What's the difference between Semax and Selank?

Semax is a 7-amino-acid peptide derived from ACTH (4-10) — drives BDNF upregulation and dopamine pathway modulation, useful for focus, attention, and neuroprotection research. Selank is a 7-amino-acid peptide derived from tuftsin — drives GABAergic and serotonergic signalling, useful for anxiolysis and stress-response research. Different parent peptides, different mechanisms, different endpoints.

Can Semax and Selank be stacked?

Yes — the mechanisms are non-overlapping. Semax provides the activating/cognitive side; Selank provides the calming/anxiolytic side. Some researchers use Semax morning + Selank evening as a balanced focus + anxiolytic protocol. There are no published combination trials; this is researcher-protocol synthesis.

Which route — intranasal or injection?

Both peptides have established intranasal protocols (matching the Russian clinical 0.1% formulation). Intranasal bypasses gastric breakdown and provides rapid CNS access via the olfactory pathway. SC injection works but is unnecessary for nootropic endpoints — intranasal is the published research route.

Where can UAE researchers buy Semax?

REVIVE LAB UAE stocks HPLC-verified Semax in 10 mg lyophilised vials with lot-level COA. Selank availability varies by lot; contact via WhatsApp for current stock. Same-day Dubai dispatch on orders before 3 PM, 24-hour delivery across the UAE.

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Cognitive · Russian Peptides

Semax vs Selank — Two Russian Nootropic Peptides, Different Mechanisms

23 June 202612 min readREVIVE LAB UAE Research Desk

Semax vs Selank Russian nootropic peptide research UAE

Russian peptide pharmacology produced two flagship nootropic compounds in the late 20th century — Semax and Selank — both 7-amino-acid synthetic peptides, both with established Russian clinical use, both routinely confused in Western peptide-research discussion. The two are not interchangeable. Different parent peptides, different molecular mechanisms, different research endpoints. This is the comparison for UAE peptide researchers running cognitive or anxiolytic protocols.

For research use only. Both peptides remain research-grade material in most markets outside Russia, where they are licensed for clinical indications. The discussion below summarises published research findings.

1. The Russian peptide-pharmacology tradition

Both peptides emerged from the Soviet/Russian neuropeptide research program centred at the Institute of Molecular Genetics (Moscow) and the Institute of Drug Research. The design philosophy was distinctive: take a known endogenous peptide (ACTH, tuftsin) with central nervous system activity, identify the active fragment, then stabilise it against protease degradation by amino acid substitutions and N/C-terminal modifications.

Both compounds went through Russian phase I-III equivalents and were registered for clinical use in Russia (Semax for cognitive indications and stroke recovery; Selank for anxiety). Neither was developed in Western pharmaceutical markets, which is why they remain research-grade material in most jurisdictions outside Russia.

2. The molecular biology — different parents

Property	Semax	Selank
Parent peptide	ACTH(4-10) fragment	Tuftsin (TKPR)
Sequence	Met-Glu-His-Phe-Pro-Gly-Pro	Thr-Lys-Pro-Arg-Pro-Gly-Pro
Length	7 amino acids (heptapeptide)	7 amino acids (heptapeptide)
Design rationale	ACTH neurocognitive effects without hormonal axis activation	Tuftsin immune + behavioural effects with extended stability
Russian clinical use	Stroke recovery, ADHD pediatric, cognitive indication	Anxiety, neurasthenia
Russian formulation	0.1% intranasal solution	0.15% intranasal solution

Both peptides retain a Pro-Gly-Pro C-terminal sequence which makes them resistant to amino-peptidase degradation — a Russian peptide-stabilisation signature seen across the broader peptide-research program.

