Desmoglein-2 is important for islet function and β-cell survival

Kay K. Myo Min; Darling Rojas-Canales; Daniella Penko; Mark DeNichilo; Michaelia P. Cockshell; Charlie B. Ffrench; Emma J. Thompson; Olof Asplund; Christopher J. Drogemuller; Rashmi B. Prasad; Leif Groop; Shane T. Grey; Helen E. Thomas; Thomas Loudovaris; Thomas W. Kay; My G. Mahoney; Claire F. Jessup; P. Toby Coates; Claudine S. Bonder

doi:10.1038/s41419-022-05326-2

Desmoglein-2 is important for islet function and β-cell survival

Kay K. Myo Min
, Darling Rojas-Canales
, Daniella Penko
, Mark DeNichilo
, Michaelia P. Cockshell
, Charlie B. Ffrench
, Emma J. Thompson
, Olof Asplund
, Christopher J. Drogemuller
, Rashmi B. Prasad
, Leif Groop
, Shane T. Grey
, Helen E. Thomas
, Thomas Loudovaris
, Thomas W. Kay
, My G. Mahoney
, Claire F. Jessup
, P. Toby Coates
, Claudine S. Bonder

Research output: Contribution to journal › Article › peer-review

7 Scopus citations

Abstract

Type 1 diabetes is a complex disease characterized by the lack of endogenous insulin secreted from the pancreatic β-cells. Although β-cell targeted autoimmune processes and β-cell dysfunction are known to occur in type 1 diabetes, a complete understanding of the cell-to-cell interactions that support pancreatic function is still lacking. To characterize the pancreatic endocrine compartment, we studied pancreata from healthy adult donors and investigated a single cell surface adhesion molecule, desmoglein-2 (DSG2). Genetically-modified mice lacking Dsg2 were examined for islet cell mass, insulin production, responses to glucose, susceptibility to a streptozotocin-induced mouse model of hyperglycaemia, and ability to cure diabetes in a syngeneic transplantation model. Herein, we have identified DSG2 as a previously unrecognized adhesion molecule that supports β-cells. Furthermore, we reveal that DSG2 is within the top 10 percent of all genes expressed by human pancreatic islets and is expressed by the insulin-producing β-cells but not the somatostatin-producing δ-cells. In a Dsg2 loss-of-function mice (Dsg2^lo/lo), we observed a significant reduction in the number of pancreatic islets and islet size, and consequently, there was less total insulin content per islet cluster. Dsg2^lo/lo mice also exhibited a reduction in blood vessel barrier integrity, an increased incidence of streptozotocin-induced diabetes, and islets isolated from Dsg2^lo/lo mice were more susceptible to cytokine-induced β-cell apoptosis. Following transplantation into diabetic mice, islets isolated from Dsg2^lo/lo mice were less effective than their wildtype counterparts at curing diabetes. In vitro assays using the Beta-TC-6 murine β-cell line suggest that DSG2 supports the actin cytoskeleton as well as the release of cytokines and chemokines. Taken together, our study suggests that DSG2 is an under-appreciated regulator of β-cell function in pancreatic islets and that a better understanding of this adhesion molecule may provide new opportunities to combat type 1 diabetes.

Original language	English (US)
Article number	911
Journal	Cell Death and Disease
Volume	13
Issue number	10
DOIs	https://doi.org/10.1038/s41419-022-05326-2
State	Published - Oct 2022
Externally published	Yes

ASJC Scopus subject areas

Immunology
Cellular and Molecular Neuroscience
Cell Biology
Cancer Research

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Myo Min, K. K., Rojas-Canales, D., Penko, D., DeNichilo, M., Cockshell, M. P., Ffrench, C. B., Thompson, E. J., Asplund, O., Drogemuller, C. J., Prasad, R. B., Groop, L., Grey, S. T., Thomas, H. E., Loudovaris, T., Kay, T. W., Mahoney, M. G., Jessup, C. F., Coates, P. T., & Bonder, C. S. (2022). Desmoglein-2 is important for islet function and β-cell survival. Cell Death and Disease, 13(10), Article 911. https://doi.org/10.1038/s41419-022-05326-2

