Primobolan (Primo)

Anabolic Steroid | Lean Mass & Low Side Effect Profile

Weight: 302.45 Da (base)
Half-life: ~10 days (enanthate)
4 studies
2007 latest
3 recent
Well Studied
Dose 400-800 mg/week (injectable) or 50-100 mg/day (oral)
Frequency 1-2x per week (enanthate) or daily (oral acetate)
Cycle 12-20 weeks (injectable) or 6-8 weeks (oral)
Storage Room temperature (68-77F). Protect from light.
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Primobolan (metenolone) is a dihydrotestosterone (DHT)-derived anabolic steroid that has been in clinical and performance use since the 1960s. It was originally marketed by Schering as Primobolan (oral acetate) and Primobolan Depot (injectable enanthate) for the treatment of muscle wasting diseases, malnutrition, and osteoporosis. Although it was once FDA-approved in the United States, it has since been discontinued from the US market and is primarily available through international pharmacies and underground production. Primobolan is widely considered one of the mildest and safest anabolic steroids in terms of side effect profile. It does not aromatize to estrogen, carries low androgenic activity relative to its anabolic effects (anabolic-to-androgenic ratio of approximately 88:44 compared to testosterone at 100:100), and the injectable form is not hepatotoxic. It gained legendary status in golden-era bodybuilding, with Arnold Schwarzenegger reportedly favoring it as part of his competition preparation. Primobolan is particularly valued for lean tissue preservation during caloric deficits, quality muscle gains without water retention, and its compatibility with longer cycle durations due to its mild nature. Its primary drawback is cost -- it is one of the most expensive anabolic steroids per milligram, and effective doses require relatively high volumes of oil for injection.

Mechanism of Action

Metenolone binds to the androgen receptor (AR) to promote nitrogen retention, protein synthesis, and anti-catabolic effects in skeletal muscle tissue. As a DHT derivative, it cannot be aromatized by the aromatase enzyme, meaning it produces no estrogenic metabolites and does not contribute to water retention, gynecomastia, or estrogen-mediated fat gain. Unlike testosterone, which is converted to the more potent DHT by 5-alpha reductase, metenolone is already a DHT derivative and undergoes no further activation in androgen-sensitive tissues, resulting in a relatively mild androgenic profile. Metenolone has a strong affinity for androgen receptors in muscle tissue and exerts significant anti-catabolic effects by reducing glucocorticoid receptor expression and inhibiting cortisol-mediated protein breakdown. This makes it particularly effective during caloric restriction, where it helps preserve lean tissue. It also enhances immune function at moderate doses, which was one of its original clinical applications in immunocompromised patients. The injectable enanthate form bypasses hepatic first-pass metabolism entirely, making it non-hepatotoxic. The oral acetate form, while possessing a 1-methyl modification that provides some degree of oral bioavailability, is not 17-alpha-alkylated in the traditional sense but still exerts measurable hepatic stress at sustained doses.

01 Lean muscle mass preservation during caloric deficits with minimal water retention
02 Does not aromatize to estrogen, eliminating estrogen-related side effects
03 One of the mildest androgenic profiles among anabolic steroids, with reduced risk of acne, aggression, and prostate issues
04 Injectable form is non-hepatotoxic, allowing extended cycle durations
05 Strong anti-catabolic properties through glucocorticoid receptor modulation
06 Immune-enhancing effects at moderate therapeutic doses
07 Quality, keepable muscle gains without the bloated appearance common with aromatizing steroids
08 Compatible with long cycle lengths (16-20 weeks) due to mild overall impact on health markers

Molecular Data

Molecular Weight
302.45 Da (base)
Type
DHT-derivative steroid (C20H30O2)
Peak 0.0 mcg
Trough 0.0 mcg
SS Peak 0.0 mcg
SS Trough 0.0 mcg

Research Indications

Body Composition
Lean Mass Preservation During Caloric Deficit most effective

Primobolan's primary strength lies in its anti-catabolic properties during energy restriction. It significantly reduces muscle protein breakdown by modulating glucocorticoid receptor activity, making it a preferred compound for contest preparation and body recomposition phases where preserving lean tissue while losing fat is the primary objective.

Lean Mass Accretion moderate

Primobolan produces moderate but high-quality muscle gains without water retention. Gains are slower and less dramatic than with more potent anabolic steroids but are more easily retained after discontinuation. Milligram-for-milligram it is less potent than testosterone, nandrolone, or trenbolone for mass building.

Body Recomposition effective

The combination of anti-catabolic effects, zero aromatization, and moderate anabolic activity makes primobolan well-suited for simultaneous fat loss and lean tissue maintenance or modest gain, particularly when combined with a testosterone base.

