What does the Primal Peptides dossier on MOTS-c // Het Mitochondriale Signalerings Dossier: De Metabole Regulator cover?

MOTS-c is een mitochondrial-derived peptide (MDP) gecodeerd in mtDNA 12S rRNA — directe AMPK-activatie, GLUT4-translocatie, nucleaire translocatie en mitokine-functie. Scientific Elite dossier · side-by-side met klassieke metabole modulatoren · 3× mission-insight · ≥99% HPLC-purity.

Is MOTS-c // Het Mitochondriale Signalerings Dossier: De Metabole Regulator a research article or a product claim?

This is an editorial research dossier authored by the Primal Research Desk. It collates publicly available structure-activity literature on the reference material; it does NOT make therapeutic, dosage, or efficacy claims. Primal Peptides supplies all materials strictly for in-vitro laboratory research.

What HPLC purity does Primal Peptides supply MOTS-c at?

Primal Peptides supplies MOTS-c at ≥99% HPLC purity, independently verified by Janoshik Analytical. The COA is supplied with every order.

What is the CAS number of MOTS-c?

MOTS-c carries CAS Registry Number 1627580-64-6. This identifier maps directly to the CAS Common Chemistry and PubChem entries for the reference material.

Where can I find the Certificate of Analysis?

Every batch ships with a Janoshik Analytical HPLC COA. The PDF is linked from the corresponding product page on primalpeptides.nl and a hard copy travels with the shipment.

Signalisation Mitochondriale MOTS-c · MDP | Primal Peptides

EMERALD ENERGY · MITOCHONDRIAL-DERIVED PEPTIDE · METABOLIC REGULATOR

MOTS-c is not a classical peptide. It is a mitochondrial signal. A 16-amino-acid peptide encoded in the mitochondrial 12S rRNA gene that communicates nuclear gene expression with cellular energy status. The first metabolic regulator to cross the cell-organelle boundary at the molecular level.

The biochemical foundation — a peptide encoded in the mitochondrion

In most research models, mitochondrion-nucleus communication is approached via classical routes: ROS signalling, calcium flux, cytochrome c release. MOTS-c (Mitochondrial Open Reading frame of the Twelve S rRNA-c) breaks fundamentally with that paradigm. It is one of the first mitochondrial-derived peptides (MDPs) functioning as a direct peptide messenger between mitochondrion and nucleus — a biological pathway identified in 2015 that has since opened a new category of metabolic research.

"MOTS-c is the mitochondrion's own SMS to the nucleus. Direct peptide messaging — no second messengers, no relay-chain attenuation."

In this respect, MOTS-c is fundamentally different from classical metabolic modulators (metformin, AMPK activators, insulin sensitizers): it is not a receptor agonist or enzyme modulator, but an encoded peptide output of the mitochondrion itself — activated in response to metabolic stress and communicated to the nucleus to reprogram gene expression.

What does MOTS-c do razor-sharp differently?

MOTS-c (sequence: MRWQEMGYIFYPRKLR) operates on multiple layers simultaneously:

Direct AMPK activation in skeletal muscle and liver cell cultures → metabolic signalling without ATP-depletion trigger
GLUT4 translocation to the plasma membrane → insulin-independent glucose uptake in muscle cultures
Folate cycle modulation → direct interaction with methionine-folate metabolism
Nuclear translocation in metabolic-stress models → MOTS-c physically relocates from mitochondrion to nucleus
Modulation of adaptive nuclear gene expression in response to physiological stress
mTOR pathway interaction → balance between anabolism and autophagy without complete suppression
Mitokine function → systemic signal from mitochondrion to peripheral tissues (the term "mitokine" was coined for MOTS-c)

MOTS-c vs Classical Metabolic Modulators — Side-by-Side

Property	MOTS-c (Mitochondrial-Derived)	Classical Metabolic Modulators (Metformin / AMPK agonists)
Origin	Endogenous · encoded in 12S rRNA mtDNA	Synthetic / xenobiotic
Operating level	Mitochondrion ↔ nucleus messaging	Cytoplasmic enzyme modulation (ETC complex I / AMPK direct)
Target pathway	Direct AMPK activation + nuclear gene modulation	Indirect AMPK via ATP/AMP ratio-shift (metformin)
Amino acid count	16 (short peptide)	n/a (small-molecule drugs)
Insulin-dependency	Independent (direct GLUT4 trigger)	Mostly insulin-sensitizing (indirect)
Mitokine function	Strong · systemic signalling	None — local enzyme effect
Folate cycle interaction	Directly modulated	No significant interaction
Lactate-acidosis risk in models	Not reported	Elevated with metformin (clinical context)
Cellular compartment-specificity	Mitochondrion → cytoplasm → nucleus	Cytoplasm / mitochondrion (no nuclear translocation)
Research position	Adaptive stress-response · longevity · metabolic flexibility	Glucose homeostasis · metabolic syndrome
HPLC-purity Primal lot	≥99%	Variable (off-the-shelf pharmaceuticals)
Reconstitution	Bacteriostatic water · −20 °C	n/a (orally available)
Half-life in-vitro	~30-60 minutes (rapid clearance)	Hours to days (varies per agent)