3. The mechanisms — fundamentally different

Semax mechanism

BDNF (brain-derived neurotrophic factor) upregulation — Dolotov 2006 J Neurochem showed Semax acutely raises BDNF mRNA in hippocampus and frontal cortex.
NGF (nerve growth factor) upregulation — additional neurotrophic effect.
Dopaminergic system modulation — Eremin 2005 showed enhanced dopamine release in prefrontal cortex.
Melanocortin receptor activity — ACTH-derived, so retains some MC receptor binding (likely MC4R-related).
Net effect: activating, focus-enhancing, neuroprotective.

Selank mechanism

GABAergic potentiation — Kozlovskaya 2003 showed Selank facilitates GABA neurotransmission without acting as a classical benzodiazepine.
Serotonergic modulation — Volkova 2016 showed serotonin metabolism effects in prefrontal cortex.
Enkephalin pathway interaction — Kost 2001 showed Selank stabilises endogenous enkephalin levels.
Immunomodulatory effects — tuftsin-derived, retains some immune-cell modulation.
Net effect: calming, anxiolytic, without benzodiazepine-class sedation or dependence profile.

4. Side-by-side comparison

Dimension	Semax	Selank
Primary endpoint	Focus, attention, neuroprotection	Anxiolysis, stress modulation
BDNF effect	↑↑ Strongly increased	Mild / variable
GABAergic effect	Neutral	↑↑ Potentiated
Dopamine effect	↑ Activating	Neutral
Serotonin effect	Neutral / mild ↑	↑ Modulated
Subjective profile	"Caffeine without jitter" / focus	Calming, reduced anxiety, similar to L-theanine ceiling
Best research context	Cognitive performance, neuroprotection, stroke recovery	Anxiety research, stress-response modulation
Time to subjective effect	Minutes (intranasal); within hour	Within hour
Tolerance / dependence	Low — published Russian record over decades	Low — no benzodiazepine-class dependence

5. The published evidence base

Semax evidence highlights

Dolotov 2006 (J Neurochem): BDNF/NGF upregulation in hippocampus and frontal cortex
Medvedeva 2014 (BMC Genomics): Genome-wide expression profiling — broad neurotrophic and synaptogenesis-related gene upregulation
Gusev 2005: Stroke recovery clinical trial — improved neurological outcome at 30 days
Ashmarin 1995: Foundational pharmacology paper
Manchenko 2010: Anxiolytic-like effects observed in some preclinical paradigms (overlap with Selank, but smaller)

Selank evidence highlights

Kost 2001: Enkephalin stabilisation mechanism
Kozlovskaya 2003: GABAergic mechanism characterisation
Volkova 2016: Serotonergic and BDNF effects
Zozulia 2008: Clinical anxiolytic trial — comparable to benzodiazepine effect without sedation
Mahmoudi 2018: Anti-inflammatory peripheral effects

6. The dosing — both peptides converge on similar routes/doses

Parameter	Semax	Selank
Intranasal dose	250-1000 μg/day, split 2-3 times	250-2250 μg/day, split 2-3 times
SC dose	0.25-1 mg/day (when used by SC route)	0.25-1 mg/day
Reconstitution	10 mg + 10 mL bac water = 1 mg/mL (matches Russian 0.1%)	10 mg + 7-10 mL bac water = ~1-1.5 mg/mL
Frequency	2-3× daily	2-3× daily
Cycle	Typically 14-30 day cycles in published research	14-30 day cycles

The 10 mL reconstitution matters. Reconstituting either peptide in 10 mL of bac water produces a 1 mg/mL solution that approximately matches the Russian clinical 0.1% formulation concentration. Intranasal delivery typically uses 1-3 drops per nostril, with each drop containing ~50 μg.

7. Stackable — and the case for stacking

The non-overlapping mechanisms make the Semax + Selank stack mechanistically coherent. Researchers running combined protocols typically use:

Semax morning + midday — for activating/focus effect during work hours
Selank evening — for anxiolytic effect during decompression / pre-sleep

The combination produces a "wide window of operation" — focused during the day, calmer in the evening — without the trade-offs that single-mechanism interventions (caffeine, stimulants, benzodiazepines) impose.

