Overview
At a Glance
Ipamorelin is a selective growth hormone secretagogue that mimics ghrelin to stimulate GH release from the pituitary, without significantly affecting cortisol or prolactin. It's popular in anti-aging and peptide therapy clinics, often combined with CJC-1295. A few clinical trials exist — notably in post-surgical recovery — but it has no FDA approval for any indication. It is sold as a research chemical, and long-term safety data in humans is lacking.
Ipamorelin is a synthetic pentapeptide — a chain of five amino acids (Aib-His-D-2-Nal-D-Phe-Lys-NH₂) — that acts as a selective growth hormone secretagogue (GHS). It stimulates the pituitary gland to release growth hormone (GH) by binding to the ghrelin receptor (GHS-R1a), mimicking the action of the endogenous hunger hormone ghrelin. Ipamorelin was originally developed by Novo Nordisk in the 1990s as part of a research program to identify compounds that could stimulate GH release with fewer side effects than earlier growth hormone-releasing peptides (Raun et al., 1998).
What distinguishes ipamorelin from earlier growth hormone secretagogues — such as GHRP-2 and GHRP-6 — is its selectivity. While those peptides stimulate GH release effectively, they also significantly elevate cortisol, prolactin, and aldosterone levels. Ipamorelin produces a dose-dependent increase in GH with minimal to no effect on these other hormones at therapeutic doses (Raun et al., 1998). This selectivity profile has made it one of the most widely used growth hormone secretagogues in clinical and anti-aging medicine settings.
Ipamorelin reached Phase 2 clinical trials for post-operative ileus (delayed gut motility after abdominal surgery), conducted by Helsinn Therapeutics. While the compound demonstrated biological activity and GH-releasing properties in humans, the Phase 2b trial did not meet its primary endpoint for ileus, and development for that indication was discontinued (Beck et al., 2008). No further FDA-track clinical development has been pursued.
Despite the lack of FDA approval, ipamorelin has become one of the most commonly prescribed peptides through compounding pharmacies and anti-aging/regenerative medicine clinics. It is frequently used alone or in combination with CJC-1295 (a growth hormone-releasing hormone analog) to amplify GH output. Ipamorelin has no FDA-approved indication for any use.
Quick Facts
| Property | Details |
|---|---|
| Molecular formula | C₃₈H₄₉N₉O₅ |
| Amino acid sequence | Aib-His-D-2-Nal-D-Phe-Lys-NH₂ |
| Molecular weight | ~711.9 Da |
| Receptor target | Growth hormone secretagogue receptor (GHS-R1a / ghrelin receptor) |
| Routes studied | Subcutaneous injection, intravenous |
| Human trials | Phase 2 for post-operative ileus (completed; did not advance) |
| FDA approval | None |
| WADA status | Prohibited (S2 — peptide hormones, growth factors) |
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
How It Works
Growth hormone release from the pituitary is controlled by two opposing signals: growth hormone-releasing hormone (GHRH), which stimulates release, and somatostatin, which inhibits it. A third pathway — the ghrelin/GHS receptor pathway — provides an additional stimulatory signal that acts synergistically with GHRH. Ipamorelin works through this third pathway.
Ghrelin Receptor Agonism
Ipamorelin binds to the growth hormone secretagogue receptor type 1a (GHS-R1a), the same receptor targeted by the endogenous hormone ghrelin. When ipamorelin occupies this receptor on somatotroph cells in the anterior pituitary, it triggers an intracellular signaling cascade involving phospholipase C and inositol trisphosphate (IP₃), leading to calcium influx and the exocytosis of stored GH vesicles (Raun et al., 1998).
The GH release follows a pulsatile pattern — mimicking the body's natural GH secretion rhythm rather than producing a sustained, unphysiologic elevation. This pulsatile release is considered more physiologically favorable than the flat, constant GH levels produced by exogenous growth hormone injection (Johansen et al., 2001).
Selectivity Advantage
The defining pharmacological feature of ipamorelin is its selectivity. In head-to-head comparisons with other growth hormone secretagogues:
| Compound | GH Release | Cortisol | Prolactin | ACTH |
|---|---|---|---|---|
| Ipamorelin | Strong, dose-dependent | No significant increase | No significant increase | No significant increase |
| GHRP-6 | Strong | Moderate increase | Moderate increase | Moderate increase |
| GHRP-2 | Strong | Mild–moderate increase | Mild increase | Mild increase |
| Hexarelin | Strong | Significant increase | Significant increase | Significant increase |
This selectivity was demonstrated in preclinical studies showing that ipamorelin at doses up to 1 mg/kg in swine produced dose-dependent GH increases while cortisol, ACTH, and prolactin remained at baseline levels. Only at very high, supratherapeutic doses did cortisol begin to rise (Raun et al., 1998).
