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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT00455325
Other study ID # 395
Secondary ID P50HL083762
Status Completed
Phase Phase 2
First received
Last updated
Start date September 2004
Est. completion date March 2012

Study information

Verified date April 2022
Source Washington University School of Medicine
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

Metabolic syndrome consists of a group of co-occuring conditions that increase an individual's risk of developing heart disease, stroke, and diabetes. The purpose of this study is to evaluate the short-term effectiveness of chloroquine, a protein-activation medication, at improving metabolic syndrome.


Description:

Metabolic syndrome is one of the most common disorders in industrialized countries. It consists of abnormal serum lipids, glucose intolerance, elevated blood pressure, and central obesity in the setting of insulin resistance. The syndrome substantially increases the risk of developing diabetes and vascular disease, but there is no clear unifying approach to treat this disorder. In animals, activation of the protein ataxia telangiectasia mutated (ATM) using the antimalarial drug chloroquine improves features of metabolic syndrome and decreases atherosclerosis, a build-up of fatty plaque within arteries. The purpose of this study is to evaluate the effectiveness of short-term treatment with low doses of chloroquine as a way of managing metabolic syndrome. Participants in this study will initially receive placebo for 3 weeks, followed by increasing doses of chloroquine in three, 3-week intervals. Following each 3-week treatment, participants will be admitted to the research center for one day. There will be a period of no active treatment for 5 to 7 weeks following each admission to the research center to allow recovery from the blood drawing of the clamp procedure before the start of the next treatment interval.


Recruitment information / eligibility

Status Completed
Enrollment 35
Est. completion date March 2012
Est. primary completion date June 2010
Accepts healthy volunteers No
Gender All
Age group 18 Years to 60 Years
Eligibility Inclusion Criteria: - Diagnosis of metabolic syndrome, as determined by at least three of the following five criteria: 1. Elevated fasting triglyceride levels greater than or equal to 150 mg/dL 2. Low HDL cholesterol levels: less than 50 mg/dL for women and less than 40 mg/dL for men 3. Hypertension (=>130/85 mm Hg =<160/100 mm Hg) untreated; or hypertension controlled (=<150/90 mm Hg) on a stable medication regimen for 4 weeks prior to baseline visit. 4. Increased waist circumference: greater than 35 inches in women and greater than 40 inches in men 5. Elevated fasting glucose levels =<100 mg/dL but =>126 mg/dL - Subjects may be on a stable doses of a statin drug for at least 3 months - Subjects may be on a stable doses of L-thyroxine for at least 3 months - Willing to use acceptable form of birth control (e.g., hormonal birth control, double barrier methods) Exclusion Criteria: - Prior travel treatment with chloroquine or hydroxychloroquine as follows: 1. any exposure in the past 2 years, 2. >30 days of therapy if exposure was between 2 and 5 years ago, 3. >90 days of therapy if exposure was between 5 and 10 years ago, 4. >6 months of therapy if exposure was 10 to 20 years ago, 5. >1 year of therapy if exposure was 20 to 30 years ago, 6. No limit if last exposure was >30 years ago, ex. during the Vietnam conflict. - Morbid obesity (body mass index [BMI] greater than 45) - Coronary artery disease or other vascular disease - History of stroke - Chronic kidney insufficiency (i.e.,estimated glomerular filtration rate (eGFR) less than 60 ml/min/1.73m2) - Diabetes - Seizure disorder - History of psoriasis - Blood disorders, including anemia (i.e., hemoglobin levels less than 13 g/dL in men and less than 12 g/dL in women) - Current malignancy or active treatment for recurrence prevention, example tamoxifen. Cancer considered to be cured, either as a result of surgery or other treatment is not exclusionary. - Asthma requiring daily beta agonist therapy or intermittent oral steroids is exclusionary. Inhaled steroids are acceptable. Obstructive sleep apnea will be allowed if Continuous Positive Airway Pressure (CPAP) or other therapy has been stable for 6 months. Other active respiratory diseases are excluded. - Liver disease, or liver function test results greater than twice the normal value - Active infection, including HIV - Serious illness requiring ongoing medical care or medication - Treatment with atypical anti-psychotic medication. Treatment with any other medication for psychiatric illness, unless on a stable dose for 6 weeks prior to enrollment. Patients with unstable psychiatric disorders are excluded per the decision of the study MD regardless of medication history. - Taking any of the following lipid lowering medications: niacin, fibrates, and greater than 1 gm fish oils - Uncontrolled hypertension (BP >150/90) at enrollment. - Need for daily over the counter medications, or currently taking cimetidine or >1000 IU vitamin E daily and unwilling to reduce or discontinue the use of vitamin E or discontinue cimetidine for the duration of the study. Persons taking >1000 IU of vitamin E should reduce the dose 30 days prior to randomization. - Pregnant, breastfeeding, or intending to become pregnant - Glucose-6-phosphate dehydrogenase (G6PD) deficiency - Retinal disease (in particular, drusen or pigmentary changes at the macula); any ocular disease that interferes with the eye examination (e.g., cataracts) - Auditory disease or hearing loss; persons with total, irreversible hearing loss can be enrolled. - Participation in another clinical trial within past 30 days prior to screening and 60 days prior to randomization. Questionnaire or observational studies are not exclusionary.

