📚 Wiki Muscle & Anabolic IGF-1 LR3

IGF-1 LR3

● Preclinical / Pharmacological tool compound
Insulin-Like Growth Factor 1 Long Arg3
Also known as: Long R3 IGF-1, LR3-IGF-1, IGF-1 LR3, Insulin-like Growth Factor-1 LR3
Brand names: IGF-1 LR3 (research grade), Long R3 IGF-I
Page last reviewed
Quick Summary

IGF-1 LR3 is a recombinant IGF-1 analog with an N-terminal extension that reduces binding to IGF binding proteins by over 1000-fold, extending active half-life to 20-30 hours from 12-15 minutes. Drives muscle protein synthesis, satellite cell activation, and anti-catabolic signaling. Most potent long-acting IGF-1 analog in research use. WADA prohibited.

Anabolic & GH Axis Extensively Studied WADA Prohibited
IGF-1 LR3 (Long Arg3 IGF-1) is a recombinant analog of human IGF-1 engineered with a 13-amino acid N-terminal extension and an Arg3 substitution. These modifications reduce binding to IGF binding proteins (IGFBPs) by over 1000-fold, dramatically extending the active half-life from ~12-15 minutes (native IGF-1) to 20-30 hours. IGF-1 LR3 is the most potent and long-acting IGF-1 analog used in research, driving anabolic signaling, satellite cell activation, protein synthesis, and anti-catabolic effects with a single daily injection.
Peptide calculator
Storage Stability
Lyophilized
1–2 years (-20°C)
Reconstituted
~30 days (2–8°C)
Room temp
Avoid

Mechanism of Action

IGF-1 LR3 acts as a potent agonist at IGF-1 receptors (IGF-1R) throughout the body, particularly in skeletal muscle, bone, and neural tissue.

IGF-1R Signaling (PI3K-Akt-mTOR Pathway)

IGF-1 LR3 binds IGF-1R with slightly lower affinity than native IGF-1 but far greater duration due to reduced IGFBP binding. Receptor activation triggers PI3K-Akt-mTOR signaling, driving protein synthesis, ribosome biogenesis, and anti-apoptotic signaling. mTORC1 activation is a central mediator of muscle protein synthesis.[1]

Satellite Cell Activation and Muscle Hypertrophy

IGF-1 LR3 activates skeletal muscle satellite cells, the myogenic progenitor cells responsible for muscle fiber repair and new nuclei addition (essential for muscle hypertrophy). Satellite cell number and activity are rate-limiting for muscle growth beyond normal fiber size limits. IGF-1 signaling via calcineurin-NFAT pathway drives satellite cell differentiation and fusion into existing fibers.[2]

Anti-catabolic and GH-Independent Anabolism

IGF-1 LR3 provides anabolic signaling independent of GH secretion, relevant for tissue repair, anti-aging, and recovery applications. It reduces glucocorticoid-driven catabolism by opposing cortisol's protein catabolic effects in muscle. This makes it useful in catabolic states (post-surgery, injury, aging-related muscle loss).[3]

Research Overview

Muscle Hypertrophy and Protein Synthesis

Most Studied

IGF-1 LR3 is among the most potent anabolic agents in preclinical research. In rodent models, direct intramuscular injection produces localized hypertrophy (30-50% increase in fiber cross-sectional area). Systemic dosing increases lean body mass, muscle protein synthesis rates, and satellite cell activation markers.[2]

Recovery from Injury and Atrophy

Strong Evidence

IGF-1 LR3 accelerates recovery from muscle disuse atrophy, immobilization, and surgical injury. It prevents atrophy-associated satellite cell depletion and promotes faster return of functional muscle mass. Animal models of spinal cord injury show improved motor recovery with systemic IGF-1 LR3.[3]

Neural and Cognitive Effects

Moderate Evidence

IGF-1R is highly expressed in brain hippocampus and prefrontal cortex. IGF-1 LR3 crosses the blood-brain barrier and promotes neurogenesis, BDNF expression, and neuroprotection in rodent models. Studies in aging animals show cognitive preservation with chronic low-dose IGF-1 treatment.[1]