Synergy with GHRH Pathway
Because ipamorelin acts through the ghrelin receptor pathway (distinct from the GHRH receptor pathway), it can act synergistically with GHRH or GHRH analogs such as CJC-1295. When both pathways are activated simultaneously, GH release is amplified beyond what either agent produces alone. This is the pharmacological rationale for the commonly used ipamorelin + CJC-1295 combination protocol (Ionescu & Bhatt, 2006).
GH-Mediated Downstream Effects
The biological effects attributed to ipamorelin are mediated by the growth hormone it releases. GH acts both directly and through hepatic production of insulin-like growth factor 1 (IGF-1):
- Lipolysis: GH promotes the breakdown of stored fat, particularly visceral adipose tissue
- Protein synthesis: GH stimulates muscle protein synthesis and supports lean body mass preservation
- Collagen synthesis: GH and IGF-1 promote collagen production in connective tissues, skin, and joints
- Bone metabolism: GH stimulates osteoblast activity and bone mineral density maintenance
- Sleep architecture: GH secretion is closely linked to slow-wave (deep) sleep; augmenting GH release may improve sleep quality
- Cellular repair: GH supports tissue turnover and recovery processes throughout the body
Go Deeper
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Research
Selectivity and GH Release Profile
The foundational research on ipamorelin established its pharmacological identity as the first truly selective growth hormone secretagogue. In swine models, ipamorelin produced dose-dependent GH elevation comparable to GHRP-6, but with no significant changes in ACTH, cortisol, prolactin, or aldosterone at doses up to 1 mg/kg. By contrast, GHRP-6 and GHRP-2 elevated all of these hormones at equivalent GH-stimulating doses (Raun et al., 1998).
In human pharmacokinetic studies, single subcutaneous doses of ipamorelin produced peak GH levels within 30–45 minutes, with GH returning to baseline within 2–3 hours. The response was dose-dependent across the 1–100 mcg/kg range tested. Repeated dosing did not lead to significant desensitization of the GH response over short treatment periods (Johansen et al., 2001).
Post-Operative Ileus (Phase 2 Clinical Trials)
Helsinn Therapeutics advanced ipamorelin into Phase 2 clinical trials for post-operative ileus (POI) — the temporary paralysis of gut motility that commonly follows abdominal surgery. The rationale was based on evidence that ghrelin receptor agonism promotes gastrointestinal motility.
- Phase 2a: Ipamorelin demonstrated prokinetic effects and was well-tolerated in patients following abdominal surgery. GH elevation was confirmed in surgical patients, and initial signals of improved gut recovery time were observed (Beck et al., 2008).
- Phase 2b: A larger, randomized, double-blind, placebo-controlled trial evaluated ipamorelin in patients undergoing open abdominal surgery. The trial did not meet its primary endpoint of reduced time to first bowel movement. While ipamorelin was well-tolerated and demonstrated GH-releasing activity, efficacy for POI was not established (Greenwood-Van Meerveld et al., 2012).
Development for the POI indication was subsequently discontinued. The trial data did, however, provide human safety and pharmacokinetic information that supports the compound's tolerability profile.
Body Composition and Metabolic Effects
Preclinical studies have demonstrated metabolic effects consistent with GH-mediated improvements in body composition:
- Fat reduction: In animal models, chronic ipamorelin administration reduced visceral adiposity without significant changes in food intake, consistent with GH-mediated lipolysis (Johansen et al., 2001).
- Lean mass preservation: Growth hormone released by ipamorelin supports protein synthesis and lean body mass maintenance, an effect well-characterized for GH itself (Andersen et al., 2001).
- Bone density: GH and IGF-1 elevation support bone turnover and mineral density. Preclinical data suggests that chronic GHS-R1a agonism may have bone-protective effects, though human bone density data specific to ipamorelin is not available (Johansen et al., 2001).
