Identification of a vimentin-expressing α-cell phenotype in CF and normal pancreas

Nicole Kattner; Yan Hang; Nicole A.J. Krentz; Lydia A. Russell; Matthew Palmer; Christine Flaxman; Nadine Plett; Rowan Coulthard; Yara Al-Selwi; Nicola Dyson; Minna Honkanen-Scott; Seung K. Kim; Dina Tiniakos; Günter Klöppel; Sarah J. Richardson; James A.M. Shaw

doi:10.1530/JOE-24-0190

Identification of a vimentin-expressing α-cell phenotype in CF and normal pancreas

Nicole Kattner
, Yan Hang
, Nicole A.J. Krentz
, Lydia A. Russell
, Matthew Palmer
, Christine Flaxman
, Nadine Plett
, Rowan Coulthard
, Yara Al-Selwi
, Nicola Dyson
, Minna Honkanen-Scott
, Seung K. Kim
, Dina Tiniakos
, Günter Klöppel
, Sarah J. Richardson
, James A.M. Shaw

Lehrstuhl für Pathologie

University of Newcastle upon Tyne
Stanford University School of Medicine
University of British Columbia
College of Medicine and Health
Royal Victoria Infirmary
Aretaieion University Hospital
Freeman Hospital

Publikation: Beitrag in Fachzeitschrift › Artikel › Begutachtung

4 Zitate (Scopus)

Abstract

Endocrine dysfunction and diabetes can develop secondary to fibrotic diseases within the pancreas, including cystic fibrosis (CF). A phenotypic shift within epithelial cells has been recognised in association with pro-fibrotic signalling. We sought evidence of endocrine cell epithelial-to-mesenchymal transition in CF and non-CF pancreas. Post-mortem pancreatic sections from 24 people with CF and 10 organ donors without CF or diabetes were stained for insulin/glucagon/vimentin and Sirius red/ fast green with collagen distribution assessed semi-quantitatively (CF) and quantitatively (non-CF). Analysis of existing single-cell RNA-sequencing datasets (three adult donors without diabetes and nine with chronic pancreatitis) for α-cell vimentin expression was performed. Cells co-expressing glucagon/vimentin were detected in a proportion (32(4,61)% (median (Q1,Q3))) of islets in all CF pancreata except donors dying perinatally. CF histopathology was characterised by peri-islet fibrosis, and 60(45,80)% of islets were surrounded by collagen strands. A positive correlation between islet fibrosis and vimentin-expressing α-cells was seen in non-CF donors <31 years (r = 0.972; P = 0.006). A possible association with donor age was seen in all donors (r = 0.343; P = 0.047). Single-cell RNA-sequencing analysis of isolated islets from non-diabetic donors and donors with chronic pancreatitis confirmed the presence of vimentin-positive and vimentin-negative α-cells. Differentiated α-cell function-associated gene expression was maintained. Differentially upregulated processes in co-expressing cells included pathways associated with extracellular matrix organisation, cell–cell adhesion, migratory capability and self-renewal. We have identified and characterised an intermediate epithelial/mesenchymal state in a sub-population of α-cells present throughout post-natal life, which may play a role in their response to extrinsic stressors, including fibrosis and ageing.

Originalsprache	Englisch
Aufsatznummer	e240190
Fachzeitschrift	Journal of Endocrinology
Jahrgang	264
Ausgabenummer	3
DOIs	https://doi.org/10.1530/JOE-24-0190
Publikationsstatus	Veröffentlicht - März 2025

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10.1530/JOE-24-0190

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Kattner, N., Hang, Y., Krentz, N. A. J., Russell, L. A., Palmer, M., Flaxman, C., Plett, N., Coulthard, R., Al-Selwi, Y., Dyson, N., Honkanen-Scott, M., Kim, S. K., Tiniakos, D., Klöppel, G., Richardson, S. J., & Shaw, J. A. M. (2025). Identification of a vimentin-expressing α-cell phenotype in CF and normal pancreas. Journal of Endocrinology, 264(3), Artikel e240190. https://doi.org/10.1530/JOE-24-0190

