Raloxifene

FDA Approved

Selective Estrogen Receptor Modulator | Gynecomastia & Bone Health

Weight: 473.58 Da
Half-life: ~28 hours
4 studies
2006 latest
FDA Approved
Dose 60mg oral daily
Frequency Once daily
Cycle 3-6 months (gynecomastia) or as directed for medical use
Storage Room temperature, protected from light and moisture
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Raloxifene is a second-generation selective estrogen receptor modulator (SERM) FDA-approved for the prevention and treatment of postmenopausal osteoporosis and for breast cancer risk reduction. Unlike tamoxifen, raloxifene has a benzothiophene core rather than a triphenylethylene backbone, giving it a distinct tissue-selectivity profile. In performance enhancement contexts, raloxifene is widely regarded as the preferred SERM for gynecomastia reversal because of its stronger antagonist activity at breast tissue estrogen receptors with fewer off-target effects. However, raloxifene is not an effective standalone post-cycle therapy drug because it does not stimulate the hypothalamic-pituitary-testicular axis as robustly as tamoxifen or enclomiphene. Its weaker antagonism at hypothalamic estrogen receptors means it produces comparatively modest elevations in LH and FSH, making it poorly suited for driving testosterone recovery after anabolic steroid cycles. Raloxifene carries a lower risk of endometrial stimulation than tamoxifen, as it acts as an estrogen antagonist rather than a partial agonist in uterine tissue.

Mechanism of Action

Raloxifene binds to both estrogen receptor alpha (ERalpha) and estrogen receptor beta (ERbeta), producing tissue-dependent agonist or antagonist effects determined by the local complement of coactivator and corepressor proteins. In breast tissue, raloxifene functions as a potent estrogen antagonist, blocking estradiol-mediated proliferative signaling with high selectivity. This strong breast-tissue antagonism underlies its effectiveness for gynecomastia treatment and breast cancer risk reduction. In bone, raloxifene acts as an estrogen agonist, maintaining bone mineral density by inhibiting osteoclast-mediated resorption. Critically, raloxifene is a weaker antagonist at hypothalamic estrogen receptors compared to tamoxifen, which means it produces less disruption of estrogen-driven negative feedback on GnRH secretion. The result is a more modest increase in LH and FSH compared to tamoxifen, limiting its utility as a standalone PCT agent. In the uterus, raloxifene does not exhibit the partial agonist activity seen with tamoxifen, which translates to a substantially lower risk of endometrial hyperplasia and endometrial cancer with long-term use. Raloxifene is metabolized primarily through glucuronidation rather than CYP450-dependent oxidation, which reduces the potential for drug-drug interactions compared to tamoxifen.

01 Superior breast tissue estrogen receptor antagonism makes it the preferred SERM for gynecomastia reversal
02 No estrogen agonist activity in the uterus, avoiding the endometrial risks associated with tamoxifen
03 Estrogen agonist activity in bone preserves bone mineral density and reduces fracture risk
04 Lower overall thromboembolic risk compared to tamoxifen
05 Metabolized via glucuronidation rather than CYP2D6, avoiding the drug interaction concerns that affect tamoxifen
06 Simple once-daily oral dosing with a manageable 28-hour half-life
07 FDA-approved with decades of clinical safety data in postmenopausal women

Molecular Data

Molecular Weight
473.58 Da
Type
Benzothiophene-derived selective estrogen receptor modulator
Peak 0.0 mcg
Trough 0.0 mcg
SS Peak 0.0 mcg
SS Trough 0.0 mcg

Research Indications

Gynecomastia Treatment
Active Gynecomastia Reversal most effective

Raloxifene is considered the most effective SERM for reversing existing gynecomastia. Its strong antagonism at breast tissue estrogen receptors directly blocks the estradiol signaling that drives glandular proliferation. Clinical and anecdotal evidence consistently favors raloxifene over tamoxifen for reducing established gynecomastia tissue.

On-Cycle Gynecomastia Prevention most effective

Blocks estrogen receptor activation in breast tissue during aromatizable steroid cycles without reducing systemic estrogen levels. Preferred over tamoxifen when the primary goal is gynecomastia prevention rather than HPTA stimulation.

