肝脏线粒体对体力活动的适应:性别二态性、PGC1α 和 BNIP3 介导的线粒体自噬的影响。
Hepatic mitochondrial adaptations to physical activity: impact of sexual dimorphism, PGC1α and BNIP3-mediated mitophagy.
机构信息
Molecular and Integrative Physiology, University of Kansas Medical Center, Kansas City, KS, 66160, USA.
Kansas City VA Medical Center, Kansas City, MO, 64128, USA.
出版信息
J Physiol. 2018 Dec;596(24):6157-6171. doi: 10.1113/JP276539. Epub 2018 Aug 28.
KEY POINTS
Hepatic mitochondrial adaptations to physical activity may be regulated by mitochondrial biogenesis (PGC1α) and mitophagy (BNIP3). Additionally, these adaptations may be sex-dependent. Chronic increase in physical activity lowers basal mitochondrial respiratory capacity in mice. Female mice have higher hepatic electron transport system protein content, elevated respiratory capacity, lowered mitophagic flux, and emit less mitochondrial H O independent of physical activity. Males require chronic daily physical activity to attain a similar mitochondrial phenotype compared to females. In contrast, females have limited hepatic adaptations to chronic physical activity. Livers deficient in PGC1α and BNIP3 display similar mitochondrial adaptations to physical activity to those found in wild-type mice.
ABSTRACT
Hepatic mitochondrial adaptations to physical activity may be regulated by biogenesis- and mitophagy-associated pathways in a sex-dependent manner. Here, we tested if mice with targeted deficiencies in liver-specific peroxisome proliferator-activated receptor γ coactivator 1α (PGC1α; LPGC1α ) and BCL2/adenovirus E1B 19 kDa protein-interacting protein 3 (BNIP3)-mediated mitophagy (BNIP3 ) would have reduced physical activity-induced adaptations in respiratory capacity, H O emission and mitophagy compared to wild-type (WT) controls and if these effects were impacted by sex. Male and female WT, LPGC1α and BNIP3 C57BL6/J mice were divided into groups that remained sedentary or had access to daily physical activity via voluntary wheel running (VWR) (n = 6-10/group) for 4 weeks. Mice had ad libitum access to low-fat diet and water. VWR reduced basal mitochondrial respiration, increased mitochondrial coupling and altered ubiquitin-mediated mitophagy in a sex-specific manner in WT mice. Female mice of all genotypes displayed higher electron transport system content, displayed increased ADP-stimulated respiration, produced less mitochondrially derived reactive oxygen species, exhibited reduced mitophagic flux, and were less responsive to VWR compared to males. Males responded more robustly to VWR-induced changes in hepatic mitochondrial function resulting in a match to adaptations found in females. Deficiencies in PGC1α and BNIP3 alone did not largely alter mitochondrial adaptations to VWR. However, VWR restored sex-dependent abnormalities in mitophagic flux in LPGC1α . Finally, BNIP3 mice had elevated mitochondrial content and increased mitochondrial respiration putatively through repressed mitophagic flux. In conclusion, hepatic mitochondrial adaptations to physical activity are more dependent on sex than PGC1α and BNIP3.
要点
肝脏对体力活动的线粒体适应可能受线粒体生物发生(PGC1α)和线粒体自噬(BNIP3)调节。此外,这些适应可能依赖于性别。慢性增加体力活动会降低小鼠的基础线粒体呼吸能力。雌性小鼠的肝电子传递系统蛋白含量较高,呼吸能力升高,线粒体自噬通量降低,并且无论体力活动如何,产生的线粒体 H2O 较少。雄性小鼠需要进行慢性日常体力活动才能达到与雌性相似的线粒体表型。相比之下,雌性小鼠对慢性体力活动的肝脏适应有限。缺乏 PGC1α 和 BNIP3 的肝脏显示出与野生型小鼠相似的线粒体对体力活动的适应。
摘要
肝脏对体力活动的线粒体适应可能通过生物发生和与自噬相关的途径以性别依赖的方式进行调节。在这里,我们测试了肝特异性过氧化物酶体增殖物激活受体 γ 共激活因子 1α(PGC1α;LPGC1α)和 BCL2/腺病毒 E1B 19 kDa 蛋白相互作用蛋白 3(BNIP3)介导的线粒体自噬(BNIP3)缺失的小鼠与野生型(WT)对照相比,在呼吸能力、H2O 排放和线粒体自噬方面是否会减少体力活动引起的适应,以及这些影响是否受性别影响。雄性和雌性 WT、LPGC1α 和 BNIP3 C57BL6/J 小鼠被分为久坐组或通过自愿轮跑(VWR)(n=6-10/组)进行每日体力活动组,持续 4 周。小鼠可以自由摄入低脂饮食和水。VWR 以性别特异性方式降低了 WT 小鼠的基础线粒体呼吸,增加了线粒体偶联并改变了泛素介导的线粒体自噬。所有基因型的雌性小鼠的电子传递系统含量较高,ADP 刺激的呼吸增加,产生的线粒体衍生活性氧较少,线粒体自噬通量降低,对 VWR 的反应不如雄性小鼠。雄性小鼠对 VWR 引起的肝线粒体功能变化的反应更为强烈,从而与雌性小鼠的适应相匹配。PGC1α 和 BNIP3 的单独缺失并没有在很大程度上改变 VWR 引起的线粒体适应。然而,VWR 恢复了 LPGC1α 中依赖于性别的线粒体自噬通量异常。最后,BNIP3 小鼠的线粒体含量增加,线粒体呼吸增加,可能是通过抑制线粒体自噬通量实现的。总之,肝脏对体力活动的线粒体适应比 PGC1α 和 BNIP3 更依赖于性别。
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