Cortagen

Monograph № 021

A tetrapeptide that appears to work not at the receptor surface but inside the nucleus itself, recalibrating the gene expression landscape of aging cortical tissue.

Sequence

4 amino acids

Half-life

Approximately 2–4 hours (estimated, in vitro)

Route

Subcutaneous · Intranasal (investigational)

Aeterna does not sell peptides. External link, vendor independently verified.

Originator

St. Petersburg Institute of Bioregulation and Gerontology

St. Petersburg, Russia · Developed under Prof. Vladimir Khavinson’s bioregulator peptide program, est. 1990s

First disclosed

1999

First described in peer-reviewed literature, Bulletin of Experimental Biology and Medicine, 1999; CAS registered as 81803-90-9

Regulatory status

Investigational

No FDA or EMA approval; studied within Russian bioregulator research framework; not listed in any active IND as of 2025

Studied for

Cortical Aging · Neuronal Gene Expression

Primary published inquiry spans cortical neuron longevity, age-related cognitive decline, and epigenetic modulation of brain tissue – St. Petersburg IBG, 1999–2019

Mechanism

What Cortagen does inside brain cells

Cortagen is a tetrapeptide – Ala-Glu-Asp-Pro – isolated originally from bovine cerebral cortex tissue. Its mechanism is not receptor-mediated in the classical pharmacological sense. Instead, the literature describes a pattern of direct chromatin interaction: short peptides of this class appear to intercalate with DNA-histone complexes, influencing transcriptional availability of genes associated with neuronal maintenance, apoptotic resistance, and antioxidant defense. The result, as observed in cell and animal models, is a shift in the gene expression landscape of aging cortical tissue – not a single-target effect, but a broad recalibration of the molecular vocabulary neurons use to sustain themselves.

Cortagen is the tetrapeptide Ala-Glu-Asp-Pro, originally isolated from bovine cerebral cortex and studied for its apparent interaction with chromatin. Fluorescence spectroscopy suggests binding at the histone-DNA interface, implying an effect on transcriptional accessibility rather than classical surface-receptor signaling.

Antioxidant gene expression appears to increase in aged cortical tissue exposed to Cortagen. In rat models, transcription of superoxide dismutase and catalase isoforms rises in older tissue, a pattern not observed in young cortex.

Apoptotic signaling is reduced in cortical neurons under oxidative stress following Cortagen treatment. Reported declines in Bax expression and caspase-3 activity support the working hypothesis that chromatin remodeling lowers transcriptional readiness across pro-apoptotic gene programs.

Neuroendocrine regulation may also shift in response to Cortagen in aged animals. Reported normalization of cortical melatonin receptor density and diurnal corticosterone rhythms remains mechanistically unresolved and may reflect either downstream chromatin effects or a separate pathway.

What we observe

Changes seen with Cortagen use

The outcomes below reflect patterns reported in cell culture, animal, and limited human observational studies from the IBG research program. These are not endpoints from randomized controlled trials. They are presented as a curriculum in what the science currently reports.

Cortical Neuron Survival

In aged rat cortical preparations, Cortagen treatment was associated with a statistically significant reduction in apoptotic cell counts relative to untreated controls. The effect was most pronounced in neurons subjected to concurrent oxidative stress, suggesting a protective rather than purely trophic mechanism.

Animal model · Oxidative stress protocol

Antioxidant Gene Upregulation

Transcriptomic analyses of cortical tissue from Cortagen-treated aged animals showed increased mRNA abundance for superoxide dismutase-1 and catalase. The magnitude of upregulation was modest – consistent with epigenetic de-repression rather than pharmacological induction – but reproducible across multiple experimental cohorts in the IBG series.

In vitro and in vivo · Aged tissue models

Cognitive Performance

Spatial memory tasks – including Morris water maze variants – showed improved performance in aged rodents following Cortagen administration compared to age-matched controls. The literature attributes this to improved cortical neuron viability rather than any acute neurotransmitter effect, though the mechanistic chain remains incompletely characterized.

Animal model · Aged cohort · Behavioral assay

Melatonin Receptor Density

Autoradiographic studies in aged animals reported partial restoration of MT1 and MT2 receptor density in cortical regions following Cortagen treatment. This finding has been interpreted as evidence of improved neuronal membrane integrity and receptor expression capacity, though direct causation has not been established.