GI Motility and Ghrelin Receptor Biology
Beyond the post-operative ileus trials, ipamorelin's action on the ghrelin receptor has relevance to broader GI motility research. Ghrelin receptor agonism stimulates gastric motility, promotes gastric emptying, and modulates appetite signaling. While ipamorelin's GI prokinetic effects were insufficient to meet clinical endpoints for POI, the underlying pharmacology is consistent with the known role of ghrelin in gut physiology (Greenwood-Van Meerveld et al., 2012).
Comparison with Other GH Secretagogues
| Feature | Ipamorelin | GHRP-2 | GHRP-6 | Hexarelin |
|---|---|---|---|---|
| GH potency | Moderate–strong | Strong | Moderate | Strong |
| Cortisol elevation | Minimal | Mild | Moderate | Significant |
| Prolactin elevation | Minimal | Mild | Mild–moderate | Significant |
| Hunger stimulation | Mild | Moderate | Strong | Moderate |
| Desensitization | Low | Moderate | Moderate | High (rapid) |
| Human trial data | Phase 2 | Phase 2 | Limited | Phase 2 |
Limitations of the Research
- No Phase 3 clinical trials: Ipamorelin has not been evaluated in large-scale, pivotal human trials for any indication.
- POI trials failed primary endpoint: The most advanced human trials did not demonstrate efficacy for the studied indication.
- Body composition data is extrapolated: Human data on fat loss, muscle gain, or anti-aging endpoints specific to ipamorelin is limited; much is inferred from the known effects of GH itself.
- Long-term safety unknown: No multi-year human safety data exists for chronic ipamorelin use.
- Combination protocols unstudied: The commonly used ipamorelin + CJC-1295 combination has not been evaluated in controlled clinical trials.
Further Reading
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Uses
FDA Status
Ipamorelin has no FDA-approved indication. It has not completed the clinical trial process required for FDA approval. The Phase 2 trial for post-operative ileus did not advance. Any clinical use is considered experimental or off-label in the context of a provider-patient relationship.
Common Clinical Applications
The following uses are reported by providers in anti-aging, regenerative, and functional medicine. They are based on ipamorelin's pharmacological mechanism and the known downstream effects of growth hormone — not on FDA-approved indications.
| Application | Evidence Basis | Notes |
|---|---|---|
| Anti-aging / GH optimization | Pharmacological rationale; GH physiology | GH declines with age (somatopause). Ipamorelin is used to restore more youthful GH pulsatility. Targeted outcomes include improved skin quality, energy, body composition, and recovery capacity. |
| Body composition | Preclinical data; GH physiology | GH promotes lipolysis and lean mass preservation. Used by individuals seeking fat loss (particularly visceral fat) and muscle mass support, typically alongside exercise and nutrition programs. |
| Recovery and repair | GH physiology | GH and IGF-1 support tissue turnover, collagen synthesis, and recovery from exercise or injury. Used by athletes and active individuals seeking faster recovery between training sessions. |
| Sleep improvement | GH physiology; clinical observation | GH secretion is closely linked to slow-wave sleep. Evening administration of ipamorelin is commonly reported to improve sleep depth and quality. This is one of the most consistently reported subjective benefits. |
| Joint and connective tissue support | GH/IGF-1 physiology | GH and IGF-1 stimulate collagen synthesis in tendons, ligaments, and cartilage. Used as adjunctive support for joint health and connective tissue recovery. |
| Combination with CJC-1295 | Pharmacological synergy | Frequently combined with CJC-1295 (a GHRH analog) to amplify GH release through dual-pathway stimulation. This combination has not been evaluated in controlled human trials. |
What Ipamorelin Is NOT Used For
- Growth hormone replacement: Ipamorelin stimulates the body's own GH production; it does not replace GH. Individuals with pituitary failure or destruction will not respond to ipamorelin.
- Direct muscle building: While GH supports lean mass, ipamorelin is not an anabolic steroid and does not produce the direct muscle-building effects of testosterone or related compounds.
- Weight loss drug: Ipamorelin is not a weight loss medication. Any body composition effects are secondary to GH-mediated metabolic changes and require appropriate diet and exercise.
- Replacement for standard medical care: Ipamorelin should be considered as a potential adjunct, not a replacement for established treatments.
Further Reading
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Dosing
Ipamorelin is not FDA-approved. No official dosing guidelines exist. The information below reflects protocols commonly reported in clinical practice and pharmacokinetic research — it is provided for informational purposes only. Do not self-administer any peptide without guidance from a qualified healthcare provider. Dosing and administration should be overseen by a licensed clinician.