There are no published combination trials. The stack is mechanism-based researcher protocol synthesis.

8. The route — intranasal as the published default

The Russian clinical formulations are intranasal (Semax 0.1%, Selank 0.15%). Intranasal delivery bypasses gastric peptidase breakdown and provides rapid CNS access via the olfactory nerve / cribriform plate pathway. The published pharmacokinetic data shows intranasal peptide concentrations in CSF within 15-30 minutes — much faster than systemic distribution from SC injection.

SC injection works (the peptides distribute systemically and reach the CNS via blood-brain barrier transport) but for nootropic research, intranasal is the published research route. The full intranasal protocol breakdown for Semax sits in our Semax dosing protocol writeup.

9. The which-one-when decision

Choose Semax if you're researching:

Cognitive performance, focus, attention endpoints
Neuroprotection (stroke research, neurodegeneration)
BDNF / neurotrophic signalling
ADHD-adjacent or pediatric cognitive research (Russian indication)
Recovery from cognitive fatigue

Choose Selank if you're researching:

Anxiety research, stress-response modulation
Sleep quality (pre-sleep anxiolysis)
GABAergic mechanisms without benzodiazepine pharmacology
Serotonin pathway research

Stack both if:

You want a combined activating/calming research protocol
Your research question spans both endpoints (e.g., cognitive performance under stress)

10. The safety record

Both peptides have multi-decade Russian clinical-use records with benign safety profiles. The published adverse event spectrum is limited to:

Nasal irritation (intranasal route)
Headache (uncommon, transient)
Occasional sleep changes (vivid dreams reported anecdotally with both)

Neither peptide has shown abuse potential, dependence syndrome, or significant withdrawal in the Russian clinical record.

11. UAE supply context

Semax is reliably stocked at REVIVE LAB UAE in 10 mg HPLC-verified lyophilised vials with lot-level COA. Selank availability varies by lot — research-grade Selank has a smaller global supply chain than Semax.

Semax UAE ships same-day on Dubai orders before 3 PM, 24 hours nationwide. WhatsApp +971 58 574 3100 to check current Selank stock.

12. The summary

Semax (ACTH-derived) → BDNF + dopamine → focus, attention, neuroprotection research.
Selank (tuftsin-derived) → GABA + serotonin → anxiolysis, stress-response research.
Both heptapeptides with Pro-Gly-Pro C-terminal stabilisation.
Both intranasal route at 1 mg/mL (matches Russian 0.1% clinical formulation).
Both 250-1000+ μg/day, split into 2-3 daily doses.
Mechanisms non-overlapping — stackable for combined activating/calming research.
REVIVE LAB UAE stocks Semax HPLC-verified in 10 mg vials.

References

Dolotov OV, Karpenko EA, Inozemtseva LS, et al. Semax, an analog of ACTH(4-10) with cognitive effects, regulates BDNF and trkB expression in the rat hippocampus. J Neurochem. 2006;97(Suppl 1):82-86. PubMed
Medvedeva EV, Dmitrieva VG, Povarova OV, et al. The peptide semax affects the expression of genes related to the immune and vascular systems in rat brain. BMC Genomics. 2014;15 Suppl 12:S7. PubMed
Kozlovskaya MM, Kozlovskii II, Val'dman EA, Seredenin SB. Selank and short peptides of the tuftsin family in the regulation of adaptive behavior in stress. Neurosci Behav Physiol. 2003;33(7):639-643. PubMed
Volkova A, Shadrina M, Kolomin T, et al. Selank Administration Affects the Expression of Some Genes Involved in GABAergic Neurotransmission. Front Pharmacol. 2016;7:31. PubMed
Gusev EI, Skvortsova VI, Miasoedov NF, et al. Semax efficacy in the treatment of stroke. Zh Nevrol Psikhiatr Im S S Korsakova. 2005;105(2):3-9.

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