A bottom-up approach to gene regulation

Guido, Nicholas; Wang, Xiao; Adalsteinsson, David; McMillen, David R.; Hasty, Jeff; Cantor, Charles R.; Elston, Timothy C.; Collins, James J.

doi:10.1038/nature04473

Cited by 297 publications

(268 citation statements)

References 28 publications

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“…Importantly, as local dynamics can then propagate through biomolecular networks-for example, via signal transduction pathways [26][27][28][29][30][31] , potentially expressing themselves in species that are otherwise directly involved only in strictly classical kinetics-the presence of just one such mechanism within a larger biological process may lead to a variety of system-wide nonclassical behavior modes 22,[32][33][34][35][36][37][38][39][40] . Given such potentially global implications of locally deviant pathway dynamics, we hope that this work may offer biologists involved with kinetic analysis or molecular modeling additional tools and intuition to help decide whether their work requires the use of discrete and stochastic chemical master equation-based methods or whether the simpler classical chemical kinetics framework is sufficient.…”

Section: Discussionmentioning

confidence: 99%

Deviant effects in molecular reaction pathways

2006

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In biological networks, any manifestations of behaviors substantially 'deviant' from the predictions of continuousdeterministic classical chemical kinetics (CCK) are typically ascribed to systems with complex dynamics and/or a small number of molecules. Here we show that in certain cases such restrictions are not obligatory for CCK to be largely incorrect. By systematically identifying properties that may cause significant divergences between CCK and the more accurate discrete-stochastic chemical master equation (CME) system descriptions, we comprehensively characterize potential CCK failure patterns in biological settings, including consequences of the assertion that CCK is closer to the 'mode' rather than the 'average' of stochastic reaction dynamics, as generally perceived. We demonstrate that mechanisms underlying such nonclassical effects can be very simple, are common in cellular networks and result in often unintuitive system behaviors. This highlights the importance of deviant effects in biotechnologically or biomedically relevant applications, and suggests some approaches to diagnosing them in situ.Although the temporal evolution of a spatially homogeneous molecular system subject to a set of (bio)chemical reactions is often described macroscopically via the classical chemical kinetics (CCK) formalism through a set of deterministic differential equations (ODEs) 1 -otherwise referred to as 'reaction rate equations' or 'mass action kinetics'-this approach does not substantially reflect the fundamentally random and discrete nature of individual molecular interactions. The latter is well described by the chemical master equation (CME) 2-4 . Although this makes CME an intrinsically much more accurate description of biological or chemical molecular system dynamics, CCK is significantly more efficient computationally and could be viewed as derived from CME via a set of limiting approximations 5 .The conditions under which these approximations hold are often considered to be broadly valid for biological and/or simple chemical systems. However, as shown here, neither is guaranteed to be the case. Breakdowns in the limiting approximations can occur in some of the most basic processes owing to mechanisms that are particularly common in biological systems. These breakdowns then manifest themselves as various 'deviant nonclassical effects'-distinctive behaviors not accounted for by the classical molecular kinetic description-whereby the discrete and/or stochastic nature of reaction events conspires to drive the characteristic behavior of the system substantially away from that predicted by classical kinetics.Notably, we demonstrate that although deviant effects may be stochastic in origin, this is by no means a requirement. The behavior of the system might be accurately characterized by a deterministic formalism, albeit not by CCK. In particular, although CCK dynamics is at times casually interpreted as describing the evolution of CME averages-this is only strictly accurate for purely linear (unimolecular and consta...

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Section: Discussionmentioning

confidence: 99%

Deviant effects in molecular reaction pathways

2006

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“…For example, Ro et al [ 60] were able to take the already optimized mevalonate pathway [ 61] and extend it to produce artemisinic acid. As the number of biologically produced molecules increases, the need to reuse and mix enzymatic pathways or subpathways will increase as well [ 62]. Creation of modular subpathways that can be easily interconnected is an area of active research with much potential.…”

Section: Production Hostmentioning

confidence: 99%

Metabolic engineering of microorganisms for biofuels production: from bugs to synthetic biology to fuels

Lee

Chou

Ham

et al. 2008

Current Opinion in Biotechnology

554

302

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The ability to generate microorganisms that can produce biofuels similar to petroleum-based transportation fuels would allow the use of existing engines and infrastructure and would save an enormous amount of capital required for replacing the current infrastructure to accommodate biofuels that have properties significantly different from petroleum-based fuels. Several groups have demonstrated the feasibility of manipulating microbes to produce molecules similar to petroleum-derived products, albeit at relatively low productivity (e.g. maximum butanol production is around 20 g/L). For cost-effective production of biofuels, the fuel-producing hosts and pathways must be engineered and optimized. Advances in metabolic engineering and synthetic biology will provide new tools for metabolic engineers to better understand how to rewire the cell in order to create the desired phenotypes for the production of economically viable biofuels.

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“…Like others, i.e., [12,19] and [38,39], we consider a simple functional form to model either repression or activation of gene transcription characterized by the values (m,n). Since genetic repression is more often observed in biochemical systems, the repression case (0,2) has been widely studied in the literature [40][41][42][43][44][45], while the activation case has been seldom used [9][10][11][12][13]. Although repression tends to stabilize a dynamical system, activation coupled with degradation can show oscillatory behavior or even complex oscillations.…”

Section: General Modelmentioning

confidence: 99%

“…In general, repression, characterized by a negative feedback, is more common in biological systems because of its tendency to stabilize the concentration of relevant metabolites [7,8]. Nevertheless, activation characterized by a positive feedback is also observed in biological systems [9][10][11][12][13], and it is considered necessary for multistability [8][9][10][11][12][13][14].…”

Section: Introductionmentioning

confidence: 99%

Self-regulation in a minimal model of chemical self-replication

Lou

Peacock‐López

2011

J Biol Phys

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In biological systems, regulation plays an important role in keeping metabolite concentrations within physiological ranges. To study the dynamical implications of selfregulation, we consider a functional form used in genetic networks and couple it to a mechanism associated with chemical self-replication. For the two-variable minimal model, we find that activation can yield chemical toggles similar to those reported for gene repression in E. coli as well as more complex dynamics.

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A bottom-up approach to gene regulation

Cited by 297 publications

References 28 publications

Deviant effects in molecular reaction pathways

Deviant effects in molecular reaction pathways

Metabolic engineering of microorganisms for biofuels production: from bugs to synthetic biology to fuels

Self-regulation in a minimal model of chemical self-replication

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