@article{cbb3fcae03534fcfba914e1d4dfeb0a1,

title = "Identification of a vimentin-expressing α-cell phenotype in CF and normal pancreas",

abstract = "Endocrine dysfunction and diabetes can develop secondary to fibrotic diseases within the pancreas, including cystic fibrosis (CF). A phenotypic shift within epithelial cells has been recognised in association with pro-fibrotic signalling. We sought evidence of endocrine cell epithelial-to-mesenchymal transition in CF and non-CF pancreas. Post-mortem pancreatic sections from 24 people with CF and 10 organ donors without CF or diabetes were stained for insulin/glucagon/vimentin and Sirius red/ fast green with collagen distribution assessed semi-quantitatively (CF) and quantitatively (non-CF). Analysis of existing single-cell RNA-sequencing datasets (three adult donors without diabetes and nine with chronic pancreatitis) for α-cell vimentin expression was performed. Cells co-expressing glucagon/vimentin were detected in a proportion (32(4,61)\% (median (Q1,Q3))) of islets in all CF pancreata except donors dying perinatally. CF histopathology was characterised by peri-islet fibrosis, and 60(45,80)\% of islets were surrounded by collagen strands. A positive correlation between islet fibrosis and vimentin-expressing α-cells was seen in non-CF donors <31 years (r = 0.972; P = 0.006). A possible association with donor age was seen in all donors (r = 0.343; P = 0.047). Single-cell RNA-sequencing analysis of isolated islets from non-diabetic donors and donors with chronic pancreatitis confirmed the presence of vimentin-positive and vimentin-negative α-cells. Differentiated α-cell function-associated gene expression was maintained. Differentially upregulated processes in co-expressing cells included pathways associated with extracellular matrix organisation, cell–cell adhesion, migratory capability and self-renewal. We have identified and characterised an intermediate epithelial/mesenchymal state in a sub-population of α-cells present throughout post-natal life, which may play a role in their response to extrinsic stressors, including fibrosis and ageing.",

keywords = "diabetes, histology, immunohistochemistry, inflammatory diseases, islet cells",

author = "Nicole Kattner and Yan Hang and Krentz, \{Nicole A.J.\} and Russell, \{Lydia A.\} and Matthew Palmer and Christine Flaxman and Nadine Plett and Rowan Coulthard and Yara Al-Selwi and Nicola Dyson and Minna Honkanen-Scott and Kim, \{Seung K.\} and Dina Tiniakos and G{\"u}nter Kl{\"o}ppel and Richardson, \{Sarah J.\} and Shaw, \{James A.M.\}",

note = "Publisher Copyright: {\textcopyright} 2025 the author(s)",

year = "2025",

month = mar,

doi = "10.1530/JOE-24-0190",

language = "English",

volume = "264",

journal = "Journal of Endocrinology",

issn = "0022-0795",

publisher = "BioScientifica Ltd.",

number = "3",

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Kattner, N, Hang, Y, Krentz, NAJ, Russell, LA, Palmer, M, Flaxman, C, Plett, N, Coulthard, R, Al-Selwi, Y, Dyson, N, Honkanen-Scott, M, Kim, SK, Tiniakos, D, Klöppel, G, Richardson, SJ & Shaw, JAM 2025, 'Identification of a vimentin-expressing α-cell phenotype in CF and normal pancreas', Journal of Endocrinology, Jg. 264, Nr. 3, e240190. https://doi.org/10.1530/JOE-24-0190

TY - JOUR

T1 - Identification of a vimentin-expressing α-cell phenotype in CF and normal pancreas

AU - Kattner, Nicole

AU - Hang, Yan

AU - Krentz, Nicole A.J.

AU - Russell, Lydia A.

AU - Palmer, Matthew

AU - Flaxman, Christine

AU - Plett, Nadine

AU - Coulthard, Rowan

AU - Al-Selwi, Yara

AU - Dyson, Nicola

AU - Honkanen-Scott, Minna

AU - Kim, Seung K.

AU - Tiniakos, Dina

AU - Klöppel, Günter

AU - Richardson, Sarah J.

AU - Shaw, James A.M.