Clinical / Therapeutic
Muscle Wasting and Cachexia effective

Originally prescribed for muscle wasting conditions, sarcopenia, and post-surgical recovery. Metenolone's mild side effect profile made it suitable for debilitated patients, including women and children, at conservative therapeutic doses.

Osteoporosis moderate

Historical clinical application for bone mineral density preservation, particularly in postmenopausal women. Its non-aromatizing nature and low androgenic activity made it a more tolerable option than other anabolic steroids for female patients.

Immune Support moderate

Metenolone was used clinically to support immune function in immunocompromised patients, including those with AIDS-related wasting. It has demonstrated the ability to enhance T-cell counts and immune competence at moderate doses.

Dosing Protocols

Primobolan Depot (metenolone enanthate) is administered via intramuscular injection. The enanthate ester provides a half-life of approximately 10 days, allowing for once or twice weekly injection schedules. The injectable form is not hepatotoxic and is the strongly preferred route of administration for both efficacy and safety. Due to metenolone's relatively low potency per milligram, effective performance doses require injecting larger volumes of oil (typically 2-4 mL per injection at standard 100 mg/mL concentration), which is a practical consideration.

GoalDoseFrequencyRoute
Lean Mass Preservation - Cutting400-600 mg/week2x per week (split dose)Intramuscular
Lean Bulking600-800 mg/week2x per week (split dose)Intramuscular
Female Protocol50-100 mg/week1x per weekIntramuscular

Reconstitution Instructions

Materials Needed:
  • Pre-filled metenolone enanthate vial (typically 100 mg/mL in sesame or grape seed oil)
  • Syringes (3 mL preferred due to larger injection volumes)
  • Drawing needle (18-21 gauge)
  • Injection needle (22-25 gauge for IM)
  • Alcohol swabs
  • Sharps container
  1. 1 Wash hands thoroughly and prepare a clean work surface
  2. 2 Wipe vial stopper with alcohol swab and allow to dry
  3. 3 Draw air into syringe equal to the volume of oil to be withdrawn
  4. 4 Insert drawing needle through vial stopper and inject air to equalize pressure
  5. 5 Invert vial and withdraw the prescribed dose, tapping to remove air bubbles
  6. 6 Switch to injection needle (do not inject with drawing needle)
  7. 7 Clean injection site with alcohol swab in circular motion outward
  8. 8 Insert needle at 90-degree angle into ventrogluteal, vastus lateralis, or deltoid muscle
  9. 9 Aspirate briefly (optional per current guidelines), then inject slowly over 15-30 seconds
  10. 10 Withdraw needle, apply gentle pressure with gauze, dispose of needle in sharps container

Protocol Variations

Multiple approaches exist - compare before choosing

Different sources recommend different protocols for this peptide. Review each approach and consider your goals, tolerance, and experience level before choosing.

Metenolone Enanthate (Primobolan Depot)

Traditional

Source: Standard Injectable Protocol

"The injectable enanthate ester is the preferred form for performance and therapeutic use. Non-hepatotoxic, longer-acting, and more cost-effective per equivalent dose than oral acetate."

Metenolone enanthate is a long-acting injectable formulation with a half-life of approximately 10 days. It is the standard and strongly preferred form for both clinical and performance applications. The enanthate ester bypasses hepatic first-pass metabolism entirely, eliminating liver toxicity concerns and allowing for extended cycle durations of 12-20 weeks. Typical concentrations are 100 mg/mL, though some underground labs produce 200 mg/mL formulations.

Key Points

  • Half-life: ~10 days -- supports once or twice weekly injection schedules
  • Non-hepatotoxic -- safe for extended cycle durations
  • More cost-effective per effective dose compared to oral acetate
  • Requires larger injection volumes due to typical 100 mg/mL concentration
  • Slower onset with steady-state blood levels achieved in approximately 4-5 weeks

Dosing Schedule

Cutting / Recomposition
400-600 mg/week · Twice weekly
Lean Bulking
600-800 mg/week · Twice weekly
Female
50-100 mg/week · Once weekly

Metenolone Acetate (Oral Primobolan)

Alternative

Source: Oral Protocol

"Short-acting oral form suited to those who prefer not to inject or who want rapid clearance. Less efficient and more hepatotoxic than the injectable, but offers dose flexibility."

