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聚糖在T淋巴细胞与抗原呈递细胞相互作用中的相关性。

Relevance of glycans in the interaction between T lymphocyte and the antigen presenting cell.

作者信息

Gómez-Henao Wilton, Tenorio Eda Patricia, Sanchez Francisco Raúl Chávez, Mendoza Miguel Cuéllar, Ledezma Ricardo Lascurain, Zenteno Edgar

机构信息

Departamento de Bioquímica, Facultad de Medicina, Universidad Nacional Autónoma de México, Coyoacan; Mexico.

Cell Growth, Tissue Repair and Regeneration (CRRET), CNRS ERL 9215, Université Paris Est Créteil (UPEC), Créteil, France.

出版信息

Int Rev Immunol. 2021;40(4):274-288. doi: 10.1080/08830185.2020.1845331. Epub 2020 Nov 18.

Abstract

The immunological synapse promotes receptors and ligands interaction in the contact interface between the T lymphocyte and the antigen presenting cell; glycosylation of the proteins involved in this biological process favors regulation of molecular interactions and development of the T lymphocyte effector response. Glycans in the immunological synapse influence cellular and molecular processes such as folding, expression, and structural stability of proteins, they also mediate ligand-receptor interaction and propagation of the intracellular signaling or inhibition of uncontrolled cellular activation that could lead to the development of autoimmunity, among others. It has been suggested that altered glycosylation of proteins that participate in the immunological synapse affects the signaling processes and cell proliferation, as well as exacerbation of the effector mechanisms of T cells that trigger systemic damage and autoimmunity. Understanding the role of glycans in the immune response has allowed for advances in the development of immunotherapies in different fields through the controlled and specific activation of the immune response. This review describes the structural and biological aspects of glycans associated with some molecules present in the immunological synapse, providing information that allows understanding the function of glycosylation in the interaction between the T lymphocyte and the antigen-presenting cell, as well as its impact on signaling and development regulation of T lymphocytes effector response.

摘要

免疫突触促进T淋巴细胞与抗原呈递细胞接触界面处受体与配体的相互作用;参与这一生物学过程的蛋白质糖基化有利于调节分子相互作用及T淋巴细胞效应反应的发展。免疫突触中的聚糖影响细胞和分子过程,如蛋白质的折叠、表达和结构稳定性,它们还介导配体-受体相互作用以及细胞内信号的传导,或抑制可能导致自身免疫发展的不受控制的细胞活化等。有人提出,参与免疫突触的蛋白质糖基化改变会影响信号传导过程和细胞增殖,以及加剧引发全身损伤和自身免疫的T细胞效应机制。通过对免疫反应的可控和特异性激活,了解聚糖在免疫反应中的作用有助于不同领域免疫疗法的发展。本综述描述了与免疫突触中一些分子相关的聚糖的结构和生物学方面,提供了有助于理解糖基化在T淋巴细胞与抗原呈递细胞相互作用中的功能及其对T淋巴细胞效应反应信号传导和发育调节影响的信息。

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