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Bistability in a Metabolic Network Underpins the De Novo Evolution of Colony Switching in Pseudomonas fluorescens
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نویسنده
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gallie j. ,libby e. ,bertels f. ,remigi p. ,jendresen c.b. ,ferguson g.c. ,desprat n. ,buffing m.f. ,sauer u. ,beaumont h.j.e. ,martinussen j. ,kilstrup m. ,rainey p.b.
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منبع
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plos biology - 2015 - دوره : 13 - شماره : 3
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چکیده
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Phenotype switching is commonly observed in nature. this prevalence has allowed the elucidation of a number of underlying molecular mechanisms. however,little is known about how phenotypic switches arise and function in their early evolutionary stages. the first opportunity to provide empirical insight was delivered by an experiment in which populations of the bacterium pseudomonas fluorescens sbw25 evolved,de novo,the ability to switch between two colony phenotypes. here we unravel the molecular mechanism behind colony switching,revealing how a single nucleotide change in a gene enmeshed in central metabolism (carb) generates such a striking phenotype. we show that colony switching is underpinned by on/off expression of capsules consisting of a colanic acid-like polymer. we use molecular genetics,biochemical analyses,and experimental evolution to establish that capsule switching results from perturbation of the pyrimidine biosynthetic pathway. of central importance is a bifurcation point at which uracil triphosphate is partitioned towards either nucleotide metabolism or polymer production. this bifurcation marks a cell-fate decision point whereby cells with relatively high pyrimidine levels favour nucleotide metabolism (capsule off),while cells with lower pyrimidine levels divert resources towards polymer biosynthesis (capsule on). this decision point is present and functional in the wild-type strain. finally,we present a simple mathematical model demonstrating that the molecular components of the decision point are capable of producing switching. despite its simple mutational cause,the connection between genotype and phenotype is complex and multidimensional,offering a rare glimpse of how noise in regulatory networks can provide opportunity for evolution. © 2015 gallie et al.
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آدرس
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new zealand institute for advanced study,massey university,auckland,new zealand,department of environmental microbiology,eawag,dübendorf,switzerland,department of environmental systems science,eth zürich,zürich, Switzerland, new zealand institute for advanced study,massey university,auckland,new zealand,santa fe institute,santa fe,nm, United States, new zealand institute for advanced study,massey university,auckland,new zealand,institute of integrative biology,eth zürich,zürich, Switzerland, new zealand institute for advanced study,massey university,auckland, New Zealand, department of systems biology,technical university of denmark,lyngby,denmark,novo nordisk foundation center for biosustainability,technical university of denmark,hørsholm, Denmark, new zealand institute for advanced study,massey university,auckland, New Zealand, laboratoire de physique statistique (umr8550),ecole normale superieure,paris,france,institut de biologie de l'ens (ibens umr 8197),ecole normale superieure,paris,france,universite paris diderot,paris, France, institute of molecular systems biology,eth zürich,zürich, Switzerland, institute of molecular systems biology,eth zürich,zürich, Switzerland, new zealand institute for advanced study,massey university,auckland,new zealand,department of bionanoscience,kavli institute of nanoscience,delft university of technology,delft, Netherlands, department of systems biology,technical university of denmark,lyngby, Denmark, department of systems biology,technical university of denmark,lyngby, Denmark, new zealand institute for advanced study,massey university,auckland,new zealand,max-planck institute for evolutionary biology,plön, Germany
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Authors
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