致糖尿病的 T 细胞识别与 IAg7 结合的胰岛素,结合方式出乎意料且亲和力较弱。
Diabetogenic T cells recognize insulin bound to IAg7 in an unexpected, weakly binding register.
机构信息
Integrated Department of Immunology, University of Colorado and National Jewish Health, Denver, CO 80206, USA.
出版信息
Proc Natl Acad Sci U S A. 2010 Jun 15;107(24):10978-83. doi: 10.1073/pnas.1006545107. Epub 2010 Jun 1.
Abstract
A peptide derived from the insulin B chain contains a major epitope for diabetogenic CD4(+) T cells in the NOD mouse model of type 1 diabetes (T1D). This peptide can fill the binding groove of the NOD MHCII molecule, IA(g7), in a number of ways or "registers." We show here that a diverse set of NOD anti-insulin T cells all recognize this peptide bound in the same register. Surprisingly, this register results in the poorest binding of peptide to IA(g7). The poor binding is due to an incompatibility between the p9 amino acid of the peptide and the unique IA(g7) p9 pocket polymorphisms that are strongly associated with susceptibility to T1D. Our findings suggest that the association of autoimmunity with particular MHCII alleles may be do to poorer, rather than more favorable, binding of the critical self-epitopes, allowing T-cell escape from thymic deletion.
摘要
从 1 型糖尿病(T1D)的 NOD 小鼠模型中的胰岛素 B 链衍生的肽含有针对致糖尿病 CD4(+)T 细胞的主要表位。该肽可以通过多种方式或“注册”填充 NOD MHCII 分子 IA(g7)的结合槽。我们在这里表明,一组不同的 NOD 抗胰岛素 T 细胞都识别结合在同一注册中的这种肽。令人惊讶的是,这种注册导致肽与 IA(g7)的结合最差。这种较差的结合是由于肽的 p9 氨基酸与强烈与 T1D 易感性相关的独特 IA(g7)p9 口袋多态性之间不兼容。我们的研究结果表明,自身免疫与特定 MHCII 等位基因的关联可能是由于关键自身表位的结合较差,而不是更有利,从而允许 T 细胞逃避胸腺删除。
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