/L)
Time Frame
Days 28, 56 and 84
Title
Percent Change From Baseline in High-sensitivity C-reactive Protein (hsCRP)
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in High-sensitivity C-reactive Protein (hsCRP)
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fibrinogen
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fibrinogen
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting Lipoprotein(a)
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting Lipoprotein(a)
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting Apolipoprotein B
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting Apolipoprotein B
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting Apolipoprotein A-I
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting Apolipoprotein A-I
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting Apolipoprotein A-II
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting Apolipoprotein A-II
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting Apolipoprotein C-II
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting Apolipoprotein C-II
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting Apolipoprotein C-III
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting Apolipoprotein C-III
Time Frame
Baseline, days 28, 56 and 84
Title
Percent Change From Baseline in Fasting Apolipoprotein E
Time Frame
Baseline, days 28, 56 and 84
Title
Change From Baseline in Fasting Apolipoprotein E
Time Frame
Baseline, days 28, 56 and 84

10. Eligibility

Sex
All
Minimum Age & Unit of Time
17 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria: Provision of written and signed informed consent (by patient or legal guardian) prior to any study-specific procedure; Male or female ≥17 years of age at time of consent; Diagnosis of HoFH by genetic confirmation (including compound heterozygosity) or a clinical diagnosis based on either (1) a history of an untreated LDL-C concentration >500 mg/dL (12.92 mmol/L) together with either appearance of xanthoma before 10 years of age, or evidence of heterozygous familial hypercholesterolemia in both parents or, if history is unavailable, (2) LDL-C >300 mg/dL (7.76 mmol/L) on maximally tolerated lipid-lowering drug therapy; Currently on a stable, low-fat, low-cholesterol diet in combination with a pre-existing, regulatory-approved, not excluded lipid-lowering therapy (i.e., statins, monoclonal antibodies to PCSK9, cholesterol absorption inhibitors, bile acid sequestrants, or nicotinic acid, or any combination thereof) at a stable dose for at least 4 weeks prior to the Screening Visit; Fasting LDL-C value >130 mg/dL (3.36 mmol/L) at the Screening Visit; Physical examination, including vital signs, that is within normal limits or clinically acceptable to the Investigator; Weight ≥50 kg; Female patients must not be pregnant or lactating. Women of child-bearing potential must have a negative serum pregnancy test at the Screening Visit and negative urine dipstick on Day 1 prior to dosing in order to qualify for the study. Women who are surgically sterile or are clinically confirmed to be post-menopausal (i.e., documented amenorrhea for ≥1 year in the absence of other biological or physiological causes) are not considered to be of child-bearing potential; and Women of child-bearing potential must agree to use acceptable methods of contraception throughout the duration of the study and for 30 days after the last dose of study drug. For this study, double-barrier contraception is required. Exclusion Criteria: Other forms of primary hyperlipoproteinemia and secondary causes of hypercholesterolemia (e.g., nephrotic syndrome or hypothyroidism); Abnormal liver function test at the Screening Visit (aspartate aminotransferase or alanine aminotransferase >2 × the upper limit of normal [ULN]; total bilirubin >1.5 × ULN; or alkaline phosphatase >2 × ULN based on appropriate age and gender normal values). Patients with bilirubin >1.5 × ULN and history of Gilbert's syndrome may be included; reflexive direct bilirubin testing will be used to confirm Gilbert's syndrome; Moderate (Grade B) or severe (Grade C) chronic hepatic impairment according to the Child Pugh classification; Active liver disease (e.g., cirrhosis, alcoholic liver disease, hepatitis B virus [HBV], hepatitis C virus [HCV], autoimmune hepatitis, liver failure, liver cancer), history of liver transplant, or known diagnosis of human immunodeficiency virus (HIV); Triglycerides value >400 mg/dL (4.52 mmol/L) at the Screening Visit; Moderate to severe renal insufficiency defined as an estimated GFR <30 mL/min/1.73m2 (calculated using The Chronic Kidney Disease Epidemiology Collaboration equation) at the Screening Visit; Abnormal urinalysis (proteinuria greater than trace or any male or non-menstruating female with greater than trace hematuria), confirmed by reflexive urine protein:creatinine ratio testing; Uncontrolled thyroid disease: hyperthyroidism or hypothyroidism as defined by thyroid stimulating hormone (TSH) below the lower limit of normal or >1.5 × ULN, respectively, at the Screening Visit. If controlled, treatment should be stable for at least 3 months prior to the Screening Visit; Type 1 diabetes mellitus or uncontrolled type 2 diabetes mellitus (hemoglobin A1c [HbA1c] value >8%), or any diabetic patient taking insulin and/or thiazolidinediones; New York Heart Association Class III or IV heart failure; Myocardial infarction, severe or unstable angina pectoris, coronary angioplasty, coronary artery bypass graft, or other major cardiovascular events resulting in hospitalization within 3 months of the Screening Visit. Patients with adequately treated stable angina, per Investigator assessment, may be included; Uncontrolled cardiac arrhythmia or prolonged QT on the Screening Visit or Day 1 prior to dosing ECG (QTcF >450 msec for men and >470 msec for women) or known family history of prolonged QT or unexplained sudden cardiac death; Uncontrolled hypertension, defined as sitting systolic blood pressure >180 mmHg or diastolic blood pressure >110 mmHg, and confirmed by repeat measurement; Currently receiving cancer treatments or, in the Investigator's opinion, at risk of relapse for recent cancer; Use of fibrate lipid-lowering agent 6 weeks prior to the Screening Visit; Hypersensitivity to or a history of significant adverse reactions to any fibrate lipid lowering agent; Use of apheresis (LDL or plasma) 8 weeks prior to the Screening Visit; Use of lomitapide 2 months prior to the Screening Visit; Use of mipomersen 5 months prior to the Screening Visit; Use of any excluded medications or supplements (e.g., potent cytochrome P450 [CYP] 3A4 inhibitors); History of drug or alcohol abuse within the past year or inability to comply with protocol requirements, including subject restrictions; Previously treated with gemcabene; Participation in another clinical study of an investigational agent or device concurrently or within 1 month prior to the Screening Visit, or use of an investigational agent within 1 month or 5 half-lives (if known), whichever is longer, prior to the Screening Visit; or Any other finding which, in the opinion of the Investigator, would compromise the patient's safety or participation in the study.
Facility Information:
Facility Name
Westside Medical Associates of Los Angeles
City
Beverly Hills
State/Province
California
Country
United States
Facility Name
Robarts Research Institute
City
London
State/Province
Ontario
Country
Canada
Facility Name
Ecogene-21
City
Chicoutimi
State/Province
Quebec
Country
Canada
Facility Name
Montreal Heart Institute
City
Montreal
State/Province
Quebec
Country
Canada
Facility Name
Wolfson Medical Center Internal Medicine Dept.
City
Holon
Country
Israel
Facility Name
Center for Research, Prevention and Treatment of Atherosclerosis - Cardiology Department of Medicine Kiryat Hadassah
City
Jerusalem
Country
Israel
Facility Name
Ziv Medical Center Internal Medicine Department
City
Safed
Country
Israel

12. IPD Sharing Statement

Citations:
PubMed Identifier
31685212
Citation
Gaudet D, Durst R, Lepor N, Bakker-Arkema R, Bisgaier C, Masson L, Golden L, Kastelein JJ, Hegele RA, Stein E. Usefulness of Gemcabene in Homozygous Familial Hypercholesterolemia (from COBALT-1). Am J Cardiol. 2019 Dec 15;124(12):1876-1880. doi: 10.1016/j.amjcard.2019.09.010. Epub 2019 Sep 26.
Results Reference
derived

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Efficacy and Safety of Gemcabene in Patients With Homozygous Familial Hypercholesterolemia on Stable, Lipid-Lowering Therapy (COBALT-1)

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