Detail
Article
Online article
FT
Medvik - BMC
  • Something wrong with this record ?

Impact of aging on mitochondrial respiration in various organs

J. Jedlička, Z. Tůma, K. Razak, R. Kunc, A. Kala, S. Proskauer Pena, T. Lerchner, K. Ježek, J. Kuncová

. 2022 ; 71 (Suppl. 2) : S227-S236. [pub] 202212031

Language English Country Czech Republic

Document type Journal Article

Persistent link   https://www.medvik.cz/link/bmc23000920

Mitochondria are considered central regulator of the aging process; however, majority of studies dealing with the impact of age on mitochondrial oxygen consumption focused on skeletal muscle concluding (although not uniformly) a general declining trend with advancing age. In addition, gender related differences in mitochondrial respiration have not been satisfactorily described yet. The aim of the present study was to evaluate mitochondrial oxygen consumption in various organs of aging male and female Fischer 344 rats at the ages of 6, 12 and 24 months. Mitochondrial respiration of homogenized (skeletal muscle, left and right heart ventricle, hippocampus, cerebellum, kidney cortex), gently mechanically permeabilized (liver) tissue or intact cells (platelets) was determined using high-resolution respirometry (oxygraphs O2k, Oroboros, Austria). The pattern of age-related changes differed in each tissue: in the skeletal muscle and kidney cortex of both sexes and in female heart, parameters of mitochondrial respiration significantly declined with age. Resting respiration of intact platelets displayed an increasing trend and it did not correlate with skeletal muscle respiratory states. In the heart of male rats and brain tissues of both sexes, respiratory states remained relatively stable over analyzed age categories with few exceptions of lower mitochondrial oxygen consumption at the age of 24 months. In the liver, OXPHOS capacity was higher in females than in males with either no difference between the ages of 6 and 24 months or even significant increase at the age of 24 months in the male rats. In conclusion, the results of our study indicate that the concept of general pattern of age-dependent decline in mitochondrial oxygen consumption across different organs and tissues could be misleading. Also, the statement of higher mitochondrial respiration in females seems to be conflicting, since the gender-related differences may vary with the tissue studied, combination of substrates used and might be better detectable at younger ages than in old animals.

