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人免疫干扰素-γ生物活性基因的化学合成。位点特异性诱变及结构-功能研究的前景。

Chemical synthesis of a biologically active gene for human immune interferon-gamma. Prospect for site-specific mutagenesis and structure-function studies.

作者信息

Jay E, MacKnight D, Lutze-Wallace C, Harrison D, Wishart P, Liu W Y, Asundi V, Pomeroy-Cloney L, Rommens J, Eglington L

出版信息

J Biol Chem. 1984 May 25;259(10):6311-7.

PMID:6327676
Abstract

A 453-base pair DNA duplex consisting of a gene coding for human interferon-gamma and initiation and termination signals plus appropriate restriction enzyme sites for plasmid insertion has been totally synthesized. The synthesis involved preparation of 66 oligodeoxynucleotides by a modified, solid phase phosphite procedure and enzymatic ligation of the oligonucleotides. The gene, when inserted into a previously constructed expression vector, was expressed in Escherichia coli, demonstrating functional activity for the synthetic gene. Several strategically located restriction cleavage sites have been introduced into the sequence. This provides a convenient system for site-specific mutagenesis for structure-function studies.

摘要

一个由编码人γ干扰素的基因、起始和终止信号以及用于质粒插入的合适限制酶位点组成的453个碱基对的DNA双链已被完全合成。合成过程包括通过改进的固相亚磷酸酯法制备66个寡脱氧核苷酸以及寡核苷酸的酶促连接。该基因插入先前构建的表达载体后在大肠杆菌中表达,证明了合成基因的功能活性。序列中引入了几个位于关键位置的限制酶切割位点。这为结构-功能研究的位点特异性诱变提供了一个便利的系统。

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