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PLCγ2 在 TCR 信号转导和 T 细胞选择中发挥作用。

Phospholipase Cγ2 plays a role in TCR signal transduction and T cell selection.

机构信息

Blood Research Institute, BloodCenter of Wisconsin, Milwaukee, WI 53226, USA.

出版信息

J Immunol. 2012 Sep 1;189(5):2326-32. doi: 10.4049/jimmunol.1103458. Epub 2012 Jul 25.

Abstract

One of the important signaling events following TCR engagement is activation of phospholipase Cγ (PLCγ). PLCγ has two isoforms, PLCγ1 and PLCγ2. It is known that PLCγ1 is important for TCR signaling and TCR-mediated T cell selection and functions, whereas PLCγ2 is critical for BCR signal transduction and BCR-mediated B cell maturation and functions. In this study, we report that PLCγ2 was expressed in primary T cells, and became associated with linker for activated T cells and Src homology 2-domain containing leukocyte protein of 76 kDa and activated upon TCR stimulation. PLCγ1/PLCγ2 double-deficient T cells displayed further block from CD4 and CD8 double-positive to single-positive transition compared with PLCγ1 single-deficient T cells. TCR-mediated proliferation was further impaired in PLCγ1/PLCγ2 double-deficient T cells compared with PLCγ1 single-deficient T cells. TCR-mediated signal transduction, including Ca²⁺ mobilization and Erk activation, was further impaired in PLCγ1/PLCγ2 double-deficient relative to PLCγ1 single-deficient T cells. In addition, in HY TCR transgenic mouse model, thymic positive and negative selections were reduced in PLCγ1 heterozygous- and PLCγ2 homozygous-deficient (PLCγ1⁺/⁻PLCγ2⁻/⁻) relative to wild-type, PLCγ2 single-deficient (PLCγ2⁻/⁻), or PLCγ1 heterozygous-deficient (PLCγ1⁺/⁻) mice. Taken together, these data demonstrate that PLCγ2 participates in TCR signal transduction and plays a role in T cell selection.

摘要

T 细胞受体(TCR)结合后,一个重要的信号事件是激活磷脂酶 Cγ(PLCγ)。PLCγ 有两种同工型,PLCγ1 和 PLCγ2。已知 PLCγ1 对于 TCR 信号转导以及 TCR 介导的 T 细胞选择和功能很重要,而 PLCγ2 对于 B 细胞受体(BCR)信号转导以及 BCR 介导的 B 细胞成熟和功能至关重要。在这项研究中,我们报告 PLCγ2 在原代 T 细胞中表达,并在 TCR 刺激后与活化 T 细胞接头蛋白和包含Src 同源 2 结构域的白细胞蛋白 76kDa 相关联并被激活。与 PLCγ1 单缺陷型 T 细胞相比,PLCγ1/PLCγ2 双缺陷型 T 细胞从 CD4 和 CD8 双阳性向单阳性转变的过程中进一步受阻。与 PLCγ1 单缺陷型 T 细胞相比,PLCγ1/PLCγ2 双缺陷型 T 细胞 TCR 介导的增殖进一步受损。PLCγ1/PLCγ2 双缺陷型 T 细胞中,TCR 介导的信号转导,包括 Ca²⁺动员和 Erk 激活,进一步受损。此外,在 HY TCR 转基因小鼠模型中,与野生型、PLCγ2 单缺陷型(PLCγ2⁻/⁻)或 PLCγ1 杂合缺陷型(PLCγ1⁺/⁻)小鼠相比,PLCγ1 杂合缺失型(PLCγ1⁺/⁻PLCγ2⁻/⁻)和 PLCγ2 纯合缺失型(PLCγ2⁻/⁻)小鼠的胸腺阳性和阴性选择减少。综上所述,这些数据表明 PLCγ2 参与 TCR 信号转导,并在 T 细胞选择中发挥作用。

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