The construction, analysis and validation of mechanistic mathematical models of protein kinetics in the context of replicative ageing in budding yeast
Abstract
Mathematical modelling constitutes a forceful tool for elucidating properties of biological systems. Using theoretical approaches in combination with experimental techniques it is possible to study specific molecular aspects of phenomena such as the ageing of human beings. In fact, as many processes are similar in simpler organisms such as the budding yeast \textit{Saccharomyces cerevisiae} it is possible to experimentally investigate for instance the accumulation of damaged proteins due to ageing in these biological systems. The aim of this thesis is to construct, analyse and validate mathematical mechanistic models of protein kinetics consisting of both ordinary and partial differential equations in the context of ageing. This is done both on a large time scale corresponding to the entire life span of cells and a short time scale corresponding to an isolated part of the cell division. The focus of the work on the large time scale is twofold, firstly the life span of individual yeast cells is modelled (Paper II) and secondly the life spans of vast numbers of cells in numerous populations are simulated (Paper III). Using a model of the accumulation of damage involving the forces cell growth, formation and repair of damage as well as the cell division, the impact of these individual parts on the overall fitness of individual cells and entire populations is investigated. On the short time scale, a more detailed model of a single protein called Cdc42 involved in the cell division is presented (Paper IV) and this theoretical framework has a high level of detail as it describes the spatial movement of the protein of interest within the cell over time. Given this precise description of the geometry of an individual cell, the mathematical properties of the model is analysed and these theoretical results are used to conduct numerical simulations of the activity of this protein. Lastly, an overall theme of the thesis is the difficulty of validating mechanistic models even in the presence of data. More precisely, as numerous and sometimes mutually exclusive models can describe a system equally well it is currently very hard, even by calibrating the models to experimental data using statistical methods, to differentiate between various models. To this end, a mathematical tool called symmetry methods is introduced as a potential remedy to this problem, and using this methodology it is possible to extract information in the data as well as in the model that is not available using standard approaches. To showcase the power of symmetries, a minimal example of the usage of these methods in the context of enzyme kinetics is presented (Paper V). In conclusion, this work suggests that novel analytical tools such as symmetry methods could complement and assist the current standard approaches for modelling protein kinetics where the purpose is to deduce the underlying mechanisms of biological systems.
Parts of work
Kappa: ISBN: 978-91-7833-911-2 (PDF), Spikblad Paper I: https://doi.org/10.1002/9783527696130.ch9 Paper II: https://doi.org/10.1038/s41598-020-58444-2 Paper III: https://doi.org/10.1101/2020.03.24.005116 Paper IV: https://doi.org/10.1101/2020.01.29.925628 Paper V: https://doi.org/10.1101/2020.01.27.922005
Degree
Doctor of Philosophy
University
Göteborgs universitet. Naturvetenskapliga fakulteten
Institution
Department of Mathematical Sciences ; Institutionen för matematiska vetenskaper
Disputation
Fredagen den 12 juni 2020, kl. 10.15, Gustaf Dalénsalen, Chalmers Campus Johanneberg, Chalmers Tvärgata 5
Date of defence
2020-06-12
johborgq@chalmers.se
Date
2020-05-04Author
Johannes, Borgqvist
Keywords
Protein kinetics
Replicative ageing
Cdc42
Ordinary differential equations
Reaction diffusion models
Parameter estimation
Model validation
Model construction
Symmetry methods
Publication type
Doctoral thesis
ISBN
978-91-7833-910-5
Language
eng