Synthetic surfaces as artificial antigen presenting cells in the study of T cell receptor triggering and immunological synapse formation.

Irvine DJ; Doh J

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Synthetic surfaces as artificial antigen presenting cells in the study of T cell receptor triggering and immunological synapse formation.

机译：合成表面作为人工抗原呈递细胞在研究T细胞受体触发和免疫突触形成中的作用。

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T cell activation occurs when T cell receptors engage peptide-major histocompatibility complex (pMHC) molecules displayed on the surface of antigen presenting cells (APCs). Clustering of TCRs and other receptors in physical patterns at the T-APC interface forms a structure known as an immunological synapse (IS). Studies of the IS are challenging due to the cell-cell contact context of the governing interactions. Model surfaces as synthetic APCs have thus been developed, where the type, quantity, and physical arrangement of ligands displayed to T cells are precisely controlled. These model systems have provided important insights into the structure and function of the IS.

机译：当T细胞受体与抗原呈递细胞（APC）表面上显示的肽-主要组织相容性复合物（pMHC）分子结合时，就会发生T细胞活化。 TCR和其他受体在T-APC界面处以物理模式聚集，形成了一种称为免疫突触（IS）的结构。由于控制相互作用的细胞-细胞接触环境，对IS的研究具有挑战性。因此，已经开发出了作为合成APC的模型表面，可以精确控制展示给T细胞的配体的类型，数量和物理排列。这些模型系统为IS的结构和功能提供了重要的见识。

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来源
《Seminars in immunology》 |2007年第4期|共10页
作者
Irvine DJ; Doh J;
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原文格式 PDF
正文语种 eng
中图分类医学免疫学;
关键词
Receptors; Antigen; T-Cell; Antigen-Presenting Cells; structure; synaptogenesis; 受体; 抗原; T细胞; 抗原提呈细胞;

机译：Receptors;Antigen;T-Cell;Antigen-Presenting Cells;structure;synaptogenesis;受体;抗原;T细胞;抗原提呈细胞;

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1. Synthetic surfaces as artificial antigen presenting cells in the study of T cell receptor triggering and immunological synapse formation. [J] . Irvine DJ, Doh J Seminars in immunology . 2007,第4期

机译：合成表面作为人工抗原呈递细胞在研究T细胞受体触发和免疫突触形成中的作用。
2. Antithymocyte globulin impairs T-cell/antigen-presenting cell interaction: disruption of immunological synapse and conjugate formation. [J] . Haidinger M, Geyeregger R, Poglitsch M, Transplantation: Official Journal of the Transplantation Society . 2007,第1期

机译：抗胸腺细胞球蛋白损害T细胞/抗原提呈细胞相互作用：破坏免疫突触和结合物。
3. Activation of the small GTPase Rac2 via the B cell receptor regulates B cell adhesion and immunological-synapse formation. [J] . Arana E, Vehlow A, Harwood NE, Immunity . 2008,第1期

机译：小GTPase Rac2通过B细胞受体的激活调节B细胞粘附和免疫突触的形成。
4. Modeling the Influence of Molecule and Cell Surface Micro-domain distribution on the formation of T cell Immunological Synapses [C] . Shulamit Kotzer, Mali Salmon-Divon, Asya Kaplan, IEEE/NIH Life Science Systems and Applications Workshop . 2007

机译：模拟分子和细胞表面微观域分布对T细胞免疫突触形成的影响
5. LAMININ: A POSSIBLE ROLE AS A MEDIATOR OF NATURAL CELL-MEDIATED FUNCTIONS (NATURAL KILLER CELLS, NATURAL CYTOTOXIC CELLS, RECEPTORS, SURFACE ANTIGEN). [D] . LAYBOURN, KATHERINE ANN. 1986

机译：层粘连蛋白：作为天然细胞介导的功能（天然杀伤细胞，天然细胞毒性细胞，受体，表面抗原）的介体的可能作用。
6. A bispecific chimeric antigen receptor molecule enhances T cell activation through dual immunological synapse formation and offsets antigen escape in glioblastoma [O] . Meenakshi Hegde, Zakaria Grada, Antonella Pignata, 2015

机译：双特异性嵌合抗原受体分子通过双重免疫突触形成增强T细胞活化并抵消胶质母细胞瘤中的抗原逃逸
7. Myosin IIA modulates T cell receptor transport and CasL phosphorylation during early immunological synapse formation. [O] . Yan Yu, Nicole C Fay, Alexander A Smoligovets, 2012

机译：肌球蛋白IIa在早期免疫突触形成期间调节T细胞受体转运和CasL磷酸化。

Synthetic surfaces as artificial antigen presenting cells in the study of T cell receptor triggering and immunological synapse formation.

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