Clinical Trial Details
— Status: Active, not recruiting
Administrative data
| NCT number |
NCT02422745 |
| Other study ID # |
2014P002768 |
| Secondary ID |
|
| Status |
Active, not recruiting |
| Phase |
Phase 4
|
| First received |
|
| Last updated |
|
| Start date |
June 2015 |
| Est. completion date |
September 30, 2023 |
Study information
| Verified date |
July 2022 |
| Source |
Brigham and Women's Hospital |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
The purpose of this study is to determine whether taking daily, dietary supplements of cocoa
extract (containing cocoa flavanols and theobromine from the cocoa bean) and/or a standard
multivitamin reduces the risk of developing cardiovascular disease (including heart attack,
stroke, coronary revascularization, unstable angina or acute coronary syndrome (ACS)
requiring hospitalization, carotid artery surgery, and peripheral artery surgery or
angioplasty, and cardiovascular mortality) and cancer.
Description:
The COcoa Supplement and Multivitamin Outcomes Study (COSMOS) is a randomized clinical trial
of cocoa extract supplement (containing a total of 600 mg/d cocoa flavanols, including 80 mg.
(-)-epicatechins), and a standard multivitamin supplement to reduce the risk of
cardiovascular disease and cancer among women aged 65 years and older and men aged 60 years
and older.
After the COSMOS trial began, an advanced method to analyze cocoa flavanols was accredited by
AOAC International as a First Action Official Method of Analysis
(https://doi.org/10.1093/jaoacint/qsaa132). This updated method relies on a reference
material (RM8403) recently standardized and made commercially available by the U.S. National
Institute of Standards and Technology. While the actual cocoa flavanol content of the COSMOS
intervention remained unchanged throughout the trial, the application of this new analytical
method led to expected changes in how the total cocoa flavanol content is now reported.
Applying AOAC 2020.05/RM8403 to the COSMOS intervention, the total cocoa flavanol content of
the COSMOS intervention is now 500 mg/day. Reporting of (-)-epicatechin content remained
unaffected. Going forward, we will therefore apply AOAC 2020.05/RM8403 and report that the
COSMOS intervention tested 500 mg/day of cocoa flavanols, including 80 mg of (-)-epicatechin.
Participants in COSMOS were recruited from among Women's Health Initiative (WHI) Extension
Study cohort members; non-randomized respondents to mailings for the VITamin D and OmegA-3
TriaL (VITAL); respondents to nationwide invitational mailings to age-eligible adults; and
volunteers who learned about the trial through the media or through ResearchMatch.org, an
electronic recruitment website.
Several small randomized trials have demonstrated benefits for cocoa flavanols on
intermediate outcomes, including blood pressure, lipids, insulin sensitivity, and
flow-mediated vasodilation. For multivitamins, a prior large-scale randomized trial in
middle-aged and older men showed a significant reduction in cancer, but comparable trial data
in women are lacking. For both interventions, a large-scale clinical trial such as COSMOS
could have major clinical and public health implications.
Eligible participants have been assigned by chance (like a coin toss) to one of four groups:
(1) daily cocoa extract and multivitamin; (2) daily cocoa extract and multivitamin placebo;
(3) daily cocoa extract placebo and multivitamin; or (4) daily cocoa extract placebo and
multivitamin placebo. Participants have an equal chance of being assigned to any of these
four groups and a 3 out of 4 chance of receiving at least one active agent.
Participants in all groups take three pills each day: two capsules that contain either cocoa
extract or cocoa extract placebo, and one tablet that contains either multivitamin or
multivitamin placebo. Participants receive their study pills in convenient calendar packs via
U.S. mail.
Participants are asked to complete mailed questionnaires each year. The questionnaires ask
about health; lifestyle habits, such as diet, physical activity, and smoking; use of
medications and dietary supplements; family history of illness and new medical diagnoses.
Occasionally, participants may receive a phone call from study staff to collect information
or clarify responses on the questionnaires.
