Transgenic substitution with Greater Amberjack Seriola dumerili fish insulin 2 in NOD mice reduces beta cell immunogenicity

Type I diabetes (T1D) is caused by immune-mediated destruction of pancreatic beta cells. This process is triggered, in part, by specific (aa 9–23) epitopes of the insulin Β chain. Previously, fish insulins were used clinically in patients allergic to bovine or porcine insulin. Fish and human insulin...

Descripción completa

Detalles Bibliográficos
Autores principales: Foo, Kylie S., Skowronski, Alicja A., Baum, Danielle, Firdessa-Fite, Rebuma, Thams, Sebastian, Shang, Linshan, Creusot, Rémi J., LeDuc, Charles A., Egli, Dieter, Leibel, Rudolph L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group UK 2019
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6428854/
https://www.ncbi.nlm.nih.gov/pubmed/30899071
http://dx.doi.org/10.1038/s41598-019-40768-3
_version_ 1783405469423894528
author Foo, Kylie S.
Skowronski, Alicja A.
Baum, Danielle
Firdessa-Fite, Rebuma
Thams, Sebastian
Shang, Linshan
Creusot, Rémi J.
LeDuc, Charles A.
Egli, Dieter
Leibel, Rudolph L.
author_facet Foo, Kylie S.
Skowronski, Alicja A.
Baum, Danielle
Firdessa-Fite, Rebuma
Thams, Sebastian
Shang, Linshan
Creusot, Rémi J.
LeDuc, Charles A.
Egli, Dieter
Leibel, Rudolph L.
author_sort Foo, Kylie S.
collection PubMed
description Type I diabetes (T1D) is caused by immune-mediated destruction of pancreatic beta cells. This process is triggered, in part, by specific (aa 9–23) epitopes of the insulin Β chain. Previously, fish insulins were used clinically in patients allergic to bovine or porcine insulin. Fish and human insulin differ by two amino acids in the critical immunogenic region (aa 9–23) of the B chain. We hypothesized that β cells synthesizing fish insulin would be less immunogenic in a mouse model of T1D. Transgenic NOD mice in which Greater Amberjack fish (Seriola dumerili) insulin was substituted for the insulin 2 gene were generated (mouse Ins1(−/−) mouse Ins2(−/−) fish Ins2(+/+)). In these mice, pancreatic islets remained free of autoimmune attack. To determine whether such reduction in immunogenicity is sufficient to protect β cells from autoimmunity upon transplantation, we transplanted fish Ins2 transgenic (expressing solely Seriola dumerili Ins2), NOD, or B16:A-dKO islets under the kidney capsules of 5 weeks old female NOD wildtype mice. The B:Y16A Β chain substitution has been previously shown to be protective of T1D in NOD mice. NOD mice receiving Seriola dumerili transgenic islet transplants showed a significant (p = 0.004) prolongation of their euglycemic period (by 6 weeks; up to 18 weeks of age) compared to un-manipulated female NOD (diabetes onset at 12 weeks of age) and those receiving B16:A-dKO islet transplants (diabetes onset at 12 weeks of age). These data support the concept that specific amino acid sequence modifications can reduce insulin immunogenicity. Additionally, our study shows that alteration of a single epitope is not sufficient to halt an ongoing autoimmune response. Which, and how many, T cell epitopes are required and suffice to perpetuate autoimmunity is currently unknown. Such studies may be useful to achieve host tolerance to β cells by inactivating key immunogenic epitopes of stem cell-derived β cells intended for transplantation.
format Online
Article
Text
id pubmed-6428854
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher Nature Publishing Group UK
record_format MEDLINE/PubMed
spelling pubmed-64288542019-03-28 Transgenic substitution with Greater Amberjack Seriola dumerili fish insulin 2 in NOD mice reduces beta cell immunogenicity Foo, Kylie S. Skowronski, Alicja A. Baum, Danielle Firdessa-Fite, Rebuma Thams, Sebastian Shang, Linshan Creusot, Rémi J. LeDuc, Charles A. Egli, Dieter Leibel, Rudolph L. Sci Rep Article Type I diabetes (T1D) is caused by immune-mediated destruction of pancreatic beta cells. This process is triggered, in part, by specific (aa 9–23) epitopes of the insulin Β chain. Previously, fish insulins were used clinically in patients allergic to bovine or porcine insulin. Fish and human insulin differ by two amino acids in the critical immunogenic region (aa 9–23) of the B chain. We hypothesized that β cells synthesizing fish insulin would be less immunogenic in