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Highly blood perfused, highly metabolically active pancreatic islets may be more susceptible for immune attack

Ullsten, Sara ; Espes, Daniel ; Quach, My ; Fex, Malin LU ; Sandberg, Monica and Carlsson, Per Ola (2020) In Physiological Reports 8(13).
Abstract

Differences in pancreatic islet susceptibility during type 1 diabetes development may be explained by interislet variations. This study aimed to investigate if heterogeneities in vascular support and metabolic activity in rat and human islets may explain why some islets are attacked earlier than other islets. In rats, highly blood perfused islets were identified by injection of microspheres into the ascending aorta, whereas a combination of anterograde and retrograde injections of microspheres into pancreas was used to determine the islet vascular drainage system. Highly blood perfused islets had superior function and lower glucose threshold for insulin release when compared with other islets. These islets had a preferential direct... (More)

Differences in pancreatic islet susceptibility during type 1 diabetes development may be explained by interislet variations. This study aimed to investigate if heterogeneities in vascular support and metabolic activity in rat and human islets may explain why some islets are attacked earlier than other islets. In rats, highly blood perfused islets were identified by injection of microspheres into the ascending aorta, whereas a combination of anterograde and retrograde injections of microspheres into pancreas was used to determine the islet vascular drainage system. Highly blood perfused islets had superior function and lower glucose threshold for insulin release when compared with other islets. These islets had a preferential direct venous drainage to the portal vein, whereas other islets mainly were incorporated into the exocrine capillary system. In BioBreeding rats, the hypothesis that islets with high islet blood perfusion was more prone to immune cell infiltration was investigated. Indeed, highly blood perfused islets were the first affected by the immune attack. In human subjects, differences in glucose threshold for insulin (C-peptide) secretion was evaluated in individuals recently diagnosed for type 1 diabetes and compared to control subjects. A preferential loss of capacity for insulin release in response to low glucose concentrations was observed at debut of type 1 diabetes. Our study indicates that highly blood perfused islets with direct venous drainage and lower glucose threshold for insulin release are of great importance for normal glucose homeostasis. At the same time, these highly metabolically active islets were the primary target of the immune system.

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author
; ; ; ; and
organization
publishing date
type
Contribution to journal
publication status
published
subject
keywords
blood flow, heterogeneity, insulitis, pancreatic islets, type 1 diabetes
in
Physiological Reports
volume
8
issue
13
article number
e14444
publisher
John Wiley & Sons Inc.
external identifiers
  • scopus:85087470740
  • pmid:32618430
ISSN
2051-817X
DOI
10.14814/phy2.14444
language
English
LU publication?
yes
id
1c72c72f-dd80-4978-9b0a-c57d716c758e
date added to LUP
2020-07-15 12:36:29
date last changed
2024-04-03 11:37:21
@article{1c72c72f-dd80-4978-9b0a-c57d716c758e,
  abstract     = {{<p>Differences in pancreatic islet susceptibility during type 1 diabetes development may be explained by interislet variations. This study aimed to investigate if heterogeneities in vascular support and metabolic activity in rat and human islets may explain why some islets are attacked earlier than other islets. In rats, highly blood perfused islets were identified by injection of microspheres into the ascending aorta, whereas a combination of anterograde and retrograde injections of microspheres into pancreas was used to determine the islet vascular drainage system. Highly blood perfused islets had superior function and lower glucose threshold for insulin release when compared with other islets. These islets had a preferential direct venous drainage to the portal vein, whereas other islets mainly were incorporated into the exocrine capillary system. In BioBreeding rats, the hypothesis that islets with high islet blood perfusion was more prone to immune cell infiltration was investigated. Indeed, highly blood perfused islets were the first affected by the immune attack. In human subjects, differences in glucose threshold for insulin (C-peptide) secretion was evaluated in individuals recently diagnosed for type 1 diabetes and compared to control subjects. A preferential loss of capacity for insulin release in response to low glucose concentrations was observed at debut of type 1 diabetes. Our study indicates that highly blood perfused islets with direct venous drainage and lower glucose threshold for insulin release are of great importance for normal glucose homeostasis. At the same time, these highly metabolically active islets were the primary target of the immune system.</p>}},
  author       = {{Ullsten, Sara and Espes, Daniel and Quach, My and Fex, Malin and Sandberg, Monica and Carlsson, Per Ola}},
  issn         = {{2051-817X}},
  keywords     = {{blood flow; heterogeneity; insulitis; pancreatic islets; type 1 diabetes}},
  language     = {{eng}},
  number       = {{13}},
  publisher    = {{John Wiley & Sons Inc.}},
  series       = {{Physiological Reports}},
  title        = {{Highly blood perfused, highly metabolically active pancreatic islets may be more susceptible for immune attack}},
  url          = {{http://dx.doi.org/10.14814/phy2.14444}},
  doi          = {{10.14814/phy2.14444}},
  volume       = {{8}},
  year         = {{2020}},
}