What question did this study set out to answer?

This research aims to explore the metabolic role of MOTS-c in adrenal cortex cells and its implications for steroidogenesis.

March 13, 2026

Mitochondrial open reading frame of the 12S rRNA type-c (MOTS-c) primes adrenal cortex metabolism without directly driving steroidogenesis.

Key Points

This research aims to explore the metabolic role of MOTS-c in adrenal cortex cells and its implications for steroidogenesis.
Investigation of MOTS-c impact on adrenal cortex cells
Assessment of calcium signaling and lipid metabolism
Analysis of stress-response protein levels and mitophagy
Evaluation of steroidogenic responsiveness under stress conditions
MOTS-c upregulates calcium signaling in adrenocortical cells
Enhances lipid metabolism without stimulating basal hormone synthesis
Downregulates stress-response proteins and inhibits mitophagy
Prepares cells for increased responsiveness to ACTH and stress stimuli

Abstract

MOTS-c functions as a metabolic conductor that primes adrenocortical cells for enhanced steroidogenic responsiveness without stimulating basal hormone synthesis. By upregulating calcium signaling, modulating lipid metabolism, downregulating stress-response proteins, and inhibiting mitophagy, MOTS-c establishes a preparatory metabolic state optimized for subsequent ACTH or stress stimulation. These findings reveal a novel preparatory mechanism in adrenal physiology and identify MOTS-c as a potential therapeutic target for HPA axis disorders requiring enhanced adrenal reserve capacity without basal hypercortisolemia.

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Mitochondrial open reading frame of the 12S rRNA type-c (MOTS-c) primes adrenal cortex metabolism without directly driving steroidogenesis.

Key Points

Abstract

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