Differences in liver TFAM binding to mtDNA and mtDNA damage between aged and extremely aged rats
Articolo
Data di Pubblicazione:
2019
Citazione:
Chimienti, G., Picca, A., Fracasso, F., Marzetti, E., Calvani, R., Leeuwenburgh, C., Russo, F., Lezza, A. M. S., Pesce, V., Differences in liver TFAM binding to mtDNA and mtDNA damage between aged and extremely aged rats, <>, 2019; 20 (10): 1-13. [doi:10.3390/ijms20102601] [https://hdl.handle.net/10807/220331]
Abstract:
While mitochondrial dysfunction is acknowledged as a major feature of aging, much less is known about the role of mitochondria in extended longevity. Livers from aged (28-month-old) and extremely aged (32-month-old) rats were analyzed for citrate synthase activity, mitochondrial transcription factor A (TFAM) amount, mitochondrial DNA (mtDNA), and 4.8 Kb “common deletion” contents. None of the assayed parameters differed significantly between age groups. TFAM-binding to mtDNA and the incidence of 8-oxo-deoxyguanosine in specific mtDNA regions, encompassing the origins of mtDNA replication (D-loop and Ori-L) and the 16-bp long direct repeat 1 (DR1) of the 4.8 Kb deletion, were determined. A decrease in TFAM binding was unveiled at all regions in extremely aged in comparison with aged rats. Reduced incidence of oxidized purines at all assayed regions was detected in 32-month-old rats compared with the 28-month-old group. A significant positive correlation between the incidence of 8-oxo-deoxoguanosine and TFAM-bound mtDNA was found at D-Loop and Ori-L regions only in 28-month-old rats. The absence of such correlation in 32-month-old rats indicates a different, fine-tuned regulation of TFAM binding in the two age groups and supports the existence of two different paces in aging and extended aging.
Tipologia CRIS:
Articolo in rivista, Nota a sentenza
Keywords:
8-oxodG incidence; Longevity; mtDNA common deletion; mtDNA content; Rat liver; TFAM binding
Elenco autori:
Chimienti, G.; Picca, A.; Fracasso, F.; Marzetti, Emanuele; Calvani, Riccardo; Leeuwenburgh, C.; Russo, F.; Lezza, A. M. S.; Pesce, V.
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