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通过内体介导的内质网滞留来抑制瞬态蛋白的功能。

Functional inhibition of transitory proteins by intrabody-mediated retention in the endoplasmatic reticulum.

机构信息

Department of Gene Regulation and Differentiation-RDIF, Helmholtz Centre for Infection Research, Braunschweig, Germany.

出版信息

Methods. 2012 Mar;56(3):338-50. doi: 10.1016/j.ymeth.2011.10.008. Epub 2011 Oct 20.

Abstract

Intrabodies are recombinantly expressed intracellular antibody fragments that can be used to specifically bind and inhibit the function of cellular proteins of interest. Intrabodies can be targeted to various cell compartments by attaching an appropriate localization peptide sequence to them. An efficient strategy with a high success rate is to anchor intrabodies in the endoplasmatic reticulum where they can inhibit transitory target proteins by binding and preventing them to reach their site of action. Intrabodies can be assembled from antibody gene fragments from various sources into dedicated expression vectors. Conventionally, antibody cDNA sequences are derived from selected hybridoma cell clones that express antibodies with the desired specificity. Alternatively, appropriate clones can be isolated by affinity selection from an antibody in vitro display library. Here an evaluation of endoplasmatic reticulum targeted intrabodies with respect to other knockdown approaches is given and the characteristics of various intrabody expression vectors are discussed. A step by step protocol is provided that was repeatedly used to construct intrabodies derived from diverse antibody isotypes producing hybridoma cell clones. The inactivation of the cell surface receptor neural cell adhesion molecule (NCAM) by a highly efficacious novel endoplasmatic reticulum-anchored intrabody is demonstrated.

摘要

内体抗体是重组表达的细胞内抗体片段,可用于特异性结合和抑制感兴趣的细胞蛋白的功能。通过将适当的定位肽序列连接到内体抗体上,它们可以靶向各种细胞区室。一种有效的策略是将内体抗体锚定在内质网中,通过结合和阻止它们到达作用部位,从而抑制瞬时靶蛋白。内体抗体可以从各种来源的抗体基因片段组装到专用表达载体中。传统上,抗体 cDNA 序列源自表达所需特异性抗体的选定杂交瘤细胞克隆。或者,可以通过从体外展示抗体文库中进行亲和选择来分离适当的克隆。在此,对内质网靶向内体抗体相对于其他敲低方法进行了评估,并讨论了各种内体表达载体的特性。提供了一个逐步方案,该方案已被反复用于构建源自不同抗体同种型的产生杂交瘤细胞克隆的内体抗体。通过一种高效的新型内质网锚定的内体抗体使细胞表面受体神经细胞黏附分子 (NCAM) 失活。

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