Commonly Reported Protocols
| Protocol | Dose | Frequency | Notes |
|---|---|---|---|
| Standard (monotherapy) | 200–300 mcg SC | 1x daily at bedtime | Bedtime dosing aligns with natural nocturnal GH pulse. Most common starting protocol. |
| Twice daily | 200–300 mcg SC | 2x daily (AM + bedtime) | Morning dose taken on an empty stomach, at least 30 min before food. Greater GH output over 24 hours. |
| Three times daily | 200–300 mcg SC | 3x daily | Used in some aggressive anti-aging protocols. Higher cost and injection burden. |
| With CJC-1295 (no DAC) | 200–300 mcg ipamorelin + 100 mcg CJC-1295 | 1–2x daily | Combined to amplify GH pulse through dual-pathway stimulation. Administered together in the same injection. |
| With CJC-1295 DAC | 200–300 mcg ipamorelin daily + 2 mg CJC-1295 DAC weekly | See notes | CJC-1295 DAC has a longer half-life (~8 days) and is dosed weekly. Ipamorelin continues daily. |
Dosing protocols above are derived from published pharmacokinetic data and reported clinical practice — not from FDA-approved labeling. Key references: Raun et al., 1998 (European Journal of Endocrinology) · Johansen et al., 2001 (European Journal of Endocrinology) · Beck et al., 2008 (Journal of Surgical Research)
Timing Considerations
- Fasting state: GH release is blunted by elevated blood sugar and insulin. Ipamorelin is most effective when administered on an empty stomach — at least 30 minutes before eating or 2 hours after a meal.
- Bedtime dosing rationale: The largest natural GH pulse occurs during early slow-wave sleep. Bedtime ipamorelin administration amplifies this natural pulse and is associated with the most consistent subjective reports of improved sleep quality.
- Post-exercise: Some protocols recommend a dose 20–30 minutes after exercise, when GH responsiveness may be enhanced. This adds a second injection to the daily regimen.
Cycling Patterns
There is no established evidence base for optimal treatment duration or cycling. Commonly reported patterns include:
- Continuous use: Many providers prescribe ipamorelin for ongoing use (months to years) with periodic blood work monitoring (IGF-1 levels, metabolic panel).
- 5 days on, 2 days off: A commonly cited cycling pattern intended to prevent receptor desensitization, though evidence for this necessity with ipamorelin specifically is limited.
- Periodic courses: 3–6 month courses followed by 1–2 month breaks, with reassessment of clinical response and blood markers.
Monitoring
Providers who prescribe ipamorelin typically monitor:
- IGF-1 levels: As a surrogate marker for GH activity. Target ranges vary by provider and clinical context.
- Fasting glucose / HbA1c: GH can affect glucose metabolism and insulin sensitivity.
- Symptoms: Joint pain, water retention, or carpal tunnel symptoms may indicate excessive GH effect.
Storage
- Lyophilized (unreconstituted) powder: Store refrigerated (2–8°C / 36–46°F). Stable for months when kept dry and cold.
- Reconstituted solution: Refrigerate and use within 3–4 weeks. Do not freeze. Discard if solution becomes cloudy or discolored.
Further Reading
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Results: What Users Report
The following timeline is compiled from clinician reports, patient surveys, and online communities — not from randomized controlled trials. Individual experiences vary significantly. Ipamorelin has not been evaluated for efficacy in Phase 3 human trials for any of these endpoints.
Reported Timeline
| Timepoint | What Users Typically Report |
|---|---|
| Days 1–7 | Improved sleep quality is the most commonly reported early effect — deeper sleep, more vivid dreams, and feeling more rested upon waking. Some users report mild water retention or transient lightheadedness. |
| Week 2–4 | Improved recovery from exercise. Increased energy and general sense of well-being. Some users report improved skin hydration and texture. Mild increase in appetite (consistent with ghrelin receptor agonism). |
| Week 4–8 | Body composition changes become noticeable: reduced midsection fat, modest lean mass improvement (particularly when combined with resistance training). Joint stiffness and minor aches may improve. |
| Month 2–4 | Continued gradual body composition improvement. Hair and nail growth quality changes reported by some users. Improved exercise capacity and recovery. Effects typically plateau if dose and lifestyle remain unchanged. |
| Month 4–6+ | Long-term users report sustained improvements in sleep, body composition, skin quality, and recovery. Some report measurable changes in IGF-1 levels on blood work. Effects are generally described as subtle and cumulative rather than dramatic. |
Most Consistently Reported Benefits
- Sleep improvement: The most frequently and consistently reported benefit across user populations. Reported as deeper, more restorative sleep — particularly with bedtime dosing.
