Cardiovascular Diseases Clinical Trial
Official title:
The Effect of Omega-3 Polyunsaturated Acids Supplementation on Endothelial Function, Oxidative Stress, Platelet Aggregation, Blood Coagulation and Inflammation in Patients With Type 2 Diabetes and Cardiovascular Disease
The major source of mortality and morbidity of diabetic patients is cardiovascular disease
(CVD). Moreover, in CVD patients the presence of diabetes is associated with the increased
risk of major adverse cardiac events as compared to patients without diabetes. The
pathophysiology of macrovascular complications in T2D is not fully understood and involves:
1/ induction of oxidative stress, 2/ the formation of advanced glycation end products, 3/
activation of blood coagulation and platelet aggregation, 4/ increased inflammation, 5/
altered secretion of adipokines in obese subjects and 6/ endothelial dysfunction. All those
mechanisms in T2D patients could potentially be a subject of new therapeutic interventions.
A therapy that continues to show promise in T2D patients with CVD is supplementation with
omega-3 polyunsaturated fatty acids (PUFA). Clinical studies have indicated that omega-3
PUFA decrease the risk of major cardiovascular events, although the mechanism of action is
not completely understood. Moreover, there were no trials exploring the mechanisms and
outcomes of omega-3 treatment in T2D patients with CVD. Despite that fact, Polish Diabetes
Association guidelines recommend the use of omega-3 PUFA in patients with diabetes in the
prevention of macrovascular complications. Moreover, it is unclear whether the benefits of
modifying the pathophysiological processes during supplementation with omega-3 PUFA occur
only in patients with their deficiency or in all patients with type 2 diabetes.
Potential benefits of omega-3 PUFA in such patients are: 1/ decreased oxidative stress, 2/
decreased platelet aggregation and reduction of hypercoagulable state, 3/ anti-inflammatory
effects, 4/ improvement in endothelial function. All those effects were explored previously
with inconsistent findings. There is very limited information from clinical studies on the
mechanisms and benefits of omega-3 PUFA in T2D patients with CVD.
The objective of the current study is to evaluate the effects of omega-3 PUFA administered
on top of optimal therapy of atherosclerotic vascular disease and T2D on endothelial
function, platelet aggregation and thrombotic, inflammatory and oxidative stress biomarkers.
The study will provide insight into:
1. The influence of the baseline level of omega-3 PUFA in patients with type 2 diabetes
mellitus (T2D) and CVD on endothelial function, platelet aggregation and thrombotic,
inflammatory, oxidative stress biomarkers.
2. The potential to improve the endothelial function, reduce the oxidative stress and to
decrease the atherothrombotic and inflammatory biomarkers with the supplementation with
a moderate dose of omega-3 PUFA
3. The mechanisms of the clinically observed effects of omega-3 PUFA in T2D patients with
CVD.
SCIENTIFIC BACKGROUND The incidence of diabetes is growing in the world and the number of
patients already exceeded 360 million and by 2030 this will rise to 552 million. The major
source of mortality and morbidity of diabetic patients is cardiovascular disease (CVD). On
average, it is estimated that people with type 2 diabetes (T2D) will die 5-10 years before
people without T2D, mostly due to CVD. The treatment of CVD accounts for a large part of the
huge healthcare costs attributable to T2D (10-12% of European health care expenditure).
Despite significant improvements in the treatment of CVD with antiplatelet agents, statin,
angiotensin converting enzyme inhibitors (ACEI) and newer antidiabetic drugs the mortality
of diabetic patients with CVD is continuously significantly higher than in people without
T2D. This pattern of elevated cardiovascular risk in diabetes has been attributed to several
possible mediating factors, including the development of more extensive, multi-vessel
coronary artery disease, the presence of impaired myocardial systolic contractility, diffuse
small vessel endothelial dysfunction and the presence of a hypercoagulable or pro-thrombotic
state attributable to diabetes.
