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首页> 外文期刊>Applied and Environmental Microbiology >In vivo monitoring system for structure-function relationship analysis of the antibacterial peptide apidaecin.
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In vivo monitoring system for structure-function relationship analysis of the antibacterial peptide apidaecin.

机译:用于抗菌肽阿霉素的结构-功能关系分析的体内监测系统。

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A unique antibacterial peptide derivative found in immune honeybee lymph, apidaecin 1b (AP1), was randomly mutagenized and characterized by a newly established system to analyze in vivo its structure-function relationship. Initially, a high-level expression host-vector system for AP1 in Escherichia coli was constructed by creating a fusion protein with the highly stable Streptomyces subtilisin inhibitor (SSI) molecule. Expression of the SSI-AP1 fusion protein was found to depend on the concentration of the transcriptional inducer isopropyl-beta-D-thio-galactopyranoside (IPTG) and to parallel the degree of growth inhibition of the transformant cells. Subsequently, apidaecin derivatives produced by localized random mutagenesis were screened with this IPTG concentration-controlled in vivo system by monitoring the growth inhibition patterns of the transformant cells. One mutant apidaecin (P9L) that had reduced activity was purified and isolated from the periplasmic fraction of an E. coli transformant. Its antibacterial activity was reduced to one-third of that of wild-type apidaecin. When considered together with the other mutations, it was concluded that several Pro residues, including that at the ninth position, are responsible for expression of the antibacterial action of apidaecin.
机译:在免疫蜜蜂淋巴液中发现的一种独特的抗菌肽衍生物,阿迪霉素1b(AP1),被随机诱变并通过新建立的系统进行特征分析,以在体内分析其结构与功能的关系。最初,通过创建具有高度稳定链霉菌枯草杆菌蛋白酶抑制剂(SSI)分子的融合蛋白,构建了大肠杆菌中AP1的高表达宿主载体系统。发现SSI-AP1融合蛋白的表达取决于转录诱导剂异丙基-β-D-硫代吡喃半乳糖苷(IPTG)的浓​​度,并与转化细胞的生长抑制程度平行。随后,通过监测转化细胞的生长抑制模式,用该IPTG浓度控制的体内系统筛选通过局部随机诱变产生的阿霉素霉素衍生物。从大肠杆菌转化体的周质部分中纯化并分离出一种活性降低的突变型阿霉素(P9L)。其抗菌活性降低到野生型阿迪霉素的三分之一。当与其他突变一起考虑时,得出的结论是,几个Pro残基(包括第9位的残基)负责表达阿霉素的抗菌作用。

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