Metabolic Syndrome Clinical Trial
Official title:
Study of Wight Reduction by Life-style Modification
Central obesity, core of metabolic syndrome, has been recognized as one of the rooting
factors for development of diabetes and cardiovascular disease. Although efforts have been
devoted to the studies of central obesity and/or metabolic syndrome, much remained unknown
as to how obesity influences cellular as well as cardiac functions, what is the central
regulation of one's body weight.
Weight loss is an undisputed way to improve cardiovascular and metabolic disorders in obese
individuals. Previous studies have demonstrated that weight loss by 5% of initial weight
universally provide substantial benefits in these subjects. However, there are little
integrated research teams, composed of different disciplines, share common weight reduction
program to look at different aspects of weight reduction in non-diabetic individuals with
metabolic syndrome. The significances of this proposal we plan to target, namely Rho kinase
activity from peripheral leukocyte, several cardiac functions measured by noninvasive
technique (VP-2000) and MRI, circulating brain-derived neurotrophic factors (BDNF) levels,
are fully explained detailed in each sub-proposal.
In order to accomplish this integrated proposal, we will form research teams including
endocrinologists, cardiologists, radiologists, and a coordinating data center. We pan to
recruit 40 non-diabetic individuals with metabolic syndrome to participate this 12-16 weeks
weight reduction program. Twenty-five age, sex matched non-diabetes lean will be served as
controls. Oral glucose tolerance test, fasting blood obtained, noninvasive vascular and MRI
examinations will be applied before and after weight reduction program in those achieving at
least 5% loss of initial weight.
In summary, this study will investigate the effects of weight loss on (1) Rho kinase
activity obtained from peripheral leukocyte; (2). Aortic stiffness, central aortic pressure
and hemodynamic by a noninvasive vascular profiling system (VP-2000); (3) Brain function
specifically reflecting by circulating BDNF; (4). Aortic elastic properties and left
ventricular function by using MRI examinations, in non-diabetic individuals of metabolic
syndrome.
Obesity, in particular central obesity, has been one of the important documented risk
factors for development of diabetes and cardiovascular disease. Recent re-delineated various
versions of definitions of metabolic syndrome, has fueled further the critical involvement
of central adiposity in these disorders through several facets, including many increased
circulating pro-inflammatory cytokines, directly or indirectly linking to visceral adipose
tissue expressions. Although lots of efforts have been devoted to the studies of central
obesity and/or metabolic syndrome, much remained unknown as to how obesity affect cellular
as well as cardiac function, what is the central regulation of one's body weight, and how to
measure fat in visceral organs precisely.
Weight loss is an undisputed way to improve cardiovascular and metabolic disorders. Both a
recent review article and data from us demonstrated that only weight loss by 5% of initial
weight universally delivered benefits on obese individuals. However, there is little
integrated research teams from different disciplines share common weight reduction protocol
and look at different aspects of weight reduction in non-diabetic individuals with metabolic
syndrome. The significances of this proposal we plan to target are explained in detail in
each sub-proposal. However, we would like to make a briefing description here.
1. . Rho kinase (ROCK) is a serine/threonine kinase that mediates the downstream signaling
of the small guanosine triphosphate- binding protein, Rho, on the actin cytoskeleton.
In mostly animal models, the inhibition of ROCK ameliorates many cardiovascular
conditions, including hypertension, atherosclerosis, myocardial fibrosis, and stroke.
Recent study from Taiwan showed that ROCK activity is increased in patients with
metabolic syndrome.
2. . Obese and overweight individuals have increased levels of arterial stiffness which is
a measure of aortic and large vessel distensibility or compliance. Weight loss could
induce significant reduction in sympathetic activity and blood pressure. However,
little is known as whether weight loss can improve arterial stiffness, central aortic
blood pressure and related hemodynamics.
3. . Brain-derived neurotrophic factor (BDNF), recently reported related to Alzheimer's
disease, is present in brain tissues extensively. It is also noted that low circulating
level of BDNF was associated with impaired glucose metabolism, and might be associated
higher BMI or body fat. We are interesting in effect of weight reduction on circulating
BDNF values in non-diabetic subjects with metabolic syndrome.
4. . Magnetic resonance imaging (MRI) of the heart is frequently used and can provide
accurate and reproducible measurement of LV mass, volumes, systolic function and aortic
pulse velocity. Although echo-cardiography has been applied to study effect of weight
loss on cardiac function, there has been no study by using cardiac MRI to measure cine
images of cardiac function and related variables before and after weight reduction in
non-diabetic subjects with metabolic syndrome.
In order to accomplish this integrated proposal, we will formulate research teams including
endocrinologists, cardiologists, radiologists, and a data center, coordinated by a PhD
researcher (infra-structure as described below). We will recruit 40 non-diabetic individuals
with metabolic syndrome (fulfilled the criteria from IDF, 2006 and DOH of Taiwan).
Twenty-five age, sex matched non-diabetes lean will be served as controls.
Written informed consent will be obtained from each subject before being enrolled into the
study after approval from IRB of Taichung VGH, Taichung, Taiwan. This weight reduction
program will be assisted by experienced dieticians and sports experts, all of whom we had
collaborated and published article previously. This program will last for 12-16 weeks with
every participants join together courses 4 hours per week. Each participant will be
introduced a dietary plan based on a caloric reduction of 1200 Kcal/day from the values
thought necessary to maintain their usual weight. Subject will be asked to follow dietary
advice and their eating habit will be reviewed by dietician at the time of their weekly
visit. Activity levels will be encouraged to reach 30 min each day and at least 5 days a
week. During each visit, weight of each participant will be recorded and announced. Meals
replacement may considered for those did not get much improvement during weekly monitoring
since recent report indicated that meals replacement may provide certain help in reducing
body weight. We are confident that adequate weight reduction (at least 5% of initial weight)
and good compliance will be achieved given our previous experience.
In aggregate, this study will investigate the effects of weight loss on (1) Rho kinase
activity obtained from peripheral leukocyte (2). Aortic stiffness, central aortic pressure
and hemodynamic by a noninvasive technique (3) Brain function specifically reflecting by
circulating BDNF levels (4). Aortic elastic properties and left ventricular function by
using MRI examinations, in non-diabetic individuals of metabolic syndrome. Findings from
this integrated proposal will provide valuable information as mild to moderate weight loss
(5% of initial body weight) in cellular, cardiac and central nervous system in additional to
well-known effects on lipids, inflammatory cytokines and insulin resistance in non-diabetic
subjects with metabolic syndrome.
Follow up- Subjects received physical check up, fasting blood tests and OGTT 6 and 12 months
after the end of study.
;
Allocation: Non-Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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