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Immunoregulatory interactions between a Lymphoid and a non-Lymphoid cell

Reactome ID: R-HSA-198933

中文名称

淋巴细胞与非淋巴细胞之间的免疫调节相互作用

通路描述

许多受体和细胞粘附分子在调节淋巴起源细胞(如 B 细胞、T 细胞和 NK 细胞)对自抗原、肿瘤抗原和病原体的反应中发挥关键作用。例如,KIRs 和 LILRs 是监视系统的一部分,用于检测 MHC 类 I 呈递中的任何紊乱,通常由癌症或病毒感染引起。体细胞也能通过展示表面应激标记物如 MICA 来报告内部功能缺陷。这些分子在体细胞上的存在被 C-lectin NK 免疫受体拾取。淋巴细胞能够根据其激活状态调节其位置和移动,并定位在表达相应配体的组织中。例如,淋巴细胞可以微调 IgSF、Selectin 和 Integrin 类粘附分子的存在和浓度,这些分子与许多炎症血管标记物相互作用。此外,淋巴细胞与抗原的相互作用有多种途径。这可以直接以 MHC 分子为上下文呈现给特定的 T 细胞受体。抗原 - 抗体复合物可以通过少数淋巴特异性 Fc 受体锚定到细胞上,进而进一步影响细胞功能。激活的补体因子 C3d 结合到抗原和细胞表面受体 CD21 上。在这种情况下,CD19 对 B 淋巴细胞功能的深远影响受到其与 CD21 相互作用的调节。
英文描述
Immunoregulatory interactions between a Lymphoid and a non-Lymphoid cell A number of receptors and cell adhesion molecules play a key role in modifying the response of cells of lymphoid origin (such as B-, T- and NK cells) to self and tumor antigens, as well as to pathogenic organisms.Molecules such as KIRs and LILRs form part of a crucial surveillance system that looks out for any derangement, usually caused by cancer or viral infection, in MHC Class I presentation. Somatic cells are also able to report internal functional impairment by displaying surface stress markers such as MICA. The presence of these molecules on somatic cells is picked up by C-lectin NK immune receptors.Lymphoid cells are able to regulate their location and movement in accordance to their state of activation, and home in on tissues expressing the appropriate complementary ligands. For example, lymphoid cells may fine tune the presence and concentration of adhesion molecules belonging to the IgSF, Selectin and Integrin class that interact with a number of vascular markers of inflammation.Furthermore, there are a number of avenues through which lymphoid cells may interact with antigen. This may be presented directly to a specific T-cell receptor in the context of an MHC molecule. Antigen-antibody complexes may anchor to the cell via a small number of lymphoid-specific Fc receptors that may, in turn, influence cell function further. Activated complement factor C3d binds to both antigen and to cell surface receptor CD21. In such cases, the far-reaching influence of CD19 on B-lymphocyte function is tempered by its interaction with CD21.

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