Metenolone acetate is the oral formulation with a half-life of approximately 4 hours. It possesses a 1-methyl modification that provides partial oral bioavailability, but it is not 17-alpha-alkylated, making it less hepatotoxic than most oral anabolic steroids. However, sustained daily dosing does produce measurable liver enzyme elevations, and cycle lengths should be limited accordingly. Oral primobolan is considerably less potent milligram-for-milligram than the injectable form and is substantially more expensive per equivalent effect.

Key Points

  • Half-life: ~4 hours -- requires twice daily dosing for stable levels
  • Mild hepatotoxicity -- limit cycles to 6-8 weeks
  • Lower bioavailability means higher mg doses needed for equivalent effect
  • Significantly more expensive per effective dose than injectable
  • Rapid clearance can be advantageous for drug testing or managing side effects
  • Preferred by some female users for the ability to stop quickly if virilization occurs

Dosing Schedule

Cutting / Lean Mass
50-100 mg/day · Split twice daily
Female
25-50 mg/day · Once or twice daily

Interactions

++
Testosterone
Testosterone is the standard base compound run alongside primobolan. A 1:1 ratio (e.g., 500 mg test / 500 mg primo per week) is the most common approach. Testosterone provides the androgenic and estrogenic signaling that primobolan lacks, maintaining libido, mood, joint lubrication, and cardiovascular-protective estrogen levels. Some users run testosterone at a lower dose and rely on primobolan's non-aromatizing nature to keep overall estrogen lower during cutting phases.
synergistic
+
Anastrozole
Aromatase inhibitors are compatible but typically unnecessary when primobolan makes up a significant portion of the total steroid load, since primobolan itself does not aromatize. AI use is dictated entirely by the testosterone dose in the stack. Some users find they can run higher testosterone doses alongside primobolan without needing an AI compared to testosterone alone, as the overall estrogen-to-androgen ratio remains favorable.
compatible
++
Growth Hormone
Growth hormone and primobolan are frequently combined for body recomposition and contest preparation. GH enhances fat mobilization and IGF-1-mediated anabolism while primobolan preserves lean tissue and provides anti-catabolic effects. The combination produces a lean, dry appearance prized in physique sports without the water retention associated with aromatizing steroids.
synergistic

What to Expect

Week 1-3
Minimal noticeable effects with the enanthate ester as blood levels are still building toward steady state. Some users report a subtle improvement in mood and well-being. No significant changes in body composition or strength yet. Oral acetate users may notice mild effects sooner due to faster onset.
Week 4-6
Blood levels approaching steady state. Early improvements in muscle hardness and fullness become apparent without accompanying water retention. Recovery between training sessions begins to improve. Strength may increase modestly. The visual quality of the physique starts to improve, particularly in leaner individuals.
Week 7-10
Primary effects are well-established. Notable improvements in lean tissue preservation during caloric deficit, improved muscle density and separation, and enhanced recovery. Anti-catabolic effects are evident in sustained strength despite caloric restriction. Skin and complexion may appear clearer compared to aromatizing compounds.
Week 11-16
Full cumulative benefits. Continued lean mass gains or preservation depending on dietary context. Body composition improvements are clearly visible. Lipid panel may show moderate HDL suppression -- bloodwork monitoring is recommended. For longer cycles, some users extend to 20 weeks given primobolan's mild impact on health markers.
Post-Cycle (Week 16+)
Gains from primobolan are generally well-retained compared to compounds that produce water retention-based weight. The enanthate ester takes approximately 4-5 weeks to fully clear the system, so natural testosterone recovery is delayed accordingly. PCT should begin approximately 2 weeks after the last injection.

Side Effects & Safety

Common Side Effects

  • Suppression of natural testosterone production (dose-dependent, less suppressive than many other anabolic steroids but still significant)
  • Hair thinning or accelerated male pattern baldness (DHT derivative -- this is the most commonly reported side effect in susceptible individuals)
  • Adverse lipid changes, particularly HDL suppression (moderate compared to other anabolic steroids)
  • Mild acne or oily skin (less pronounced than testosterone or other androgens)
  • Injection site discomfort from larger oil volumes required at performance doses
  • Gradual decline in natural testosterone production requiring post-cycle therapy

Stop Signs - Discontinue if:

  • Severe chest pain, tightness, or pressure
  • Sudden shortness of breath or difficulty breathing at rest
  • Yellowing of skin or eyes (jaundice) -- particularly with oral acetate
  • Signs of stroke: sudden numbness, confusion, trouble speaking, loss of coordination
  • Severe or persistent headaches with visual disturbances
  • Rapid or unexplained hair loss beyond gradual thinning
  • Women: rapid onset of voice deepening, significant facial hair growth, or menstrual cessation

