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Guía de Investigación · Actualizada Marzo 2026

Sleep Enhancement Research

Slow-wave sleep modulation and stress-induced insomnia in EEG models

Solo para investigación: Toda la información es exclusivamente para fines de investigación científica. Estos péptidos no están no aprobados para uso terapéutico humano. Cumpla con los requisitos éticos y regulatorios de su institución.

Péptidos en esta categoría:

Selank — Comparar precios LATAM →DSIP — Comparar precios LATAM →

¿Qué es esta Categoría?

Sleep quality is increasingly recognised as one of the most powerful levers for health, cognitive performance, and longevity. DSIP (Delta Sleep-Inducing Peptide) was discovered in 1977 when researchers isolated it from rabbit blood during natural sleep and found that injecting it into alert rabbits induced slow-wave (deep) sleep within 30 minutes. Unlike sleeping pills, which work by broadly suppressing brain activity, DSIP specifically promotes delta-wave (slow-wave) sleep — the deepest and most restorative stage — without sedation, respiratory depression, or dependence. Selank contributes to this category through its anxiolytic mechanism: by reducing the hyperarousal (racing thoughts, elevated cortisol, difficulty switching off) that underlies stress-induced insomnia, without the muscle-relaxing or respiratory effects of benzodiazepines.

Para Qué se Investiga

→Improving deep (slow-wave) sleep duration and quality
→Reducing sleep onset latency without sedation or "drugged" feeling
→Stress-related insomnia and hyperarousal at bedtime
→Studying alternatives to benzodiazepines for sleep research models
→Circadian rhythm support and normalisation of sleep architecture
→Combined Selank use for anxiety-driven sleep disruption

Pros y Contras

+DSIP improves sleep architecture (specifically slow-wave sleep) rather than simply increasing total sedation

+No respiratory depression — critical safety advantage over conventional sleep medications

+Selank shows no withdrawal or dependence effects in published rodent studies — unlike benzodiazepines

+Selank is intranasal — no injections required

+Cortisol-reducing effect of Selank may have positive downstream effects beyond sleep

+Non-addictive mechanism — neither compound acts on GABA-A receptors the way benzodiazepines do

−DSIP has an extremely short plasma half-life (~30 minutes) — the compound degrades quickly, making dosing protocols challenging

−DSIP is practically unavailable from LATAM-accessible vendors as of 2026 — specialised custom synthesis required

−Human clinical data for DSIP is very limited and inconsistent across published studies

−Selank's sleep benefits are a secondary effect of its anxiolytic action — it is not a direct sleep-inducing agent

−Effects of DSIP in human volunteers have shown high inter-individual variability in the few published trials

−Without access to sleep EEG monitoring, it is difficult to verify sleep architecture improvement objectively

Cronología de Efectos

Basado en cronogramas de estudios publicados. La extrapolación humana es aproximada — los resultados individuales varían.

Inicio

30–60 minutes (DSIP, animal studies); 30–90 minutes (Selank anxiolytic)

Efecto Máximo

Ongoing with consistent use; Selank effects stable within days

Notas

DSIP-induced delta sleep changes are measurable within the first sleep cycle in animal polysomnography studies. Selank's anxiolytic effects are measurable within 30–60 minutes in animal models and may require 3–7 days of consistent use for stable baseline improvement in self-researchers.

Estatus Legal en LATAM: DSIP and Selank are unscheduled compounds in most Latin American countries. Neither is a controlled substance or approved medicine in Latin America. Selank is available from LATAM-accessible vendors; DSIP is practically unavailable and would need to be specially ordered. Selank is an approved drug in Russia (Selank® nasal drops).

Resumen Científico

Sleep enhancement peptide research focuses primarily on DSIP (Delta Sleep-Inducing Peptide), a nonapeptide originally isolated from rabbit venous blood during natural sleep, and Selank, which has secondary anxiolytic-mediated sleep-improving effects. DSIP was discovered by Schoenenberger and colleagues in 1977 and characterised by its ability to increase the proportion of slow-wave (delta) sleep in multiple species. Research models include polysomnographic recording in freely moving rodents, stress-induced insomnia models, and neonatal/aged animal sleep architecture studies.

Mecanismo de Acción

DSIP interacts with opioid receptors (µ and δ) and modulates GABA-B receptor activity, collectively shifting sleep architecture toward slow-wave dominance. It also suppresses corticotropin-releasing hormone (CRH) release, providing indirect stress-axis modulation that may contribute to sleep onset facilitation. Selank's sleep benefits are mediated through its GABAergic and anxiolytic mechanisms — reducing the hyperarousal that characterises stress-induced insomnia without the respiratory depression associated with benzodiazepines.