Bone Health
Osteoporosis Prevention and Treatment most effective

FDA-approved for prevention and treatment of postmenopausal osteoporosis. Raloxifene acts as an estrogen agonist in bone tissue, maintaining bone mineral density and reducing the risk of vertebral fractures. The MORE trial demonstrated a 30-50% reduction in vertebral fracture risk.

Medical (FDA-Approved)
Breast Cancer Risk Reduction most effective

FDA-approved for reducing the risk of invasive breast cancer in postmenopausal women with osteoporosis and in postmenopausal women at high risk of breast cancer. The STAR trial demonstrated equivalent efficacy to tamoxifen for invasive breast cancer risk reduction with fewer side effects.

Dosing Protocols

Raloxifene is administered orally as a tablet (raloxifene hydrochloride). It has approximately 60% oral absorption, though extensive first-pass glucuronidation results in an absolute bioavailability of about 2%. Despite the low bioavailability, the 60mg dose produces reliable clinical effects. Peak plasma concentrations are reached within 0.5-6 hours. The 28-hour half-life supports once-daily dosing. Can be taken with or without food.

GoalDoseFrequencyRoute
Gynecomastia reversal60mgOnce daily for 3-6 monthsOral
On-cycle gynecomastia prevention60mgOnce daily throughout cycleOral
Osteoporosis prevention/treatment (medical)60mgOnce dailyOral

Interactions

!
Tamoxifen
Both are SERMs that compete for the same estrogen receptors. Combining two SERMs provides no meaningful additive benefit for gynecomastia or PCT and increases the risk of side effects including thromboembolic events. Choose one SERM based on the clinical goal: raloxifene for gynecomastia, tamoxifen for HPTA recovery.
avoid
+
Anastrozole
Raloxifene and anastrozole work through complementary mechanisms. Anastrozole reduces estrogen production via aromatase inhibition, while raloxifene blocks estrogen receptor signaling in breast tissue. Unlike tamoxifen, raloxifene is not metabolized via CYP pathways, so anastrozole does not impair its efficacy. Can be used together when both aromatase inhibition and breast tissue protection are desired.
compatible
+
Testosterone (exogenous)
Raloxifene can be used alongside exogenous testosterone for on-cycle gynecomastia prevention or treatment. It blocks estrogen receptors in breast tissue without interfering with testosterone's anabolic effects or the beneficial effects of estradiol in other tissues. Note that raloxifene will not prevent or reverse HPTA suppression caused by exogenous testosterone.
compatible

What to Expect

Day 1-3
Raloxifene begins binding to estrogen receptors in breast tissue. With a 28-hour half-life, near-steady-state plasma levels are reached within approximately 5 days. Early effects are subclinical.
Week 1-2
Steady-state levels are established. Users treating active gynecomastia may notice a reduction in breast tissue tenderness and sensitivity. The estrogen-blocking effect in breast tissue is building.
Week 2-4
Measurable reduction in gynecomastia symptoms in responsive individuals. Breast tissue firmness and size may begin to decrease. Bone-protective estrogen agonist effects are accumulating.
Month 1-3
Progressive reduction in gynecomastia glandular tissue in most users. Optimal results for gyno reversal typically require 3-6 months of consistent use. Earlier-stage gynecomastia responds more favorably than long-standing fibrotic tissue.

Side Effects & Safety

Common Side Effects

  • Hot flashes and increased sweating
  • Leg cramps and muscle spasms
  • Joint pain or stiffness
  • Peripheral edema (mild swelling in extremities)
  • Flu-like symptoms during initial weeks

Stop Signs - Discontinue if:

  • Signs of blood clots: sudden leg pain or swelling, chest pain, shortness of breath, or coughing up blood
  • Sudden vision changes: blurred vision, loss of vision in one eye, or visual field deficits
  • Severe or persistent headache, confusion, or neurological symptoms suggestive of stroke
  • Unexplained calf tenderness with warmth or redness

Contraindications

  • History of deep vein thrombosis, pulmonary embolism, retinal vein thrombosis, or other venous thromboembolic events
  • Active or past history of stroke or transient ischemic attack
  • Known hypersensitivity to raloxifene hydrochloride or any excipients
  • Pregnancy or planned pregnancy (category X -- contraindicated)
  • Prolonged immobilization (e.g., post-surgical recovery, extended bed rest) due to elevated DVT risk
  • Severe hepatic impairment

