Regulation of Human Mitochondrial DNA Replication and Transcription
Abstract
Regulation of Human Mitochondrial DNA Replication and Transcription
Majda Mehmedović
Department of Medical Biochemistry and Cell biology, Institute of Biomedicine
Sahlgrenska Academy, University of Gothenburg
Gothenburg, Sweden
ABSTRACT
Mitochondria are organelles in eukaryotic cells, which through oxidative phosphorylation (OXPHOS) produce most of the ATP used to drive cellular processes. The organelle contains its own genetic material, mitochondrial DNA (mtDNA), which encodes 13 key components of the OXPHOS machinery. For its maintenance and expression, mtDNA is dependent on a large number of nuclear factors. Our understanding of these processes has progressed significantly during the last years, but much is still unknown.
The mitochondrial genome is completely coated by TFAM, which acts to compact mtDNA molecules into nucleoid structures. In this thesis we have examined how nucleoid formation contributes to regulation of mitochondrial replication and transcription. Our studies demonstrate that TFAM packaging regulates mtDNA availability, thereby directing levels of replication and transcription in vitro. These findings therefore reveal that TFAM has the potential to function as an epigenetic regulator of mtDNA transactions.
Second, we investigate the characteristics of a newly discovered mutation in TFAM that causes severe mtDNA depletion and early onset-liver failure in infants. Using a combined effort with biochemical, biophysical and cell biology techniques, we demonstrate that the mutant form of TFAM impairs transcription initiation from mitochondrial promoters. The mutant protein also impairs compaction of mtDNA.
Finally, we investigate a replication pre-termination event that leads to the formation of a displacement loop (D-loop) structure in mtDNA. We demonstrate that replication initiated at the origin of heavy-strand replication and transcription coming from the opposite direction (initiated at the heavy strand promoter) are both terminated at an evolutionary conserved sequence, which we term coreTAS. We also provide data, which suggest that coreTAS plays an important role in the regulated switch between D-loop formation and full-length replication.
Keywords: mitochondria, mtDNA, TFAM, transcription, replication
ISBN 978-91-8009-146-6 (PRINT)
ISBN 978-91-8009-147-3 (PDF)
http://hdl.handle.net/2077/66819
Parts of work
I. In vitro-reconstituted nucleoids can block mitochondrial DNA replication and transcription
Farge G*, Mehmedovic M*, Baclayon M, van den Wildenberg SM, Roos WH, Gustafsson CM, Falkenberg M.
Cell Rep. 2014 July 10; 8(1):66-74. ::doi::10.1016/j.celrep.2014.05.046 II. Mehmedović M, Martucci M, Spåhr H, Ishak L, Peter B, Mishra A, van den
Wildenberg SM, Falkenberg M, Farge G.
Disease causing mutation (P178L) in mitochondrial transcription factor A results
in impaired mitochondrial transcription initiation. Manuscript 2021 III. Regulation of DNA replication at the end of the mitochondrial D-loop involves the helicase TWINKLE and a conserved sequence element
Jemt E, Persson Ö, Shi Y, Mehmedovic M, Uhler JP, Dávila López M, Freyer C, Gustafsson CM, Samuelsson T, Falkenberg M.
Nucleic Acids Res. 2015 October 30; 43(19):9262-75. ::doi::10.1093/nar/gkv804
Degree
Doctor of Philosophy (Medicine)
University
University of Gothenburg. Sahlgrenska Academy
Institution
Institute of Biomedicine. Department of Medical Biochemistry and Cell Biology
Disputation
Fredagen den 5 februari, 2021, kl 9.00, Hörsal Arvid Carlsson, Academicum, Medicinaregatan 3, Göteborg. https://gu-se.zoom.us/j/66282399263?pwd=VzdHSXFMMVhqaE5ZS3diQkZZUGlaZz09
Date of defence
2021-02-05
majda.mehmedovic@gu.com
majda.mehmedovic@gmail.com
Date
2021-01-18Author
Mehmedović, Majda
Keywords
Mitochondria
mtDNA
replication
transcription
TFAM
Publication type
Doctoral thesis
ISBN
978-91-8009-146-6
978-91-8009-147-3
Language
eng