The increased cardiovascular risk in T2D patients is generated by the metabolic disturbances
related to diabetes (both hyperglycaemia and hypoglycaemia) and that includes:
- irreversible glycation of intra- and extracellular proteins leading to changes in gene
expression and induction of oxidative stress leading to endothelial dysfunction,
- activation of protein kinase C resulting in activation of blood coagulation,
- increase in the levels of various pro-atherothrombotic and inflammatory biomarkers e.g.
markers of platelet activation, thrombin generation, endothelin, von Willebrand factor,
adhesion molecules (eg.VCAM-1, vascular endothelial cell adhesion molecule), growth
factors (VEGF), factor VII, CRP, IL-6 (interleukin-6). Moreover it was recently
described that hyperglycemia in T2D leads to nonenzymatic glycation of fibrinogen.
Glycated fibrinogen leads to denser fibrin clots that are stiffer and more resistant to
fibrinolysis, thus leading to an increased thrombotic burden,
- altered secretion of adipokines by adipose tissue in obese subjects with T2D. It was
demonstrated that greater adiposity e.g. down-regulates secretion of adiponectin, an
adipokine with anti-inflammatory and insulin-sensitizing properties.
All those pro-atherothrombotic mechanisms in T2D patients could potentially be a subject of
new developments in the treatment, especially in patients with CVD. A therapy that continues
to show great promise in this indication is supplementation with omega-3 polyunsaturated
fatty acids (PUFA) although the underlying mechanism of their beneficial action is not
precisely known. Numerous prospective and retrospective trials have shown that omega-3 PUFA
supplementation decreases the risk of major cardiovascular events, such as myocardial
infarction, sudden cardiac death, coronary heart disease, atrial fibrillation, and most
recently, death in patients with heart failure. However, none of those trials was performed
in T2D patients with CVD who are at the highest risk of events and where benefits could have
considerable clinical importance. Moreover to our knowledge, there are very few randomized,
double-blind, placebo-controlled clinical trials exploring the mechanisms of omega-3
treatment in T2D patients with documented cardiovascular disease. Despite that fact, Polish
Diabetes Association guidelines recommend the use of omega-3 PUFA in patients with diabetes
in the prevention of macrovascular complications. Moreover, it is unclear whether the
benefits of modifying the pathophysiological processes during supplementation with omega-3
PUFA occur only in patients with their deficiency or in all patients with type 2 diabetes.
Although there are several potential benefits considering therapy with omega-3 PUFA in T2D
patients with atherosclerotic vascular disease, some of those effects require a detailed
appraisal in a clinical study. They are:
1. Platelet activation and resistance to antiplatelet agents. Platelet dysfunction in
diabetes mellitus is related to several mechanisms - including metabolic derangements,
oxidative stress, and endothelial dysfunction. They lead to high platelet reactivity
which has been associated with atherothrombotic complications in patients with T2DM.
Therefore antiplatelet therapy is one of the cornerstones of secondary prevention of
atherothrombotic events in patients with T2DM.
Recent evidence suggests that the clinical efficacy of both aspirin and clopidogrel is
compromised in subjects in diabetes by mechanisms that are not entirely clear. This is
one of the reasons why diabetic patients continue to have a higher risk of adverse
cardiovascular events compared with that in non-diabetic patients.
The antiplatelet effect of n-3 PUFA has been explored with inconsistent findings.
Recently, the investigators have demonstrated that the addition of n-3 PUFA to the
combination of aspirin and clopidogrel significantly potentiates platelet response to
clopidogrel after percutaneous coronary intervention (PCI).
So far, there are no studies evaluating the effects of n-3 PUFA on platelet reactivity
and response to antiplatelet agents in patients with T2D and CVD.
2. Coagulation and fibrinolysis. In patients with T2D there is a general increase in
plasma levels of procoagulant factors accompanied by a decreased fibrinolytic capacity.
The mechanisms for these alterations are complex, with insulin resistance and
hyperglycaemia being clear culprits. The net result of the above changes is an
increased tendency to clot formation, with the fibrin network displaying a compact
structure and resistance to fibrinolysis. Moreover, increased fibrinogen levels
observed in diabetes correlate with the degree of hyperglycemia and with fibrinogen
glycation affecting fibrin polymerization and factor XIII-mediated crosslinking. Of
note, impaired metabolic control and marked fluctuations in plasma glucose levels have
been shown to be related to hypofibrinolysis associated with the formation of dense
fibrin clots. The differences in fibrin clot structure and its susceptibility to lysis
found to occur in type 2 diabetes may contribute to the increase in CVD risk in
diabetic patients.