Animal model · Autoradiography · Aged cohort

Pro Apoptotic Markers

Western blot analyses from treated cortical tissue preparations showed reduced Bax:Bcl-2 ratios and diminished caspase-3 cleavage products in Cortagen-treated groups. These findings are consistent across several publications from the IBG group, though independent replication in non-affiliated laboratories remains limited.

In vitro · Protein expression analysis

Animal Longevity Signals

Long-term administration studies in aged rats and mice, conducted over 12–18 month periods, reported modest but consistent increases in median lifespan in Cortagen-treated cohorts relative to controls. The IBG group has contextualized these findings within a broader bioregulator longevity framework; the data have not been replicated in primate models.

Animal model · Long-term administration · IBG series

Evidence

Studies on Cortagen

The evidence base for Cortagen is concentrated within the St. Petersburg Institute of Bioregulation and Gerontology. Independent replication is sparse. The studies below represent the most substantive peer-reviewed entries in the published record as of 2025.

Bulletin of Experimental Biology and Medicine

2002

Effect of Cortagen on Apoptosis and Antioxidant Enzyme Expression in Aged Rat Cortical Neurons

Cortical neurons isolated from 24-month-old rats and treated with Cortagen at 0.1 µg/mL showed a 34% reduction in TUNEL-positive cells relative to untreated aged controls. Concurrent upregulation of SOD-1 mRNA was observed by RT-PCR. Authors concluded that the peptide exerts a cytoprotective effect consistent with epigenetic modulation of stress-response gene clusters.

34%

reduction in apoptotic cortical neurons, aged rat model, treated vs. untreated controls

Neuroendocrinology Letters

2008

Cortagen Administration and Melatonin Receptor Restoration in the Aging Cerebral Cortex: An Autoradiographic Study

Aged Wistar rats (22 months) receiving subcutaneous Cortagen over a 30-day protocol demonstrated a 28% increase in MT1 receptor binding density in frontal cortical regions compared to saline controls, as measured by tritiated melatonin autoradiography. The authors proposed that improved neuronal membrane integrity, rather than direct receptor synthesis induction, accounts for the observed restoration.

28%

increase in MT1 melatonin receptor binding density, frontal cortex, aged rat model

Advances in Gerontology (St. Petersburg)

2014

Long-Term Bioregulator Peptide Administration and Lifespan in Aged Rodents: A Comparative Series Including Cortagen

In a 14-month longitudinal study, aged C57BL/6 mice receiving Cortagen as part of a bioregulator peptide series showed a median lifespan extension of 11.2% relative to untreated age-matched controls. Histological examination at endpoint revealed reduced cortical neuron loss and lower lipofuscin accumulation in treated animals. The authors noted that no single peptide in the series could be isolated as solely responsible for the longevity signal.

11.2%

median lifespan extension in aged C57BL/6 mice, Cortagen-inclusive bioregulator series vs. controls

Reconstitution

From lyophilized powder to a usable solution.

Reconstitution is the act of dissolving lyophilized peptide in bacteriostatic water. Done correctly, it takes under two minutes.

Peptide

20 mg lyophilized powder

Diluent

3.0 mL bacteriostatic water

Final concentration

6.67 mg/mL

Prepare the vial

Allow the lyophilized vial to reach room temperature. Wipe the stopper with an alcohol swab. Do not shake the powder.

Draw the diluent

Using a sterile syringe, draw 1 mL of bacteriostatic water (0.9% benzyl alcohol). Use a fresh needle for the draw.

Add slowly

Inject the water against the inside wall of the peptide vial, drop by drop.

Prepare the vial

Rotate or shake the vial until the solution clears. It should be visually transparent within sixty seconds. You can wait up to 20 minutes.

Note

Most reconstituted peptides are stable for approximately 10-28 days under refrigeration (2–8 °C). Bacteriostatic water is preferred because the benzyl alcohol prevents microbial growth across the usable window. You can use sterile water with shorter timeframes.

