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Embryonic Pig Pancreatic Tissue Transplantation for the Treatment of Diabetes

BACKGROUND: Transplantation of embryonic pig pancreatic tissue as a source of insulin has been suggested for the cure of diabetes. However, previous limited clinical trials failed in their attempts to treat diabetic patients by transplantation of advanced gestational age porcine embryonic pancreas....

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Autores principales: Eventov-Friedman, Smadar, Tchorsh, Dalit, Katchman, Helena, Shezen, Elias, Aronovich, Anna, Hecht, Gil, Dekel, Benjamin, Rechavi, Gideon, Blazar, Bruce R, Feine, Ilan, Tal, Orna, Freud, Enrique, Reisner, Yair
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2006
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1479387/
https://www.ncbi.nlm.nih.gov/pubmed/16768546
http://dx.doi.org/10.1371/journal.pmed.0030215
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author Eventov-Friedman, Smadar
Tchorsh, Dalit
Katchman, Helena
Shezen, Elias
Aronovich, Anna
Hecht, Gil
Dekel, Benjamin
Rechavi, Gideon
Blazar, Bruce R
Feine, Ilan
Tal, Orna
Freud, Enrique
Reisner, Yair
author_facet Eventov-Friedman, Smadar
Tchorsh, Dalit
Katchman, Helena
Shezen, Elias
Aronovich, Anna
Hecht, Gil
Dekel, Benjamin
Rechavi, Gideon
Blazar, Bruce R
Feine, Ilan
Tal, Orna
Freud, Enrique
Reisner, Yair
author_sort Eventov-Friedman, Smadar
collection PubMed
description BACKGROUND: Transplantation of embryonic pig pancreatic tissue as a source of insulin has been suggested for the cure of diabetes. However, previous limited clinical trials failed in their attempts to treat diabetic patients by transplantation of advanced gestational age porcine embryonic pancreas. In the present study we examined growth potential, functionality, and immunogenicity of pig embryonic pancreatic tissue harvested at different gestational ages. METHODS AND FINDINGS: Implantation of embryonic pig pancreatic tissues of different gestational ages in SCID mice reveals that embryonic day 42 (E42) pig pancreas can enable a massive growth of pig islets for prolonged periods and restore normoglycemia in diabetic mice. Furthermore, both direct and indirect T cell rejection responses to the xenogeneic tissue demonstrated that E42 tissue, in comparison to E56 or later embryonic tissues, exhibits markedly reduced immunogenicity. Finally, fully immunocompetent diabetic mice grafted with the E42 pig pancreatic tissue and treated with an immunosuppression protocol comprising CTLA4-Ig and anti–CD40 ligand (anti-CD40L) attained normal blood glucose levels, eliminating the need for insulin. CONCLUSIONS: These results emphasize the importance of selecting embryonic tissue of the correct gestational age for optimal growth and function and for reduced immunogenicity, and provide a proof of principle for the therapeutic potential of E42 embryonic pig pancreatic tissue transplantation in diabetes.
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spelling pubmed-14793872006-07-18 Embryonic Pig Pancreatic Tissue Transplantation for the Treatment of Diabetes Eventov-Friedman, Smadar Tchorsh, Dalit Katchman, Helena Shezen, Elias Aronovich, Anna Hecht, Gil Dekel, Benjamin Rechavi, Gideon Blazar, Bruce R Feine, Ilan Tal, Orna Freud, Enrique Reisner, Yair PLoS Med Research Article BACKGROUND: Transplantation of embryonic pig pancreatic tissue as a source of insulin has been suggested for the cure of diabetes. However, previous limited clinical trials failed in their attempts to treat diabetic patients by transplantation of advanced gestational age porcine embryonic pancreas. In the present study we examined growth potential, functionality, and immunogenicity of pig embryonic pancreatic tissue harvested at different gestational ages. METHODS AND FINDINGS: Implantation of embryonic pig pancreatic tissues of different gestational ages in SCID mice reveals that embryonic day 42 (E42) pig pancreas can enable a massive growth of pig islets for prolonged periods and restore normoglycemia in diabetic mice. Furthermore, both direct and indirect T cell rejection responses to the xenogeneic tissue demonstrated that E42 tissue, in comparison to E56 or later embryonic tissues, exhibits markedly reduced immunogenicity. Finally, fully immunocompetent diabetic mice grafted with the E42 pig pancreatic tissue and treated with an immunosuppression protocol comprising CTLA4-Ig and anti–CD40 ligand (anti-CD40L) attained normal blood glucose levels, eliminating the need for insulin. CONCLUSIONS: These results emphasize the importance of selecting embryonic tissue of the correct gestational age for optimal growth and function and for reduced immunogenicity, and provide a proof of principle for the therapeutic potential of E42 embryonic pig pancreatic tissue transplantation in diabetes. Public Library of Science 2006-07 2006-06-20 /pmc/articles/PMC1479387/ /pubmed/16768546 http://dx.doi.org/10.1371/journal.pmed.0030215 Text en Copyright: © 2006 Eventov-Friedman et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Eventov-Friedman, Smadar
Tchorsh, Dalit
Katchman, Helena
Shezen, Elias
Aronovich, Anna
Hecht, Gil
Dekel, Benjamin
Rechavi, Gideon
Blazar, Bruce R
Feine, Ilan
Tal, Orna
Freud, Enrique
Reisner, Yair
Embryonic Pig Pancreatic Tissue Transplantation for the Treatment of Diabetes
title Embryonic Pig Pancreatic Tissue Transplantation for the Treatment of Diabetes
title_full Embryonic Pig Pancreatic Tissue Transplantation for the Treatment of Diabetes
title_fullStr Embryonic Pig Pancreatic Tissue Transplantation for the Treatment of Diabetes
title_full_unstemmed Embryonic Pig Pancreatic Tissue Transplantation for the Treatment of Diabetes
title_short Embryonic Pig Pancreatic Tissue Transplantation for the Treatment of Diabetes
title_sort embryonic pig pancreatic tissue transplantation for the treatment of diabetes
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1479387/
https://www.ncbi.nlm.nih.gov/pubmed/16768546
http://dx.doi.org/10.1371/journal.pmed.0030215
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