Affiliation:
1. 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, Denmark2
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.
Publisher
American Society for Microbiology
Subject
Ecology,Applied Microbiology and Biotechnology,Food Science,Biotechnology
Cited by
83 articles.
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