Literature DB >> 11095720

Coevolution of transcriptional and allosteric regulation at the chorismate metabolic branch point of Saccharomyces cerevisiae.

S Krappmann1, W N Lipscomb, G H Braus.   

Abstract

Control of transcription and enzyme activities are two interwoven regulatory systems essential for the function of a metabolic node. Saccharomyces cerevisiae strains differing in enzyme activities at the chorismate branch point of aromatic amino acid biosynthesis were constructed by recombinant DNA technology. Expression of an allosterically unregulated, constitutively activated chorismate mutase encoded by the ARO7(T226I) (ARO7(c)) allele depleted the chorismate pool. The resulting tryptophan limitation caused growth defects, which could be counteracted only by transcriptional induction of TRP2 encoding the competing enzyme anthranilate synthase. ARO7 expression is not transcriptionally regulated by amino acids. Transcriptional activation of the ARO7(c) allele led to stronger growth retardation upon tryptophan limitation. The same effect was achieved by removing the competing enzyme anthranilate synthase, which is encoded by the TRP2 gene, from the transcriptional control. The allelic situation of ARO7(c) being under general control instead of TRP2 resulted in severe growth defects when cells were starved for tryptophan. In conclusion, the specific regulatory pattern acting on enzymatic activities at the first metabolic node of aromatic amino acid biosynthesis is necessary to maintain proper flux distribution. Therefore, the evolution of the sophisticated allosteric regulation of yeast chorismate mutase requires as prerequisite (i) that the encoding ARO7 gene is not transcriptionally regulated, whereas (ii) the transcription of the competing feedback-regulated anthranilate synthase-encoding gene is controlled by availability of amino acids.

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Year:  2000        PMID: 11095720      PMCID: PMC17619          DOI: 10.1073/pnas.240469697

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  32 in total

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Authors:  G Miozzari; P Niederberger; R Hütter
Journal:  Arch Microbiol       Date:  1977-12-15       Impact factor: 2.552

5.  Transition-state stabilization and enzymic catalysis. Kinetic and molecular orbital studies of the rearrangement of chorismate to prephenate.

Authors:  P R Andrews; G D Smith; I G Young
Journal:  Biochemistry       Date:  1973-08-28       Impact factor: 3.162

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Authors:  S Krappmann; K Helmstaedt; T Gerstberger; S Eckert; B Hoffmann; M Hoppert; G Schnappauf; G H Braus
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8.  Nucleotide sequence of Saccharomyces cerevisiae genes TRP2 and TRP3 encoding bifunctional anthranilate synthase: indole-3-glycerol phosphate synthase.

Authors:  H Zalkin; J L Paluh; M van Cleemput; W S Moye; C Yanofsky
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Authors:  A F Egan; F Gibson
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Authors:  G Schnappauf; S Krappmann; G H Braus
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  8 in total

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2.  Refined molecular hinge between allosteric and catalytic domain determines allosteric regulation and stability of fungal chorismate mutase.

Authors:  Kerstin Helmstaedt; Gabriele Heinrich; William N Lipscomb; Gerhard H Braus
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Review 4.  The diversity of allosteric controls at the gateway to aromatic amino acid biosynthesis.

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5.  CRISPR-mediated multigene integration enables Shikimate pathway refactoring for enhanced 2-phenylethanol biosynthesis in Kluyveromyces marxianus.

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6.  Metabolic engineering of Saccharomyces cerevisiae for hydroxytyrosol overproduction directly from glucose.

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7.  Silencing of Vlaro2 for chorismate synthase revealed that the phytopathogen Verticillium longisporum induces the cross-pathway control in the xylem.

Authors:  Seema Singh; Susanna A Braus-Stromeyer; Christian Timpner; Van Tuan Tran; Gertrud Lohaus; Michael Reusche; Jessica Knüfer; Thomas Teichmann; Andreas von Tiedemann; Gerhard H Braus
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8.  Yarrowia lipolytica chassis strains engineered to produce aromatic amino acids via the shikimate pathway.

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  8 in total

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