References provided by Crossref.org

000      
00000naa a2200000 a 4500
001      
bmc23000920
003      
CZ-PrNML
005      
20250108153118.0
007      
ta
008      
230307s2022 xr a f 000 0|eng||
009      
AR
024    7_
$a 10.33549/physiolres.934995 $2 doi
035    __
$a (PubMed)36647911
040    __
$a ABA008 $b cze $d ABA008 $e AACR2
041    0_
$a eng
044    __
$a xr
100    1_
$a Jedlička, Jan, $u Institute of Physiology, Faculty of Medicine in Plzeň, Charles University, Plzeň, Czech Republic $d 1991- $7 xx0230803 $u Biomedical Centre, Faculty of Medicine in Plzeň, Charles University, Plzeň, Czech Republic
245    10
$a Impact of aging on mitochondrial respiration in various organs / $c J. Jedlička, Z. Tůma, K. Razak, R. Kunc, A. Kala, S. Proskauer Pena, T. Lerchner, K. Ježek, J. Kuncová
520    9_
$a Mitochondria are considered central regulator of the aging process; however, majority of studies dealing with the impact of age on mitochondrial oxygen consumption focused on skeletal muscle concluding (although not uniformly) a general declining trend with advancing age. In addition, gender related differences in mitochondrial respiration have not been satisfactorily described yet. The aim of the present study was to evaluate mitochondrial oxygen consumption in various organs of aging male and female Fischer 344 rats at the ages of 6, 12 and 24 months. Mitochondrial respiration of homogenized (skeletal muscle, left and right heart ventricle, hippocampus, cerebellum, kidney cortex), gently mechanically permeabilized (liver) tissue or intact cells (platelets) was determined using high-resolution respirometry (oxygraphs O2k, Oroboros, Austria). The pattern of age-related changes differed in each tissue: in the skeletal muscle and kidney cortex of both sexes and in female heart, parameters of mitochondrial respiration significantly declined with age. Resting respiration of intact platelets displayed an increasing trend and it did not correlate with skeletal muscle respiratory states. In the heart of male rats and brain tissues of both sexes, respiratory states remained relatively stable over analyzed age categories with few exceptions of lower mitochondrial oxygen consumption at the age of 24 months. In the liver, OXPHOS capacity was higher in females than in males with either no difference between the ages of 6 and 24 months or even significant increase at the age of 24 months in the male rats. In conclusion, the results of our study indicate that the concept of general pattern of age-dependent decline in mitochondrial oxygen consumption across different organs and tissues could be misleading. Also, the statement of higher mitochondrial respiration in females seems to be conflicting, since the gender-related differences may vary with the tissue studied, combination of substrates used and might be better detectable at younger ages than in old animals.
650    _2
$a zvířata $7 D000818
650    _2
$a ženské pohlaví $7 D005260
650    _2
$a mužské pohlaví $7 D008297
650    _2
$a krysa rodu Rattus $7 D051381
650    _2
$a stárnutí $7 D000375
650    _2
$a buněčné dýchání $7 D019069
650    12
$a mitochondrie $7 D008928
650    12
$a svalové mitochondrie $x metabolismus $7 D008931
650    _2
$a kosterní svaly $x metabolismus $7 D018482
650    _2
$a spotřeba kyslíku $x fyziologie $7 D010101
650    _2
$a dýchání $7 D012119
650    _2
$a anestezie $7 D000758
655    _2
$a časopisecké články $7 D016428
700    1_
$a Tůma, Zdeněk, $d 1980- $7 xx0128863 $u Biomedical Centre, Faculty of Medicine in Plzeň, Charles University, Plzeň, Czech Republic
700    1_
$a Razak, Karim $u Institute of Physiology, Faculty of Medicine in Plzeň, Charles University, Plzeň, Czech Republic
700    1_
$a Kunc, Radovan $7 xx0301066 $u Institute of Physiology, Faculty of Medicine in Plzeň, Charles University, Plzeň, Czech Republic
700    1_
$a Kala, Annu $7 _AN116826 $u Biomedical Centre, Faculty of Medicine in Plzeň, Charles University, Plzeň, Czech Republic
700    1_
$a Proskauer Peña, Stephanie $7 xx0327367 $u Biomedical Centre, Faculty of Medicine in Plzeň, Charles University, Plzeň, Czech Republic
700    1_
$a Lerchner, Tobias $7 _AN113890 $u Institute of Physiology, Faculty of Medicine in Plzeň, Charles University, Plzeň, Czech Republic
700    1_
$a Ježek, Karel, $d 1973- $7 xx0076240 $u Biomedical Centre, Faculty of Medicine in Plzeň, Charles University, Plzeň, Czech Republic
700    1_
$a Kuncová, Jitka, $d 1964- $7 xx0078884 $u Institute of Physiology, Faculty of Medicine in Plzeň, Charles University, Plzeň, Czech Republic
773    0_
$w MED00003824 $t Physiological research $x 1802-9973 $g Roč. 71, Suppl. 2 (2022), s. S227-S236
856    41
$u https://pubmed.ncbi.nlm.nih.gov/36647911 $y Pubmed
910    __
$a ABA008 $b A 4120 $c 266 $y p $z 0
990    __
$a 20230307 $b ABA008
991    __
$a 20250108153113 $b ABA008
999    __
$a ok $b bmc $g 1928841 $s 1187115
BAS    __
$a 3
BAS    __
$a PreBMC-MEDLINE
BMC    __
$a 2022 $b 71 $c Suppl. 2 $d S227-S236 $e 202212031 $i 1802-9973 $m Physiological research $n Physiol. Res. (Print) $x MED00003824
LZP    __
$b NLK198 $a Pubmed-20230307

Find record

Citation metrics

Archiving options