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Assessment of β-Cell Mass and α- and β-Cell Survival and Function by Arginine Stimulation in Human Autologous Islet Recipients

We used intravenous arginine with measurements of insulin, C-peptide, and glucagon to examine β-cell and α-cell survival and function in a group of 10 chronic pancreatitis recipients 1–8 years after total pancreatectomy and autoislet transplantation. Insulin and C-peptide responses correlated robust...

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Autores principales: Robertson, R. Paul, Bogachus, Lindsey D., Oseid, Elizabeth, Parazzoli, Susan, Patti, Mary Elizabeth, Rickels, Michael R., Schuetz, Christian, Dunn, Ty, Pruett, Timothy, Balamurugan, A.N., Sutherland, David E.R., Beilman, Gregory, Bellin, Melena D.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Diabetes Association 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4303963/
https://www.ncbi.nlm.nih.gov/pubmed/25187365
http://dx.doi.org/10.2337/db14-0690
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author Robertson, R. Paul
Bogachus, Lindsey D.
Oseid, Elizabeth
Parazzoli, Susan
Patti, Mary Elizabeth
Rickels, Michael R.
Schuetz, Christian
Dunn, Ty
Pruett, Timothy
Balamurugan, A.N.
Sutherland, David E.R.
Beilman, Gregory
Bellin, Melena D.
author_facet Robertson, R. Paul
Bogachus, Lindsey D.
Oseid, Elizabeth
Parazzoli, Susan
Patti, Mary Elizabeth
Rickels, Michael R.
Schuetz, Christian
Dunn, Ty
Pruett, Timothy
Balamurugan, A.N.
Sutherland, David E.R.
Beilman, Gregory
Bellin, Melena D.
author_sort Robertson, R. Paul
collection PubMed
description We used intravenous arginine with measurements of insulin, C-peptide, and glucagon to examine β-cell and α-cell survival and function in a group of 10 chronic pancreatitis recipients 1–8 years after total pancreatectomy and autoislet transplantation. Insulin and C-peptide responses correlated robustly with the number of islets transplanted (correlation coefficients range 0.81–0.91; P < 0.01–0.001). Since a wide range of islets were transplanted, we normalized the insulin and C-peptide responses to the number of islets transplanted in each recipient for comparison with responses in normal subjects. No significant differences were observed in terms of magnitude and timing of hormone release in the two groups. Three recipients had a portion of the autoislets placed within their peritoneal cavities, which appeared to be functioning normally up to 7 years posttransplant. Glucagon responses to arginine were normally timed and normally suppressed by intravenous glucose infusion. These findings indicate that arginine stimulation testing may be a means of assessing the numbers of native islets available in autologous islet transplant candidates and is a means of following posttransplant α- and β-cell function and survival.
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spelling pubmed-43039632016-01-31 Assessment of β-Cell Mass and α- and β-Cell Survival and Function by Arginine Stimulation in Human Autologous Islet Recipients Robertson, R. Paul Bogachus, Lindsey D. Oseid, Elizabeth Parazzoli, Susan Patti, Mary Elizabeth Rickels, Michael R. Schuetz, Christian Dunn, Ty Pruett, Timothy Balamurugan, A.N. Sutherland, David E.R. Beilman, Gregory Bellin, Melena D. Diabetes Immunology and Transplantation We used intravenous arginine with measurements of insulin, C-peptide, and glucagon to examine β-cell and α-cell survival and function in a group of 10 chronic pancreatitis recipients 1–8 years after total pancreatectomy and autoislet transplantation. Insulin and C-peptide responses correlated robustly with the number of islets transplanted (correlation coefficients range 0.81–0.91; P < 0.01–0.001). Since a wide range of islets were transplanted, we normalized the insulin and C-peptide responses to the number of islets transplanted in each recipient for comparison with responses in normal subjects. No significant differences were observed in terms of magnitude and timing of hormone release in the two groups. Three recipients had a portion of the autoislets placed within their peritoneal cavities, which appeared to be functioning normally up to 7 years posttransplant. Glucagon responses to arginine were normally timed and normally suppressed by intravenous glucose infusion. These findings indicate that arginine stimulation testing may be a means of assessing the numbers of native islets available in autologous islet transplant candidates and is a means of following posttransplant α- and β-cell function and survival. American Diabetes Association 2015-02 2014-09-02 /pmc/articles/PMC4303963/ /pubmed/25187365 http://dx.doi.org/10.2337/db14-0690 Text en © 2015 by the American Diabetes Association. Readers may use this article as long as the work is properly cited, the use is educational and not for profit, and the work is not altered.
spellingShingle Immunology and Transplantation
Robertson, R. Paul
Bogachus, Lindsey D.
Oseid, Elizabeth
Parazzoli, Susan
Patti, Mary Elizabeth
Rickels, Michael R.
Schuetz, Christian
Dunn, Ty
Pruett, Timothy
Balamurugan, A.N.
Sutherland, David E.R.
Beilman, Gregory
Bellin, Melena D.
Assessment of β-Cell Mass and α- and β-Cell Survival and Function by Arginine Stimulation in Human Autologous Islet Recipients
title Assessment of β-Cell Mass and α- and β-Cell Survival and Function by Arginine Stimulation in Human Autologous Islet Recipients
title_full Assessment of β-Cell Mass and α- and β-Cell Survival and Function by Arginine Stimulation in Human Autologous Islet Recipients
title_fullStr Assessment of β-Cell Mass and α- and β-Cell Survival and Function by Arginine Stimulation in Human Autologous Islet Recipients
title_full_unstemmed Assessment of β-Cell Mass and α- and β-Cell Survival and Function by Arginine Stimulation in Human Autologous Islet Recipients
title_short Assessment of β-Cell Mass and α- and β-Cell Survival and Function by Arginine Stimulation in Human Autologous Islet Recipients
title_sort assessment of β-cell mass and α- and β-cell survival and function by arginine stimulation in human autologous islet recipients
topic Immunology and Transplantation
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4303963/
https://www.ncbi.nlm.nih.gov/pubmed/25187365
http://dx.doi.org/10.2337/db14-0690
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