Quality Checklist

Good Signs

  • White to off-white tablets with uniform appearance and consistent size
  • Pharmaceutical-grade product from a licensed manufacturer or compounding pharmacy
  • Third-party certificate of analysis (COA) confirming identity, purity (>98%), and potency
  • Proper packaging with batch number, expiration date, and raloxifene hydrochloride content clearly labeled
  • HPLC or mass spectrometry testing verifying raloxifene content matches label claim

Warning Signs

  • No COA or third-party testing documentation available
  • Product labeled ambiguously (e.g., generic 'anti-estrogen' or 'SERM' without specifying raloxifene)
  • Tablets that crumble easily, vary significantly in size, or have inconsistent coloring

Bad Signs

  • Discolored, crumbling, or visibly degraded tablets
  • Unusual chemical odor or taste
  • No labeling, batch information, or expiration date
  • COA shows underdosed or contaminated product
  • Sourced from unverified vendors with no quality documentation or regulatory oversight

References

  • Raloxifene for the treatment of pubertal gynecomastia
    Lawrence SE, Faught KA, Vethamuthu J, Lawson ML
    Journal of Pediatric Endocrinology and Metabolism (2004)

    Raloxifene 60mg daily produced a significant reduction in breast tissue volume in adolescents with pubertal gynecomastia. Over 90% of subjects experienced measurable reduction in glandular tissue, establishing raloxifene as an effective pharmacological option for gynecomastia treatment.

  • Effect of raloxifene on bone mineral density, serum cholesterol concentrations, and uterine endometrium in postmenopausal women (MORE trial)
    Ettinger B, Black DM, Mitlak BH, Knickerbocker RK, Nickelsen T, Genant HK, Christiansen C, Delmas PD, Zanchetta JR, Stakkestad J, Gluer CC, Krueger K, Cohen FJ, Eckert S, Ensrud KE, Avioli LV, Lips P, Cummings SR
    JAMA (1999)

    The Multiple Outcomes of Raloxifene Evaluation (MORE) trial demonstrated that raloxifene 60mg daily increased bone mineral density by 2-3% and reduced the risk of vertebral fractures by 30-50% over 3 years in postmenopausal women with osteoporosis, without stimulating endometrial tissue. This trial was pivotal for FDA approval.

  • Effects of tamoxifen vs raloxifene on the risk of developing invasive breast cancer and other disease outcomes: the NSABP Study of Tamoxifen and Raloxifene (STAR) P-2 trial
    Vogel VG, Costantino JP, Wickerham DL, Cronin WM, Cecchini RS, Atkins JN, Bevers TB, Fehrenbacher L, Pajon ER Jr, Wade JL 3rd, Robidoux A, Margolese RG, James J, Lippman SM, Runowicz CD, Ganz PA, Reis SE, McCaskill-Stevens W, Ford LG, Jordan VC, Wolmark N
    JAMA (2006)

    The STAR trial directly compared raloxifene with tamoxifen for breast cancer risk reduction. Raloxifene was equally effective at reducing invasive breast cancer risk while producing fewer thromboembolic events, fewer cataracts, and no increase in endometrial cancer risk. Established raloxifene as the SERM with the more favorable side effect profile.

  • Raloxifene: a selective estrogen receptor modulator with tissue-specific pharmacological effects
    Muchmore DB
    Journal of Clinical Endocrinology and Metabolism (2000)

    Comprehensive review of raloxifene's tissue-selective mechanism of action, detailing its antagonist effects in breast and uterine tissue and agonist effects in bone. Explained the molecular basis for its distinct profile compared to tamoxifen, including differences in coactivator recruitment across tissue types.

Related Peptides

Anastrozole compatible

Raloxifene and anastrozole work through complementary mechanisms. Anastrozole reduces estrogen production via aromatase inhibition, while raloxifene blocks estrogen receptor signaling in breast tissue. Unlike tamoxifen, raloxifene is not metabolized via CYP pathways, so anastrozole does not impair its efficacy. Can be used together when both aromatase inhibition and breast tissue protection are desired.

Disclaimer

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