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Mots-C

Mitochondrial open reading frame of the 12S rRNA-c, MT-RNR1, Mitochondrial-derived peptide MOTS-c

Quick Stats
Studies 137
Trials 5
Score 3
2023 pubmed 17 citations

MOTS-c Functionally Prevents Metabolic Disorders.

Gao. Yue Y; Wei. Xinran X; Wei. Pingying P; Lu. Huijie H; Zhong. Luying L; Tan. Jie J; Liu. Hongbo H; Liu. Zheng Z

Key Findings

  • MOTS‑c activates the AICAR‑AMPK signaling cascade, improving cellular energy balance.
  • It modulates key metabolic genes (GLUT4, STAT3, IL‑10) linked to glucose uptake, inflammation, and bone turnover.
  • Animal and early human studies suggest MOTS‑c can reduce insulin resistance, protect against obesity, and enhance muscle and bone function.

Practical Outcomes

  • For biohackers, MOTS‑c looks promising as a metabolic‑boosting supplement, especially for insulin sensitivity and body‑composition goals. However, the literature is still at a pre‑clinical/early‑clinical stage, so dosing protocols are not established yet. Keep an eye on emerging human trials for safety data before trying it, and consider pairing any future MOTS‑c use with proven AMPK‑activators like intermittent fasting or metformin-like strategies.

Summary

MOTS‑c is a tiny peptide made by mitochondria that acts like a hormone. It can improve insulin sensitivity, help prevent weight gain, boost muscle and bone health, support the immune system, and may slow aging. It does this mainly by turning on the AMPK energy‑sensing pathway and tweaking the folate‑methionine cycle, which in turn changes genes such as GLUT4, STAT3 and IL‑10.

Abstract

Mitochondrial-derived peptides are a family of peptides encoded by short open reading frames in the mitochondrial genome, which have regulatory effects on mitochondrial functions, gene expression, and metabolic homeostasis of the body. As a new member of the mitochondrial-derived peptide family, mitochondrial open reading frame of the 12S rRNA-c (MOTS-c) is regarding a peptide hormone that could reduce insulin resistance, prevent obesity, improve muscle function, promote bone metabolism, enhance immune regulation, and postpone aging. MOTS-c plays these physiological functions mainly through activating the AICAR-AMPK signaling pathways by disrupting the folate-methionine cycle in cells. Recent studies have shown that the above hormonal effect can be achieved through MOTS-c regulating the expression of genes such as GLUT4, STAT3, and IL-10. However, there is a lack of articles summarizing the genes and pathways involved in the physiological activity of MOTS-c. This article aims to summarize and interpret the interesting and updated findings of MOTS-c-associated genes and pathways involved in pathological metabolic processes. Finally, it is expected to develop novel diagnostic markers and treatment approaches with MOTS-c to prevent and treat metabolic disorders in the future.

Study Information

Provider

pubmed

Year

2023

Date

2023-01-13T00:00:00.000Z

DOI

10.3390/metabo13010125

Citations

17

References

82