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Research Protocols

GoalDoseFrequencyRoute
Muscle recovery / repair50–100 µgOnce daily post-exerciseSubcutaneous or intramuscular
Anti-catabolic / injury20–50 µgOnce dailySubcutaneous
Bilateral site injection50 µg per sitePost-workout, bilateral injection near target musclesIntramuscular
Conservative start20–30 µgOnce dailySubcutaneous

Post-workout administration capitalizes on elevated blood flow and IGF-1R expression in recently exercised muscle. Some protocols use bilateral intramuscular injection near target muscles for localized hyperplasia signals, though evidence for site-specific hypertrophy advantage is mixed. 20-30 hour half-life means once-daily dosing provides sustained anabolic elevation.

Research protocols only. Not medical advice.

Peptide Interactions

compatible
Ipamorelin / CJC-1295
GH-axis peptides drive endogenous IGF-1; exogenous IGF-1 LR3 adds direct downstream signaling. Monitor for supraphysiological IGF-1 levels when combining.
compatible
BPC-157
BPC-157 provides local repair signaling; IGF-1 LR3 provides systemic anabolic and anti-catabolic support. Common recovery combination.
compatible
TB-500
TB-500 drives cell migration and angiogenesis; IGF-1 LR3 drives satellite cell activation and protein synthesis. Complementary recovery mechanisms.
caution
Insulin
IGF-1 LR3 has insulin-like activity at the insulin receptor (~8% binding affinity). Hypoglycemia risk when combined with exogenous insulin. Monitor blood glucose carefully.
monitor
Somatostatin analogs
Somatostatin reduces IGF-1 production and may blunt IGF-1 LR3 effects. Relevant for acromegaly management contexts.

Safety Profile

IGF-1 LR3 is a potent anabolic compound requiring careful use and monitoring.

WADA Status: Prohibited by WADA as an anabolic agent. Athletes subject to testing must not use this compound.

Hypoglycemia: The most significant acute risk. IGF-1 LR3 has ~8% binding affinity at insulin receptors. At doses above 100 mcg, hypoglycemia is possible, particularly in the fasted state. Always have fast-acting carbohydrates available.

Acromegaly-like effects: Chronic supraphysiological IGF-1 elevation can cause soft tissue and organ growth (jaw, hands, feet, heart). Effects are dose and duration dependent. Periodic IGF-1 level monitoring is essential for long-duration protocols.

Tumor risk: IGF-1 signaling promotes cell proliferation. Not recommended for anyone with a personal or family history of cancer. Theoretical risk is a primary safety concern for long-term use.

No FDA approval: Research compound. Not approved for any human use.

References

  • [1]Clemmons DR. "Modifying IGF1 activity: an approach to treat endocrine disorders, atherosclerosis and cancer." Nat Rev Drug Discov. 2007;6(10):821-833.
  • [2]Adams GR, McCue SA. "Localized infusion of IGF-I results in skeletal muscle hypertrophy in rats." J Appl Physiol. 1998;84(5):1716-1722.
  • [3]Hameed M, et al. "Expression of IGF-I splice variants in young and old human skeletal muscle after high resistance exercise." J Physiol. 2003;547(Pt 1):247-254.
Key Terms
Peptide Reconstitution Guide
Reconstitution is the process of dissolving lyophilized (freeze-dried) peptide powder with a sterile diluent to create a…
Bacteriostatic Water
Bacteriostatic water (BAC water) is sterile water for injection containing 0.9% benzyl alcohol as a preservative. It is …
Peptide Injection Guide
Subcutaneous injection is the standard administration route for most lyophilized research peptides. The technique is str…
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See Also

IpamorelinCJC-1295TB-500BPC-157HexarelinPeptide Reconstitution GuideBacteriostatic WaterPeptide Injection Guide
Categories: AnabolicGH AxisMuscleRecovery
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Verified Scientific Data Last audited:
Data Sources & External References
⬡ PubMed / NCBI, Research Literature ⬡ NCBI, Full-Text Articles ⬡ PubChem, Chemical Database
CAS Registry: 946870-92-4  ·  Molecular Formula: C400H625N111O115S9  ·  Source: peer-reviewed literature  ·  Domain: ascendpeptide.org
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