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Generating low immunogenic pig pancreatic islet cell clusters for xenotransplantation

Xenotransplantation of pancreatic islets offers a promising alternative to overcome the shortage of allogeneic donors. Despite significant advances, either immune rejection or oxygen supply in immune protected encapsulated islets remains major bottlenecks for clinical application. To decrease xenoge...

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Autores principales: Carvalho Oliveira, Marco, Valdivia, Emilio, Verboom, Murielle, Yuzefovych, Yuliia, Sake, Hendrik Johannes, Pogozhykh, Olena, Niemann, Heiner, Schwinzer, Reinhard, Petersen, Björn, Seissler, Jochen, Blasczyk, Rainer, Figueiredo, Constança
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7205796/
https://www.ncbi.nlm.nih.gov/pubmed/32212307
http://dx.doi.org/10.1111/jcmm.15136
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author Carvalho Oliveira, Marco
Valdivia, Emilio
Verboom, Murielle
Yuzefovych, Yuliia
Sake, Hendrik Johannes
Pogozhykh, Olena
Niemann, Heiner
Schwinzer, Reinhard
Petersen, Björn
Seissler, Jochen
Blasczyk, Rainer
Figueiredo, Constança
author_facet Carvalho Oliveira, Marco
Valdivia, Emilio
Verboom, Murielle
Yuzefovych, Yuliia
Sake, Hendrik Johannes
Pogozhykh, Olena
Niemann, Heiner
Schwinzer, Reinhard
Petersen, Björn
Seissler, Jochen
Blasczyk, Rainer
Figueiredo, Constança
author_sort Carvalho Oliveira, Marco
collection PubMed
description Xenotransplantation of pancreatic islets offers a promising alternative to overcome the shortage of allogeneic donors. Despite significant advances, either immune rejection or oxygen supply in immune protected encapsulated islets remains major bottlenecks for clinical application. To decrease xenogeneic immune responses, we generated tissue engineered swine leucocyte antigen (SLA)‐silenced islet cell clusters (ICC). Single‐cell suspensions from pancreatic islets were generated by enzymatic digestion of porcine ICCs. Cells were silenced for SLA class I and class II by lentiviral vectors encoding for short hairpin RNAs targeting beta2‐microglobulin or class II transactivator, respectively. SLA‐silenced ICCs‐derived cells were then used to form new ICCs in stirred bioreactors in the presence of collagen VI. SLA class I silencing was designed to reach a level of up to 89% and class II by up to 81% on ICCs‐derived cells. Xenogeneic T cell immune responses, NK cell and antibody‐mediated cellular‐dependent immune responses were significantly decreased in SLA‐silenced cells. In stirred bioreactors, tissue engineered islets showed the typical 3D structure and insulin production. These data show the feasibility to generate low immunogenic porcine ICCs after single‐cell engineering and post‐transduction islet reassembling that might serve as an alternative to allogeneic pancreatic islet cell transplantation.
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spelling pubmed-72057962020-05-11 Generating low immunogenic pig pancreatic islet cell clusters for xenotransplantation Carvalho Oliveira, Marco Valdivia, Emilio Verboom, Murielle Yuzefovych, Yuliia Sake, Hendrik Johannes Pogozhykh, Olena Niemann, Heiner Schwinzer, Reinhard Petersen, Björn Seissler, Jochen Blasczyk, Rainer Figueiredo, Constança J Cell Mol Med Original Articles Xenotransplantation of pancreatic islets offers a promising alternative to overcome the shortage of allogeneic donors. Despite significant advances, either immune rejection or oxygen supply in immune protected encapsulated islets remains major bottlenecks for clinical application. To decrease xenogeneic immune responses, we generated tissue engineered swine leucocyte antigen (SLA)‐silenced islet cell clusters (ICC). Single‐cell suspensions from pancreatic islets were generated by enzymatic digestion of porcine ICCs. Cells were silenced for SLA class I and class II by lentiviral vectors encoding for short hairpin RNAs targeting beta2‐microglobulin or class II transactivator, respectively. SLA‐silenced ICCs‐derived cells were then used to form new ICCs in stirred bioreactors in the presence of collagen VI. SLA class I silencing was designed to reach a level of up to 89% and class II by up to 81% on ICCs‐derived cells. Xenogeneic T cell immune responses, NK cell and antibody‐mediated cellular‐dependent immune responses were significantly decreased in SLA‐silenced cells. In stirred bioreactors, tissue engineered islets showed the typical 3D structure and insulin production. These data show the feasibility to generate low immunogenic porcine ICCs after single‐cell engineering and post‐transduction islet reassembling that might serve as an alternative to allogeneic pancreatic islet cell transplantation. John Wiley and Sons Inc. 2020-03-25 2020-05 /pmc/articles/PMC7205796/ /pubmed/32212307 http://dx.doi.org/10.1111/jcmm.15136 Text en © 2020 The Authors. Journal of Cellular and Molecular Medicine published by Foundation for Cellular and Molecular Medicine and John Wiley & Sons Ltd. This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Articles
Carvalho Oliveira, Marco
Valdivia, Emilio
Verboom, Murielle
Yuzefovych, Yuliia
Sake, Hendrik Johannes
Pogozhykh, Olena
Niemann, Heiner
Schwinzer, Reinhard
Petersen, Björn
Seissler, Jochen
Blasczyk, Rainer
Figueiredo, Constança
Generating low immunogenic pig pancreatic islet cell clusters for xenotransplantation
title Generating low immunogenic pig pancreatic islet cell clusters for xenotransplantation
title_full Generating low immunogenic pig pancreatic islet cell clusters for xenotransplantation
title_fullStr Generating low immunogenic pig pancreatic islet cell clusters for xenotransplantation
title_full_unstemmed Generating low immunogenic pig pancreatic islet cell clusters for xenotransplantation
title_short Generating low immunogenic pig pancreatic islet cell clusters for xenotransplantation
title_sort generating low immunogenic pig pancreatic islet cell clusters for xenotransplantation
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7205796/
https://www.ncbi.nlm.nih.gov/pubmed/32212307
http://dx.doi.org/10.1111/jcmm.15136
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