Understanding the influence of the neural efferent and afferent regulation of ?-cell health and function would be an important advancement. Although it is known that neural input plays a critical role in the health of the pancreas, details of the neuroanatomy and neurobiology of the human pancreas remains largely unexplored. It may be that T1D patients, wherein residual ?-cells continue to secrete C-peptide, could benefit from neuromodulation therapies that stimulate neurovascular regrowth and result in anti-inflammatory effects in the pancreas. Furthermore, neuromodulation therapies may help to improve insulin secretion in patients with T2D or perhaps delay onset of disease for those at high risk for T1D (e.g. first-degree relative with T1D, multiple islet autoantibodies, genetic risk factors). Both knowledge of the functional neuroanatomy and enabling technologies to test this hypothesis do not currently exist. This project brings together a potent combination of experts in islet biology, neurophysiology, bioengineering, and clinical endocrinology with an innovative approach to define the comparative neuroanatomy of the human and rat pancreatic neural network. Our hypothesis is that pancreatic ?-cells, functioning like peripheral neurons, maintain blood glucose levels, in part, due to the neural regulation of islet blood flow. This novel hypothesis will be tested by one specific aim: 1) To determine pancreatic neuroanatomy. These studies will enable understanding and mapping of the autonomic and sensory efferent and afferent networks in normal human and rat pancreas. Importantly, our studies will map the human pancreatic neural networks utilizing specimens already collected from human organ donors without diabetes and those with T1D or T2D using optical clearing methodologies and high resolution 3D microscopy. The outcomes of these studies will provide critical design data for logical application of next-generation neuromodulation technologies to improve islet health. This proposed work is directly in-line with the SPARC program to understand comparative neuroanatomy of the endocrine pancreas to enable neuromodulation strategies for amelioration of end organ diseases.

Public Health Relevance

Within the United States, diabetes affects ~30 million people and is the seventh leading cause of death while prediabetes affects an estimated 8 million adults. Understanding the influence of the autonomic and sensory neural regulation of insulin-producing ?-cell health and function would be an important advance for improving glucose metabolism through regulation of islet blood flow and neuroendocrine secretion.

Agency
National Institute of Health (NIH)
Institute
Office of The Director, National Institutes of Health (OD)
Project #
3OT2OD023861-01S1
Application #
9531858
Study Section
Anatomical and Functional Mapping of the Innervation of Marjor Internal Organs (AFMI)
Program Officer
Qashu, Felicia M
Project Start
2016-09-28
Project End
2018-07-31
Budget Start
2017-08-01
Budget End
2018-01-31
Support Year
1
Fiscal Year
2017
Total Cost
Indirect Cost
Name
University of Florida
Department
Pathology
Type
Schools of Medicine
DUNS #
969663814
City
Gainesville
State
FL
Country
United States
Zip Code
32611
Tang, Shiue-Cheng; Jessup, Claire F; Campbell-Thompson, Martha (2018) The Role of Accessory Cells in Islet Homeostasis. Curr Diab Rep 18:117