A number of measures can reduce the hypercoagulable environment in diabetes including
glycaemic control, with avoidance of hypoglycaemia and improvement in insulin
sensitivity. Of the pharmacological agents used in patients with T2D and CVD,
metformin, aspirin, statins and angiotensin converting enzyme inhibitors have a
favourable effect on the coagulation system and all have been shown to reduce
cardiovascular events in diabetes.
Although it is unclear whether n-3 PUFA has clinically relevant effects on insulin
resistance in humans, they may affect coagulation system directly via several
mechanisms. It has been shown that in apparently healthy subjects, omega-3 PUFA can
increase or decrease plasma fibrinogen and clotting factors, in particular factor VII
activity, factor VIII and von Willebrand factor concentrations. There are studies
indicating that fish oil supplementation may reduce thrombin generation. Conversely,
other studies failed to demonstrate significant changes in circulating markers of
thrombosis following administration of omega-3 PUFA. Of note, these studies have been
conducted in patients without diabetes, so the knowledge on the effects of omega-3 in
T2D patients with CVD treated on optimal pharmacotherapy (including drugs affecting the
coagulation) is limited.
Regarding the effects of omega-3 PUFAs on fibrinolytic activity the findings are
controversial. In a single study performed 20 years ago intake of omega-3 PUFAs has
been associated with increased plasma plasminogen activator inhibitor (PAI-1) activity
in non-insulin-dependent diabetes mellitus patients. Interestingly, in a recent study,
PAI-1 concentration and activity increased more following high omega-3 PUFAs beverage
compared with low omega-3 PUFAs beverage in men with metabolic syndrome. It was also
demonstrated that with respect to fibrinolytic measurements, acute and chronic intake
of fish oil may show opposite effects, although the underlying mechanistic basis for
this is not understood. Further research is needed on this potentially adverse effect
on the coagulation in patients with glycometabolic disorders.
3. Endothelial dysfunction and oxidative stress A large body of evidence links endothelial
dysfunction to human diabetes mellitus. Endothelial dysfunction in T2D contributes to
the pathogenesis and clinical expression of atherosclerosis by promoting inflammation,
thrombosis, arterial stiffness, and impaired regulation of arterial tone and flow.
Increased oxidative stress in the vasculature is an important mechanism of endothelial
dysfunction and insulin resistance in diabetes mellitus. For example, circulating
markers of oxidative stress, including F2 isoprostanes and antibodies against oxidized
low density lipoprotein, are increased in humans with T2D.
In recent years, growing evidence links the intake of omega-3 PUFA with an improvement
in endothelial function. The mechanisms by which omega-3 PUFAs might influence
endothelial function are likely to be multiple and complex. They could include the
suppression of thromboxane A2 or cyclic endoperoxides, a reduced production of
cytokines, the augmented endothelial synthesis of nitric oxide, an improvement of
vascular smooth muscle cell sensitivity to nitric oxide, and a reduced expression of
endothelial adhesion molecules. The reduction of oxidative stress with omega-3 PUFA in
patients with T2D may be an important factor responsible for the improvement of
endothelial function. However, there is not enough data on the improvement of
endothelial function and the reduction of oxidative stress in patients with T2D and
established CVD.
4. Inflammation Chronic inflammation may participate in the pathogenesis of insulin
resistance, type 2 diabetes, and cardiovascular disease and may be a common denominator
that links obesity to these disease states. A variety of circulating proinflammatory
cytokines and acute-phase reactants are increased in obesity, type 2 diabetes, and
cardiovascular disease. Moreover, chronic low-grade inflammation occurring in the
adipose tissue of obese individuals is linked to increased insulin resistance and leads
to disturbances in the adipokines secretion.
Although there are divergent data whether omega-3 PUFA reduce inflammation they may modulate
adipokine secretion from adipose tissue. It was demonstrated that they increase plasma
adiponectin levels, which could be a potential mechanism by which EPA and DHA improve
insulin sensitivity. They also induce leptin and visfatin secretion and reduce the
expression of several proinflammatory cytokines from the adipose tissue, including tumor
necrosis factor TNFα, IL-6, monocyte chemotactic protein MCP-1, and PAI-1. However, there
are no clinical studies whether omega-3 PUFA supplementation can modulate adipose tissue
inflammation in T2D patients with CVD.
;
Allocation: Randomized, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Basic Science
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