- Recovery from exercise: Reduced soreness, faster return to training readiness, and improved exercise tolerance.
- Body composition: Gradual reduction in body fat (particularly abdominal) and preservation or modest improvement in lean mass. Effects are described as supportive rather than transformative — requiring consistent diet and exercise.
- Skin and connective tissue: Improved skin elasticity, hydration, and texture. Some users report improved joint comfort.
What "Results" Means Without Phase 3 Data
Important context for interpreting these reports:
- Placebo effect: Cannot be excluded, particularly for subjective outcomes like sleep quality, energy, and general well-being.
- Lifestyle confounding: Individuals who begin ipamorelin often simultaneously improve their diet, exercise, and sleep habits — making it difficult to attribute changes to the peptide alone.
- Selection bias: Positive experiences are shared more frequently than neutral or negative ones.
- GH effects are well-characterized: Many reported benefits are consistent with the known effects of growth hormone, lending biological plausibility — but also raising the question of whether similar benefits could be achieved through lifestyle optimization of natural GH production (sleep, exercise, fasting).
Further Reading
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Side Effects
Reported Side Effects
| Side Effect | Frequency | Notes |
|---|---|---|
| Headache | Uncommon | Typically mild and self-limiting, more common during the first week of use. May relate to transient changes in intracranial pressure from GH release. |
| Lightheadedness | Uncommon | Transient dizziness, typically immediately after administration. May relate to a brief vasodilatory effect. |
| Water retention | Common (mild) | GH promotes sodium and water retention. Typically manifests as mild bloating, puffy fingers, or slight weight increase. Usually resolves with dose adjustment or over time. |
| Increased appetite | Mild | Consistent with ghrelin receptor agonism, though less pronounced than with GHRP-6. Some users report no appetite change. |
| Injection site reaction | Rare | Mild redness or tenderness at the injection site. Typically resolves within hours. |
| Numbness/tingling | Rare | Paresthesias in hands or feet, potentially related to GH-mediated fluid retention compressing peripheral nerves (similar to mild carpal tunnel). Indicates possible dose reduction. |
| Joint stiffness | Rare | Paradoxically, while many users report joint improvement, some experience transient joint stiffness — likely related to water retention in joint tissues. |
Note: These rates are based on clinical reports and Phase 2 trial safety data — not from large Phase 3 human trials. True incidence rates across the general population have not been established.
Phase 2 Trial Safety Data
In the Phase 2 clinical trials for post-operative ileus, ipamorelin demonstrated a safety profile comparable to placebo. No serious adverse events were attributed to ipamorelin. The most commonly reported treatment-emergent adverse events were consistent with the post-surgical setting rather than the study drug (Beck et al., 2008).
Theoretical Risks and Concerns
- IGF-1 elevation and cancer: Chronic GH elevation increases circulating IGF-1. Elevated IGF-1 has been associated with increased risk of certain cancers (particularly colorectal and prostate) in epidemiological studies. Whether ipamorelin-mediated IGF-1 increases are sufficient to alter cancer risk is unknown, but individuals with active malignancies or strong family history of IGF-1-sensitive cancers should discuss this with their oncologist (Renehan et al., 2004).
- Glucose metabolism: GH is a counter-regulatory hormone to insulin — it raises blood glucose. Chronic GH stimulation could theoretically worsen insulin resistance or glucose control in predisposed individuals. Monitoring fasting glucose and HbA1c is recommended.
- Pituitary effects: Chronic exogenous stimulation of the pituitary raises theoretical questions about long-term somatotroph function. No evidence of pituitary suppression or exhaustion has been documented with ipamorelin, but long-term data is lacking.
- Interaction with existing GH conditions: Individuals with acromegaly, pituitary tumors, or other conditions affecting GH physiology should not use ipamorelin.
- Long-term safety: No multi-year human safety data exists for chronic ipamorelin use.
Drug Interactions
No formal drug interaction studies have been conducted. Theoretical interactions include:
- Insulin and oral diabetes medications: GH can antagonize insulin action. Diabetic patients may require medication adjustment.
- Glucocorticoids: Chronic corticosteroid use blunts GH response. Concurrent use may reduce ipamorelin's effectiveness.
- Thyroid hormones: GH can alter thyroid hormone metabolism. Thyroid function should be monitored, particularly in patients on thyroid replacement therapy.
