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Expression of mouse metallothionein-I cDNA in E.coli

机译:小鼠金属硫蛋白-I cDNA在大肠杆菌中的表达

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Metallothioneins (MT) are a family of cysteine-rich, low molecular weightm metal-binding proteins [1]. They play an important role in the homeostasis of essential metal ions, e.g., zinc and copper [2], as well as in the detoxification of heavy metals such as cadimum and mercury. They are also important in mammalian UV response. MTs are usually single-chain proteins, without a alpha -helix or beta -sheet, and bind a total of 7 equivalents of bivalent metal ions. In this regard, MTs are ideal proteins for hte examination of structure/function relationships by site-directed mutagenesis or other molecular biological methods. The expression of MT in E.coli has been reported previously, but attempts to produce high levels of recombinatn proteins had only limited success because of their low stability [3,4]. We describe here the expression in E.Coli of mouse MT-I cDNA as a carboxyl-terminal extension of glutathione-S-transferase.
机译:Metallothioneins(MT)是一种富含半胱氨酸的低分子量金属结合蛋白[1]。它们在必需金属离子的稳态中发挥着重要作用,例如锌和铜[2],以及在最大和汞的重金属的解毒中。它们在哺乳动物UV反应中也很重要。 MTS通常是单链蛋白,没有α-helix或β-曲线,并结合总共7当量的二价金属离子。在这方面,MTS是用于通过点定向诱变或其他分子生物学方法检查结构/功能关系的理想蛋白质。先前已经报道了MT在大肠杆菌中的表达,但由于它们的低稳定性[3,4],试图产生高水平的重组蛋白的成功仅有限。我们在此描述小鼠MT-I cDNA的大肠杆菌中的表达作为谷胱甘肽-S-转移酶的羧基 - 末端延伸。

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