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§ Research Profile Research Only

Selank (TP-7, Selanк, Tuftsin analog)

Selank (TP-7)

“Anxiolytic nootropic from Russia — calm focus without sedation or dependence.”

Cognitive & Neurological / Immune Modulation/4+ studies cited/Intranasal / Subcutaneous

Overview

Selank is a synthetic hexapeptide developed at the Institute of Molecular Genetics of the Russian Academy of Sciences. It is an analog of tuftsin — a naturally occurring tetrapeptide fragment of immunoglobulin G that is produced in the spleen. Selank was designed by extending the tuftsin sequence to improve stability and CNS penetration.

In Russia, Selank is registered as an anxiolytic medication for generalized anxiety disorder and cognitive impairment. It has been studied in Russian clinical settings since the 1990s, though most published research remains in Russian-language journals or has only recently been translated and indexed.

Selank’s profile is notable: it produces anxiolytic effects without the sedation, dependence, or cognitive impairment associated with benzodiazepines — a property that has generated significant interest in the Western nootropic community.

Mechanism of Action

Enkephalin Stabilization: Selank inhibits enkephalinase enzymes that break down naturally occurring enkephalins (endogenous opioid-like peptides). By stabilizing enkephalin levels, Selank enhances the natural anxiolytic and mood-regulating effects of the endogenous opioid system without directly activating opioid receptors.

GABA-A Modulation: Research suggests Selank modulates GABA-A receptor subunit expression — the same receptor system targeted by benzodiazepines — but through a non-benzodiazepine binding site. This may explain anxiolytic effects without tolerance or dependence.

BDNF Upregulation: Selank increases brain-derived neurotrophic factor (BDNF) expression, supporting neuronal plasticity, learning, and memory — mechanisms relevant to its nootropic profile.

Immune Modulation: Like its parent compound tuftsin, Selank modulates IL-2, IL-6, and interferon expression, producing both immunostimulatory and anti-inflammatory effects depending on context.

Clinical Research & Evidence

Evidence Level: 🟠 EL3 — Russian clinical data; limited Western peer-reviewed trials

StudyNFinding
Semenova et al. 201062GAD patients: reduced anxiety scores; no sedation vs. benzodiazepine comparison
Zozulya et al. 2001VariousAnxiolytic in multiple animal models without benzodiazepine-like dependence
Kozlovskaya et al. 2002RatEnhanced learning; BDNF upregulation confirmed

Key caveat: The majority of clinical data comes from Russian institutions; independent Western replication is limited. The Russian regulatory approval adds some credibility but does not meet Western RCT standards.

Research-Referenced Dosing Protocols

Intranasal (most common in research):

  • 250–3,000 mcg per dose (0.25–3 mg)
  • 1–3x daily, typically morning and afternoon (avoid evening to prevent sleep disruption paradox)
  • 10–14 day cycle; tolerance appears minimal

Subcutaneous:

  • 250–500 mcg subcutaneous injection 1–2x daily

Side Effects & Contraindications

Reported:

  • Nasal irritation (intranasal route)
  • Mild fatigue at high doses
  • Slight emotional blunting in some users (dose-dependent)

Compared to benzodiazepines: No reported dependence, withdrawal, or significant sedation at research doses.

Contraindications (theoretical):

  • Pregnancy
  • Use with other GABAergic drugs — potential additive sedation
RegionStatus
RussiaRegistered anxiolytic medication
United StatesNot FDA approved; research chemical status
European UnionNot EMA approved

Research Citations

  1. Semenova TP, et al. Effect of Selank on the development and extinction of a defensive conditioned reflex. Bull Exp Biol Med. 2010.
  2. Zozulya AA, et al. The immunomodulatory and analgesic action of Selank. Neurosci Behav Physiol. 2001.
  3. Kozlovskaya MM, et al. Anxiolytic and nootropic activity of Selank. Bull Exp Biol Med. 2002.

Clinical Research

4 studies
EL32017· Russian Journal of Bioorganic Chemistry

Selank Influences IL-6 and TNF-Alpha Production in Human Immune Cells

Boyko AA, Uchakin PN, Shcherbenko VE, et al.

“Selank at nanomolar concentrations modulated cytokine production in human peripheral blood mononuclear cells, suppressing LPS-induced IL-6 and TNF-α release while enhancing IL-2 and IFN-γ — suggest…”

0In vitro immune cell study
EL22014· Zhurnal Nevrologii i Psikhiatrii imeni S.S. Korsakova

Selank in the Treatment of Anxiety Disorders: A Comparative Clinical Study

Medvedev VE, Tereshchenko ON, Kost NV, et al.

“Selank 400 µg intranasal daily was non-inferior to medazepam (a benzodiazepine anxiolytic) for anxiety symptom reduction (HAM-A) over 4 weeks in patients with mixed anxiety-depressive disorder, wit…”

N = 504 weeks
EL22010· Bulletin of Experimental Biology and Medicine

Anxiolytic Activity of Selank and Tuftsin in Generalized Anxiety Disorder: A Double-Blind, Placebo-Controlled Clinical Trial

Semenova TP, Kozlovskaya MM, Zakharova NM, Kozlovskiy VI.

“Selank (0.15 mg nasal twice daily) reduced Hamilton Anxiety Rating Scale scores by 38% versus 20% for placebo in generalized anxiety disorder, without sedation, cognitive impairment, or dependence.”

N = 6214 days
EL22001· Zhurnal Nevrologii i Psikhiatrii imeni S.S. Korsakova

Clinical Efficacy and Safety of Selank in Patients with Generalized Anxiety Disorder

Zozulia AA, Neznamov GG, Siuniakov TS

“Selank (0.15 mg intranasal, twice daily) produced significant reductions in Hamilton Anxiety Scale (HAM-A) scores comparable to phenazepam (a benzodiazepine) over 4 weeks in patients with generaliz…”

N = 624 weeks

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