Myo Min, KK, Rojas-Canales, D, Penko, D, DeNichilo, M, Cockshell, MP, Ffrench, CB, Thompson, EJ, Asplund, O, Drogemuller, CJ, Prasad, RB, Groop, L, Grey, ST, Thomas, HE, Loudovaris, T, Kay, TW, Mahoney, MG, Jessup, CF, Coates, PT & Bonder, CS 2022, 'Desmoglein-2 is important for islet function and β-cell survival', Cell Death and Disease, vol. 13, no. 10, 911. https://doi.org/10.1038/s41419-022-05326-2

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title = "Desmoglein-2 is important for islet function and β-cell survival",

abstract = "Type 1 diabetes is a complex disease characterized by the lack of endogenous insulin secreted from the pancreatic β-cells. Although β-cell targeted autoimmune processes and β-cell dysfunction are known to occur in type 1 diabetes, a complete understanding of the cell-to-cell interactions that support pancreatic function is still lacking. To characterize the pancreatic endocrine compartment, we studied pancreata from healthy adult donors and investigated a single cell surface adhesion molecule, desmoglein-2 (DSG2). Genetically-modified mice lacking Dsg2 were examined for islet cell mass, insulin production, responses to glucose, susceptibility to a streptozotocin-induced mouse model of hyperglycaemia, and ability to cure diabetes in a syngeneic transplantation model. Herein, we have identified DSG2 as a previously unrecognized adhesion molecule that supports β-cells. Furthermore, we reveal that DSG2 is within the top 10 percent of all genes expressed by human pancreatic islets and is expressed by the insulin-producing β-cells but not the somatostatin-producing δ-cells. In a Dsg2 loss-of-function mice (Dsg2lo/lo), we observed a significant reduction in the number of pancreatic islets and islet size, and consequently, there was less total insulin content per islet cluster. Dsg2lo/lo mice also exhibited a reduction in blood vessel barrier integrity, an increased incidence of streptozotocin-induced diabetes, and islets isolated from Dsg2lo/lo mice were more susceptible to cytokine-induced β-cell apoptosis. Following transplantation into diabetic mice, islets isolated from Dsg2lo/lo mice were less effective than their wildtype counterparts at curing diabetes. In vitro assays using the Beta-TC-6 murine β-cell line suggest that DSG2 supports the actin cytoskeleton as well as the release of cytokines and chemokines. Taken together, our study suggests that DSG2 is an under-appreciated regulator of β-cell function in pancreatic islets and that a better understanding of this adhesion molecule may provide new opportunities to combat type 1 diabetes.",

author = "\{Myo Min\}, \{Kay K.\} and Darling Rojas-Canales and Daniella Penko and Mark DeNichilo and Cockshell, \{Michaelia P.\} and Ffrench, \{Charlie B.\} and Thompson, \{Emma J.\} and Olof Asplund and Drogemuller, \{Christopher J.\} and Prasad, \{Rashmi B.\} and Leif Groop and Grey, \{Shane T.\} and Thomas, \{Helen E.\} and Thomas Loudovaris and Kay, \{Thomas W.\} and Mahoney, \{My G.\} and Jessup, \{Claire F.\} and Coates, \{P. Toby\} and Bonder, \{Claudine S.\}",

note = "Publisher Copyright: {\textcopyright} 2022, The Author(s).",

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doi = "10.1038/s41419-022-05326-2",

language = "English (US)",

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AU - Myo Min, Kay K.

AU - Rojas-Canales, Darling

AU - Penko, Daniella

AU - DeNichilo, Mark

AU - Cockshell, Michaelia P.

AU - Ffrench, Charlie B.

AU - Thompson, Emma J.

AU - Asplund, Olof

AU - Drogemuller, Christopher J.

AU - Prasad, Rashmi B.

AU - Groop, Leif

AU - Grey, Shane T.

AU - Thomas, Helen E.

AU - Loudovaris, Thomas

AU - Kay, Thomas W.

AU - Mahoney, My G.

