Abstract

The glucagon response to insulin-induced hypoglycemia (IIH) is markedly impaired early in type 1 diabetes. We have previously demonstrated that this glucagon response is largely autonomically mediated in nondiabetic animals and humans. More recently we discovered an early sympathetic islet neuropathy (eSIN) in human subjects with type 1 diabetes and animal models thereof and therefore hypothesized that eSIN contributes to this glucagon impairment. The purpose of this grant is to determine the mechanism by which 1) only sympathetic nerves are lost, 2) only from the islets and 3) only in autoimmune diabetes. The mechanism that accounts for all three is based on emerging concepts in developmental neurobiology. We hypothesize that brain derived neurotrophic factor (BDNF), secreted by B-lymphocytes invading the islet during the development of autoimmune diabetes, shifts the balance of islet neurotrophins away from """"""""axonal maintenance"""""""" via Trk receptors towards """"""""axonal pruning"""""""" via the p75 pan-neurotrophin receptor (NTR), causing a selective loss of islet sympathetic nerves and thereby dysfunction of the sympathetic alpha-cell pathway. Therefore our first Specific Aim is to demonstrate the necessity of BDNF for the loss of islet sympathetic nerves. We will localize BDNF in the diabetic islet by a combination of transgenically tagging BDNF and immunohistochemically staining the tag. We will quantify BDNF mRNA in these islets by laser capturing them and using RT-PCR. We will demonstrate the sympathetic neurotoxicity of BDNF by knocking out the BDNF gene and thereby sparing these nerves and preventing the impairment of the glucagon response to sympathetic nerve activation. In our second Specific Aim we will demonstrate the necessity of B-lymphocytes by knocking them out, thus preventing both the loss of islet sympathetic nerves and the impairment of the glucagon response to sympathetic activation. In our third Specific Aim we will prevent the loss of islet sympathetic nerves by knocking out p75NTR, again preserving the glucagon response to sympathetic nerve activation. Significance: Determining the mechanism for the loss of islet sympathetic nerves in type 1 diabetes will allow us to prevent or reverse that loss. Since the sympathetic-alpha cell pathway is activated during IIH and contributes to the glucagon response to IIH, we expect such prevention to improve this glucagon response in type 1 diabetes. Normalizing this glucagon response will reduce the incidence and severity of insulin induced hypoglycemia, allowing more intensive treatment of patients with type 1 diabetes, thereby reducing the chronic hyperglycemia that causes the long-term complications of this disease.

Public Health Relevance

This grant seeks to understand why certain nerves are lost from the islets of people with type 1 diabetes. That understanding will allow us to prevent the nerve loss, which in turn should reduce the incidence of hypoglycemia during diabetes treatment. Prevention of hypoglycemia will allow tighter control of blood sugar, which is known to reduce the long-term complications of diabetes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
2R01DK050154-13A1
Application #
8185862
Study Section
Integrative Physiology of Obesity and Diabetes Study Section (IPOD)
Program Officer
Arreaza-Rubin, Guillermo
Project Start
1996-12-19
Project End
2015-04-30
Budget Start
2011-08-01
Budget End
2012-04-30
Support Year
13
Fiscal Year
2011
Total Cost
$337,423
Indirect Cost

  Institution

Name
Seattle Institute for Biomedical/Clinical Research
Department
Type
DUNS #
928470061
City
Seattle
State
WA
Country
United States
Zip Code
98108

  Publications

Morton, Gregory J; Muta, Kenjiro; Kaiyala, Karl J et al. (2017) Evidence That the Sympathetic Nervous System Elicits Rapid, Coordinated, and Reciprocal Adjustments of Insulin Secretion and Insulin Sensitivity During Cold Exposure. Diabetes 66:823-834
Mundinger, Thomas O; Taborsky Jr, Gerald J (2016) Early sympathetic islet neuropathy in autoimmune diabetes: lessons learned and opportunities for investigation. Diabetologia 59:2058-67
Mundinger, Thomas O; Mei, Qi; Foulis, Alan K et al. (2016) Human Type 1 Diabetes Is Characterized by an Early, Marked, Sustained, and Islet-Selective Loss of Sympathetic Nerves. Diabetes 65:2322-30
Mundinger, Thomas O; Cooper, Ellis; Coleman, Michael P et al. (2015) Short-term diabetic hyperglycemia suppresses celiac ganglia neurotransmission, thereby impairing sympathetically mediated glucagon responses. Am J Physiol Endocrinol Metab 309:E246-55
Meek, Thomas H; Dorfman, Mauricio D; Matsen, Miles E et al. (2015) Evidence That in Uncontrolled Diabetes, Hyperglucagonemia Is Required for Ketosis but Not for Increased Hepatic Glucose Production or Hyperglycemia. Diabetes 64:2376-87
Taborsky Jr, G J; Mei, Q; Hackney, D J et al. (2014) The search for the mechanism of early sympathetic islet neuropathy in autoimmune diabetes. Diabetes Obes Metab 16 Suppl 1:96-101
Taborsky Jr, Gerald J; Mei, Qi; Bornfeldt, Karin E et al. (2014) The p75 neurotrophin receptor is required for the major loss of sympathetic nerves from islets under autoimmune attack. Diabetes 63:2369-79
Meek, Thomas H; Wisse, Brent E; Thaler, Joshua P et al. (2013) BDNF action in the brain attenuates diabetic hyperglycemia via insulin-independent inhibition of hepatic glucose production. Diabetes 62:1512-8
Meek, Thomas H; Matsen, Miles E; Dorfman, Mauricio D et al. (2013) Leptin action in the ventromedial hypothalamic nucleus is sufficient, but not necessary, to normalize diabetic hyperglycemia. Endocrinology 154:3067-76
Taborsky Jr, Gerald J; Mundinger, Thomas O (2012) Minireview: The role of the autonomic nervous system in mediating the glucagon response to hypoglycemia. Endocrinology 153:1055-62

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