Efficiency of acetate-based isopropanol synthesis in Escherichia coli W is controlled by ATP demand.

Background: Due to increasing ecological concerns, microbial production of biochemicals from sustainable carbon sources like acetate is rapidly gaining importance. However, to successfully establish large-scale production scenarios, a solid understanding of metabolic driving forces is required to inform bioprocess design. To generate such knowledge, we constructed isopropanol-producing Escherichia coli W strains.

Network-wide thermodynamic constraints shape NAD(P)H cofactor specificity of biochemical reactions.

The ubiquitous coexistence of the redox cofactors NADH and NADPH is widely considered to facilitate an efficient operation of cellular redox metabolism. However, it remains unclear what shapes the NAD(P)H specificity of specific redox reactions. Here, we present a computational framework to analyze the effect of redox cofactor swaps on the maximal thermodynamic potential of a metabolic network and use it to investigate key aspects of redox cofactor redundancy in Escherichia coli.

StrainDesign: a comprehensive Python package for computational design of metabolic networks.

Summary: Various constraint-based optimization approaches have been developed for the computational analysis and design of metabolic networks. Herein, we present StrainDesign, a comprehensive Python package that builds upon the COBRApy toolbox and integrates the most popular metabolic design algorithms, including nested strain optimization methods such as OptKnock, RobustKnock and OptCouple as well as the more general minimal cut sets approach. The optimization approaches are embedded in individual modules, which can also be combined for setting up more elaborate strain design problems.

CNApy: a CellNetAnalyzer GUI in Python for analyzing and designing metabolic networks.

Summary: Constraint-based reconstruction and analysis (COBRA) is a widely used modeling framework for analyzing and designing metabolic networks. Here, we present CNApy, an open-source cross-platform desktop application written in Python, which offers a state-of-the-art graphical front-end for the intuitive analysis of metabolic networks with COBRA methods. While the basic look-and-feel of CNApy is similar to the user interface of the MATLAB toolbox CellNetAnalyzer, it provides various enhanced features by using components of the powerful Qt library.

Designing microbial communities to maximize the thermodynamic driving force for the production of chemicals.

Microbial communities have become a major research focus due to their importance for biogeochemical cycles, biomedicine and biotechnological applications. While some biotechnological applications, such as anaerobic digestion, make use of naturally arising microbial communities, the rational design of microbial consortia for bio-based production processes has recently gained much interest. One class of synthetic microbial consortia is based on specifically designed strains of one species.

Automatic construction of metabolic models with enzyme constraints.

Background: In order to improve the accuracy of constraint-based metabolic models, several approaches have been developed which intend to integrate additional biological information. Two of these methods, MOMENT and GECKO, incorporate enzymatic (kcat) parameters and enzyme mass constraints to further constrain the space of feasible metabolic flux distributions. While both methods have been proven to deliver useful extensions of metabolic models, they may considerably increase size and complexity of the models and there is currently no tool available to fully automate generation and calibration of such enzyme-constrained models from given stoichiometric models.

Computational exploration of cis-regulatory modules in rhythmic expression data using the "Exploration of Distinctive CREs and CRMs" (EDCC) and "CRM Network Generator" (CNG) programs.

Understanding the effect of cis-regulatory elements (CRE) and clusters of CREs, which are called cis-regulatory modules (CRM), in eukaryotic gene expression is a challenge of computational biology. We developed two programs that allow simple, fast and reliable analysis of candidate CREs and CRMs that may affect specific gene expression and that determine positional features between individual CREs within a CRM. The first program, "Exploration of Distinctive CREs and CRMs" (EDCC), correlates candidate CREs and CRMs with specific gene expression patterns.