Métodos de Administración

Vía 1Intravenous / intracerebroventricular (DSIP, animal models)

Preparación

Dissolve lyophilised DSIP in sterile saline immediately before administration. IV bolus or slow infusion over 10 minutes.

Concentración Típica

25–100 µg/mL

Notas

ICV administration is used to demonstrate CNS-direct effects and establish receptor pharmacology. IV is used for systemic pharmacokinetic studies. DSIP crosses the BBB, but BBB penetration rate is dose-dependent.

Vía 2Intranasal (Selank)

Preparación

Same as Cognitive Enhancement protocol. 0.1% solution in sterile saline.

Concentración Típica

1 mg/mL

Notas

Selank intranasal administration is preferred for sleep models to replicate the direct CNS route without the stress of injection.

Protocolos de Investigación

Polysomnography Model (DSIP)

DSIP

Duración

Acute (single dose) to 5-day chronic

Frecuencia

Acute: single IV bolus; chronic: once daily IV

Rango de Dosificación

25–200 µg/kg

Criterios de Evaluación

EEG delta power (0.5–4 Hz band), NREM/REM ratio, sleep latency (time to first NREM epoch), total sleep time

Notas del protocolo: Chronic EEG electrode implantation under stereotaxic surgery is required. Animals must have ≥7-day recovery before baseline recordings.

Stress-Induced Insomnia Model (Selank)

Selank

Duración

7 days

Frecuencia

Once daily intranasal, 60 min before lights-off

Rango de Dosificación

100–300 µg per animal

Criterios de Evaluación

Sleep onset latency (EEG), serum corticosterone (evening sample), NREM delta power, open-field locomotion (to control for sedation)

Notas del protocolo: Restraint stress (60 min daily) is used to model chronic psychosocial stress insomnia. Diazepam positive control group is standard.

Estudios Publicados Clave

A delta sleep-inducing peptide (DSIP): the first sleep factor?

1977

Intravenous injection of DSIP extracted from sleeping rabbit blood into alert rabbits produced a significant and reproducible increase in delta wave activity and facilitated transition to NREM sleep within 30 minutes.

Metodología: Alert rabbit model, IV infusion, EEG recording, n=6, crossover design

PubMed: 409316 ↗

Resultados Esperados

Basado en la evidencia preclínica publicada. Los resultados pueden variar según el modelo, la dosis y la vía de administración.

✓Increased delta band power (0.5–4 Hz) in EEG during NREM sleep (DSIP)
✓Reduced sleep onset latency in both acute and stress-model paradigms
✓Increased total NREM sleep time without suppression of REM sleep
✓Reduced serum corticosterone in stress models (Selank)
✓No significant respiratory depression or muscle relaxation (distinguishing from benzodiazepines)

Consideraciones de Seguridad

⚠DSIP has a very short half-life (~30 min in plasma) due to rapid enzymatic degradation; formulation stability must be verified before use.
⚠ICV administration requires survival surgery with attendant anaesthetic and surgical risks.
⚠Selank has shown no withdrawal or dependence effects in published rodent studies; contrast with benzodiazepine positive controls.
⚠Not approved for human therapeutic use.

Preguntas Frecuentes

Does DSIP induce sleep immediately, like a sedative?

No. DSIP modulates sleep architecture by increasing slow-wave (delta) sleep proportion rather than inducing acute sedation. It reduces sleep latency and shifts sleep pressure toward NREM, but does not produce the sedation or anxiolysis associated with benzodiazepines or barbiturates.

Why is DSIP difficult to source from LATAM-accessible vendors?

DSIP is a relatively low-demand research peptide with a very short plasma half-life that makes in vivo studies technically demanding. Few LATAM-accessible vendors stock it routinely; researchers typically order from specialised synthesis laboratories on a custom basis.

Notas Prácticas para Auto-Investigadores

Solo con fines educativos. La autoadministración de compuestos de investigación conlleva riesgos significativos y no respaldado por PeptideLATAM. Consulte a un profesional de salud calificado antes de considerar cualquier protocolo de autoinvestigación.

What time of day should I use Selank for sleep benefits?

For sleep applications, self-researchers typically use Selank 60–90 minutes before bedtime. This timing allows the anxiolytic effect to develop before sleep onset, helping reduce the hyperarousal and racing thoughts that prevent falling asleep. Morning use is more common when the goal is daytime anxiety reduction — the compound can be used at either time.

Can DSIP actually be sourced for research?

DSIP is not stocked by most LATAM-accessible vendors due to low demand and synthesis complexity. Researchers requiring DSIP typically contact specialised custom peptide synthesis laboratories directly. The short half-life also means freshly synthesised material is preferable. This category is included because the research literature is extensive, but practical sourcing is significantly harder than for BPC-157 or Selank.

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