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[title] => [First signature of islet beta-cell-derived naturally processed peptides selected by diabetogenic class II MHC molecules.]
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<div class="biblio_authors"><h3>Authors:</h3> <a href="/biblio/author/Suri+A">Suri A , Walters JJ , Rohrs HW , Gross ML , Unanue ER ,</a></div>
<div class="biblio_source"><h3>Source: </h3> Journal of immunology (Baltimore, Md. : 1950), Volume 180, p.3849-56 (2008)</div>
<h3>URL:</h3><a href="http://www.jimmunol.org/cgi/pmidlookup?view=long&pmid=18322192">http://www.jimmunol.org/cgi/pmidlookup?view=long&pmid=18322192</a>
<h3>Abstract:</h3> <p>The diversity of Ags targeted by T cells in autoimmune diabetes is unknown. In this study, we identify and characterize a limited number of naturally processed peptides from pancreatic islet beta-cells selected by diabetogenic I-A(g7) molecules of NOD mice. We used insulinomas transfected with the CIITA transactivator, which resulted in their expression of class II histocompatibility molecules and activation of diabetogenic CD4 T cells. Peptides bound to I-A(g7) were isolated and examined by mass spectrometry: some peptides derived from proteins present in secretory granules of endocrine cells, and a number were shared with cells of neuronal lineage. All proteins to which peptides were identified were expressed in beta cells from normal islets. Peptides bound to I-A(g7) molecules contained the favorable binding motif characterized by acidic amino acids at the P9 position. The draining pancreatic lymph nodes of prediabetic NOD mice contained CD4 T cells that recognized three different natural peptides. Furthermore, four different peptides elicited CD4 T cells, substantiating the presence of such self-reactive T cells. The overall strategy of identifying natural peptides from islet beta-cells opens up new avenues to evaluate the repertoire of self-reactive T cells and its role in onset of diabetes.</p>
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[biblio_secondary_title] => [Journal of immunology (Baltimore, Md. : 1950)]
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[biblio_authors] => [Suri A , Walters JJ , Rohrs HW , Gross ML , Unanue ER ,]
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[biblio_abst_e] => [<p>The diversity of Ags targeted by T cells in autoimmune diabetes is unknown. In this study, we identify and characterize a limited number of naturally processed peptides from pancreatic islet beta-cells selected by diabetogenic I-A(g7) molecules of NOD mice. We used insulinomas transfected with the CIITA transactivator, which resulted in their expression of class II histocompatibility molecules and activation of diabetogenic CD4 T cells. Peptides bound to I-A(g7) were isolated and examined by mass spectrometry: some peptides derived from proteins present in secretory granules of endocrine cells, and a number were shared with cells of neuronal lineage. All proteins to which peptides were identified were expressed in beta cells from normal islets. Peptides bound to I-A(g7) molecules contained the favorable binding motif characterized by acidic amino acids at the P9 position. The draining pancreatic lymph nodes of prediabetic NOD mice contained CD4 T cells that recognized three different natural peptides. Furthermore, four different peptides elicited CD4 T cells, substantiating the presence of such self-reactive T cells. The overall strategy of identifying natural peptides from islet beta-cells opens up new avenues to evaluate the repertoire of self-reactive T cells and its role in onset of diabetes.</p>]
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<div class="biblio_authors"><h3>Authors:</h3> <a href="/biblio/author/Suri+A">Suri A , Walters JJ , Rohrs HW , Gross ML , Unanue ER ,</a></div>
<div class="biblio_source"><h3>Source: </h3> Journal of immunology (Baltimore, Md. : 1950), Volume 180, p.3849-56 (2008)</div>
<h3>URL:</h3><a href="http://www.jimmunol.org/cgi/pmidlookup?view=long&pmid=18322192">http://www.jimmunol.org/cgi/pmidlookup?view=long&pmid=18322192</a>
<h3>Abstract:</h3> <p>The diversity of Ags targeted by T cells in autoimmune diabetes is unknown. In this study, we identify and characterize a limited number of naturally processed peptides from pancreatic islet beta-cells selected by diabetogenic I-A(g7) molecules of NOD mice. We used insulinomas transfected with the CIITA transactivator, which resulted in their expression of class II histocompatibility molecules and activation of diabetogenic CD4 T cells. Peptides bound to I-A(g7) were isolated and examined by mass spectrometry: some peptides derived from proteins present in secretory granules of endocrine cells, and a number were shared with cells of neuronal lineage. All proteins to which peptides were identified were expressed in beta cells from normal islets. Peptides bound to I-A(g7) molecules contained the favorable binding motif characterized by acidic amino acids at the P9 position. The draining pancreatic lymph nodes of prediabetic NOD mice contained CD4 T cells that recognized three different natural peptides. Furthermore, four different peptides elicited CD4 T cells, substantiating the presence of such self-reactive T cells. The overall strategy of identifying natural peptides from islet beta-cells opens up new avenues to evaluate the repertoire of self-reactive T cells and its role in onset of diabetes.</p>
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<div class="biblio_authors"><h3>Authors:</h3> <a href="/biblio/author/Suri+A">Suri A , Walters JJ , Rohrs HW , Gross ML , Unanue ER ,</a></div>
<div class="biblio_source"><h3>Source: </h3> Journal of immunology (Baltimore, Md. : 1950), Volume 180, p.3849-56 (2008)</div>
<h3>URL:</h3><a href="http://www.jimmunol.org/cgi/pmidlookup?view=long&pmid=18322192">http://www.jimmunol.org/cgi/pmidlookup?view=long&pmid=18322192</a>
<h3>Abstract:</h3> <p>The diversity of Ags targeted by T cells in autoimmune diabetes is unknown. In this study, we identify and characterize a limited number of naturally processed peptides from pancreatic islet beta-cells selected by diabetogenic I-A(g7) molecules of NOD mice. We used insulinomas transfected with the CIITA transactivator, which resulted in their expression of class II histocompatibility molecules and activation of diabetogenic CD4 T cells. Peptides bound to I-A(g7) were isolated and examined by mass spectrometry: some peptides derived from proteins present in secretory granules of endocrine cells, and a number were shared with cells of neuronal lineage. All proteins to which peptides were identified were expressed in beta cells from normal islets. Peptides bound to I-A(g7) molecules contained the favorable binding motif characterized by acidic amino acids at the P9 position. The draining pancreatic lymph nodes of prediabetic NOD mice contained CD4 T cells that recognized three different natural peptides. Furthermore, four different peptides elicited CD4 T cells, substantiating the presence of such self-reactive T cells. The overall strategy of identifying natural peptides from islet beta-cells opens up new avenues to evaluate the repertoire of self-reactive T cells and its role in onset of diabetes.</p>
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