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促进G蛋白吸附的混合单层:与甲酰基末端寡肽共吸附的α2A肾上腺素能受体衍生肽

Mixed monolayers to promote g-protein adsorption: alpha2A-adrenergic receptor-derived peptides coadsorbed with formyl-terminated oligopeptides.

作者信息

Balau Luminita Savitchi, Vahlberg Cecilia, Petoral Rodrigo M, Uvdal Kajsa

机构信息

Division of Sensor Science and Molecular Physics, Department of Physics, Chemistry and Biology, IFM, Linköping University, SE-581 83 Linköping, Sweden.

出版信息

Langmuir. 2007 Jul 31;23(16):8474-9. doi: 10.1021/la063447f. Epub 2007 Jul 10.

Abstract

Pure and mixed monolayers of a synthetic peptide, GPR-i3n, derived from the third intracellular loop of the alpha2 adrenergic receptor and a shorter inactive oligopeptide, N-formyl-(Gly)3-(Cys) (called 3GC), were prepared on gold surfaces. The mixing ratio of the GPR-i3n and 3GC was used to control G-protein binding capability. The GPR-i3n peptide is specially designed for bovine G-protein selectivity and has been proven to have high affinity to G-proteins [Vahlberg, C.; Petoral, R. M., Jr.; Lindell, C.; Broo, K.; Uvdal, K. Langmuir 2006, 22 (17), 7260-7264]. Pure 3GC monolayers show very low protein adsorption capability. In this study, 3GC is chosen as a coadsorbent, with the aim to induce molecular conformational changes during monolayer formation to enhance G-protein adsorption. A full characterization of the mixed monolayers was done. The monolayer thickness and the mass-related surface coverage for both GPR-i3n and 3GC were investigated using radio labeling. The GPR-i3n was labeled by 125I-targeting tyrosine, and the activity was measured by using radioimmunoassay (RIA). The formation and chemical composition of GPR-i3n and 3GC monolayers were investigated using X-ray photoelectron spectroscopy, and it is shown that both GPR-i3n and 3GC bind chemically to the gold surface. The interaction between the mixed monolayers and G-proteins was investigated by means of real-time surface plasmon resonance. There is a higher protein binding capacity to the monolayer when the GPR-i3n peptide is intermixed with the 3GC coadsorbent, despite the fact that the 3GC itself has a very low G-protein binding capability. This supports a molecular reorientation at the surface, while 3GC is intermixed with GPR-i3n.

摘要

在金表面制备了源自α2肾上腺素能受体第三细胞内环的合成肽GPR-i3n以及较短的无活性寡肽N-甲酰基-(甘氨酸)3-(半胱氨酸)(称为3GC)的纯单层和混合单层。GPR-i3n和3GC的混合比例用于控制G蛋白结合能力。GPR-i3n肽是专门为牛G蛋白选择性设计的,并且已被证明对G蛋白具有高亲和力[瓦尔贝里,C;佩托拉尔,R.M.,Jr.;林德尔,C.;布鲁,K.;乌瓦尔,K.《朗缪尔》2006年,22(17),7260 - 7264]。纯3GC单层显示出非常低的蛋白质吸附能力。在本研究中,选择3GC作为共吸附剂,目的是在单层形成过程中诱导分子构象变化以增强G蛋白吸附。对混合单层进行了全面表征。使用放射性标记研究了GPR-i3n和3GC的单层厚度和质量相关表面覆盖率。GPR-i3n用125I标记靶向酪氨酸,并通过放射免疫测定法(RIA)测量活性。使用X射线光电子能谱研究了GPR-i3n和3GC单层的形成和化学成分,结果表明GPR-i3n和3GC都与金表面发生化学结合。通过实时表面等离子体共振研究了混合单层与G蛋白之间的相互作用。尽管3GC本身具有非常低的G蛋白结合能力,但当GPR-i3n肽与3GC共吸附剂混合时,单层对蛋白质的结合能力更高。这支持了在表面发生分子重排,而3GC与GPR-i3n混合在一起。

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