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dc.contributor.authorJohanna, Hörberg
dc.date.accessioned2022-10-13T07:03:37Z
dc.date.available2022-10-13T07:03:37Z
dc.date.issued2022-10-13
dc.identifier.isbn978-91-8009-993-6 (PRINT), 978-91-8009-994-3 (PDF)
dc.identifier.urihttps://hdl.handle.net/2077/73631
dc.description.abstractDNA transcription involves the association of multiple proteins with DNA to convert the genetic information into messenger-RNA transcripts, which later will be translated into proteins. Con-trolled regulation of transcription is imperative for preserving the healthy and homeostatic state of cells. In eukaryotes, where the accessibility of DNA is limited by the chromatin packaging, transcriptional control occurs primarily at the initiation stage. The initiation of transcription is regulated by a class of proteins termed transcription factors, which recognise and bind with high specificity short non-coding DNA fragments, so-called response elements, to modulate the re-cruitment of the transcription machinery. The mapping of how transcription factors achieve binding specificity for their genomic target sites, shielded by the massive amount of non-specific DNA, remains incomplete despite decades of dedicated research. Over the years, traditional structure determination techniques have provided multiple insights into specificity of transcrip-tion factors-DNA interactions, though from a more static perspective. We still lack information on why transcription factors bind related sequences with different affinity and unrelated se-quences with similar affinity. Furthermore, the response elements occur more frequently in the genome than the actual genes regulated by the transcription factors. To understand these aspects of transcriptional control, it is imperative also to study the dynamic aspects of the transcription factors-DNA interactions. Until relatively recently, DNA has been looked at as a rather passive component in the recognition process. However, DNA is highly polymorphic and its flexibility is sequence specific, allowing DNA to adapt in response to various conditions. In addition, DNA state constantly changes during the life time of a cell as a consequence of DNA supercoiling, the predominant regulatory force of transcriptional control. DNA supercoiling, introduced by molec-ular motors, can propagate along the chromatin fibre, altering the accessibility of the genetic code, which in turn could affect the binding of transcription factors. Taken together, reveals DNA as the key driver of many biological processes. In this thesis, I use computational meth-ods, to unravel mechanistic details of eukaryotic transcriptional control. I study naked DNA and DNA interactions with various transcription factors, in particular BZIP- and BHTH-factors. In my quest, I have uncovered the mechanism of how DNA epigenetic modifications and transcrip-tion factors binding modulate the torsional rigidity of DNA; and how these properties can be utilised in the regulation of transcription. I have also contributed to the understanding of how transcription factors exploit the local sequence specific plasticity of DNA in recognition of their genomic target sites, and how small alterations in DNA flexibility due to DNA methylation could make their targets sites unrecognisable. The major conclusion from this thesis work, is that the enigma of selective binding of transcription factors has its solution in the dynamics of transcrip-tion factor-DNA complexation combined with sequence specific DNA flexibility of response elements but also their flanking sites. The flanking sites modulate the conformational adaptability of the response elements, making them more shape-complementary for the transcription factor to form specific contacts, which increases the stability of the complex. The level of conformational adaptability of the DNA response elements to the binding by transcription factor, could modulate the degree of torsional rigidity of DNA to undergo supercoiling transitions, which in turn may modulate the recruitment of different collaborative transcription factors control how long gene promoters stay open and consequently being transcribed.en_US
dc.language.isoengen_US
dc.relation.haspart1. Hörberg, J., Moreau, K., Tamás, M. J. & Reymer, A. Sequence-specific dynamics of DNA response elements and their flanking sites regulate the recognition by AP-1 transcription factors. Nucleic Acids Res. 49, 9280-9293 (2021). http://dx.doi.org/10.1093/nar/gkab691en_US
dc.relation.haspart2. Hörberg, J. & Reymer, A. A sequence environment modulates the impact of methylation on the torsional rigidity of DNA. Chem. Commun. 54, 11885-11888 (2018). http://dx.doi.org/10.1039/c8cc06550ken_US
dc.relation.haspart3. Hörberg, J. & Reymer, A. Specifically bound BZIP transcription factors modulate DNA super-coiling transitions. Sci. Rep. 10, 1-10 (2020). http://dx.doi.org/10.1038/s41598-020-75711-4en_US
dc.relation.haspart4. Hörberg, J., Moreau, K. & Reymer, A. Homologous BHLH transcription factors induce distinct deformations of torsionally-stressed DNA: a potential transcription regulation mechanism. QRB Discovery, 3, e4 (2022). http://dx.doi.org/10.1017/qrd.2022.5en_US
dc.relation.haspart5. Hörberg, J., Hallbäck, B., Moreau, K. & Reymer, A. Abnormal methylation in NDUFA13 gene promoter of breast cancer cells breaks the cooperative DNA recognition by transcription factors. Manuscript https://doi.org/10.1101/2022.06.01.494372en_US
dc.subjectTranscriptional controlen_US
dc.subjectGene expression regulationen_US
dc.subjectDNA supercoilingen_US
dc.subjectDNA methylationen_US
dc.subjectDNA-protein recognitionen_US
dc.subjectBasic-Leucine-Zipper transcription factorsen_US
dc.subjectBasic-Helix-Loop-Helix transcription factorsen_US
dc.subjectSequence specific DNA plasticityen_US
dc.subjectTranscription factor cooperativityen_US
dc.subjectCanceren_US
dc.subjectMolecular modellingen_US
dc.subjectMolecular dynamicsen_US
dc.titleUnravelling Mechanistic Insights of Eukaryotic Transcriptional Controlen_US
dc.typeTextswe
dc.type.svepDoctoral thesiseng
dc.gup.mailjohanna.horberg@gu.seen_US
dc.type.degreeDoctor of Philosophyen_US
dc.gup.originUniversity of Gothenburg. Faculty of Scienceen_US
dc.gup.departmentDepartment of Chemistry and Molecular Biology ; Institutionen för kemi och molekylärbiologien_US
dc.gup.defenceplaceTorsdagen den 10 november 2022, kl. 10:00, Hörsal Arvid Carlsson, Academicum, Medicinaregatan 3en_US
dc.gup.defencedate2022-11-10
dc.gup.dissdb-fakultetMNF


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