Human pancreatic capillaries and nerve fibers persist in type 1 diabetes despite beta cell loss

The autonomic nervous system regulates pancreatic function. Islet capillaries are essential for the extension of axonal projections into islets, and both of these structures are important for appropriate islet hormone secretion. Because beta cells provide important paracrine cues for islet glucagon...

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Published in:American journal of physiology: endocrinology and metabolism 2023-03, Vol.324 (3), p.E251-E267
Main Authors: Richardson, Tiffany M, Saunders, Diane C, Haliyur, Rachana, Shrestha, Shristi, Cartailler, Jean-Philippe, Reinert, Rachel B, Petronglo, Jenna, Bottino, Rita, Aramandla, Radhika, Bradley, Amber M, Jenkins, Regina, Phillips, Sharon, Kang, Hakmook, Caicedo, Alejandro, Powers, Alvin C, Brissova, Marcela
Format: Article
Language:English
Subjects:
Animals
Capillaries - metabolism
Diabetes Mellitus, Type 1 - metabolism
Diabetes Mellitus, Type 2 - metabolism
Glucagon - metabolism
Glucagon-Secreting Cells - metabolism
Humans
Islets of Langerhans - metabolism
Mice
Nerve Fibers - metabolism
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Summary:The autonomic nervous system regulates pancreatic function. Islet capillaries are essential for the extension of axonal projections into islets, and both of these structures are important for appropriate islet hormone secretion. Because beta cells provide important paracrine cues for islet glucagon secretion and neurovascular development, we postulated that beta cell loss in type 1 diabetes (T1D) would lead to a decline in intraislet capillaries and reduction of islet innervation, possibly contributing to abnormal glucagon secretion. To define morphological characteristics of capillaries and nerve fibers in islets and acinar tissue compartments, we analyzed neurovascular assembly across the largest cohort of T1D and normal individuals studied thus far. Because innervation has been studied extensively in rodent models of T1D, we also compared the neurovascular architecture between mouse and human pancreas and assembled transcriptomic profiles of molecules guiding islet angiogenesis and neuronal development. We found striking interspecies differences in islet neurovascular assembly but relatively modest differences at transcriptome level, suggesting that posttranscriptional regulation may be involved in this process. To determine whether islet neurovascular arrangement is altered after beta cell loss in T1D, we compared pancreatic tissues from non-diabetic, recent-onset T1D (10-yr duration) donors. Recent-onset T1D showed greater islet and acinar capillary density compared to non-diabetic and longstanding T1D donors. Both recent-onset and longstanding T1D had greater islet nerve fiber density compared to non-diabetic donors. We did not detect changes in sympathetic axons in either T1D cohort. Additionally, nerve fibers overlapped with extracellular matrix (ECM), supporting its role in the formation and function of axonal processes. These results indicate that pancreatic capillaries and nerve fibers persist in T1D despite beta cell loss, suggesting that alpha cell secretory changes may be decoupled from neurovascular components. Defining the neurovascular architecture in the pancreas of individuals with type 1 diabetes (T1D) is crucial to understanding the mechanisms of dysregulated glucagon secretion. In the largest T1D cohort of biobanked tissues analyzed to date, we found that pancreatic capillaries and nerve fibers persist in human T1D despite beta cell loss, suggesting that alpha cell secretory changes may be deco
ISSN:0193-1849
1522-1555
DOI:10.1152/ajpendo.00246.2022