Regulation of T cell receptor expression in immature CD4+CD8+ thymocytes by p56lck tyrosine kinase: basis for differential signaling by CD4 and CD8 in immature thymocytes expressing both coreceptor molecules.

D L Wiest; L Yuan; J Jefferson; P Benveniste; M Tsokos; R D Klausner; L H Glimcher; L E Samelson; A Singer

首页> 外文期刊>The Journal of Experomental Medicine >Regulation of T cell receptor expression in immature CD4+CD8+ thymocytes by p56lck tyrosine kinase: basis for differential signaling by CD4 and CD8 in immature thymocytes expressing both coreceptor molecules.

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Regulation of T cell receptor expression in immature CD4+CD8+ thymocytes by p56lck tyrosine kinase: basis for differential signaling by CD4 and CD8 in immature thymocytes expressing both coreceptor molecules.

机译：p56lck酪氨酸激酶对未成熟CD4 + CD8 +胸腺细胞中T细胞受体表达的调节：表达两个共受体分子的未成熟胸腺细胞中CD4和CD8差异信号传导的基础。

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Signals transduced through the T cell antigen receptor (TCR) are modulated by the src family tyrosine kinase p56lck (lck), which associates in mature T cells with the coreceptor molecules CD4 and CD8. Here we describe a novel function of lck in immature CD4+CD8+ thymocytes, that of regulating TCR expression. Activation of lck in immature CD4+CD8+ thymocytes by intrathymic engagement of CD4 maintains low TCR expression by causing most TCR components to be retained and degraded within the endoplasmic reticulum. Importantly, activation of lck in immature CD4+CD8+ thymocytes results from engagement of surface CD4 molecules, but not surface CD8 molecules, despite the nearly fourfold greater surface expression of CD8 than CD4. The competence of CD4 to activate lck in CD4+CD8+ thymocytes relates to the fact that a relatively large fraction of surface CD4 molecules (25-50%) are associated with intracellular lck molecules, whereas only 2% of surface CD8 molecules are associated with lck. The amount of lck associated with CD4 in CD4+CD8+ thymocytes is diminished by chronic CD4 engagement in the thymus, as activated lck molecules subsequently dissociate from CD4. Indeed, the amount of lck associated with CD4 in CD4+CD8+ thymocytes is markedly increased in major histocompatibility complex (MHC) class II- mice that lack the intrathymic ligand for CD4 and in which surface CD4 molecules are consequently not engaged. Thus, the present study demonstrates that (a) activation of lck in CD4+CD8+ thymocytes regulates distribution and expression of TCR components; (b) unlike CD4 molecules, CD8 molecules on CD4+CD8+ thymocytes cannot efficiently activate lck despite their significantly greater surface expression; and (c) the amount of lck associated with CD4 in the CD4+CD8+ thymocytes is inversely related to the extent of CD4 engagement by MHC class II molecules in the thymus.

机译：通过T细胞抗原受体（TCR）传导的信号由src家族酪氨酸激酶p56lck（lck）调节，后者在成熟T细胞中与共受体分子CD4和CD8相关联。在这里，我们描述了lck在未成熟的CD4 + CD8 +胸腺细胞中的新功能，即调节TCR表达的功能。 CD4的胸腺内结合通过激活未成熟的CD4 + CD8 +胸腺细胞中的lck来维持大多数TCR成分在内质网内保留和降解，从而维持了低TCR表达。重要的是，尽管CD8的表面表达比CD4高近四倍，但未成熟的CD4 + CD8 +胸腺细胞中lck的活化是由表面CD4分子而非表面CD8分子的结合引起的。 CD4激活CD4 + CD8 +胸腺细胞中lck的能力与以下事实有关：表面CD4分子的相对较大部分（25-50％）与细胞内lck分子相关，而仅2％的表面CD8分子与lck相关。。 CD4 + CD8 +胸腺细胞中与CD4相关的lck量由于胸腺中慢性CD4参与而减少，因为随后激活的lck分子从CD4上解离。实际上，在缺少CD4的胸腺内配体并且因此未参与表面CD4分子的主要组织相容性复合体（MHC）II类小鼠中，CD4 + CD8 +胸腺细胞中与CD4相关的lck的量显着增加。因此，本研究证明：（a）CD4 + CD8 +胸腺细胞中lck的激活调节TCR成分的分布和表达; （b）与CD4分子不同，CD4 + CD8 +胸腺细胞上的CD8分子尽管表面表达明显增强，但不能有效激活lck。（c）CD4 + CD8 +胸腺细胞中与CD4相关的lck量与胸腺中MHC II类分子与CD4的结合程度成反比。