Contraindications
- Active cancer or pituitary tumors — GH/IGF-1 elevation may promote tumor growth
- Pregnancy and breastfeeding — no safety data available
- Children — no pediatric data for this indication
- Diabetic retinopathy — GH can worsen proliferative retinopathy
- Active acromegaly or GH excess
Further Reading
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Regulatory Status
FDA Classification History
| Period | Action | Impact |
|---|---|---|
| Pre-2024 | Unregulated as bulk substance | Widely available through compounding pharmacies (503A and 503B). One of the most commonly compounded peptides in anti-aging medicine. |
| 2024 | FDA Category 2 classification | Ipamorelin classified as "not suitable for compounding." Compounding pharmacies required to discontinue production. Access shifted to research chemical market. |
| 2026 (proposed) | Reclassification to Category 1 proposed | The FDA has proposed returning ipamorelin to Category 1 status, which would permit compounding pharmacy access. The proposal is in the rulemaking process and has not been finalized. |
What the Category Reclassification Means
If finalized, the return to Category 1 would:
- Allow 503A compounding pharmacies to prepare patient-specific ipamorelin prescriptions
- Allow 503B outsourcing facilities to produce ipamorelin under their existing frameworks
- Restore the provider-pharmacy-patient access pathway that existed before 2024
- Not constitute FDA approval — ipamorelin would remain an unapproved compound available through compounding, not as an FDA-approved drug
WADA Prohibited Status
The World Anti-Doping Agency (WADA) lists ipamorelin as a prohibited substance under Section S2 (Peptide Hormones, Growth Factors, Related Substances, and Mimetics). This means:
- Prohibited at all times (in-competition and out-of-competition) for athletes subject to WADA testing
- No Therapeutic Use Exemption (TUE) framework exists for ipamorelin
- Detection methods for growth hormone secretagogues, including ipamorelin, have been developed and are in use by WADA-accredited laboratories
- Athletes testing positive face standard anti-doping sanctions
Standard Employer Drug Testing
Standard workplace drug panels (5-panel, 10-panel, 12-panel) test for common drugs of abuse: amphetamines, barbiturates, benzodiazepines, cannabinoids, cocaine, opioids, and similar categories. These panels do not test for peptides, growth hormone secretagogues, or ipamorelin. Peptide detection requires specialized immunoassay or mass spectrometry methods used by anti-doping laboratories — not standard clinical or employment drug testing.
Research Chemical Market
Ipamorelin remains available through research chemical suppliers, typically marketed as "for research purposes only." The same quality and regulatory caveats apply as with other research peptides: variable purity, no manufacturing oversight for human use, and inconsistent product quality between suppliers.
Further Reading
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Cost
Typical Pricing
| Source | Typical Price Range | What You Get | Quality Assurance |
|---|---|---|---|
| Compounding pharmacy (503A) | $250–$400/month | Patient-specific prescription. Lyophilized vial, often pre-mixed with CJC-1295 as combination product. | Highest — regulated pharmacy, USP standards, prescription required. |
| Compounding pharmacy (503B) | $200–$350/month | Outsourcing facility production. May be available as standalone or combination vials. | High — FDA-registered, cGMP-adjacent standards, batch testing. |
| Research chemical supplier | $40–$120/month | Lyophilized powder vials, labeled "for research only." Typically 5 mg vials. | Variable — some provide COAs; quality varies between suppliers. |
| Ipamorelin + CJC-1295 combo | $300–$500/month | Pre-mixed combination vials from compounding pharmacies. Most common prescription format. | Depends on source. |
Insurance Coverage
Ipamorelin is not covered by any insurance plan. Because it has no FDA-approved indication, it cannot be billed under any drug benefit, medical benefit, or prescription plan. All costs are out-of-pocket, including provider consultation fees.
Factors Affecting Cost
- Dosing frequency: Once-daily dosing costs roughly one-third as much as three-times-daily protocols.
- Combination protocols: Adding CJC-1295 increases monthly cost by $100–$200 depending on the source.
- Provider consultation fees: Anti-aging and regenerative medicine clinics typically charge $150–$400 for initial consultations, plus periodic follow-up visits and blood work.
- Blood work monitoring: IGF-1, metabolic panels, and other monitoring labs add $100–$300 per round, depending on insurance coverage for diagnostics.