a mouse model of T1D. Transgenic NOD mice in which Greater Amberjack fish (Seriola dumerili) insulin was substituted for the insulin 2 gene were generated (mouse Ins1(−/−) mouse Ins2(−/−) fish Ins2(+/+)). In these mice, pancreatic islets remained free of autoimmune attack. To determine whether such reduction in immunogenicity is sufficient to protect β cells from autoimmunity upon transplantation, we transplanted fish Ins2 transgenic (expressing solely Seriola dumerili Ins2), NOD, or B16:A-dKO islets under the kidney capsules of 5 weeks old female NOD wildtype mice. The B:Y16A Β chain substitution has been previously shown to be protective of T1D in NOD mice. NOD mice receiving Seriola dumerili transgenic islet transplants showed a significant (p = 0.004) prolongation of their euglycemic period (by 6 weeks; up to 18 weeks of age) compared to un-manipulated female NOD (diabetes onset at 12 weeks of age) and those receiving B16:A-dKO islet transplants (diabetes onset at 12 weeks of age). These data support the concept that specific amino acid sequence modifications can reduce insulin immunogenicity. Additionally, our study shows that alteration of a single epitope is not sufficient to halt an ongoing autoimmune response. Which, and how many, T cell epitopes are required and suffice to perpetuate autoimmunity is currently unknown. Such studies may be useful to achieve host tolerance to β cells by inactivating key immunogenic epitopes of stem cell-derived β cells intended for transplantation. Nature Publishing Group UK 2019-03-21 /pmc/articles/PMC6428854/ /pubmed/30899071 http://dx.doi.org/10.1038/s41598-019-40768-3 Text en © The Author(s) 2019 Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/.
spellingShingle Article
Foo, Kylie S.
Skowronski, Alicja A.
Baum, Danielle
Firdessa-Fite, Rebuma
Thams, Sebastian
Shang, Linshan
Creusot, Rémi J.
LeDuc, Charles A.
Egli, Dieter
Leibel, Rudolph L.
Transgenic substitution with Greater Amberjack Seriola dumerili fish insulin 2 in NOD mice reduces beta cell immunogenicity
title Transgenic substitution with Greater Amberjack Seriola dumerili fish insulin 2 in NOD mice reduces beta cell immunogenicity
title_full Transgenic substitution with Greater Amberjack Seriola dumerili fish insulin 2 in NOD mice reduces beta cell immunogenicity
title_fullStr Transgenic substitution with Greater Amberjack Seriola dumerili fish insulin 2 in NOD mice reduces beta cell immunogenicity
title_full_unstemmed Transgenic substitution with Greater Amberjack Seriola dumerili fish insulin 2 in NOD mice reduces beta cell immunogenicity
title_short Transgenic substitution with Greater Amberjack Seriola dumerili fish insulin 2 in NOD mice reduces beta cell immunogenicity
title_sort transgenic substitution with greater amberjack seriola dumerili fish insulin 2 in nod mice reduces beta cell immunogenicity
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6428854/
https://www.ncbi.nlm.nih.gov/pubmed/30899071
http://dx.doi.org/10.1038/s41598-019-40768-3
work_keys_str_mv AT fookylies transgenicsubstitutionwithgreateramberjackserioladumerilifishinsulin2innodmicereducesbetacellimmunogenicity
AT skowronskialicjaa transgenicsubstitutionwithgreateramberjackserioladumerilifishinsulin2innodmicereducesbetacellimmunogenicity
AT baumdanielle transgenicsubstitutionwithgreateramberjackserioladumerilifishinsulin2innodmicereducesbetacellimmunogenicity
AT firdessafiterebuma transgenicsubstitutionwithgreateramberjackserioladumerilifishinsulin2innodmicereducesbetacellimmunogenicity
AT thamssebastian transgenicsubstitutionwithgreateramberjackserioladumerilifishinsulin2innodmicereducesbetacellimmunogenicity
AT shanglinshan transgenicsubstitutionwithgreateramberjackserioladumerilifishinsulin2innodmicereducesbetacellimmunogenicity
AT creusotremij transgenicsubstitutionwithgreateramberjackserioladumerilifishinsulin2innodmicereducesbetacellimmunogenicity
AT leduccharlesa transgenicsubstitutionwithgreateramberjackserioladumerilifishinsulin2innodmicereducesbetacellimmunogenicity
AT eglidieter transgenicsubstitutionwithgreateramberjackserioladumerilifishinsulin2innodmicereducesbetacellimmunogenicity
AT leibelrudolphl transgenicsubstitutionwithgreateramberjackserioladumerilifishinsulin2innodmicereducesbetacellimmunogenicity

Ejemplares similares