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H19X-encoded miR-322(424)/miR-503 regulates muscle mass by targeting translation initiation factors.

Rui LiangXiaopeng ShenFan WangXin WangAlex DesJarlaisAnam SyedRaymond SabaZhi TanFang YuXuan JiShreesti ShresthaYinghong RenJin YangYoonjung ParkRobert J SchwartzBenjamin SoibamBradley K McConnellM David StewartAshok KumarYu Liu
Published in: Journal of cachexia, sarcopenia and muscle (2021)
Our study illustrates a novel pathway wherein H19X microRNAs regulate skeletal muscle growth and atrophy through regulating the abundance of translation initiation factors, thereby protein synthesis. The study highlights how translation initiation factors lie at the crux of multiple signalling pathways that control skeletal muscle mass.
Keyphrases
  • skeletal muscle
  • cell proliferation
  • long non coding rna
  • long noncoding rna
  • type diabetes