PY - 2025/3

Y1 - 2025/3

N2 - Endocrine dysfunction and diabetes can develop secondary to fibrotic diseases within the pancreas, including cystic fibrosis (CF). A phenotypic shift within epithelial cells has been recognised in association with pro-fibrotic signalling. We sought evidence of endocrine cell epithelial-to-mesenchymal transition in CF and non-CF pancreas. Post-mortem pancreatic sections from 24 people with CF and 10 organ donors without CF or diabetes were stained for insulin/glucagon/vimentin and Sirius red/ fast green with collagen distribution assessed semi-quantitatively (CF) and quantitatively (non-CF). Analysis of existing single-cell RNA-sequencing datasets (three adult donors without diabetes and nine with chronic pancreatitis) for α-cell vimentin expression was performed. Cells co-expressing glucagon/vimentin were detected in a proportion (32(4,61)% (median (Q1,Q3))) of islets in all CF pancreata except donors dying perinatally. CF histopathology was characterised by peri-islet fibrosis, and 60(45,80)% of islets were surrounded by collagen strands. A positive correlation between islet fibrosis and vimentin-expressing α-cells was seen in non-CF donors <31 years (r = 0.972; P = 0.006). A possible association with donor age was seen in all donors (r = 0.343; P = 0.047). Single-cell RNA-sequencing analysis of isolated islets from non-diabetic donors and donors with chronic pancreatitis confirmed the presence of vimentin-positive and vimentin-negative α-cells. Differentiated α-cell function-associated gene expression was maintained. Differentially upregulated processes in co-expressing cells included pathways associated with extracellular matrix organisation, cell–cell adhesion, migratory capability and self-renewal. We have identified and characterised an intermediate epithelial/mesenchymal state in a sub-population of α-cells present throughout post-natal life, which may play a role in their response to extrinsic stressors, including fibrosis and ageing.

AB - Endocrine dysfunction and diabetes can develop secondary to fibrotic diseases within the pancreas, including cystic fibrosis (CF). A phenotypic shift within epithelial cells has been recognised in association with pro-fibrotic signalling. We sought evidence of endocrine cell epithelial-to-mesenchymal transition in CF and non-CF pancreas. Post-mortem pancreatic sections from 24 people with CF and 10 organ donors without CF or diabetes were stained for insulin/glucagon/vimentin and Sirius red/ fast green with collagen distribution assessed semi-quantitatively (CF) and quantitatively (non-CF). Analysis of existing single-cell RNA-sequencing datasets (three adult donors without diabetes and nine with chronic pancreatitis) for α-cell vimentin expression was performed. Cells co-expressing glucagon/vimentin were detected in a proportion (32(4,61)% (median (Q1,Q3))) of islets in all CF pancreata except donors dying perinatally. CF histopathology was characterised by peri-islet fibrosis, and 60(45,80)% of islets were surrounded by collagen strands. A positive correlation between islet fibrosis and vimentin-expressing α-cells was seen in non-CF donors <31 years (r = 0.972; P = 0.006). A possible association with donor age was seen in all donors (r = 0.343; P = 0.047). Single-cell RNA-sequencing analysis of isolated islets from non-diabetic donors and donors with chronic pancreatitis confirmed the presence of vimentin-positive and vimentin-negative α-cells. Differentiated α-cell function-associated gene expression was maintained. Differentially upregulated processes in co-expressing cells included pathways associated with extracellular matrix organisation, cell–cell adhesion, migratory capability and self-renewal. We have identified and characterised an intermediate epithelial/mesenchymal state in a sub-population of α-cells present throughout post-natal life, which may play a role in their response to extrinsic stressors, including fibrosis and ageing.

KW - diabetes

KW - histology

KW - immunohistochemistry

KW - inflammatory diseases

KW - islet cells

UR - https://www.scopus.com/pages/publications/85219500516

U2 - 10.1530/JOE-24-0190

DO - 10.1530/JOE-24-0190

M3 - Article

C2 - 39836539

AN - SCOPUS:85219500516

SN - 0022-0795

VL - 264

JO - Journal of Endocrinology

JF - Journal of Endocrinology

IS - 3

M1 - e240190

ER -

Identification of a vimentin-expressing α-cell phenotype in CF and normal pancreas

Abstract

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