Dosing rythm

A patient titration

Schedule below mirrors the peptidedosages.com educational protocol (typical daily range: 1000–2000 mcg once daily (morning administration preferred)).

For educational reference only. Actual dosing decisions belong to a licensed practitioner with full knowledge of the member’s history.

Weeks 1–2

1000 mcg

Once daily · 15 units (0.15 mL)

Weeks 3–4

2000 mcg

Once daily · 30 units (0.30 mL)

Course Duration | 10–20 days | Per cycle · Repeat at 3–6 month intervals

10–20 days per course

Repeated courses at 3–6 month intervals · IBG series employed 2 courses per year in aged animal models

Research Ceiling | 1 mg maximum | Daily · Aged-tissue protocols only · Not established in human data

1 mg

per day (research ceiling in published IBG protocols – not a recommended target)

Reserved for specific aged-tissue protocols · Not established in human data

Handling

Storage, caution, contradiction

The molecule is delicate, the schedule is forgiving, and the contraindications are non-negotiable. Members are taught to take all three with equal seriousness.

Storage

Cold, dark, undisturbed

Lyophilized: freeze at −20 °C (−4 °F).
After reconstitution, refrigerate at 2–8 °C (35.6–46.4 °F).
Avoid freeze–thaw cycles.
Keep away from direct light at all stages; amber vials or foil wrapping are appropriate precautions.
Label each vial with reconstitution date and concentration; discard any solution showing particulate matter or discoloration.

Side effects

What members describe

Mild injection-site reactions - transient erythema or induration - have been noted in human observational reports; typically self-resolving within 24 hours.
Transient fatigue or mild somnolence has been reported anecdotally in some users, possibly reflecting neuroendocrine modulation; the mechanism is not established.
Headache of mild intensity has been noted in a minority of subjects in IBG observational series; causality has not been confirmed.
No significant hematological, hepatic, or renal adverse signals have been reported in published animal toxicology studies at research doses.
Long-term safety data in humans are absent; the absence of reported adverse events in limited observational series should not be interpreted as a safety guarantee.

Contradictions

Reasons to abstain

Known hypersensitivity to any component of the formulation, including the tetrapeptide sequence Ala-Glu-Asp-Pro.
Active neurological malignancy or history of cortical neoplasm - epigenetic modulators carry theoretical risk of altered gene expression in proliferating cells.
Pregnancy and lactation - no safety data exist; use is not supported by any published evidence in these populations.
Concurrent use of agents with significant epigenetic activity (e.g., HDAC inhibitors, DNA methyltransferase inhibitors) - additive or unpredictable transcriptional effects cannot be excluded.
Pediatric populations - the peptide has been studied exclusively in aged adult and animal models; use in developing nervous systems is without evidence and carries unknown risk.

Synergies

Cortagen combos that make sense

The pairings below reflect patterns observed in the IBG bioregulator research series and in the broader neuroprotective peptide literature. They are not prescriptive protocols. Aeterna does not dispense or sell. These combinations are presented as a vocabulary for informed conversation with a qualified clinician – not as a recommended stack for self-administration.

For educational reference only. Actual dosing decisions belong to a licensed practitioner with full knowledge of the member’s history.

Epithalon

Epithalon, the tetrapeptide Ala-Glu-Asp-Gly, shares the IBG bioregulator lineage and acts on telomerase expression and pineal gland function. The two peptides have been studied together in the IBG longevity series; their combined epigenetic activity on cortical and neuroendocrine tissue is the most documented pairing in the Khavinson literature.

Longevity · Epigenetic Regulation

Semax

Semax, an ACTH(4-7) analogue, acts through BDNF upregulation and melanocortin receptor pathways to support neuronal survival and cognitive function. Where Cortagen is proposed to act at the chromatin level, Semax operates through growth factor signaling – a complementary rather than redundant axis of neuroprotection.

Neuroprotection · BDNF Signaling

Selank

Selank’s anxiolytic and immunomodulatory profile addresses the neuroendocrine stress axis that Cortagen does not directly target. In aged populations, chronic cortisol dysregulation accelerates cortical neuron loss; Selank’s reported normalization of anxiety-related signaling may create a more favorable environment for Cortagen’s proposed cytoprotective activity.

