Literature DB >> 12853648

Streptomyces-derived quorum-sensing systems engineered for adjustable transgene expression in mammalian cells and mice.

Wilfried Weber1, Ronald Schoenmakers, Manuela Spielmann, Marie Daoud El-Baba, Marc Folcher, Bettina Keller, Cornelia C Weber, Nils Link, Petra van de Wetering, Christoph Heinzen, Benoît Jolivet, Urs Séquin, Dominique Aubel, Charles J Thompson, Martin Fussenegger.   

Abstract

Prokaryotic transcriptional regulatory elements have been adopted for controlled expression of cloned genes in mammalian cells and animals, the cornerstone for gene-function correlations, drug discovery, biopharmaceutical manufacturing as well as advanced gene therapy and tissue engineering. Many prokaryotes have evolved specific molecular communication systems known as quorum-sensing to coordinate population-wide responses to physiological and/or physicochemical signals. A generic bacterial quorum-sensing system is based on a diffusible signal molecule that prevents binding of a repressor to corresponding operator sites thus resulting in derepression of a target regulon. In Streptomyces, a family of butyrolactones and their corresponding receptor proteins, serve as quorum-sensing systems that control morphological development and antibiotic biosynthesis. Fusion of the Streptomyces coelicolor quorum-sensing receptor (ScbR) to a eukaryotic transactivation domain (VP16) created a mammalian transactivator (SCA) which binds and adjusts transcription from chimeric promoters containing an SCA-specific operator module (P(SPA)). Expression of erythropoietin or the human secreted alkaline phosphatase (SEAP) by this quorum-sensor-regulated gene expression system (QuoRex) could be fine-tuned by non-toxic butyrolactones in a variety of mammalian cells including human primary and mouse embryonic stem cells. Following intraperitoneal implantation of microencapsulated Chinese hamster ovary cells transgenic for QuoRex-controlled SEAP expression into mice, the serum levels of this model glycoprotein could be adjusted to desired concentrations using different butyrolactone dosing regimes.

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Year:  2003        PMID: 12853648      PMCID: PMC167645          DOI: 10.1093/nar/gng071

Source DB:  PubMed          Journal:  Nucleic Acids Res        ISSN: 0305-1048            Impact factor:   16.971


  34 in total

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Review 4.  Immunosuppressive drugs: the first 50 years and a glance forward.

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5.  A transcriptional regulator of a pristinamycin resistance gene in Streptomyces coelicolor.

Authors:  M Folcher; R P Morris; G Dale; K Salah-Bey-Hocini; P H Viollier; C J Thompson
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Authors:  D Aubel; R Morris; B Lennon; M Rimann; H Kaufmann; M Folcher; J E Bailey; C J Thompson; M Fussenegger
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6.  2-Alkyl-4-hydroxymethylfuran-3-carboxylic acids, antibiotic production inducers discovered by Streptomyces coelicolor genome mining.

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