AU - Jessup, Claire F.

AU - Coates, P. Toby

AU - Bonder, Claudine S.

PY - 2022/10

Y1 - 2022/10

N2 - Type 1 diabetes is a complex disease characterized by the lack of endogenous insulin secreted from the pancreatic β-cells. Although β-cell targeted autoimmune processes and β-cell dysfunction are known to occur in type 1 diabetes, a complete understanding of the cell-to-cell interactions that support pancreatic function is still lacking. To characterize the pancreatic endocrine compartment, we studied pancreata from healthy adult donors and investigated a single cell surface adhesion molecule, desmoglein-2 (DSG2). Genetically-modified mice lacking Dsg2 were examined for islet cell mass, insulin production, responses to glucose, susceptibility to a streptozotocin-induced mouse model of hyperglycaemia, and ability to cure diabetes in a syngeneic transplantation model. Herein, we have identified DSG2 as a previously unrecognized adhesion molecule that supports β-cells. Furthermore, we reveal that DSG2 is within the top 10 percent of all genes expressed by human pancreatic islets and is expressed by the insulin-producing β-cells but not the somatostatin-producing δ-cells. In a Dsg2 loss-of-function mice (Dsg2lo/lo), we observed a significant reduction in the number of pancreatic islets and islet size, and consequently, there was less total insulin content per islet cluster. Dsg2lo/lo mice also exhibited a reduction in blood vessel barrier integrity, an increased incidence of streptozotocin-induced diabetes, and islets isolated from Dsg2lo/lo mice were more susceptible to cytokine-induced β-cell apoptosis. Following transplantation into diabetic mice, islets isolated from Dsg2lo/lo mice were less effective than their wildtype counterparts at curing diabetes. In vitro assays using the Beta-TC-6 murine β-cell line suggest that DSG2 supports the actin cytoskeleton as well as the release of cytokines and chemokines. Taken together, our study suggests that DSG2 is an under-appreciated regulator of β-cell function in pancreatic islets and that a better understanding of this adhesion molecule may provide new opportunities to combat type 1 diabetes.

AB - Type 1 diabetes is a complex disease characterized by the lack of endogenous insulin secreted from the pancreatic β-cells. Although β-cell targeted autoimmune processes and β-cell dysfunction are known to occur in type 1 diabetes, a complete understanding of the cell-to-cell interactions that support pancreatic function is still lacking. To characterize the pancreatic endocrine compartment, we studied pancreata from healthy adult donors and investigated a single cell surface adhesion molecule, desmoglein-2 (DSG2). Genetically-modified mice lacking Dsg2 were examined for islet cell mass, insulin production, responses to glucose, susceptibility to a streptozotocin-induced mouse model of hyperglycaemia, and ability to cure diabetes in a syngeneic transplantation model. Herein, we have identified DSG2 as a previously unrecognized adhesion molecule that supports β-cells. Furthermore, we reveal that DSG2 is within the top 10 percent of all genes expressed by human pancreatic islets and is expressed by the insulin-producing β-cells but not the somatostatin-producing δ-cells. In a Dsg2 loss-of-function mice (Dsg2lo/lo), we observed a significant reduction in the number of pancreatic islets and islet size, and consequently, there was less total insulin content per islet cluster. Dsg2lo/lo mice also exhibited a reduction in blood vessel barrier integrity, an increased incidence of streptozotocin-induced diabetes, and islets isolated from Dsg2lo/lo mice were more susceptible to cytokine-induced β-cell apoptosis. Following transplantation into diabetic mice, islets isolated from Dsg2lo/lo mice were less effective than their wildtype counterparts at curing diabetes. In vitro assays using the Beta-TC-6 murine β-cell line suggest that DSG2 supports the actin cytoskeleton as well as the release of cytokines and chemokines. Taken together, our study suggests that DSG2 is an under-appreciated regulator of β-cell function in pancreatic islets and that a better understanding of this adhesion molecule may provide new opportunities to combat type 1 diabetes.

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JO - Cell Death and Disease

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Desmoglein-2 is important for islet function and β-cell survival

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