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Fluoxymesterone (Halo)

Oral steroid

Halo · Fluoxymesterone

⚠️ Reserved for very experienced athletes seeking maximum pre-competition aggression. Very high anabolic/androgenic ratio but extreme hepatotoxic and psychological effects. Last-resort use, 2-4 weeks maximum.

Half-life

6–8 heures

Detection

2 mois

Anabolic ratio

1900

Androgenic ratio

1600

OralHepatotoxicPCT required

Dosages

BeginnerNon recommandé débutants
Intermediate10–20 mg/j (max 4 sem)
Advanced20–40 mg/j (pré-compétition uniquement)
FemaleContraindicated

Frequency : 2-3× / day

Effects

  • Extreme aggression and training rage
  • Maximum explosive strength
  • Hardness
  • No significant mass gain

Side effects

  • Extreme hepatotoxicity
  • Pathological aggression
  • Severe acne
  • Hypertension
  • LDL↑↑↑
  • Total HPTA shutdown

Support supplements

TUDCA +++NACOmega-3Antihypertensive if needed

Synergies & stacks

Test (base)Pre-contest only (last 2-3 weeks)

Avoid

  • Cycle > 4 weeks
  • Cardiovascular issues
  • Beginners
  • Stacking with other orals

AnaProtoKol is a health and performance tracking tool. This information is provided for educational purposes only and does not constitute medical advice. Consult a qualified healthcare professional before starting any protocol.

Sources

Studies and scientific publications this guide relies on.

  1. Hudson B (1959). Fluoxymesterone ("halotestin"): a new androgen. Medical Journal of Australia. pmid: 14403738

    Article princeps présentant la fluoxymestérone (Halotestin) : dérivé testostérone 9-fluoré, 11β-hydroxylé, 17α-méthylé — affinité androgénique extrême (ratio 1900/1600 vs testostérone), non aromatisable, hépatotoxique marqué, indication clinique en hypogonadisme sévère et cancer du sein.

  2. Saartok T, Dahlberg E, Gustafsson JA (1984). Relative binding affinity of anabolic-androgenic steroids: comparison of the binding to the androgen receptors in skeletal muscle and in prostate, as well as to sex hormone-binding globulin. Endocrinology. doi: 10.1210/endo-114-6-2100

    Étude de référence : fluoxymestérone montre une affinité androgénique très élevée avec un effet sur l'agressivité et la force comportementale documenté, sans effet majeur sur la masse musculaire — d'où son usage en sports de combat plutôt qu'en bodybuilding.

  3. Kicman AT (2008). Pharmacology of anabolic steroids. British Journal of Pharmacology. doi: 10.1038/bjp.2008.165

    Revue de pharmacologie : fluoxymestérone partage l'hépatotoxicité des oraux 17α-alkylés, demi-vie orale ~6-8 h, profil androgénique très marqué (gynécomastie progestative-like, agressivité, sécheresse cutanée) — usage clinique aujourd'hui rare.

  4. Niedfeldt MW (2018). Anabolic Steroid Effect on the Liver. Current Sports Medicine Reports. doi: 10.1249/JSR.0000000000000467

    Revue clinique : halotestin présente une hépatotoxicité parmi les plus sévères des oraux 17α-alkylés en raison de la fluoration combinée à l'alkylation 17α — usage limité aux fenêtres pré-compétition (2-4 sem max) avec monitoring hépatique rapproché.

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AnaProtoKol is a health and performance tracking tool. This information is provided for educational purposes only and does not constitute medical advice. Consult a qualified healthcare professional before starting any protocol.