Spectratyping analysis of the islet-reactive T cell repertoire in diabetic NOD Igμ(null )mice after polyclonal B cell reconstitution

BACKGROUND: Non Obese Diabetic mice lacking B cells (NOD.Igμ(null )mice) do not develop diabetes despite their susceptible background. Upon reconstitution of B cells using a chimera approach, animals start developing diabetes at 20 weeks of age. METHODS: We have used the spectratyping technique to f...

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Autores principales: Vong, Allen M, Daneshjou, Nazila, Norori, Patricia Y, Sheng, Huiming, Braciak, Todd A, Sercarz, Eli E, Gabaglia, Claudia Raja
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2011
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3141497/
https://www.ncbi.nlm.nih.gov/pubmed/21722394
http://dx.doi.org/10.1186/1479-5876-9-101
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author Vong, Allen M
Daneshjou, Nazila
Norori, Patricia Y
Sheng, Huiming
Braciak, Todd A
Sercarz, Eli E
Gabaglia, Claudia Raja
author_facet Vong, Allen M
Daneshjou, Nazila
Norori, Patricia Y
Sheng, Huiming
Braciak, Todd A
Sercarz, Eli E
Gabaglia, Claudia Raja
author_sort Vong, Allen M
collection PubMed
description BACKGROUND: Non Obese Diabetic mice lacking B cells (NOD.Igμ(null )mice) do not develop diabetes despite their susceptible background. Upon reconstitution of B cells using a chimera approach, animals start developing diabetes at 20 weeks of age. METHODS: We have used the spectratyping technique to follow the T cell receptor (TCR) V beta repertoire of NOD.Igμ(null )mice following B cell reconstitution. This technique provides an unbiased approach to understand the kinetics of TCR expansion. We have also analyzed the TCR repertoire of reconstituted animals receiving cyclophosphamide treatment and following tissue transplants to identify common aggressive clonotypes. RESULTS: We found that B cell reconstitution of NOD.Igμ(null )mice induces a polyclonal TCR repertoire in the pancreas 10 weeks later, gradually diversifying to encompass most BV families. Interestingly, these clonotypic BV expansions are mainly confined to the pancreas and are absent from pancreatic lymph nodes or spleens. Cyclophosphamide-induced diabetes at 10 weeks post-B cell reconstitution reorganized the predominant TCR repertoires by removing potential regulatory clonotypes (BV1, BV8 and BV11) and increasing the frequency of others (BV4, BV5S2, BV9, BV16-20). These same clonotypes are more frequently present in neonatal pancreatic transplants under the kidney capsule of B-cell reconstituted diabetic NOD.Igμ(null )mice, suggesting their higher invasiveness. Phenotypic analysis of the pancreas-infiltrating lymphocytes during diabetes onset in B cell reconstituted animals show a predominance of CD19(+ )B cells with a B:T lymphocyte ratio of 4:1. In contrast, in other lymphoid organs (pancreatic lymph nodes and spleens) analyzed by FACS, the B:T ratio was 1:1. Lymphocytes infiltrating the pancreas secrete large amounts of IL-6 and are of Th1 phenotype after CD3-CD28 stimulation in vitro. CONCLUSIONS: Diabetes in NOD.Igμ(null )mice appears to be caused by a polyclonal repertoire of T cell accumulation in pancreas without much lymphoid organ involvement and is dependent on the help by B cells.
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spelling pubmed-31414972011-07-23 Spectratyping analysis of the islet-reactive T cell repertoire in diabetic NOD Igμ(null )mice after polyclonal B cell reconstitution Vong, Allen M Daneshjou, Nazila Norori, Patricia Y Sheng, Huiming Braciak, Todd A Sercarz, Eli E Gabaglia, Claudia Raja J Transl Med Research BACKGROUND: Non Obese Diabetic mice lacking B cells (NOD.Igμ(null )mice) do not develop diabetes despite their susceptible background. Upon reconstitution of B cells using a chimera approach, animals start developing diabetes at 20 weeks of age. METHODS: We have used the spectratyping technique to follow the T cell receptor (TCR) V beta repertoire of NOD.Igμ(null )mice following B cell reconstitution. This technique provides an unbiased approach to understand the kinetics of TCR expansion. We have also analyzed the TCR repertoire of reconstituted animals receiving cyclophosphamide treatment and following tissue transplants to identify common aggressive clonotypes. RESULTS: We found that B cell reconstitution of NOD.Igμ(null )mice induces a polyclonal TCR repertoire in the pancreas 10 weeks later, gradually diversifying to encompass most BV families. Interestingly, these clonotypic BV expansions are mainly confined to the pancreas and are absent from pancreatic lymph nodes or spleens. Cyclophosphamide-induced diabetes at 10 weeks post-B cell reconstitution reorganized the predominant TCR repertoires by removing potential regulatory clonotypes (BV1, BV8 and BV11) and increasing the frequency of others (BV4, BV5S2, BV9, BV16-20). These same clonotypes are more frequently present in neonatal pancreatic transplants under the kidney capsule of B-cell reconstituted diabetic NOD.Igμ(null )mice, suggesting their higher invasiveness. Phenotypic analysis of the pancreas-infiltrating lymphocytes during diabetes onset in B cell reconstituted animals show a predominance of CD19(+ )B cells with a B:T lymphocyte ratio of 4:1. In contrast, in other lymphoid organs (pancreatic lymph nodes and spleens) analyzed by FACS, the B:T ratio was 1:1. Lymphocytes infiltrating the pancreas secrete large amounts of IL-6 and are of Th1 phenotype after CD3-CD28 stimulation in vitro. CONCLUSIONS: Diabetes in NOD.Igμ(null )mice appears to be caused by a polyclonal repertoire of T cell accumulation in pancreas without much lymphoid organ involvement and is dependent on the help by B cells. BioMed Central 2011-07-02 /pmc/articles/PMC3141497/ /pubmed/21722394 http://dx.doi.org/10.1186/1479-5876-9-101 Text en Copyright ©2011 Vong et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Vong, Allen M
Daneshjou, Nazila
Norori, Patricia Y
Sheng, Huiming
Braciak, Todd A
Sercarz, Eli E
Gabaglia, Claudia Raja
Spectratyping analysis of the islet-reactive T cell repertoire in diabetic NOD Igμ(null )mice after polyclonal B cell reconstitution
title Spectratyping analysis of the islet-reactive T cell repertoire in diabetic NOD Igμ(null )mice after polyclonal B cell reconstitution
title_full Spectratyping analysis of the islet-reactive T cell repertoire in diabetic NOD Igμ(null )mice after polyclonal B cell reconstitution
title_fullStr Spectratyping analysis of the islet-reactive T cell repertoire in diabetic NOD Igμ(null )mice after polyclonal B cell reconstitution
title_full_unstemmed Spectratyping analysis of the islet-reactive T cell repertoire in diabetic NOD Igμ(null )mice after polyclonal B cell reconstitution
title_short Spectratyping analysis of the islet-reactive T cell repertoire in diabetic NOD Igμ(null )mice after polyclonal B cell reconstitution
title_sort spectratyping analysis of the islet-reactive t cell repertoire in diabetic nod igμ(null )mice after polyclonal b cell reconstitution
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3141497/
https://www.ncbi.nlm.nih.gov/pubmed/21722394
http://dx.doi.org/10.1186/1479-5876-9-101
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