Anxiolytic · GABAergic Modulation

Pinealon

Pinealon (Glu-Asp-Arg), another IBG-derived tripeptide, is studied for its activity in pineal and cortical tissue with particular attention to circadian gene expression. Its reported complementarity with Cortagen in the IBG series – where both were administered in aged animal longevity protocols – makes it a natural companion in any curriculum focused on cortical aging.

Neuroprotection · Circadian Regulation

FAQ

Your questions, patiently answered

We are an educational website, and we take that responsibility seriously. If your question is not here, write to us at [email protected]

What distinguishes Cortagen from other neuroprotective peptides?

Most neuroprotective peptides act through defined receptor pathways – growth factor receptors, melanocortin receptors, or ion channel modulation. Cortagen’s proposed mechanism is different in kind: it is described as a chromatin-interacting peptide, one that may influence which genes are transcriptionally available rather than which receptors are activated. This distinction matters because the effect, if real, would be broader and more durable than receptor agonism – but also harder to characterize and verify with standard pharmacological tools.

Is there human clinical trial data for Cortagen?

No randomized controlled human trials have been published for Cortagen as of 2025. The evidence base consists of in vitro studies, aged animal models, and limited observational series conducted within the St. Petersburg IBG research program. This is a meaningful limitation. The patterns reported are internally consistent, but they have not been subjected to the scrutiny of blinded, placebo-controlled human trials. Readers should weight the evidence accordingly.

How does the epigenetic mechanism proposed for Cortagen actually work?

The working model, as described in the IBG literature, holds that short peptides with the right charge distribution and spatial geometry can associate with histone proteins and linker DNA in chromatin. This association is proposed to alter the accessibility of gene promoter regions – effectively de-repressing genes that have been silenced by age-related chromatin compaction. The model is biologically plausible and consistent with what is known about chromatin remodeling, but direct structural evidence for Cortagen-chromatin binding at atomic resolution has not been published.

What is the relationship between Cortagen and the broader Khavinson bioregulator series?

Cortagen is one of approximately 20 short peptide bioregulators developed and studied by Prof. Vladimir Khavinson and colleagues at the St. Petersburg IBG over several decades. The series includes tissue-specific peptides derived from or modeled on brain, thymus, pineal gland, retina, and other organs. Cortagen is the cortex-specific entry. The series shares a common theoretical framework – that short peptides carry tissue-specific epigenetic information – and a common research methodology, which means the evidence base is coherent but not independently diverse.

Can Cortagen be administered intranasally?

Intranasal administration has been explored in the IBG literature as a route that may allow direct access to the olfactory-cortical pathway, bypassing the blood-brain barrier challenge that limits many neuropeptides. Some animal studies have employed intranasal delivery. However, the pharmacokinetic data for intranasal Cortagen in humans are not published, and no standardized intranasal protocol has been established. Subcutaneous administration remains the better-documented route.

How should Cortagen be positioned relative to established neuroprotective interventions?

Cortagen should be understood as an investigational compound with a plausible mechanism and a coherent but limited evidence base – not as a replacement for established neuroprotective practices. The literature on sleep quality, aerobic exercise, dietary pattern, and cognitive engagement as modulators of cortical aging is vastly more robust. Cortagen, if it is to be considered at all, belongs in a conversation with a qualified clinician, positioned as an adjunct to – not a substitute for – those foundational practices.

In the same family

Further entries in the curriculum.

Neuroprotective

Epithalon

The pineal tetrapeptide that anchors the IBG bioregulator series. Epithalon’s evidence base for telomerase activation and neuroendocrine normalization is the most extensive in the Khavinson corpus – a natural companion to Cortagen in any study of epigenetic aging.

Neuroprotective

Semax

An ACTH-derived heptapeptide with a well-characterized BDNF-upregulating mechanism. Where Cortagen addresses the chromatin architecture of aging neurons, Semax addresses the growth factor signaling that sustains them – two different vocabularies for the same underlying problem.

Neuroprotective

Pinealon

The IBG tripeptide studied for pineal and cortical tissue, with particular attention to circadian gene expression and neuronal apoptosis. Pinealon and Cortagen appear together in several IBG longevity protocols, making this the most contextually proximate entry in the library.

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