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2型非T细胞依赖性抗原

T cell-independent antigens type 2.

作者信息

Mond J J, Lees A, Snapper C M

机构信息

Department of Medicine, Uniformed Services University of the Health Sciences, Bethesda, Maryland 20814-4799, USA.

出版信息

Annu Rev Immunol. 1995;13:655-92. doi: 10.1146/annurev.iy.13.040195.003255.

Abstract

In this review we have attempted to define the characteristics of TI-2 antigens that enable them to stimulate antibody production in the absence of T cell help. One of the most critical properties of this group of antigens is their ability to deliver prolonged and persistent signaling to the B cell. This by itself is not however sufficient to stimulate Ig synthesis, and they must therefore stimulate non-T cells to interact with the B cells either directly or indirectly via cytokine production. There is evidence implicating the NK cell and T cell as playing this important role in response to TI antigens. Furthermore, we discuss the importance of cytokines such as IL-3, GMCSF, and IFN-gamma, which significantly enhance antibody production by these antigens. Finally, we present evidence demonstrating that B cell activation via TI stimuli does not play merely a permissive role in allowing for cell cycle entry and enhanced responsiveness to other stimuli. Rather, the nature of the B cell activating signal is critical in determining the quantitative and qualitative profile of Ig isotype production.

摘要

在本综述中,我们试图定义TI-2抗原的特征,这些特征使它们能够在没有T细胞辅助的情况下刺激抗体产生。这类抗原最关键的特性之一是它们向B细胞传递延长且持续信号的能力。然而,仅此一点不足以刺激Ig合成,因此它们必须刺激非T细胞通过细胞因子产生直接或间接与B细胞相互作用。有证据表明NK细胞和T细胞在对TI抗原的应答中发挥这一重要作用。此外,我们讨论了诸如IL-3、GMCSF和IFN-γ等细胞因子的重要性,它们可显著增强这些抗原诱导的抗体产生。最后,我们提供的证据表明,通过TI刺激激活B细胞不仅仅在允许细胞进入细胞周期以及增强对其他刺激的反应性方面起许可作用。相反,B细胞激活信号的性质对于确定Ig同种型产生的数量和质量特征至关重要。

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