The Impact of Potential Islet Precursor Cells on Islet Autotransplantation Outcomes

Islet autotransplant patients represent excellent subjects to assess the posttransplant impact of islet precursors, as chronic pancreatitis (CP) causes an elevation of ductal cells, pancreatic precursors cells, and hormone-positive acinar cells. The relationship between these cell types and autograf...

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Main Authors: M. A. Webb, J. J. Chen, S. C. Illouz, C. A. Pollard, B. Dennison, K. P. West, R. F. L. James, A. R. Dennison
Format: Article
Language:English
Published: SAGE Publishing 2013-06-01
Series:Cell Transplantation
Online Access:https://doi.org/10.3727/096368912X655046
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spelling doaj-08163d570622478d86028994e3300de52020-11-25T01:20:36ZengSAGE PublishingCell Transplantation0963-68971555-38922013-06-012210.3727/096368912X655046The Impact of Potential Islet Precursor Cells on Islet Autotransplantation OutcomesM. A. Webb0J. J. Chen1S. C. Illouz2C. A. Pollard3B. Dennison4K. P. West5R. F. L. James6A. R. Dennison7Department of Hepatobiliary Surgery, University Hospitals of Leicester, NHS Trust, Leicester General Hospital, Leicester, UKDepartment of Hepatobiliary Surgery, University Hospitals of Leicester, NHS Trust, Leicester General Hospital, Leicester, UKDepartment of Hepatobiliary Surgery, University Hospitals of Leicester, NHS Trust, Leicester General Hospital, Leicester, UKDepartment of Hepatobiliary Surgery, University Hospitals of Leicester, NHS Trust, Leicester General Hospital, Leicester, UKDepartment of Hepatobiliary Surgery, University Hospitals of Leicester, NHS Trust, Leicester General Hospital, Leicester, UKDepartment of Pathology, University Hospitals of Leicester, NHS Trust, Leicester General Hospital, Leicester, UKDepartment of Infection, Immunity and Inflammation, University of Leicester, Leicester, UKDepartment of Hepatobiliary Surgery, University Hospitals of Leicester, NHS Trust, Leicester General Hospital, Leicester, UKIslet autotransplant patients represent excellent subjects to assess the posttransplant impact of islet precursors, as chronic pancreatitis (CP) causes an elevation of ductal cells, pancreatic precursors cells, and hormone-positive acinar cells. The relationship between these cell types and autograft outcomes should be more apparent than would be the case in the context of an allograft program with confounding immunological variables. To improve diabetic control following total pancreatectomy for CP, nonpurified islets were autotransplanted into the liver. Pancreas specimens were recovered from 23 patients and stained for antigens including: insulin, glucagon, cytokeratin 19, cytokeratin 7, and PDX-1. In line with previous reports, the prevalence of ductal cells, non-islet endocrine cells and non-islet PDX-1-expressing cells was significantly higher in CP glands compared with normal pancreata. When correlating follow-up data (i.e., fasting and stimulated C-peptide/glucose levels and HbA1c%) with pancreas immunoreactivity, high levels of ductal cells, non-islet PDX-1-positive cells, and non-islet glucagon-positive cells were associated with superior outcomes, detectable up to 2 years posttransplant. To conclude, the acinar parenchyma and ductal epithelium of the CP pancreas show an upregulation of both endocrine and pre-endocrine cell types, which appear to have a positive effect on islet graft outcomes in autotransplantation setting.https://doi.org/10.3727/096368912X655046
collection DOAJ
language English
format Article
sources DOAJ
author M. A. Webb
J. J. Chen
S. C. Illouz
C. A. Pollard
B. Dennison
K. P. West
R. F. L. James
A. R. Dennison
spellingShingle M. A. Webb
J. J. Chen
S. C. Illouz
C. A. Pollard
B. Dennison
K. P. West
R. F. L. James
A. R. Dennison
The Impact of Potential Islet Precursor Cells on Islet Autotransplantation Outcomes
Cell Transplantation
author_facet M. A. Webb
J. J. Chen
S. C. Illouz
C. A. Pollard
B. Dennison
K. P. West
R. F. L. James
A. R. Dennison
author_sort M. A. Webb
title The Impact of Potential Islet Precursor Cells on Islet Autotransplantation Outcomes
title_short The Impact of Potential Islet Precursor Cells on Islet Autotransplantation Outcomes
title_full The Impact of Potential Islet Precursor Cells on Islet Autotransplantation Outcomes
title_fullStr The Impact of Potential Islet Precursor Cells on Islet Autotransplantation Outcomes
title_full_unstemmed The Impact of Potential Islet Precursor Cells on Islet Autotransplantation Outcomes
title_sort impact of potential islet precursor cells on islet autotransplantation outcomes
publisher SAGE Publishing
series Cell Transplantation
issn 0963-6897
1555-3892
publishDate 2013-06-01
description Islet autotransplant patients represent excellent subjects to assess the posttransplant impact of islet precursors, as chronic pancreatitis (CP) causes an elevation of ductal cells, pancreatic precursors cells, and hormone-positive acinar cells. The relationship between these cell types and autograft outcomes should be more apparent than would be the case in the context of an allograft program with confounding immunological variables. To improve diabetic control following total pancreatectomy for CP, nonpurified islets were autotransplanted into the liver. Pancreas specimens were recovered from 23 patients and stained for antigens including: insulin, glucagon, cytokeratin 19, cytokeratin 7, and PDX-1. In line with previous reports, the prevalence of ductal cells, non-islet endocrine cells and non-islet PDX-1-expressing cells was significantly higher in CP glands compared with normal pancreata. When correlating follow-up data (i.e., fasting and stimulated C-peptide/glucose levels and HbA1c%) with pancreas immunoreactivity, high levels of ductal cells, non-islet PDX-1-positive cells, and non-islet glucagon-positive cells were associated with superior outcomes, detectable up to 2 years posttransplant. To conclude, the acinar parenchyma and ductal epithelium of the CP pancreas show an upregulation of both endocrine and pre-endocrine cell types, which appear to have a positive effect on islet graft outcomes in autotransplantation setting.
url https://doi.org/10.3727/096368912X655046
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