Contraindications

  • Prostate cancer (active or history of hormone-sensitive prostate cancer)
  • Breast cancer in males or females
  • Pregnancy or potential for pregnancy (teratogenic risk -- fetal virilization)
  • Severe hepatic impairment (particularly relevant for oral acetate form)
  • Known hypersensitivity to metenolone or formulation components
  • Hypercalcemia
  • Polycythemia (hematocrit above 54% at baseline)
  • Uncontrolled cardiovascular disease or severe dyslipidemia

Quality Checklist

Good Signs

  • Clear, pale yellow oil with no visible particles or cloudiness
  • Pharmaceutical-grade product with valid lot number and manufacturer identification (e.g., Bayer Primobolan Depot)
  • Proper labeling with concentration (typically 100 mg/mL), ester type (enanthate), and expiration date
  • Intact rubber stopper and tamper-evident seal
  • Oil draws smoothly with appropriate viscosity
  • Consistent with known pharmaceutical packaging for the stated manufacturer

Warning Signs

  • Underground lab product -- primobolan is one of the most frequently counterfeited steroids due to high raw material cost
  • Concentration claims above 200 mg/mL (metenolone enanthate has limited solubility at higher concentrations)
  • Price significantly below market rate (genuine primobolan is expensive; cheap product is likely substituted with another steroid)
  • Oral tablets without pharmaceutical branding (high counterfeit rate for oral primo)
  • Vial label with spelling errors, misaligned printing, or unprofessional appearance

Bad Signs

  • Cloudy, discolored, or particulate-containing solution (contamination risk)
  • Crashed product (crystallized steroid visible in vial)
  • Broken or missing tamper-evident seal on vial or tablet blister pack
  • No labeling, incorrect labeling, or missing expiration date
  • Product testing reveals a different compound (common substitutions include boldenone undecylenate or testosterone)
  • Severe post-injection pain, redness, or swelling lasting more than 72 hours

References

  • Methyltestosterone, related steroids, and liver function
    Westaby, D., Ogle, S.J., Paradinas, F.J., et al.
    British Medical Journal (1977)

    Early clinical documentation of the hepatic effects of various oral anabolic steroids, including metenolone acetate. Found that metenolone acetate, while not 17-alpha-alkylated, could produce mild liver enzyme elevations at sustained therapeutic doses, distinguishing it from the non-hepatotoxic injectable enanthate form.

  • Comparative androgenic, myotrophic and antigonadotrophic properties of some anabolic steroids
    Potts, G.O., Arnold, A., Beyler, A.L.
    Endocrinology (1976)

    Established the anabolic-to-androgenic ratio of metenolone and other anabolic steroids in animal models. Demonstrated metenolone's favorable separation of anabolic and androgenic activity, supporting its clinical use in populations where androgenic side effects are undesirable.

  • The Effects of Supraphysiologic Doses of Testosterone on Muscle Size and Strength in Normal Men
    Bhasin, S., Storer, T.W., Berman, N., et al.
    The New England Journal of Medicine (1996)

    Landmark study establishing dose-dependent anabolic effects of supraphysiological androgens on muscle size and strength. While focused on testosterone, this trial provided the foundational framework for understanding anabolic steroid dose-response relationships applicable to DHT derivatives including metenolone.

  • Anabolic steroid abuse and cardiac death
    Fineschi, V., Riezzo, I., Centini, F., et al.
    International Journal of Legal Medicine (2007)

    Review of cardiovascular risks associated with anabolic steroid abuse. Documented that while milder compounds like metenolone carry lower cardiovascular risk per dose than more potent androgens, chronic supraphysiological use of any anabolic steroid poses risks including adverse lipid changes, left ventricular hypertrophy, and sudden cardiac events.

Related Peptides

Testosterone synergistic

Testosterone is the standard base compound run alongside primobolan. A 1:1 ratio (e.g., 500 mg test / 500 mg primo per week) is the most common approach. Testosterone provides the androgenic and estrogenic signaling that primobolan lacks, maintaining libido, mood, joint lubrication, and cardiovascular-protective estrogen levels. Some users run testosterone at a lower dose and rely on primobolan's non-aromatizing nature to keep overall estrogen lower during cutting phases.

Anastrozole compatible

Aromatase inhibitors are compatible but typically unnecessary when primobolan makes up a significant portion of the total steroid load, since primobolan itself does not aromatize. AI use is dictated entirely by the testosterone dose in the stack. Some users find they can run higher testosterone doses alongside primobolan without needing an AI compared to testosterone alone, as the overall estrogen-to-androgen ratio remains favorable.

Disclaimer

This information is for educational and research purposes only. Consult a healthcare professional before use.