HIV Infections Clinical Trial
Official title:
The Effects of HIV Protease Inhibitors on Glucose Metabolism
The purpose of this study is to determine the mechanisms by which HIV protease inhibitors contribute to the development of diabetes in HIV-infected patients. The investigators propose that some HIV protease inhibitors impair insulin secretion and increase the production of glucose by the liver.
HIV protease inhibitors (PIs) have been associated with type 2 diabetes. To design future
HIV drugs that have have the least adverse metabolic effects, it is necessary to identify
the disorders of glucose metabolism with PI therapy. Previously PIs have been shown to
acutely induce insulin resistance in the periphery. Preliminary data show that PIs also
impair insulin secretion and increase hepatic glucose production in humans. These lesions
are key contributors to the development of type 2 diabetes. Due to the difficulty in
separating out factors related to HIV infection from the direct effect of PIs, an effective
design is to study HIV-negative subjects to define the direct effects of PIs on the liver
and pancreas on glucose metabolism:
Specific Aim 1: To determine which PIs acutely inhibit insulin secretion in humans;
randomized, double-blind, placebo-controlled trials will be performed on healthy normal
volunteers given either a single dose of PI or placebo using the hyperglycemic clamp to
assess insulin secretion in relation to insulin sensitivity.
Specific Aim 2: To determine which PIs acutely increase hepatic glucose production,
glycogenolysis, and gluconeogenesis; measurements will be assessed in the fasting and
hyperinsulinemic states using stable isotope analysis techniques. Samples have already been
collected from double-blind, placebo-controlled trials of the effects of a single dose of PI
on insulin sensitivity during the euglycemic hyperinsulinemic clamp.
Specific Aim 3: To determine the mechanism by which certain PIs increase hepatic glucose
production; an infusion of somatostatin during the fasting state and hyperinsulinemic state
will be used to suppress the effects of glucagon. Subjects will undergo a randomized,
double-blind, placebo-controlled trial of a single dose of PI or placebo on insulin
sensitivity using the euglycemic hyperinsulinemic clamp. Somatostatin, glucagon, and growth
hormone will be infused before and during the clamp study. Hepatic glucose production,
glycogenolysis, and gluconeogenesis will be assessed using stable isotope tracer techniques.
Results will be compared to PIs acutely given in the absence of somatostatin, as stated in
Specific Aim 2.
Determination of the effects of PI therapy allows clinicians to identify patients who may be
at particular risk for developing diabetes on certain PIs and treat them more effectively.
In the future, drugs for the treatment of HIV can be developed that avoid these disorders of
glucose metabolism.
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