Study Design


Intervention

Drug:
Placebo Comparator: First Intervention (3 weeks)
once daily placebo tablet for 3 weeks followed by: euglycemic clamp procedure; 24 hour Ambulatory Blood Pressure; Oral Glucose tolerance Test; serum collection; 24 hour urine collection; collection of peripheral blood mononuclear cells
Active Comparator: Second Intervention (3 weeks)
Once daily 80mg chloroquine or placebo tablet 3 Weeks followed by euglycemic clamp procedure; 24 hour Ambulatory Blood Pressure; Oral Glucose tolerance Test; serum collection; 24 hour urine collection; collection of peripheral blood mononuclear cells
Active Comparator: Third Intervention (3 weeks)
Once daily 80mg tablet for 3 weeks followed by: euglycemic clamp procedure; 24 hour Ambulatory Blood Pressure; Oral Glucose tolerance Test; serum collection; 24 hour urine collection; collection of peripheral blood mononuclear cells
Active Comparator: Fourth Intervention (3 weeks)
Once daily 250mg tablet for 3 weeks followed by: euglycemic clamp procedure; 24 hour Ambulatory Blood Pressure; Oral Glucose tolerance Test; serum collection; 24 hour urine collection; collection of peripheral blood mononuclear cells

Locations

Country Name City State
United States Washington University in St. Louis Saint Louis Missouri

Sponsors (2)

Lead Sponsor Collaborator
Washington University School of Medicine National Heart, Lung, and Blood Institute (NHLBI)

Country where clinical trial is conducted

United States, 

References & Publications (1)

Schneider JG, Finck BN, Ren J, Standley KN, Takagi M, Maclean KH, Bernal-Mizrachi C, Muslin AJ, Kastan MB, Semenkovich CF. ATM-dependent suppression of stress signaling reduces vascular disease in metabolic syndrome. Cell Metab. 2006 Nov;4(5):377-89. — View Citation

Outcome

Type Measure Description Time frame Safety issue
Primary Insulin Sensitivity Hepatic insulin sensitivity was measured by comparing glucose production at baseline of zero insulin infusion rate with glucose production at 56 pmol/m2/min. Hepatic insulin sensitivity was expressed as the percent suppression, such that greater percent suppression indicated greater hepatic insulin sensitivity. There are no reference values, since the patients served as their own controls. assessed every 8 - 10 weeks at the end of each treatment period
Secondary Systolic Blood Pressure Two techniques were employed: auscultation of seated subjects at rest was performed by a trained observer who recorded the first and fifth phases of the Korotkoff sounds; and, a portable oscillometric device (SpaceLabs Medical) recorded results every 20 min during the day and every hour during the night. Data were analyzed as mean values over 24 hours. Assessed every 8-10 weeks at the end of each treatment period
Secondary Diastolic Blood Pressure Two techniques were employed: auscultation of seated subjects at rest was performed by a trained observer who recorded the first and fifth phases of the Korotkoff sounds; and, a portable oscillometric device (SpaceLabs Medical) recorded results every 20 min during the day and every hour during the night. Data were analyzed as mean values over 24 hours. Assessed every 8-10 weeks at the end of each treatment period.
Secondary Total Cholesterol Fasting Serum Blood Sample Assessed every 8-10 weeks at the end of each treatment period.
Secondary Non-HDL Cholesterol Fasting Serum Blood Sample Assessed every 8-10 weeks at the end of each treatment period.
Secondary Low-density Lipoprotein Fasting Serum Blood Sample Assessed every 8-10 weeks at the end of each treatment period.
Secondary Triglycerides Fasting Serum Blood Sample Assessed every 8-10 weeks at the end of each treatment period.
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