4.7 Article

Hypertrophy of Rat Skeletal Muscle Is Associated with Increased SIRT1/Akt/mTOR/S6 and Suppressed Sestrin2/SIRT3/FOXO1 Levels

INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES (2021)

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Journal

INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES
Volume 22, Issue 14, Pages -

Publisher

MDPI
DOI: 10.3390/ijms22147588

Keywords

overload-induced hypertrophy; skeletal muscle; anabolic signaling pathways; redox regulation

Categories

Biochemistry & Molecular Biology Chemistry, Multidisciplinary

Funding

  1. National Excellence Program at the University of Physical Education, Innovation and Technology Ministry, Hungary [126823]
  2. Scientific Excellence Program at the University of Physical Education, Innovation and Technology Ministry, Hungary [TUDFO/51757/2019-ITM]
  3. Hungarian Thematic Excellence Program from the Hungarian National Research, Development and Innovation Office [TKP2020-NKA-26]

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The study used an overload model in rats to investigate the molecular signaling pathways involved in skeletal muscle hypertrophy. Results showed an increase in muscle mass and upregulation of anabolic signaling pathways like SIRT1, Akt, mTOR, and S6, while downregulation of FOXO1 and SIRT3 suggested reduced protein breakdown and mitophagy. Additionally, decreased levels of NAD(+), sestrin2, and OGG1 indicated a change in the redox milieu of the skeletal muscle during overload-induced hypertrophy.
Despite the intensive investigation of the molecular mechanism of skeletal muscle hypertrophy, the underlying signaling processes are not completely understood. Therefore, we used an overload model, in which the main synergist muscles (gastrocnemius, soleus) of the plantaris muscle were surgically removed, to cause a significant overload in the remaining plantaris muscle of 8-month-old Wistar male rats. SIRT1-associated pro-anabolic, pro-catabolic molecular signaling pathways, NAD and H2S levels of this overload-induced hypertrophy were studied. Fourteen days of overload resulted in a significant 43% (p < 0.01) increase in the mass of plantaris muscle compared to sham operated animals. Cystathionine-beta-synthase (CBS) activities and bioavailable H2S levels were not modified by overload. On the other hand, overload-induced hypertrophy of skeletal muscle was associated with increased SIRT1 (p < 0.01), Akt (p < 0.01), mTOR, S6 (p < 0.01) and suppressed sestrin 2 levels (p < 0.01), which are mostly responsible for anabolic signaling. Decreased FOXO1 and SIRT3 signaling (p < 0.01) suggest downregulation of protein breakdown and mitophagy. Decreased levels of NAD(+), sestrin2, OGG1 (p < 0.01) indicate that the redox milieu of skeletal muscle after 14 days of overloading is reduced. The present investigation revealed novel cellular interactions that regulate anabolic and catabolic processes in the hypertrophy of skeletal muscle.

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