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通过 Phos-tag SDS- 和 Blue Native-PAGE 检测磷酸化的 T 和 B 细胞抗原受体种类。

Detection of phosphorylated T and B cell antigen receptor species by Phos-tag SDS- and Blue Native-PAGE.

机构信息

Department for Molecular Immunology, Max Planck-Institute for Immunobiology, Freiburg, Germany.

出版信息

Immunol Lett. 2010 May 4;130(1-2):51-6. doi: 10.1016/j.imlet.2009.12.012. Epub 2009 Dec 22.

Abstract

Detection of phospho-proteins and differently phosphorylated forms of the same protein are important in understanding cell behaviour. One novel method is Phos-tag SDS-PAGE. A dinuclear Mn(2+) complex that binds to phosphate groups (the Phos-tag) is covalently attached to the polyacrylamide gel matrix. Thus, phosphorylated proteins are retarded in their migration and can be distinguished from their non-phosphorylated counterparts. We applied Phos-tag SDS-PAGE to the analysis of the zeta, CD3epsilon and CD3delta subunits of the T cell antigen receptor (TCR-CD3). Pervanadate stimulation generated six different phospho-zeta and each two different CD3epsilon and CD3delta forms. This corresponds to the phosphorylatable tyrosines on their cytoplasmic tails. The phosphorylation pattern was compatible with random phosphorylation events. Further, we showed that the Phos-tag technology can be applied to Blue Native (BN)-PAGE. This extends the applicability to the analysis of native protein complexes. Upon pervanadate stimulation the TCR-CD3 complex was predominantly detected as two distinct phospho-complexes. In contrast, the B cell antigen receptor (BCR) appeared as one phospho-form. Thus, Phos-tag BN-PAGE is useful for the analysis of different phosphorylation states of multiprotein complexes.

摘要

检测磷酸化蛋白和同一蛋白的不同磷酸化形式对于理解细胞行为非常重要。一种新方法是 Phos-tag SDS-PAGE。一种与磷酸基团结合的双核 Mn(2+) 配合物(Phos-tag)被共价连接到聚丙烯酰胺凝胶基质上。因此,磷酸化蛋白在迁移过程中受到阻滞,可以与非磷酸化蛋白区分开来。我们将 Phos-tag SDS-PAGE 应用于 T 细胞抗原受体 (TCR-CD3) 的 ζ、CD3ε 和 CD3δ 亚基的分析。过氧化物酶刺激产生了六种不同的磷酸化 ζ,每种都有两种不同的 CD3ε 和 CD3δ 形式。这与它们胞质尾部的可磷酸化酪氨酸相对应。磷酸化模式与随机磷酸化事件兼容。此外,我们表明 Phos-tag 技术可应用于 Blue Native (BN)-PAGE。这将适用性扩展到了天然蛋白复合物的分析。在用过氧化物酶刺激后,TCR-CD3 复合物主要以两种不同的磷酸化复合物形式检测到。相比之下,B 细胞抗原受体 (BCR) 仅显示一种磷酸化形式。因此,Phos-tag BN-PAGE 可用于分析多蛋白复合物的不同磷酸化状态。

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