Anastrozole vs MK-2866

FDA Approved vs Moderate Research

avoid Mechanism-based · 64% Both Anastrozole and MK-2866 carry hepatotoxic risk. Combining hepatotoxic compounds significantly increases liver damage potential. If unavoidable, include liver support (TUDCA/NAC) and monitor ALT/AST frequently.

Molecular Data

Anastrozole MK-2866

Weight 293.37 Da 389.33 Da

Half-life ~40-50 hours ~24 hours

Type Nonsteroidal aromatase inhibitor (triazole derivative) Non-steroidal selective androgen receptor modulator (C19H14F3N3O3)

Key Benefits

Anastrozole

01 Potent reduction of circulating estradiol levels (70-80% at standard dose)

02 Prevents gynecomastia during testosterone or anabolic steroid cycles

03 Reduces estrogen-driven water retention and bloating

04 Helps control estrogen-related blood pressure elevation

05 Oral dosing with long half-life allows flexible scheduling (EOD or E3D)

06 Reversible inhibition allows estrogen recovery after discontinuation

07 Well-characterized pharmacokinetics with decades of clinical data

MK-2866

01 Increases lean body mass in a dose-dependent manner with clinical trial support

02 Preserves muscle mass during caloric deficit or catabolic conditions

03 Selective tissue activity reduces androgenic side effects compared to anabolic steroids

04 Oral bioavailability eliminates the need for injections

05 Does not aromatize to estrogen, avoiding gynecomastia and water retention

06 Improves physical function and stair-climbing power in clinical populations

07 Long 24-hour half-life allows convenient once-daily dosing

08 Mild side effect profile at commonly studied doses

Side Effects

Anastrozole

Joint pain, stiffness, or dryness (from reduced estrogen-mediated joint lubrication)

Hot flashes or flushing

Fatigue and general malaise

Mood changes (flat affect, irritability, or low mood)

Decreased libido (when estrogen is suppressed too aggressively)

Headache

MK-2866

Mild testosterone suppression (dose-dependent, typically 10-30% reduction at 25 mg)

HDL cholesterol reduction (10-20% suppression observed in clinical trials)

Headaches, particularly during the first 1-2 weeks

Mild back pain or muscle cramps

Transient fatigue toward the end of longer cycles

Slight reduction in libido at higher doses or extended cycle lengths

Contraindications

Known hypersensitivity to anastrozole or any excipients

Premenopausal women (not indicated and potentially harmful to reproductive function)

Pregnancy or breastfeeding (teratogenic risk)

Severe hepatic impairment

Pre-existing severe osteoporosis or high fracture risk

Concurrent use with tamoxifen or estrogen-containing therapies

Active liver disease or significantly elevated liver enzymes

Hormone-sensitive cancers (breast, prostate) without oncologist clearance

Pregnancy or breastfeeding (potential endocrine disruption to fetus/infant)

Individuals under 21 years of age (risk of premature HPTA disruption during development)

Concurrent use of hepatotoxic medications without liver function monitoring

Known hypersensitivity to MK-2866 or any formulation excipients

Competitive athletes subject to WADA or USADA anti-doping testing

Research Evidence

Anastrozole MK-2866

Status FDA Approved Moderate Research

References 5 studies 5 studies

FDA Approved Yes No

Full Anastrozole profile Full MK-2866 profile Anastrozole calculator MK-2866 calculator

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