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用于矿化芳烃的细菌条件自杀遏制系统。

Conditional-suicide containment system for bacteria which mineralize aromatics.

机构信息

Estación Experimental del Zaidín, Consejo Superior de Investigaciones Científicas, Apto. 419, 18080 Granada, Spain, and Department of Microbiology, Technical University of Denmark, DK-2800 Lyngby, Denmark.

出版信息

Appl Environ Microbiol. 1991 May;57(5):1504-8. doi: 10.1128/aem.57.5.1504-1508.1991.

Abstract

A model conditional-suicide system to control genetically engineered microorganisms able to degrade substituted benzoates is reported. The system is based on two elements. One element consists of a fusion between the promoter of the Pseudomonas putida TOL plasmid-encoded meta-cleavage pathway operon (P(m)) and the lacI gene encoding Lac repressor plus xylS, coding for the positive regulator of P(m). The other element carries a fusion between the P(tac) promoter and the gef gene, which encodes a killing function. In the presence of XylS effectors, LacI protein is synthesized, preventing the expression of the killing function. In the absence of effectors, expression of the P(tac)::gef cassette is no longer prevented and a high rate of cell killing is observed. The substitution of XylS for XylSthr45, a mutant regulator with altered effector specificity and increased affinity for benzoates, allows the control of populations able to degrade a wider range of benzoates at micromolar substrate concentrations. Given the wide effector specificity of the key regulators, the wild-type and mutant XylS proteins, the system should allow the control of populations able to metabolize benzoate; methyl-, dimethyl-, chloro-, dichloro-, ethyl-, and methoxybenzoates; salicylate; and methyl- and chlorosalicylates. A small population of genetically engineered microorganisms became Gef resistant; however, the mechanism of such survival remains unknown.

摘要

报道了一种用于控制能够降解取代苯甲酸的基因工程微生物的条件自杀系统。该系统基于两个要素。一个要素是由恶臭假单胞菌 TOL 质粒编码的 meta 裂解途径操纵子(P(m))启动子和编码 Lac 阻遏物的 lacI 基因融合而成,Lac 阻遏物加上 xylS,编码 P(m)的正调节剂。另一个要素携带 P(tac)启动子和 gef 基因的融合,该基因编码杀伤功能。在 XylS 效应物存在的情况下,合成 LacI 蛋白,阻止杀伤功能的表达。在没有效应物的情况下,P(tac)::gef 盒的表达不再受到阻止,观察到细胞高死亡率。用 XylSthr45 替代 XylS,XylSthr45 是一种具有改变的效应物特异性和增加的对苯甲酸亲和力的突变调节剂,允许控制能够在微摩尔底物浓度下降解更广泛范围的苯甲酸的群体。鉴于关键调节剂、野生型和突变型 XylS 蛋白的广泛效应物特异性,该系统应允许控制能够代谢苯甲酸;甲基-、二甲基-、氯-、二氯-、乙基-和甲氧基苯甲酸;水杨酸;和甲基和氯水杨酸的群体。一小部分基因工程微生物对 Gef 产生了抗性;然而,这种生存机制仍然未知。

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