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The cytosolic domain of T-cell receptor ζ associates with membranes in a dynamic equilibrium and deeply penetrates the bilayer

机译:T细胞受体ζ的胞质结构域与膜动态平衡地结合并深度渗透双层

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摘要

Interactions between lipid bilayers and the membrane-proximal regions of membrane-associated proteins play important roles in regulating membrane protein structure and function. The T-cell antigen receptor is an assembly of eight single-pass membrane-spanning subunits on the surface of T lymphocytes that initiates cytosolic signaling cascades upon binding antigens presented by MHC-family proteins on antigen-presenting cells. Its ζ-subunit contains multiple cytosolic immunoreceptor tyrosine-based activation motifs involved in signal transduction, and this subunit by itself is sufficient to couple extracellular stimuli to intracellular signaling events. Interactions of the cytosolic domain of ζ (ζcyt) with acidic lipids have been implicated in the initiation and regulation of transmembrane signaling. ζcyt is unstructured in solution. Interaction with acidic phospholipids induces structure, but its disposition when bound to lipid bilayers is controversial. Here, using surface plasmon resonance and neutron reflection, we characterized the interaction of ζcyt with planar lipid bilayers containing mixtures of acidic and neutral lipids. We observed two binding modes of ζcyt to the bilayers in dynamic equilibrium: one in which ζcyt is peripherally associated with lipid headgroups and one in which it penetrates deeply into the bilayer. Such an equilibrium between the peripherally bound and embedded forms of ζcyt apparently controls accessibility of the immunoreceptor tyrosine-based activation signal transduction pathway. Our results reconcile conflicting findings of the ζ structure reported in previous studies and provide a framework for understanding how lipid interactions regulate motifs to tyrosine kinases and may regulate the T-cell antigen receptor biological activities for this cell-surface receptor system.
机译:脂质双层与膜相关蛋白的膜近端区域之间的相互作用在调节膜蛋白的结构和功能中起重要作用。 T细胞抗原受体是T淋巴细胞表面上八个单次跨膜亚单位的集合,当结合MHC家族蛋白在抗原呈递细胞上呈递的抗原时,启动胞质信号级联反应。它的ζ亚基包含多个参与信号转导的基于胞浆免疫受体酪氨酸的活化基序,并且该亚基本身足以将细胞外刺激物与细胞内信号转导事件耦合。 ζ(ζcyt)的胞质域与酸性脂质的相互作用已经牵涉到跨膜信号传导的启动和调节中。 ζcyt在溶液中无结构。与酸性磷脂的相互作用可诱导结构,但与脂质双层结合时其结构却存在争议。在这里,我们使用表面等离振子共振和中子反射,表征了cycy与包含酸性和中性脂质混合物的平面脂质双层的相互作用。我们观察到了动态平衡状态下cycy与双层的两种结合模式:一种在其中cycy与脂质头基团相关联,而另一种则深入渗透到双层中。外围结合和嵌入的cycyt形式之间的这种平衡显然控制了基于免疫受体酪氨酸的激活信号转导途径的可及性。我们的结果调和了先前研究中报道的ζ结构的矛盾发现,并为理解脂质相互作用如何调节酪氨酸激酶的基序以及可能调节该细胞表面受体系统的T细胞抗原受体生物学活性提供了框架。

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