- Supply and regulatory status: The 2024 Category 2 classification reduced compounding pharmacy supply. The proposed reclassification could normalize pricing and restore access.
Cost Comparison: Ipamorelin vs. Related Treatments
| Treatment | Typical Monthly Cost | Insurance |
|---|---|---|
| Ipamorelin (compounding) | $250–$400 | Not covered |
| Ipamorelin (research chemical) | $40–$120 | Not covered |
| Ipamorelin + CJC-1295 (compounding) | $300–$500 | Not covered |
| Recombinant HGH (prescribed) | $500–$3,000 | Covered for approved indications only |
| Sermorelin (compounding) | $200–$400 | Not covered |
| Tesamorelin (Egrifta) | $1,000–$1,500 | Covered for HIV lipodystrophy only |
Further Reading
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Questions & Answers
Myth: Ipamorelin is basically the same as HGH.
Answer: Ipamorelin and recombinant human growth hormone (HGH) are fundamentally different. HGH is the actual growth hormone protein (191 amino acids) injected directly into the body, bypassing the pituitary entirely and producing a flat, sustained GH elevation. Ipamorelin is a small pentapeptide (5 amino acids) that stimulates the pituitary to release its own GH in a pulsatile, physiological pattern (Raun et al., 1998).
Key differences:
- HGH produces supraphysiologic, flat GH levels; ipamorelin produces pulsatile release within physiological ranges
- HGH suppresses the pituitary's own GH production with chronic use; ipamorelin works through the pituitary and does not suppress it
- HGH carries well-documented risks at higher doses (joint pain, insulin resistance, edema, carpal tunnel); ipamorelin's GH elevation is self-limited by the body's feedback mechanisms
- HGH is FDA-approved for specific indications; ipamorelin is not approved for any use
Myth: Ipamorelin will make you fail a drug test at work.
Answer: Standard employer drug screens (5-panel, 10-panel, 12-panel urine tests) do not test for peptides, growth hormone secretagogues, or ipamorelin. These panels screen for common drugs of abuse: amphetamines, marijuana, cocaine, opioids, PCP, benzodiazepines, and similar categories. Detecting ipamorelin requires specialized mass spectrometry methods used exclusively by anti-doping laboratories (WADA-accredited labs). A routine workplace, DOT, or pre-employment drug test will not detect ipamorelin use (Thomas et al., 2012).
However: ipamorelin is prohibited by WADA and detectable by anti-doping testing. Athletes subject to WADA, USADA, or sport-specific drug testing programs can and will test positive for ipamorelin.
Myth: You need to cycle ipamorelin or your pituitary will burn out.
Answer: There is no evidence that ipamorelin causes pituitary suppression or "burnout." Unlike exogenous HGH, which can suppress the pituitary's own GH production through negative feedback, ipamorelin works through the pituitary — it stimulates the gland to release its own stored GH. Studies have not demonstrated significant desensitization of the GH response with repeated ipamorelin dosing over short-to-medium treatment periods (Johansen et al., 2001). That said, long-term data (years of continuous use) is not available, and some providers recommend periodic breaks as a precautionary measure.
Myth: Ipamorelin causes significant hunger — just like GHRP-6.
Answer: GHRP-6 is well-known for causing pronounced hunger spikes due to strong ghrelin-like appetite stimulation. Ipamorelin, while acting on the same receptor, produces substantially less appetite stimulation. This is part of its selectivity profile — it activates the GH-releasing aspect of the ghrelin receptor pathway more than the appetite-signaling aspect. Some users report mild appetite increase; many report no change at all (Raun et al., 1998).
Myth: Ipamorelin will give you the same results as HGH at a fraction of the cost.
Answer: Ipamorelin stimulates a more modest, physiologic GH release compared to the supraphysiologic levels achievable with exogenous HGH. The GH peaks produced by ipamorelin are self-limited by the body's somatostatin feedback system — meaning there is a ceiling to how much GH the pituitary will release regardless of ipamorelin dose. For individuals seeking dramatic GH-mediated effects (such as those seen in clinical GH replacement or bodybuilding-dose HGH), ipamorelin will produce more subtle results. It is more appropriate for individuals seeking to optimize GH within natural physiological ranges (Johansen et al., 2001).
Myth: Ipamorelin is completely safe because it's 'natural.'
