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来自大肠杆菌的重组盘基网柄菌钙调节的34,000道尔顿F-肌动蛋白成束蛋白的过表达、纯化及特性分析

Overexpression, purification, and characterization of recombinant Dictyostelium discoideum calcium-regulated 34,000-dalton F-actin bundling protein from Escherichia coli.

作者信息

Lim R W, Fechheimer M

机构信息

Department of Cellular Biology, University of Georgia, Athens 30602, USA.

出版信息

Protein Expr Purif. 1997 Mar;9(2):182-90. doi: 10.1006/prep.1996.0692.

DOI:10.1006/prep.1996.0692
PMID:9056483
Abstract

The Dictyostelium discoideum 34-kDa protein is an F-actin bundling protein that demonstrates diverse distributions in the cell during cell shape changes and cell movement. The protein is expressed at a very low level in the amoeba, just 0.4% of the total cell protein. This presents a challenging problem when purifying sufficient protein for structural and biochemical studies. The purification procedure is lengthy and yields only a few milligrams of protein. An alternative protein expression system, that of the bacterial T7 expression system, was used to produce large quantities of recombinant 34-kDa protein (r34-kDa). The soluble r34-kDa protein constitutes up to a quarter of the total bacterial protein, and was purified to homogeneity by a modification of the purification procedure for the native D. discoideum 34-kDa protein (N34-kDa). The r34-kDa possesses all the same functional characteristics as the N34-kDa protein with respect to its interactions with F-actin in vitro: it bound to and cross-linked F-actin, mediated F-actin bundle formation, directly bound calcium, and demonstrated calcium-sensitive F-actin binding activities.

摘要

盘基网柄菌的34 kDa蛋白是一种F-肌动蛋白成束蛋白,在细胞形态变化和细胞运动过程中,该蛋白在细胞内呈现出多样的分布。该蛋白在变形虫中的表达水平非常低,仅占细胞总蛋白的0.4%。在为结构和生化研究纯化足够量的蛋白时,这带来了一个具有挑战性的问题。纯化过程冗长,仅能获得几毫克的蛋白。一种替代的蛋白表达系统,即细菌T7表达系统,被用于大量生产重组34 kDa蛋白(r34 kDa)。可溶性r34 kDa蛋白占细菌总蛋白的四分之一,通过对天然盘基网柄菌34 kDa蛋白(N34 kDa)纯化程序的改进,将其纯化至同质。就其在体外与F-肌动蛋白的相互作用而言,r34 kDa具有与N34 kDa蛋白所有相同的功能特性:它能结合并交联F-肌动蛋白,介导F-肌动蛋白束的形成,直接结合钙,并表现出钙敏感的F-肌动蛋白结合活性。

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Formation of Hirano bodies induced by expression of an actin cross-linking protein with a gain-of-function mutation.由具有功能获得性突变的肌动蛋白交联蛋白表达诱导的 Hirano 小体的形成。
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