The expected rates for our original primary composite cardiovascular disease (CVD) endpoint
were based on the projected age and sex distribution of the trial cohort and CVD event rates
from our previously conducted trials. However, we determined that the observed rates of CVD
endpoints among COSMOS participants were lower than expected due to a younger population of
women, increasing use of statins and other pharmacotherapies as seen in other recently
published clinical trials, and the impact of COVID-19 on fewer reports of CVD diagnoses,
hospitalizations, and procedures. As a result, the COSMOS Data and Safety Monitoring Board
(DSMB) approved a proposal to add three new outcomes to our primary composite CVD endpoint:
(1) unstable angina or acute coronary syndrome requiring hospitalization, (2) carotid artery
surgery, and (3) peripheral artery surgery or angioplasty. These additional CVD outcomes are
consistent with the atherosclerotic mechanisms underlying the postulated effects for the
randomized interventions. COSMOS participants have already provided self-reports of these
diagnoses since the start of the COSMOS trial that will be adjudicated via medical records.
The original primary composite CVD endpoint will still be evaluated as a secondary outcome.
At baseline, approximately 7,000 COSMOS participants provided optional blood and urine
samples, which will be used to determine whether the study agents significantly change
biomarkers and other risk factors related to cardiovascular disease and cancer. Selected
participants either have specimens collected through mailed specimen collection kits that are
returned by the participant, or have blood, urine, blood pressure, and anthropometric
measurements collected by technicians from Examination Management Services, Inc. (EMSI), a
national clinical services provider. A subgroup of those who provide baseline specimens and
measurements are asked to provide follow-up samples and measurements.
At baseline and year 2 of the trial, approximately 600 participants living within driving
distance of Boston, Massachusetts provide additional measurements from in-clinic study visits
at the Clinical and Translational Science Center (CTSC) of Brigham and Women's Hospital.
These visits include cognitive function assessments, anthropometrics, physical function
assessments, blood pressure and other measurements. The trial will assess whether the study
agents significantly affect changes in these variables over time.
Primary Hypotheses:
1. A cocoa extract supplement will reduce the risk of major cardiovascular events, defined
as a composite endpoint of myocardial infarction, stroke, cardiovascular mortality,
coronary revascularization, unstable angina or ACS requiring hospitalization, carotid
artery surgery, and peripheral artery surgery or angioplasty;
2. A daily multivitamin will reduce the risk of invasive cancer (excluding non-melanoma
skin cancer).
Secondary Hypotheses:
1. Cocoa extract will reduce the risk of a composite endpoint of MI, stroke, cardiovascular
mortality, and coronary revascularization;
2. Cocoa extract will reduce the risk of invasive cancer (excluding non-melanoma skin
cancer);
3. A daily multivitamin will reduce the risk of major cardiovascular events;
4. Cocoa extract and/or a daily multivitamin will reduce the combined endpoint of major
cardiovascular events plus all-cause mortality;
5. Cocoa extract and/or a daily multivitamin will reduce the risk of individual
cardiovascular events, including myocardial infarction, stroke, cardiovascular
mortality, coronary revascularization, unstable angina or ACS requiring hospitalization,
carotid artery surgery, and peripheral artery surgery or angioplasty, and total
mortality; plus site-specific cancers, including breast, colorectal, and lung cancer;
6. A daily multivitamin will reduce the risk of cancer among women and men with a history
of cancer at baseline;
7. In a subset of equal numbers of female and male COSMOS respondents who provide baseline
bloods, cocoa extract and/or a daily multivitamin will significantly change levels of
blood flavonoids from baseline to 2 years of follow-up.
Tertiary Aim:
To assess whether the cocoa extract and/or a daily multivitamin exhibit synergistic effects
on risk of major cardiovascular events or cancer, and if the effects vary by nutritional
status or medication use.
Aims of Clinical and Translational Science Center (CTSC) Component:
To test whether the cocoa extract and/or a daily multivitamin has beneficial effects on:
1. Systolic and diastolic blood pressure;
2. Pulse wave velocity (PWV) and central blood pressure indices as measured by pulse wave
analysis;
3. Cognitive function and memory;
4. Physical performance as assessed by balance tests, grip strength, timed chair stands,
and walking speed,
5. Bone loss in the spine, hip and total body as assessed by bone-mineral density (BMD) and
changes in body composition as assessed by dual x-ray absorpiometry (DXA);