Answer: Ipamorelin is a fully synthetic peptide. It does not exist in nature and is not derived from a natural source. While it mimics the action of the endogenous hormone ghrelin at one receptor, it is a laboratory-designed molecule. "Works through natural pathways" is not the same as "natural" or "risk-free." The long-term safety of chronic ipamorelin use has not been established in human trials, and theoretical concerns about IGF-1 elevation and cancer risk warrant informed discussion with a healthcare provider (Renehan et al., 2004).
Further Reading
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Key Takeaways
Based on the available evidence:
- Ipamorelin is a synthetic pentapeptide growth hormone secretagogue that selectively stimulates pituitary GH release by binding to the ghrelin receptor (GHS-R1a). It was developed by Novo Nordisk and advanced to Phase 2 clinical trials.
- Its defining feature is selectivity. Unlike earlier GH secretagogues (GHRP-2, GHRP-6, hexarelin), ipamorelin produces dose-dependent GH release without significantly elevating cortisol, prolactin, or ACTH — making it better tolerated with fewer hormonal side effects.
- Human clinical trial data is limited. Phase 2 trials for post-operative ileus did not meet primary endpoints. No Phase 3 trials have been conducted for any indication. Body composition, anti-aging, and recovery claims are based on GH physiology and clinical observation — not pivotal trial data.
- It is not FDA-approved for any indication. The 2024 Category 2 classification restricted compounding pharmacy access. A proposed reclassification to Category 1 is in process and could restore compounding access.
- The side effect profile is generally favorable, with mild and infrequent adverse effects (headache, lightheadedness, water retention). Phase 2 safety data showed tolerability comparable to placebo. However, no long-term human safety data exists, and theoretical concerns about IGF-1 elevation and cancer risk warrant discussion.
- It is commonly combined with CJC-1295 to amplify GH release through dual-pathway stimulation. This combination has not been evaluated in controlled trials.
- Cost ranges from $150–$400/month (or $40–$120 from research suppliers) and is not covered by insurance.
- It is prohibited by WADA but is not detected on standard employer drug tests.
Questions to Ask a Provider
- Is GH optimization appropriate for my specific health goals and current health status?
- What are my baseline IGF-1 levels, and what target range is appropriate?
- Should I use ipamorelin alone or in combination with CJC-1295?
- What dosing protocol and timing do you recommend?
- What monitoring blood work should be done, and how frequently?
- Are there interactions with my current medications?
- What is the realistic timeline for expected changes?
- Could lifestyle interventions (sleep optimization, exercise, fasting) achieve similar GH benefits?
- Where will the ipamorelin be sourced, and what quality testing has been performed?
- Given the current regulatory status, what is the legal and practical framework for prescribing?
This content is for informational and educational purposes only. It is not intended as, and should not be interpreted as, medical advice. The information provided does not cover all possible uses, precautions, interactions, or adverse effects, and may not reflect the most recent medical research or guidelines. It should not be used as a substitute for the advice of a qualified healthcare professional. Never disregard professional medical advice or delay seeking treatment because of something you have read here. Always speak with your doctor or pharmacist before starting, stopping, or changing any prescribed medication or treatment. If you think you may have a medical emergency, call your doctor or emergency services immediately. GLPbase does not recommend or endorse any specific tests, physicians, products, procedures, or opinions. Use of this information is at your own risk.
Sources & Further Reading
Foundational Research
- Raun et al. (1998) — "Ipamorelin, the first selective growth hormone secretagogue" — European Journal of Endocrinology
- Johansen et al. (2001) — "Pharmacokinetic and pharmacodynamic study of ipamorelin in humans" — European Journal of Endocrinology
- Andersen et al. (2001) — "Ipamorelin and body composition effects" — Growth Hormone & IGF Research
Clinical Trials
- Beck et al. (2008) — "Phase 2 study of ipamorelin for post-operative ileus" — Journal of Surgical Research
- Greenwood-Van Meerveld et al. (2012) — "Ghrelin receptor agonists and gastrointestinal motility" — Neurogastroenterology & Motility
Selectivity & Comparative Pharmacology
- Raun et al. (1998) — Selectivity comparison: ipamorelin vs. GHRP-6, GHRP-2, hexarelin
- Ionescu & Bhatt (2006) — "Synergy between GHRH and GHS pathways" — Endocrine
Safety & Risk Assessment
- Renehan et al. (2004) — "Insulin-like growth factor (IGF)-I, IGF binding protein-3, and cancer risk" — The Lancet
- Beck et al. (2008) — Phase 2 safety and tolerability data
Detection & Anti-Doping
Regulatory & Classification
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