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《The Journal of Experomental Medicine》 |1993年第5期|共12页
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D L Wiest; L Yuan; J Jefferson; P Benveniste; M Tsokos; R D Klausner; L H Glimcher; L E Samelson; A Singer;
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1. ZAP-70 Protein Promotes Tyrosine Phosphorylation of T Cell Receptor Signaling Motifs (ITAMs) in Immature CD4+8+ Thymocytes with Limiting p56lck [J] . Jennifer M. Ashe, David L. Wiest, Ryo Abe, The Journal of Experomental Medicine . 1999,第7期

机译：ZAP-70蛋白通过限制p56lck促进未成熟CD4 + 8 +胸腺细胞中T细胞受体信号基元（ITAM）的酪氨酸磷酸化
2. Commitment of Immature CD4+8+ Thymocytes to the CD4 Lineage Requires CD3 Signaling but Does Not Require Expression of Clonotypic T Cell Receptor (TCR) Chains [J] . Harumi Suzuki, Yoichi Shinkai, Lawrence G. Granger, The Journal of Experomental Medicine . 1997,第1期

机译：未成熟的CD4 + 8 +胸腺细胞对CD4谱系的承诺需要CD3信号传导，但不需要表达克隆型T细胞受体（TCR）链
3. Immature thymocytes become sensitive to calcium-mediated apoptosis with the onset of CD8, CD4, and the T cell receptor expression: a role for bcl-2? [J] . S Andjeli?, N Jain, J Nikoli?-Zugi? The Journal of Experomental Medicine . 1993,第5期

机译：随着CD8，CD4和T细胞受体的表达，未成熟的胸腺细胞对钙介导的细胞凋亡变得敏感：对bcl-2？
4. Regulation of VH replacement in human immature B cells by B cell receptor (BCR)-mediated signaling. [D] . Liu, Jing. 2009

机译：通过B细胞受体（BCR）介导的信号传导调节人类未成熟B细胞中VH的替换。
5. Regulation of T cell receptor expression in immature CD4+CD8+ thymocytes by p56lck tyrosine kinase: basis for differential signaling by CD4 and CD8 in immature thymocytes expressing both coreceptor molecules [O] . 1993

机译：p56lck酪氨酸激酶对未成熟CD4 + CD8 +胸腺细胞中T细胞受体表达的调节：表达两个共受体分子的未成熟胸腺细胞中CD4和CD8差异信号传导的基础
6. Regulation of T cell receptor expression in immature CD4+CD8+ thymocytes by p56lck tyrosine kinase: basis for differential signaling by CD4 and CD8 in immature thymocytes expressing both coreceptor molecules. [O] . D L Wiest, L Yuan, J Jefferson, 1993

机译：P56LCK酪氨酸激酶在未成熟的CD4 + CD8 +胸腺酶中的T细胞受体表达的调节：CD4和CD8在表达血栓细胞中CD4和CD8的差分信号。
7. Ligand-Stimulated Signaling Events in Immature CD4+CD8+Thymocytes ExpressingCompetent T-Cell Receptor Complexes [R] . Nakayama, T., Samelson, L. E., Nakayama, Y., 1991

机译：未成熟CD4 + CD8 +胸腺细胞中的配体刺激信号事件表达感受态T细胞受体复合物

Regulation of T cell receptor expression in immature CD4+CD8+ thymocytes by p56lck tyrosine kinase: basis for differential signaling by CD4 and CD8 in immature thymocytes expressing both coreceptor molecules.

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