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首页> 外文期刊>Biochemical and Biophysical Research Communications >Novel protein engineering strategy for creating highly receptor-selective mutant TNFs.
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Novel protein engineering strategy for creating highly receptor-selective mutant TNFs.

机译:用于创建高度受体选择性突变TNF的新型蛋白质工程策略。

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摘要

Tumor necrosis factor (TNF) plays important roles in host defense and in preventing tumor formation by acting via its receptors, TNFR1 and TNFR2, functions of which are less understood. To this end, we have been isolating TNF receptor-selective mutants using phage display technique. However, generation of a phage library with large repertoire (>10(8)) is impeded by the limited transformation efficiency of Escherichia coli. Therefore, it is currently difficult to create a mutant library containing amino acid substitutions in more than seven residues. To overcome this problem, here we have used two different TNF mutant libraries, each containing random substitutions at six selected amino acid residues, and utilized a gene shuffling method to construct a randomized mutant library containing substitutions at 12 different amino acid residues of TNF. Consequently, using this library, we identified TNF mutants with greater receptor-selectivity and enhanced receptor-specific bioactivity than the existing mutants.
机译:肿瘤坏死因子(TNF)通过其受体TNFR1和TNFR2发挥作用,在宿主防御和预防肿瘤形成中起重要作用,人们对其功能的了解较少。为此,我们一直在使用噬菌体展示技术分离TNF受体选择性突变体。但是,由于大肠埃希氏大肠杆菌的转化效率有限,因此无法生成具有较大保留库(> 10(8))的噬菌体文库。因此,目前难以创建在七个以上的残基中包含氨基酸取代的突变体文库。为了克服这个问题,这里我们使用了两个不同的TNF突变体文库,每个突变体文库在六个选定的氨基酸残基上包含随机取代,并利用一种基因改组方法构建了一个在TNF的12个不​​同氨基酸残基上包含取代基的随机化突变体文库。因此,使用该文库,我们确定了比现有突变体具有更大的受体选择性和更高的受体特异性生物活性的TNF突变体。

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