Analysis of Biochemical Reaction Networks using Tropical and Polyhedral Geometry Methods

The field of systems biology makes an attempt to realise various biological functions and processes as the emergent properties of the underlying biochemical network model. The area of computational systems biology deals with the computational methods to compute such properties. In this context, the thesis primarily discusses novel computational methods to compute the emergent properties as well as to recognize the essence in complex network models. The computational methods described in the thesis are based on the computer algebra techniques, namely tropical geometry and extreme currents. Tropical geometry is based on ideas of dominance of monomials appearing in a system of differential equations, which are often used to describe the dynamics of the network model. In such differential equation based models, tropical geometry deals with identification of the metastable regimes, defined as low dimensional regions of the phase space close to which the dynamics is much slower compared to the rest of the phase space. The application of such properties in model reduction and symbolic dynamics are demonstrated in the network models obtained from a public database namely Biomodels. Extreme currents are limiting edges of the convex polyhedrons describing the admissible fluxes in biochemical networks, which are helpful to decompose a biochemical network into a set of irreducible pathways. The pathways are shown to be associated with given clinical outcomes thereby providing some mechanistic insights associated with the clinical phenotypes. Similar to the tropical geometry, the method based on extreme currents is evaluated on the network models derived from a public database namely KEGG. Therefore, this thesis makes an attempt to explain the emergent properties of the network model by determining extreme currents or metastable regimes. Additionally, their applicability in the real world network models are discussed

Analysis of Reaction Network Systems Using Tropical Geometry

We discuss a novel analysis method for reaction network systems with polynomial or rational rate functions. This method is based on computing tropical equilibrations defined by the equality of at least two dominant monomials of opposite signs in the differential equations of each dynamic variable. In algebraic geometry, the tropical equilibration problem is tantamount to finding tropical prevarieties, that are finite intersections of tropical hypersurfaces. Tropical equilibrations with the same set of dominant monomials define a branch or equivalence class. Minimal branches are particularly interesting as they describe the simplest states of the reaction network. We provide a method to compute the number of minimal branches and to find representative tropical equilibrations for each branch.Comment: Proceedings Computer Algebra in Scientific Computing CASC 201

A geometric method for model reduction of biochemical networks with polynomial rate functions

Model reduction of biochemical networks relies on the knowledge of slow and fast variables. We provide a geometric method, based on the Newton polytope, to identify slow variables of a biochemical network with polynomial rate functions. The gist of the method is the notion of tropical equilibration that provides approximate descriptions of slow invariant manifolds. Compared to extant numerical algorithms such as the intrinsic low dimensional manifold method, our approach is symbolic and utilizes orders of magnitude instead of precise values of the model parameters. Application of this method to a large collection of biochemical network models supports the idea that the number of dynamical variables in minimal models of cell physiology can be small, in spite of the large number of molecular regulatory actors

Geometric analysis of pathways dynamics: application to versatility of TGF-β receptors

International audienceWe propose a new geometric approach to describe the qualitative dynamics of chemical reactions networks. By this method we identify metastable regimes, defined as low dimensional regions of the phase space close to which the dynamics is much slower compared to the rest of the phase space. These metastable regimes depend on the network topology and on the orders of magnitude of the kinetic parameters. Benchmarking of the method on a computational biology model repository suggests that the number of metastable regimes is sub-exponential in the number of variables and equations. The dynamics of the network can be described as a sequence of jumps from one metastable regime to another. We show that a geometrically computed con-nectivity graph restricts the set of possible jumps. We also provide finite state machine (Markov chain) models for such dynamic changes. Applied to signal transduction models, our approach unravels dynamical and functional * corresponding author capacities of signalling pathways, as well as parameters responsible for speci-ficity of the pathway response. In particular, for a model of TGFβ signalling, we find that the ratio of TGFBR2 to TGFBR1 receptors concentrations can be used to discriminate between metastable regimes. Using expression data from the NCI60 panel of human tumor cell lines, we show that aggressive and non-aggressive tumour cell lines function in different metastable regimes and can be distinguished by measuring the relative concentrations of receptors of the two types

The SYMBIONT Project: Symbolic Methods for Biological Networks

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