Hypoglycemia Clinical Trial
Official title:
Evaluation of the Effect of Hypoglycemia on the Noradrenergic System With PET and a Highly Selective Norepinephrine Transporter Ligand
The aim of this study is to use Positron Emission Tomography (PET) imaging to measure changes
in norepinephrine transporter (NET) concentrations in the brain and periphery of healthy
individuals during hypoglycemia.
We hypothesize that during hypoglycemia, NE levels will increase within the brain, especially
the hypothalamus, and this likely contributes to activation of glucose counterregulatory
responses. We further hypothesize that during hypoglycemia, NET concentrations in key
glucoregulatory regions will change in order to sustain or prolong sympathetic nervous system
activation of counterregulatory responses.
Hypoglycemia elicits a multifaceted hormonal response that aims to restore glycemic levels to
normal. As blood glucose levels start to fall, there is a cessation of insulin secretion. At
the top of this hierarchy of counterregulatory responses are glucagon and epinephrine, which
are the two principal circulating hormones that increase glucose production and inhibit
glucose utilization to raise plasma glucose levels back to normal. In conjunction with these
circulating hormones there is activation of the sympathetic nervous system, which acts to
stimulate hepatic glucose production and lipolysis and suppress peripheral glucose uptake. In
cases of prolonged and/or more severe hypoglycemia, growth hormone and cortisol are mobilized
to stimulate the synthesis of gluconeogenic enzymes and inhibit glucose utilization.In
non-diabetic individuals, glucagon and epinephrine are usually very effective and the latter
responses are rarely required in the acute situation. In contrast, impaired glucose
counterregulation presents itself in longstanding diabetes and with antecedent
hypoglycemia.Within the first five years after the onset of type 1 diabetes, the primary
defense against hypoglycemia, the release of glucagon, either becomes significantly
attenuated or is completely absent and this impairment appears to be specific for the
stimulus of hypoglycemia. Hence, patients with diabetes primarily depend on the release of
catecholamines as their main defense against hypoglycemia. Unfortunately, with longer
duration of diabetes and especially with poor glycemic control, epinephrine secretion and
sympathetic activation are also compromised, making these patients even more vulnerable to
the threat of hypoglycemia. In patients with diabetes, hypoglycemia arises from the interplay
of a relative excess of exogenous insulin and defective glucose counterregulation and it
remains a limiting factor in attaining proper glycemic management. Both the Diabetes Control
and Complications Trial (DCCT) conducted in type 1 patients and the United Kingdom
Prospective Diabetes Study (UKPDS) conducted in type 2 patients have established the
importance of maintaining good glucose control over a lifetime of diabetes to avoid
ophthalmologic, renal and neurological complications. However, lowering glycemic goals for
patients with diabetes increases their risk for hypoglycemia exposure. According to the DCCT,
type 1 patients put on intensive insulin therapy, though having improved outcomes for
diabetic complications, are at a 3-fold higher risk of experiencing severe hypoglycemia
compared to those on conventional insulin therapy9. Moreover, recent antecedent hypoglycemia
reduces autonomic response (catecholamines) and development of symptoms (which normally
prompts behavioral defenses such as eating) to subsequent hypoglycemia10-13. Thus begins the
vicious cycle of recurrent hypoglycemia where hypoglycemia leads to further impairment of
counterregulatory responses which in turn, begets more hypoglycemia and so forth. Because of
the imperfections of current insulin therapies, those patients attempting to achieve tight
glycemic control suffer an untold number of asymptomatic hypoglycemic episodes. Current
estimates of symptomatic hypoglycemic episodes range from 2-3 incidences per week on average
and severe, debilitating episodes occur once or twice each year. Therefore, understanding how
the body senses falling blood glucose levels and initiates counterregulatory mechanisms will
be crucial if we are to prevent or eliminate hypoglycemia. Sensors that detect changes in
blood glucose levels and initiate glucose counterregulatory responses have been identified in
the hepatic portal vein, the carotid body and most importantly in the brain. In the brain,
the predominant sensors are located in the VMH and they are crucial for detecting falling
blood glucose levels and for initiating counterregulatory responses. Although the VMH has
been implicated as the primary glucose sensor in rodents, no human data are available.
Moreover, the exact mechanism leading to VMH activation is not well understood. It was
proposed that during hypoglycemia, a rise in VMH norepinephrine (NE) levels improves the
counterregulatory response to hypoglycemia27. While these studies highlight the importance of
the local NE elevation in the VMH, no one has examined the mechanisms that regulate local NE
levels during hypoglycemia. NETs limit the action of NE through reuptake into the cytoplasm,
regulating the extent of time that NE remains in the synapse28. Studies in rats showed that
chronic elevations of intracerebral insulin can significantly decrease NET mRNA expression in
the locus coeruleus, while hypoinsulinemia resulting from streptozotocin-induced diabetes
significantly elevates NET mRNA levels. These data suggest that endogenous insulin may be one
factor that regulates the synthesis and re-uptake of NE in the CNS. This hypothesis has been
confirmed and showed that treating hippocampal tissue and cervical ganglion neurons cells
with insulin led to a decrease in NET surface expression. However, the direct effect of
insulin on NET levels in humans has never been studied.
We have developed a novel approach to measure noradrenergic function using PET scanning and a
highly selective norepinephrine transporter (NET) ligand, (S,S)-[11C]O-methylreboxetine
([11C]MRB). Measuring changes in brain NET concentration is now possible with the use of
[11C]MRB and a high resolution HRRT PET system.
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