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請用此 Handle URI 來引用此文件: http://scholars.ntou.edu.tw/handle/123456789/18755
標題: Prediction of HLA-DQ8 β cell peptidome using a computational program and its relationship to autoreactive T cells
作者: Kuan Y. Chang 
Emil R. Unanue
關鍵字: HLA-DQ8;MHC class II molecules;T cell epitope prediction;type I diabetes mellitus
公開日期: 六月-2009
出版社: OXFORD ACADEMIC
卷: 21
期: 6
起(迄)頁: 705–713
來源出版物: International Immunology
摘要: 
The goal was to identify HLA-DQ8-bound β cell epitopes important in the T cell response in autoimmune diabetes. We first identified HLA-DQ8 (DQA1*0301/DQB1*0302) β cell epitopes using a computational approach and then related their identification to CD4 T cell responses. The computational program (TEA-DQ8) was adapted from one previously developed for identifying peptides bound to the I-Ag7 molecule and based on a library of naturally processed peptides bound to HLA-DQ8 molecules of antigen-presenting cells. We then examined experimentally the response of NOD.DQ8 mice immunized with peptides derived from the Zinc transporter 8 protein. Log-of-odds scores on peptides were experimentally validated as an indicator of peptide binding to HLA-DQ8 molecules. We also examined previously published data on diabetic autoantigens, including glutamic acid decarboxylase-65, insulin and insulinoma-associated antigen-2, all tested in NOD.DQ8 transgenic mice. In all examples, many peptides identified with a favorable binding motif generated an autoimmune T cell response, but importantly many did not. Moreover, some peptides with weak-binding motifs were immunogenic. These results indicate the benefits and limitations in predicting autoimmune T cell responses strictly from MHC-binding data. TEA-DQ8 performed significantly better than other prediction programs
URI: http://scholars.ntou.edu.tw/handle/123456789/18755
ISSN: 0953-8178
DOI: 10.1093/intimm/dxp039
://WOS:000266499800008
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