Winstrol
Stanozolol — un oral de sèche réputé pour un physique dur et défini. Améliore la vascularisation et la performance athlétique.
Composé
En un coup d'œil
En un coup d'œil
- Concentration
- 50 × 25mg
- Pureté
- Équivalent USP ≥98 %
- Voie
- Orale
- Conservation
- À température ambiante, au sec, à l'abri de la lumière.
Stanozolol is a DHT-derived anabolic steroid developed by Winthrop Laboratories in 1962. Its structural modification — a pyrazole ring fused to the A-ring of the steroid nucleus — gives it unique pharmacological properties among DHT derivatives: it does not convert to a more potent androgen in target tissues (unlike testosterone), yet maintains strong anabolic activity with an anabolic:androgenic ratio of approximately 320:30. Stanozolol is one of the few oral anabolics that exists in both oral (C17-alpha-alkylated) and injectable aqueous suspension forms.
Stanozolol exerts its effects through high-affinity androgen receptor binding in skeletal muscle, but its most distinctive mechanism involves a potent reduction in sex hormone-binding globulin (SHBG). By lowering SHBG, Stanozolol increases the proportion of free (bioactive) testosterone and other androgens circulating in the bloodstream — making companion compounds in a stack functionally more potent. It does not aromatize to estrogen and carries no progestogenic activity. Additionally, Stanozolol has documented anti-estrogenic effects at the receptor level.
Winstrol is the definitive cutting oral. It produces a hard, dry, vascular aesthetic without subcutaneous water retention — the compound most closely associated with the "shrink-wrapped" contest look. Beyond cosmetics, it reliably increases speed, power output, and muscular endurance, which is why it has historically appeared in athletic performance contexts (including the widely cited 1988 Olympic disqualification). Strength gains are notable but lean toward functional power rather than sheer mass.
Best suited for intermediate to advanced researchers who already carry meaningful lean tissue and are working in a caloric deficit or at maintenance. Winstrol pairs excellently with Testosterone Propionate, Trenbolone Acetate, or Anavar in cutting stacks. It is not ideal for bulking or for researchers seeking mass, as it offers minimal weight gain and can exacerbate joint discomfort due to its drying effect on synovial fluid.
Stanozolol has a half-life of approximately 9 hours orally. Research dosages range from 25–50 mg daily for males, typically administered in two divided doses. Female researchers should exercise caution — virilization risk is moderate at standard dosages (5–10 mg daily is the typical female range). This is a C17-alpha-alkylated compound; hepatotoxicity is moderate and cycle lengths should not exceed 6–8 weeks. Joint dryness is a well-known side effect — researchers often co-administer Nandrolone or supplement with glucosamine/chondroitin for joint support. Lipid impact is significant: Stanozolol is among the harshest orals on HDL cholesterol.
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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