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POLKADOTS Are Foci of Functional Interactions in T-Cell Receptor–mediated Signaling to NF-κB

机译:POLKADOTS是T细胞受体介导的NF-κB信号传导中功能相互作用的焦点

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摘要

Stimulation of the T-cell receptor (TCR) results in the activation of several transcription factors, including NF-κB, that are crucial for T-cell proliferation and gain of effector functions. On TCR engagement, several proteins within the TCR-directed NF-κB signaling pathway undergo dynamic spatial redistribution, but the significance of these redistribution events is largely unknown. We have previously described TCR-induced cytoplasmic structures called POLKADOTS (punctate and oligomeric killing or activating domains transducing signals) that are enriched in the NF-κB signaling intermediate, Bcl10. We now show that these structures are formed only under conditions that promote efficient NF-κB activation. Furthermore, POLKADOTS formation is dependent on functional domains of specific NF-κB signal transducers. Through use of a photoactivatable GFP, we demonstrate that POLKADOTS contain both a highly stable and a rapidly equilibrating protein component. FRET analyses show that POLKADOTS are sites of enriched interactions between Bcl10 and partner signaling proteins. These observations strongly suggest that POLKADOTS are focal sites of dynamic information exchange between cytosolic intermediates in the process of TCR activation of NF-κB.
机译:T细胞受体(TCR)的刺激导致几种转录因子(包括NF-κB)的激活,这对于T细胞增殖和效应功能的获得至关重要。在TCR参与下,TCR定向的NF-κB信号传导途径中的几种蛋白质会经历动态的空间再分布,但是这些再分布事件的意义在很大程度上是未知的。我们先前已经描述了TCR诱导的胞质结构,称为POLKADOTS(点状和寡聚的杀伤或激活结构域,转导信号),富含NF-κB信号传导中间物Bcl10。现在我们显示这些结构仅在促进有效NF-κB活化的条件下形成。此外,POLKADOTS的形成取决于特定NF-κB信号转导子的功能域。通过使用可光激活的GFP,我们证明POLKADOTS包含高度稳定和快速平衡的蛋白质成分。 FRET分析表明,POLKADOTS是Bcl10与伴侣信号蛋白之间丰富相互作用的位点。这些观察结果强烈表明,POLKADOTS是TCR激活NF-κB过程中胞质中间体之间动态信息交换的焦点。

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