The biochemical conclusion: Classical metabolic modulators intervene at downstream enzymes. MOTS-c is an upstream messenger from the mitochondrion itself — encoded in the organelle genome that evolved independently from the nuclear genome. A fundamentally different research instrument for fundamentally different metabolic research.

The Molecular Mechanics

MISSION INSIGHT · METABOLIC PATHWAY ACTIVATION

At the level of metabolic pathway activation in skeletal muscle and liver cell cultures, the following molecular effects are documented:

Direct AMPK phosphorylation at Thr172 → AMPK activation without ATP/AMP ratio-shift (unlike metformin)
GLUT4 translocation from intracellular vesicles to plasma membrane within 30-60 min → insulin-independent glucose uptake
Glycolysis flux increase in fasted-state muscle cultures → metabolic flexibility
Folate cycle interaction → modulation of one-carbon metabolism (relevant for methylation research)
Elevated mitochondrial biogenesis markers (PGC-1α expression) in animal models
mTOR pathway balance → autophagy response without complete suppression of protein synthesis

MISSION INSIGHT · NUCLEAR TRANSLOCATION & STRESS RESPONSE

The most unique MOTS-c property is physical translocation from mitochondrion to nucleus — a research domain that classical peptides do not make accessible:

Nuclear translocation within 60-90 min after metabolic stress in cell cultures (glucose deprivation, oxidative stress)
Direct transcription modulation → MOTS-c binds regulatory gene regions in the nucleus, not only surface receptors
Adaptive gene expression program activation → cellular stress resistance, mitochondrial biogenesis, anti-oxidative response
Heat-shock response synergy → amplifies HSP-mediated cytoprotection in stress models
Mitokine systemic signal → MOTS-c detected in circulation, influences peripheral tissues at distance
Age-related decline reversal in animal models → MOTS-c serum levels decline with age, supplementation restores baseline metabolic flexibility

MISSION INSIGHT · LONGEVITY & METABOLIC FLEXIBILITY

For research into longevity pathways and metabolic flexibility, MOTS-c delivers reproducible research data that other peptides do not replicate:

Increased metabolic flexibility in animal models → smoother switch between carbohydrate and lipid oxidation
Reduced insulin-resistance markers in obese/aged mouse models (HOMA-IR equivalent)
Mitochondrial capacity restoration in aging research → restoration of baseline ATP production capacity
Senescence-marker reduction (p21, p16) in cell cultures with chronic metabolic stress
Compatible with caloric-restriction research → MOTS-c pathway is one of the common endpoints of CR protocols in animal models

The Primal Peptides standard

Every batch is independently validated. The Certificate of Analysis (COA) is the binding source of truth for each lot — publicly available, batch-specific and generated by an independent third-party laboratory prior to shipment. We publish no claims that are not per-lot supported by the COA.

01RP-HPLC with UV-detection → purity ≥ 98–99%
02Mass spectrometry → molecular-mass confirmation
03Janoshik 3rd-party verification → public COA per lot

Our validation architecture is deliberately minimalist and strict: three reproducible assays, one independent verification, one public certificate. For the complete analytical dossier of your specific batch, consult the COA with your shipment or via our public verification page.

Waarschuwing

MOTS-c modulates mitochondrion-nucleus signalling at a pathway level not reached by classical modulators — in research models, nuclear-translocation kinetics and downstream transcription response must be strictly controlled via time-course baselines. Folate-cycle modulation may produce secondary effects on methylation-dependent processes.

Legal disclaimer: MOTS-c is intended exclusively for IN-VITRO RESEARCH. Not for human use. Not for consumption. Not for clinical or performance application.

Conclusion — The metabolic regulator encoded in the mitochondrion

MOTS-c is not the peptide that activates enzymes. It is the peptide that the mitochondrion itself uses to inform the nucleus of metabolic status — a 16-amino-acid biological SMS encoded in the mtDNA that evolved independently from the nuclear genome for billions of years. For researchers studying metabolic flexibility, longevity pathways and mitochondrion-nucleus communication at the most fundamental level, MOTS-c is the missing mitochondrial-tuned instrument.

From organelle to nucleus. Signal before substrate.

MOTS-c

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