Primobolan Acetate
Acétate de méthénolone oral — un oral doux mais efficace pour des gains secs. Qualité premium avec une hépatotoxicité minimale.
Composé
En un coup d'œil
En un coup d'œil
- Concentration
- 50 × 20mg
- Pureté
- Équivalent USP ≥98 %
- Voie
- Orale
- Conservation
- À température ambiante, au sec, à l'abri de la lumière.
Methenolone Acetate is a dihydrotestosterone (DHT)-derived anabolic steroid that exists in both injectable (Enanthate ester) and oral (Acetate ester) forms. The oral variant carries a 1-methyl modification that provides oral bioavailability without the standard 17-alpha-alkylation used by most oral steroids — a structural distinction that makes Primobolan Acetate one of the mildest orals on the liver. Originally marketed by Schering (as Primobolan) for the treatment of muscle-wasting conditions and malnutrition, it earned a reputation as one of the safest and most well-tolerated anabolic steroids in clinical and research applications.
Methenolone's mechanism of action is straightforward androgen receptor activation with strong nitrogen-retention effects. It does not aromatize to estrogen, carries no progestogenic activity, and exerts minimal androgenic effects relative to its anabolic potency (anabolic:androgenic ratio of approximately 88:44). Its DHT-derived structure means it cannot interact with the 5-alpha reductase enzyme, so there is no conversion to a more androgenic metabolite in target tissues. Primobolan also has documented immune-enhancing properties — clinical studies have shown it can increase T-cell counts, which is part of why it was explored in HIV/AIDS wasting treatment.
Oral Primobolan is valued for its clean lean-gain profile and its exceptional tolerability. It produces gradual, high-quality lean tissue accrual with no water retention, no estrogenic effects, and minimal post-cycle loss. It is not a compound for researchers seeking rapid mass — it rewards patience with dense, retainable muscle. Its mild nature has made it historically popular among competitive bodybuilders during pre-contest phases, where its lack of water retention and estrogen-free profile are particularly advantageous.
Primobolan Acetate suits novice through advanced researchers who prioritize tolerability and lean-tissue quality over rapid mass. Female researchers frequently select it due to its low virilization risk (at 25–75 mg daily). It stacks exceptionally well with Testosterone, Anavar, and Winstrol for cutting and recomposition protocols. Its premium price point reflects limited manufacturing availability and consistent demand.
Oral Methenolone Acetate has a half-life of approximately 4–6 hours, requiring multiple daily doses (2–3 administrations) to maintain stable blood levels. Research dosages for males range from 50–150 mg daily; effective doses for females are typically 25–75 mg daily. Because it lacks the C17-alpha-alkylated structure, hepatotoxicity is minimal — making it one of the few orals that can be run for longer periods (8–12 weeks) with reduced liver concern. The trade-off for this mildness is dose-for-dose potency: milligram-for-milligram, Primobolan Acetate is less potent than most C17-alpha-alkylated orals, which contributes to both its higher dosage requirements and its higher cost per cycle.
Dose ranges published in the peptide-research literature vary considerably. Research protocols should be designed by a qualified researcher and use the lowest effective dose consistent with the hypothesis being tested. Half-life determines dosing frequency — shorter half-lives usually require daily dosing, while long-acting analogues tolerate weekly administration.
For compound-specific dose theory, see the half-life dosing math guide and the stacking theory reference.
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