AOX delays the onset of the lethal phenotype in a mouse model of Uqcrh (complex III) disease
Jacobs, Howard T.; Szibor, Marten; Rathkolb, Birgit; da Silva-Buttkus, Patricia; Aguilar-Pimentel, Juan Antonio; Amarie, Oana V.; Becker, Lore; Calzada-Wack, Julia; Dragano, Nathalia; Garrett, Lillian; Gerlini, Raffaele; Hölter, Sabine M.; Klein-Rodewald, Tanja; Kraiger, Markus; Leuchtenberger, Stefanie; Marschall, Susan; Östereicher, Manuela A.; Pfannes, Kristina; Sanz-Moreno, Adrián; Seisenberger, Claudia; Spielmann, Nadine; Stoeger, Claudia; Wurst, Wolfgang; Fuchs, Helmut; Hrabě de Angelis, Martin; Gailus-Durner, Valérie (2023-10)
Jacobs, Howard T.
Szibor, Marten
Rathkolb, Birgit
da Silva-Buttkus, Patricia
Aguilar-Pimentel, Juan Antonio
Amarie, Oana V.
Becker, Lore
Calzada-Wack, Julia
Dragano, Nathalia
Garrett, Lillian
Gerlini, Raffaele
Hölter, Sabine M.
Klein-Rodewald, Tanja
Kraiger, Markus
Leuchtenberger, Stefanie
Marschall, Susan
Östereicher, Manuela A.
Pfannes, Kristina
Sanz-Moreno, Adrián
Seisenberger, Claudia
Spielmann, Nadine
Stoeger, Claudia
Wurst, Wolfgang
Fuchs, Helmut
Hrabě de Angelis, Martin
Gailus-Durner, Valérie
10 / 2023
166760
Julkaisun pysyvä osoite on
https://urn.fi/URN:NBN:fi:tuni-202306086624
https://urn.fi/URN:NBN:fi:tuni-202306086624
Kuvaus
Peer reviewed
Tiivistelmä
The alternative oxidase, AOX, provides a by-pass of the cytochrome segment of the mitochondrial respiratory chain when the chain is unavailable. AOX is absent from mammals, but AOX from Ciona intestinalis is benign when expressed in mice. Although non-protonmotive, so does not contribute directly to ATP production, it has been shown to modify and in some cases rescue phenotypes of respiratory-chain disease models. Here we studied the effect of C. intestinalis AOX on mice engineered to express a disease-equivalent mutant of Uqcrh, encoding the hinge subunit of mitochondrial respiratory complex III, which results in a complex metabolic phenotype beginning at 4–5 weeks, rapidly progressing to lethality within a further 6–7 weeks. AOX expression delayed the onset of this phenotype by several weeks, but provided no long-term benefit. We discuss the significance of this finding in light of the known and hypothesized effects of AOX on metabolism, redox homeostasis, oxidative stress and cell signaling. Although not a panacea, the ability of AOX to mitigate disease onset and progression means it could be useful in treatment.
Kokoelmat
- TUNICRIS-julkaisut [19879]