Bio-inspired crossover and a model of neuronal reprogramming
Författare
Summary, in English
Bio-inspired crossover:
Natural genomes are affected by various kinds of mutations, manifesting as variations in the genome. This includes modifications to individual base pairs (single nucleotide polymorphism, SNP), but also short insertions and deletions (indels), and variations in the position (translocations) or multiplicity (copy number variations) of genetic sequences. While SNPs are historically the most studied, the other, structural variations are now known to affect a large fraction of the human genome, and can result in clinically relevant expressions in the phenotype. In biology, structural variations are also known to affect evolutionary dynamics of a population. For example, most genes originate through duplication, followed by divergent evolution of the two copies. However, in computer programs simulating evolution, structural variations are rarely included. Their absence makes it difficult to study the evolutionary consequences of translocation and copy number variation in simulated models. Including them may also have positive consequences for bio-inspired computation such as genetic algorithms. In this dissertation, a theoretical framework with algorithmic implementations is presented for sexual reproduction between linear genomes structures with structural variation, including permutations, and DNA-like strings.
A model of neuronal reprogramming:
In multicellular organisms, cells typically follow a hierarchical progression from embryonal stem cells to increasingly specialised cell types. However, by manipulating the expression of key genes, it is possible to reverse this specialisation, or convert directly between terminal cell types. This technology has been applied to convert human skin cells to neurons, with promising applications in disease modelling and regenerative medicine. Understanding the gene regulation network (GRN) governing this transition is crucial for improving the efficiency of this conversion in the future. In this dissertation, we integrated known interactions described in the literature into a holistic GRN model. We measured the activity of genes that are known to play pivotal roles during a reprogramming process, and compared these data to our modelling system. We found that the reprogramming process could be accurately modelled. The interaction between two genes, PTB and nPTB, played a different role from its usual interpretation in the literature, acting as a negative feedback loop.
Natural genomes are affected by various kinds of mutations, manifesting as variations in the genome. This includes modifications to individual base pairs (single nucleotide polymorphism, SNP), but also short insertions and deletions (indels), and variations in the position (translocations) or multiplicity (copy number variations) of genetic sequences. While SNPs are historically the most studied, the other, structural variations are now known to affect a large fraction of the human genome, and can result in clinically relevant expressions in the phenotype. In biology, structural variations are also known to affect evolutionary dynamics of a population. For example, most genes originate through duplication, followed by divergent evolution of the two copies. However, in computer programs simulating evolution, structural variations are rarely included. Their absence makes it difficult to study the evolutionary consequences of translocation and copy number variation in simulated models. Including them may also have positive consequences for bio-inspired computation such as genetic algorithms. In this dissertation, a theoretical framework with algorithmic implementations is presented for sexual reproduction between linear genomes structures with structural variation, including permutations, and DNA-like strings.
A model of neuronal reprogramming:
In multicellular organisms, cells typically follow a hierarchical progression from embryonal stem cells to increasingly specialised cell types. However, by manipulating the expression of key genes, it is possible to reverse this specialisation, or convert directly between terminal cell types. This technology has been applied to convert human skin cells to neurons, with promising applications in disease modelling and regenerative medicine. Understanding the gene regulation network (GRN) governing this transition is crucial for improving the efficiency of this conversion in the future. In this dissertation, we integrated known interactions described in the literature into a holistic GRN model. We measured the activity of genes that are known to play pivotal roles during a reprogramming process, and compared these data to our modelling system. We found that the reprogramming process could be accurately modelled. The interaction between two genes, PTB and nPTB, played a different role from its usual interpretation in the literature, acting as a negative feedback loop.
Publiceringsår
2020-03-28
Språk
Engelska
Fulltext
Dokumenttyp
Doktorsavhandling
Förlag
Lund University, Faculty of Science
Ämne
- Bioinformatics (Computational Biology)
Nyckelord
- evolutionary comuptation
- crossover
- genetic recombination
- permutation
- flexible genome
- direct neuronal reprogramming
Status
Published
Projekt
- Modelling cellular decision making in direct reprogramming to neurons
- Crossover in evolutionary algorithms with dynamic linear genome representations
Handledare
ISBN/ISSN/Övrigt
- ISBN: 978-91-7895-451-3
- ISBN: 978-91-7895-450-6
Försvarsdatum
20 april 2020
Försvarstid
13:15
Försvarsplats
Lecture hall F (K404), Sölvegatan 14 A, Lund (Live streaming: https://lu-se.zoom.us/j/68849170218)
Opponent
- Arend Hintze (Professor)