Cabergoline vs Dianabol

FDA Approved vs Well Studied

synergistic Mechanism-based · 55% Dianabol supports hormonal recovery from suppression caused by Cabergoline. Standard protocol — begin PCT after the suppressive compound has cleared based on its half-life.

Molecular Data

Cabergoline Dianabol

Weight 451.60 Da 300.44 Da

Half-life ~63-69 hours ~4-6 hours

Type Ergoline-derived dopamine D2 receptor agonist 17-alpha-alkylated anabolic steroid (C20H28O2)

Key Benefits

Cabergoline

01 Potent suppression of prolactin levels, often normalizing them within days

02 Prevents and reverses prolactin-related gynecomastia from 19-nor compounds

03 Restores sexual function impaired by hyperprolactinemia (libido, erectile function, orgasm)

04 Long half-life (63-69 hours) allows convenient twice-weekly dosing

05 Significantly better tolerated than bromocriptine with fewer gastrointestinal side effects

06 Effective at shrinking prolactin-secreting pituitary tumors

07 Low doses required for bodybuilding prolactin management (0.25-0.5mg twice weekly)

Dianabol

01 Rapid and dramatic increases in muscle mass and bodyweight

02 Significant strength gains within the first 1-2 weeks

03 Enhanced nitrogen retention and protein synthesis

04 Improved glycogenolysis and muscular endurance

05 Pronounced muscle fullness and pumps from increased intracellular water and glycogen

06 Effective oral kickstart while waiting for injectable compounds to saturate

07 One of the fastest-acting anabolic compounds available

Side Effects

Cabergoline

Nausea (especially during initial doses; mitigated by taking with food)

Dizziness or lightheadedness

Headache

Nasal congestion or stuffiness

Fatigue or drowsiness

Orthostatic hypotension (feeling faint when standing up quickly)

Dianabol

Significant water retention and bloating (estrogen-mediated)

Elevated blood pressure from fluid retention and increased red blood cell mass

Liver stress with elevated ALT/AST enzymes (dose and duration dependent)

Back pumps (painful lower back cramping during exercise)

Increased appetite

Oily skin and acne

Suppression of endogenous testosterone production (HPTA suppression)

Mild mood changes (increased aggression, irritability, or euphoria)

Contraindications

Known hypersensitivity to cabergoline or any ergot alkaloid

History of cardiac valvular disease or clinically significant valvular regurgitation

History of pulmonary, pericardial, or retroperitoneal fibrotic disorders

Uncontrolled hypertension

Concurrent use of dopamine antagonists (antipsychotics, antiemetics acting on D2 receptors)

Severe hepatic impairment (cabergoline is extensively metabolized by the liver)

Pre-existing liver disease or impaired hepatic function

Active or history of hormone-sensitive cancers (prostate, breast)

Uncontrolled hypertension or significant cardiovascular disease

Elevated hematocrit (above 54%) at baseline

Concurrent use of other hepatotoxic oral steroids (do not stack C17-aa orals)

Pregnancy or potential exposure to pregnant women

Heavy alcohol use (compounded hepatotoxicity risk)

Cholestatic liver conditions or history of drug-induced liver injury

Research Evidence

Cabergoline Dianabol

Status FDA Approved Well Studied

References 5 studies 5 studies

Latest — 2017

FDA Approved Yes No

Full Cabergoline profile Full Dianabol profile Cabergoline calculator Dianabol calculator

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