Truncation of the class II beta-chain cytoplasmic domain influences the level of class II/invariant chain-derived peptide complexes.

机译：II类β链胞质结构域的截短影响II类/不变链衍生肽复合物的水平。

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Previous studies have established that antigen presenting cells (APC) expressing major histocompatibility complex class II beta chains with truncated cytoplasmic domains are impaired in their capacity to activate T cells. While it had been widely accepted that this impairment is due to a defect in class II cytoplasmic domain-dependent signal transduction, we recently generated transgenic mice expressing only truncated class II beta chains, and functional analyses of APC from these mice revealed signaling-independent defects in antigen presentation. Here, we demonstrate that T cells primed on such transgenic APC respond better to stimulation by APC expressing truncated beta chains than by wild-type APC. This finding suggests that APC expressing truncated class II beta chains are not inherently defective in their antigen presenting capacity but, rather, may differ from wild-type APC in the peptide antigens that they present. Indeed, analysis of the peptides bound to class II molecules isolated from normal and transgenic spleen cells revealed clear differences. Most notably, the level of class II-associated invariant chain-derived peptides (CLIP) is significantly reduced in cells expressing only truncated beta chains. Prior studies have established that CLIP and antigenic peptides compete for binding to class II molecules. Thus, our results suggest that the cytoplasmic domain of the class II beta chain affects antigen presentation by influencing the level of CLIP/class II complexes.

机译：先前的研究已经确定，表达具有截短的胞质结构域的主要组织相容性复合物II类β链的抗原呈递细胞（APC）激活T细胞的能力受到损害。虽然这种损伤是由于II类细胞质结构域依赖性信号转导的缺陷引起的，但我们最近产生了只表达截短的II类β链的转基因小鼠，对这些小鼠进行的APC功能分析显示了信号独立的缺陷在抗原呈递中。在这里，我们证明了在这种转基因APC上引发的T细胞对表达截短的β链的APC的刺激比对野生型APC的刺激反应更好。该发现表明表达APC的截短的II类β链在其抗原呈递能力上不是天生的缺陷，而是在它们呈递的肽抗原上可能不同于野生型APC。实际上，对与分离自正常和转基因脾细胞的II类分子结合的肽的分析显示出明显的差异。最值得注意的是，在仅表达截短的β链的细胞中，II类相关的不变链衍生肽（CLIP）的水平显着降低。先前的研究已经确定CLIP和抗原性肽竞争与II类分子的结合。因此，我们的结果表明II类β链的胞质结构域通过影响CLIP / II类复合物的水平来影响抗原呈递。

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期刊名称 Proceedings of the National Academy of Sciences of the United States of America
作者
S T Smiley; A Y Rudensky; L H Glimcher; M J Grusby;
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年(卷),期 1996(93),1
年度 1996
页码 241–244
总页数 4
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1. Truncation of the class II β-chain cytoplasmic domain influences the level of class II/invariant chain-derived peptide complexes [J] . Stephen T. Smiley, Alexander Y. Rudensky, Laurie H. Glimche Proceedings of the National Academy of Sciences of the United States of America . 1996,第1期

机译：II类β链胞质结构域的截断影响II类/不变链衍生肽复合物的水平
2. Binding of major histocompatibility complex class II to the invariant chain-derived peptide, CLIP, is regulated by allelic polymorphism in class II. [J] . A Sette, S Southwood, J Miller, The Journal of Experomental Medicine . 1995,第2期

机译：主要的组织相容性复合物II类与不变链衍生肽CLIP的结合受II类的等位基因多态性调控。
3. Variation in HLA-DM expression influences conversion of MHC class II alpha beta:class II-associated invariant chain peptide complexes to mature peptide-bound class II alpha beta dimers in a normal B cell line. [J] . Ramachandra L, Kovats S, Eastman S, The Journal of Immunology: Official Journal of the American Association of Immunologists . 1996,第6期

机译：HLA-DM表达的变化会影响正常B细胞系中MHC II类αβ：与II类相关的恒定链肽复合物向成熟肽结合的II类αββ二聚体的转化。
4. PEPTIDE ANALOGUES DERIVED FROM THE CYTOPLASMIC DOMAIN OF AIIBβ3 INTEGRIN RECEPTOR INHIBIT PLATELET AGGREGATION [C] . Vassiliki Koloka, Panagiotis Stathopoulos, Eugenia Panou-Pomonis the European Peptide Symposium . 2007

机译：衍生自AIIBβ3整联蛋白受体的细胞质结构域的肽类似物抑制血小板聚集
5. Defining the mechanism of MHC class II peptide editing by HLA-DM: I. HLA-DM recognizes the flexible conformation of major histocompatibility complex class II. II. Mapping the interaction surface of DR1 with DM by superantigen blocking. III. Determinati [D] . Chou, Chih-Ling. 2003

机译：定义HLA-DM编辑MHC II类肽的机制：I. HLA-DM识别II类主要组织相容性复合物的柔性构象。二。通过超抗原阻断作用绘制DR1与DM的相互作用表面。三，确定性
6. Binding of major histocompatibility complex class II to the invariant chain-derived peptide CLIP is regulated by allelic polymorphism in class II [O] . 1995

机译：主要组织相容性复合物II类与不变链衍生肽CLIP的结合受II类等位基因多态性的调节
7. Truncation of the class II beta-chain cytoplasmic domain influences the level of class II/invariant chain-derived peptide complexes. [O] . Smiley, S T, Rudensky, A Y, Glimcher, L H, 1996

机译：II类β链胞质结构域的截短影响II类/不变链衍生肽复合物的水平。
8. Small Peptide (CEL-1000) Derived from the Beta-Chain of the Human Major Histocompatibility Complex Class II Molecule Induces Complete Protection Against Malaria in an Antigen-Independent Manner [R] . Charoenvit, Y. , Brice, G. T. , Bacon, D. , 2004

机译：源自人类主要组织相容性复合物II类分子的β-链的小肽（CEL-1000）以抗原非依赖性方式诱导针对疟疾的完全保护

Truncation of the class II beta-chain cytoplasmic domain influences the level of class II/invariant chain-derived peptide complexes.

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