首页> 外文期刊>Molecular biotechnology >Vectors for Expression of Signal Peptide-Dependent Proteins in Baculovirus/Insect Cell Systems and Their Application to Expression and Purification of the High-Affinity Immunoglobulin Gamma Fc Receptor I in Complex with Its Gamma Chain
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Vectors for Expression of Signal Peptide-Dependent Proteins in Baculovirus/Insect Cell Systems and Their Application to Expression and Purification of the High-Affinity Immunoglobulin Gamma Fc Receptor I in Complex with Its Gamma Chain

机译:用于表达杆状病毒/昆虫体系中信号肽依赖性蛋白的载体及其在γ链中复合物中的高亲和力免疫球蛋白γFC受体I的表达和纯化的应用

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摘要

Integral membrane proteins play a central role in various cellular functions and are important therapeutic targets. However, technical challenges in the overexpression and purification of membrane proteins often represent a limiting factor for biochemical and structural studies. Here, we constructed a set of vectors, derivatives of MultiBac vectors that can be used to express proteins with a cleavable N-terminal signal peptide in insect cells. We propose these vectors for expression of type I membrane proteins and other secretory pathway proteins that require the signal recognition particle for translocation to the endoplasmic reticulum (ER). The vectors code for N-terminal and C-terminal affinity tags including 3 x FLAG and Twin-Strep, which represent tags compatible with efficient translocation to the ER as well as with purification under mild conditions that preserve protein structure and function. As a model, we used our system to express and purify the engineered high-affinity immunoglobulin gamma Fc receptor I (CD64) in complex with its gamma subunit (gamma-chain). We demonstrate that CD64 expressed in complex with the gamma-chain is functional in immunoglobulin G (IgG) binding. The sedimentation of CD64 in complex with IgG suggests individual CD64/IgG complexes in addition to formation of high-molecular weight complexes. In summary, our vectors can be used as a tool for expression of membrane proteins, other secretory pathway proteins and their protein complexes.
机译:整体膜蛋白在各种细胞功能中起着核心作用,是重要的治疗靶标。然而,膜蛋白过表达和纯化的技术挑战通常代表生化和结构研究的限制因素。这里,我们构建了一组载体,多元型载体的衍生物,其可用于表达昆虫细胞中可切割的N-末端信号肽的蛋白质。我们提出了这些载体,用于表达I型膜蛋白和其他分泌途径蛋白,其需要信号识别颗粒以将用于转移到内质网(ER)的易位。 N终端和C末端亲和力标签的向量代码包括3 x标志和双击,其代表与ER的有效易位相兼容的标签,以及在保持蛋白质结构和功能的温和条件下纯化。作为一种模型,我们使用我们的系统以与其γ亚基(γ链)复杂的工程化的高亲和力免疫球蛋白γFc受体I(CD64)。我们证明CD64与γ链表达的CD64在免疫球蛋白G(IgG)结合中具有功能性。除了形成高分子量复合物之外,CD64络合物中CD64的沉降表明单个CD64 / IgG复合物。总之,我们的载体可以用作表达膜蛋白,其他分泌途径蛋白及其蛋白质复合物的工具。

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