|
|
Home
Search
Study Topics
Glossary
|
 |
|
|
|
|
|
|
|
|
|
|
|
|
||||||||||||||||||||||||||||||||||||
| Sponsor: | Albert Einstein College of Medicine of Yeshiva University |
|---|---|
| Collaborator: |
National Institutes of Health (NIH) |
| Information provided by: | Albert Einstein College of Medicine of Yeshiva University |
| ClinicalTrials.gov Identifier: | NCT00678145 |
Purpose
Many studies have demonstrated that when people with diabetes are intensively treated with insulin in order to maintain their glucose within the normal range, all the complications of diabetes can be prevented or delayed. However, such treatment carries a significant risk of severe hypoglycemia (excessively low blood glucose levels), which may be life-threatening. Thus, ideal treatment with insulin in patients with diabetes can be seen as a double-edged sword: intensive treatment will delay the complications but is also associated with an increased risk of disabling hypoglycemia. In normal conditions, when hypoglycemia occurs, the body responds by secreting a variety of hormones and by activating the autonomous nervous system which ultimately will result in increasing the blood glucose to normal levels. Patients with diabetes, lose this capacity to effectively respond to hypoglycemia and become more susceptible to a fall in plasma glucose. Paradoxically, repeated episodes of hypoglycemia—especially in the most vulnerable persons with type 1 who need insulin for life--induce a metabolic deterioration that further increases the risk of developing hypoglycemia.
Our proposal focuses on understanding the mechanisms the body uses in order to respond to hypoglycemia and on potential tools (medicines) that may be used in order to prevent this metabolic deterioration associated with repeated episodes of hypoglycemia.
Based on previous data generated in our laboratory (and others), we propose that repeated episodes of hypoglycemia are associated with a deterioration in the "body sensor" for hypoglycemia in diabetes. Moreover, since many studies have shown that such deterioration in the response to hypoglycemia can be induced also by exercise (patients with diabetes are at greater risk for hypoglycemia after exercise), we propose that exercise (and other stresses) affect the hypoglycemia response by endorphin release (endorphins are proteins responsible for inhibition of the neuroendocrine response system).
Developing a method that will decrease the incidence of severe hypoglycemia will result in safer control of blood glucose, a decrease in the complications of diabetes, and ultimately in a better quality and longer life for many patients with diabetes.
| Condition | Intervention |
|---|---|
|
Diabetes Mellitus Hypoglycemia Autonomic Failure |
Drug: naloxone Dietary Supplement: fructose Behavioral: exercise |
| Study Type: | Interventional |
| Study Design: | Basic Science, Open Label, Placebo Control, Single Group Assignment |
| Official Title: | Mechanisms of Hypoglycemia Associated Autonomic Failure |
| Estimated Enrollment: | 116 |
| Study Start Date: | March 2008 |
| Estimated Study Completion Date: | January 2013 |
| Estimated Primary Completion Date: | February 2009 (Final data collection date for primary outcome measure) |
| Arms | Assigned Interventions |
|---|---|
|
1: Experimental
Healthy individuals and patients with type 1 diabetes mellitus
|
Drug: naloxone
Administering fructose or naloxone or exercise on Day 1, and quantifying the counterregulatory responses to hypoglycemia on Day 2.
Dietary Supplement: fructose
Administering fructose or naloxone or exercise on Day 1, and quantifying the counterregulatory responses to hypoglycemia on Day 2.
Behavioral: exercise
Administering fructose or naloxone or exercise on Day 1, and quantifying the counterregulatory responses to hypoglycemia on Day 2.
|
Severe hypoglycemia (SH) is the major limitation of intensive insulin treatment in type 1 diabetes (T1DM), and the near-term prospects for perfected insulin therapy without this risk are dim. Intensively treated T1DM patients suffer from impaired counterregulation of hypoglycemia (HYPO)—ie, HYPO-Associated Autonomic Failure (HAAF) and HYPO unawareness (HU)—which enhance their susceptibility to SH. The precise mechanisms of HAAF and HU, however, have not been clarified, though multiple redundant control systems are implicated. Experimental HYPO and exercise in normal and T1DM subjects reproduce HAAF and HU, providing a robust experimental paradigm of these disorders. We have shown that fructose, infused in a catalytic dose for modulating glucokinase activity, results in augmentation of the counterregulatory responses to HYPO in nondiabetic and in T1DM individuals. We hypothesize that an equivalent infusion of fructose will prevent HAAF in nondiabetic and in T1DM persons. Furthermore, since both HYPO and exercise are associated with endogenous opioid (EO) release, and blocking EO improves HYPO counterregulation, we hypothesize that repeated HYPO episodes induce alterations in the modulatory effects of EO on hormonal and glucose counterregulation, ultimately leading to HAAF. We also propose that HYPO autoregulation, and hepatic glycogen metabolism play important roles in the development of HAAF and HU. The specific aims are: 1) to determine the effects of previous modulation of glucokinase activity on the counterregulatory hormonal and glucose recovery responses to subsequent HYPO in nondiabetic and T1DM subjects, 2) to examine the effects of blocking the inhibitory action of endorphins on the central neuroendocrine response system (with naloxone), during recurrent HYPO or exercise, on subsequent HYPO counterregulatory responses in nondiabetic and T1DM subjects, 3) to analyze the effects of recurrent mild HYPO (autoregulation), on subsequent HYPO counterregulation in nondiabetic and in T1DM subjects, and 4) to determine the effects of recurrent HYPO on hepatic glycogen content in nondiabetic and T1DM subjects, and the effects of normalization of liver glycogen content, by means of insulin and glucose administration, on experimental HAAF in T1DM subjects.
Eligibility| Ages Eligible for Study: | 19 Years to 64 Years |
| Genders Eligible for Study: | Both |
| Accepts Healthy Volunteers: | Yes |
Inclusion Criteria:
Exclusion Criteria:
Contacts and Locations| Contact: Cynthia Rivera | 718-430-8670 | carivera@aecom.yu.edu |
| United States, New York | |
| Albert Einstein College of Medicine / General Clinical Research Center | Recruiting |
| Bronx, New York, United States, 10461 | |
| Principal Investigator: | Ilan Gabriely, M.D. | Albert Einstein College of Medicine of Yeshiva University |
More Information
| Responsible Party: | Albert Einstein College of Medicine ( Ilan Gabriely, MD ) |
| Study ID Numbers: | 2008-202, R01 DK079974-01 |
| Study First Received: | May 14, 2008 |
| Last Updated: | August 5, 2009 |
| ClinicalTrials.gov Identifier: | NCT00678145 History of Changes |
| Health Authority: | United States: Institutional Review Board |
|
Diabetes Hypoglycemia HAAF Counterregulation |
|
Hypocalcemia Hypoglycemia Metabolic Diseases Nervous System Diseases Narcotic Antagonists Physiological Effects of Drugs Diabetes Mellitus Endocrine System Diseases Pharmacologic Actions |
Naloxone Calcium Metabolism Disorders Autonomic Nervous System Diseases Sensory System Agents Therapeutic Uses Water-Electrolyte Imbalance Peripheral Nervous System Agents Glucose Metabolism Disorders Central Nervous System Agents |
