Molecular adaptations to diving-induced hypoxia. Diurnal variations in cellular and mitochondrial hypoxia tolerance in the hooded seal (Cystophora cristata)

Ciccone, Chiara

dc.contributor.advisor	Folkow, Lars
dc.contributor.author	Ciccone, Chiara
dc.date.accessioned	2024-11-05T13:44:45Z
dc.date.available	2024-11-05T13:44:45Z
dc.date.embargoEndDate	2025-11-26
dc.date.issued	2024-11-26
dc.description.abstract	<p>Hypoxia may be defined as a state of O<sub>2</sub> deficiency in which cellular energetic homeostasis is challenged. Prolonged exposure to hypoxia can lead to a bioenergetic collapse as it induces a switch from mitochondrial oxidative metabolism to a mainly glycolytic one, which is not sustainable over time. Recent evidence shows that mitochondrial metabolic response to hypoxia also depends on the circadian clock. Although most species are not able to tolerate hypoxia over time, some live permanently or periodically under hypoxic conditions. Breath-hold diving mammals, like the deep-diving hooded seal (<i>Cystophora cristata</i>), display a set of systemic and cellular/molecular adaptations that convey them enhanced hypoxia tolerance. It has been hypothesised that the hooded seal brain is endowed with alternate metabolic pathways between neurons and astrocytes, in which neurons may periodically rely on glycolysis, with astrocytes metabolising the produced lactate, enabling their brain to tolerate repeated exposure to severely hypoxic conditions. The objectives of this thesis were to investigate 1) mitochondria-clock interactions in this hypoxia-tolerant species and 2) the role of mitochondrial oxidative metabolism in hooded seal neurons and astrocytes. <p>In paper I, we show that hooded seals display diurnal variation in diving behaviour, with longer dives during day than night. Further, by using primary skin fibroblasts we characterised the hooded seal circadian clock: two core clock genes displayed circadian expression which was maintained also under constant conditions. Finally, we show the presence of a clock-mediated change in mitochondrial metabolic efficiency, possibly in coordination with daily changes in diving efforts. In paper II, we found that adult hooded seal astrocytes have higher mitochondrial density than seal neurons, which is opposite to the situation in mice. In addition, via high resolution respirometry of primary astrocytic and neuronal cultures, we show that mitochondria of hooded seal astrocytes have a similar or possibly higher oxidative capacity than neurons. Finally, in paper III, we present three cell lines immortalised from hooded seal primary astrocytes that may serve as <i>in vitro</i> models in future studies into brain function and hypoxia tolerance in diving mammals. High resolution respirometry showed that these astrocytic cell lines have the capacity to oxidise both glucose and lactate for mitochondrial energy production. <p>Overall, the results presented in this thesis work highlight the importance of regulation of mitochondrial oxidative metabolism in hypoxia tolerance physiology and add new knowledge on some of the various hypoxia-induced adaptations in a remarkable species such as the hooded seal.	en_US
dc.description.doctoraltype	ph.d.	en_US
dc.description.popularabstract	Diving mammals, like the hooded seal (Cystophora cristata), routinely experience conditions of low oxygen availability (hypoxia). To be able to face this challenge, diving mammals have evolved a series of systemic and cellular/molecular adaptations conveying them enhanced hypoxia tolerance. The objective of this thesis was to investigate how mitochondria, the organelles were oxygen is consumed to produce energy, are adapted to hypoxia. To do so we used primary cell cultures and high resolution respirometry to investigate cell-specific brain mitochondrial metabolism and the interaction between the mitochondria and molecular clock. The latter is indeed involved in circadian regulation of mitochondrial metabolism and regulation of the hypoxia response in tissues and cells. Finally, we present a new stable cell line which could be used as in vitro model for future studies on hypoxia tolerance in diving mammals.	en_US
dc.identifier.isbn	978-82-8266-269-7
dc.identifier.uri	https://hdl.handle.net/10037/35447
dc.language.iso	eng	en_US
dc.publisher	UiT The Arctic University of Norway	en_US
dc.publisher	UiT Norges arktiske universitet	en_US
dc.relation.haspart	<p>Paper I: Ciccone, C., Kante, F., Folkow, L.P., Hazlerigg, D.G., West, A.C. & Wood, S.H. (2024). Circadian coupling of mitochondria in a deep diving mammal. <i>Journal of Experimental Biology, 227</i>(7), jeb246990. Also available in Munin at <a href=https://hdl.handle.net/10037/35199>https://hdl.handle.net/10037/35199</a>. <p>Paper II: Ciccone, C., Dötterer, S.E., Geßner, C., West, A.C., Wood, S.H., Hazlerigg, D.G. & Folkow, L.P. The metabolic roles of neurons and astrocytes in the diving brain. (Manuscript). <p>Paper III: Ciccone, C., Wood, S.H., Hazlerigg, D.G., Folkow, L.P. & West, A.C. AstroSel: a stable astrocytic cell line to study hypoxia tolerance and lactate oxidation in the brain of an Arctic pinniped. (Manuscript).	en_US
dc.rights.accessRights	embargoedAccess	en_US
dc.rights.holder	Copyright 2024 The Author(s)
dc.rights.uri	https://creativecommons.org/licenses/by-nc-sa/4.0	en_US
dc.rights	Attribution-NonCommercial-ShareAlike 4.0 International (CC BY-NC-SA 4.0)	en_US
dc.subject	Hypoxia	en_US
dc.subject	Diving mammals	en_US
dc.subject	Mitochondria	en_US
dc.subject	Biological clock	en_US
dc.title	Molecular adaptations to diving-induced hypoxia. Diurnal variations in cellular and mitochondrial hypoxia tolerance in the hooded seal (Cystophora cristata)	en_US
dc.type	Doctoral thesis	en_US
dc.type	Doktorgradsavhandling	en_US