Diabetes Clinical Trial
Official title:
Pilot Study of Mitochondrial Biology in Human Platelets
Type II diabetes mellitus is rapidly becoming a global pandemic with a deleterious impact on
cardiovascular morbidity and mortality. Understanding its pathophysiology is important for
the development of future therapeutic interventions. Emerging evidence suggests interplay
between mitochondrial dysfunction and the development of insulin resistance. Interestingly,
mitochondrial dysfunction in skeletal muscle and adipose tissue are early events in the
development of type II diabetes mellitus and are proposed to play a role in exacerbating
insulin resistance. Although it has been demonstrated that skeletal muscle of
insulin-resistant individuals has reduced mitochondria and mitochondrial dysfunction, whether
this disruption of mitochondrial function is more widespread has not been explored. We
hypothesize that this disruption of mitochondrial function is more systemic and thereby may
contribute to the development of peripheral insulin resistance and possibly promote the
myriad of complications associated with diabetes.
To test these assumptions, we propose an initial proof of concept study to evaluate
mitochondrial biology in human platelets in normal volunteers, pre-diabetic and diabetic
subjects to assess whether mitochondrial disruption/dysfunction evolves with the progression
to type II diabetes. In parallel, proteomic analysis will be performed to evaluate whether
the development of insulin resistance and diabetes confers a specific modulation in the
biological signature of human platelets with disease progression. To delineate these
concepts, we will evaluate study subject's glucose tolerance and insulin sensitivity and draw
blood in parallel to study their platelets. Biological readouts will include: 1) the
quantification of the mitochondrial proteome and electron transfer chain content; 2) the
evaluation of platelet mitochondrial respiratory function and 3) to determine the
mitochondrial reactive oxygen species capacity and defenses. If this hypothesis is validated,
this study will show that the mitochondrial disruption/dysfunction is a more generalized
finding in type II diabetes. Additionally, it would propose the use of platelets as potential
biomarkers for early detection of mitochondrial function and assessment of disease. Finally,
this would establish a peripheral blood readout of the modification of mitochondrial function
as a novel approach to monitor the prevention and/or reversal of insulin resistance and
diabetes in response to therapeutic strategies.
Type II diabetes mellitus is rapidly becoming a global pandemic with a deleterious impact on
cardiovascular morbidity and mortality. Understanding its pathophysiology is important for
the development of future therapeutic interventions. Emerging evidence suggests interplay
between mitochondrial dysfunction and the development of insulin resistance. Interestingly,
mitochondrial dysfunction in skeletal muscle and adipose tissue are early events in the
development of type II diabetes mellitus and are proposed to play a role in exacerbating
insulin resistance. Although it has been demonstrated that skeletal muscle of
insulin-resistant individuals has reduced mitochondria and mitochondrial dysfunction, whether
this disruption of mitochondrial function is more widespread has not been explored. We
hypothesize that this disruption of mitochondrial function is more systemic and thereby may
contribute to the development of peripheral insulin resistance and possibly promote the
myriad of complications associated with diabetes.
To test these assumptions, we propose an initial proof of concept study to evaluate
mitochondrial biology in human platelets in normal volunteers, pre-diabetic and diabetic
subjects to assess whether mitochondrial disruption/dysfunction evolves with the progression
to type II diabetes. In parallel, proteomic analysis will be performed to evaluate whether
the development of insulin resistance and diabetes confers a specific modulation in the
biological signature of human platelets with disease progression. To delineate these
concepts, we will evaluate study subject's glucose tolerance and insulin sensitivity and draw
blood in parallel to study their platelets. Biological readouts will include: 1) the
quantification of the mitochondrial proteome and electron transfer chain content; 2) the
evaluation of platelet mitochondrial respiratory function and 3) to determine the
mitochondrial reactive oxygen species capacity and defenses. If this hypothesis is validated,
this study will show that the mitochondrial disruption/dysfunction is a more generalized
finding in type II diabetes. Additionally, it would propose the use of platelets as potential
biomarkers for early detection of mitochondrial function and assessment of disease. Finally,
this would establish a peripheral blood readout of the modification of mitochondrial function
as a novel approach to monitor the prevention and/or reversal of insulin resistance and
diabetes in response to therapeutic strategies.
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