Raloxifene

The standard dosage for Raloxifene is consistent across all approved indications, simplifying the treatment regimen for patients and providers.

• Osteoporosis (Prevention and Treatment): The recommended dose is 60 mg taken orally once daily.
• Reduction of Invasive Breast Cancer Risk: The recommended dose is 60 mg taken orally once daily.

Clinical trials, such as the MORE (Multiple Outcomes of Raloxifene Evaluation) trial, utilized this 60 mg daily dose to demonstrate significant reductions in vertebral fracture risk. There is no evidence that increasing the dose beyond 60 mg provides additional clinical benefit, and higher doses may increase the risk of adverse events.

Raloxifene is not approved for use in pediatric patients. Its safety and efficacy have not been established in children or adolescents. Because the drug's mechanism involves the modulation of estrogen receptors, which are critical for growth and development, its use in a pediatric population could have significant and unpredictable effects on bone maturation and hormonal balance.

Renal Impairment

For patients with mild to moderate renal (kidney) impairment, no specific dose adjustment is typically required. However, Raloxifene should be used with extreme caution in patients with severe renal impairment. Data in this population are limited, and because the drug can affect systemic mineral balance, close monitoring by a healthcare provider is essential.

Hepatic Impairment

Raloxifene is extensively metabolized in the liver. In patients with hepatic (liver) impairment (such as cirrhosis), safety and efficacy have not been fully established. Clinical studies have shown that plasma concentrations of Raloxifene can be significantly higher in patients with liver dysfunction. Therefore, Raloxifene is generally not recommended for patients with moderate to severe hepatic impairment.

Elderly Patients

No dose adjustment is necessary based solely on age. Clinical trials included a significant number of women over the age of 65 and 75, and no overall differences in safety or effectiveness were observed between these patients and younger postmenopausal women. However, older patients may be at a higher baseline risk for venous thromboembolism (VTE), which requires careful consideration.

To ensure the best results and safety, follow these administration guidelines:

• Consistency: Take Raloxifene at the same time every day to maintain steady levels in your bloodstream.
• With or Without Food: You may take the tablet with or without food. It does not affect the drug's absorption.
• Swallow Whole: The tablet should be swallowed whole with a full glass of water. Do not crush, chew, or break the tablet, as this may interfere with the controlled release of the medication.
• Calcium and Vitamin D: For the treatment or prevention of osteoporosis, your doctor will likely recommend supplemental calcium and vitamin D if your dietary intake is inadequate. Raloxifene works best when the body has sufficient building blocks for bone formation.
• Storage: Store the medication at room temperature (68°F to 77°F or 20°C to 25°C), away from moisture and heat.

If you miss a dose of Raloxifene, take it as soon as you remember. However, if it is almost time for your next scheduled dose, skip the missed dose and return to your regular schedule. Do not double the dose to catch up. Consistency is key to the long-term effectiveness of the medication in protecting bone density and reducing cancer risk.

Reports of Raloxifene overdose are rare. In clinical trials, daily doses up to 600 mg (ten times the standard dose) were administered for several weeks and were generally well-tolerated. However, an acute overdose may lead to an increase in side effects, particularly leg cramps and dizziness. In children, accidental ingestion has resulted in symptoms such as ataxia (lack of muscle coordination), dizziness, vomiting, and rash.

In the event of a suspected overdose, contact your local poison control center or seek emergency medical attention immediately. Treatment is generally supportive, as there is no specific antidote for Raloxifene.

> Important: Follow your healthcare provider's dosing instructions exactly. Do not adjust your dose or stop taking the medication without first consulting your medical team.

Raloxifene is generally well-tolerated, but because it blocks estrogen in certain parts of the body, it can cause symptoms similar to those experienced during menopause. The most frequently reported side effects include:

• Hot Flashes (Vasomotor Symptoms): This is the most common side effect, occurring in approximately 10-25% of patients. Unlike hormone replacement therapy, which treats hot flashes, Raloxifene may trigger or worsen them because it acts as an estrogen antagonist in the brain's thermoregulatory center. These usually appear within the first six months of treatment.
• Leg Cramps: Many women report muscle spasms or cramps, particularly in the calves or feet, often occurring at night.
• Peripheral Edema: Swelling of the hands, feet, or lower legs due to fluid retention is common and should be monitored.
• Joint Pain (Arthralgia): Generalised aching in the joints is frequently reported but is usually mild to moderate in intensity.

• Flu-like Symptoms: Some patients may experience fever, chills, or body aches shortly after starting the medication.
• Sweating: Increased perspiration, often associated with hot flashes.
• Gastrointestinal Issues: Nausea, vomiting, or abdominal pain may occur.
• Weight Gain: Some women report modest increases in weight, though clinical trials have shown this to be similar to placebo groups in many cases.

• Skin Rash: Allergic-type skin reactions or hives.
• Breast Tenderness: While Raloxifene generally blocks estrogen in the breast, some women may still experience mild tenderness or enlargement.
• Gallstones: There is a slightly increased risk of gallbladder disease, similar to other medications that affect estrogen pathways.

While rare, some side effects of Raloxifene are life-threatening. You must be vigilant for the following symptoms:

> Warning: Stop taking Raloxifene and call your doctor immediately if you experience any of these.

1. 1Venous Thromboembolism (VTE): This includes Deep Vein Thrombosis (DVT) and Pulmonary Embolism (PE). Symptoms include sudden swelling, pain, or tenderness in one leg (DVT), or sudden shortness of breath, chest pain, and coughing up blood (PE).
2. 2Stroke: Raloxifene increases the risk of death from stroke in women with established coronary heart disease or those at high risk for cardiovascular events. Seek emergency care for sudden numbness or weakness (especially on one side of the body), sudden confusion, or trouble speaking.
3. 3Vision Changes: Sudden blurring of vision or loss of vision could indicate a blood clot in the eye (retinal vein thrombosis).
4. 4Severe Allergic Reaction: Symptoms include swelling of the face, lips, or tongue, and difficulty breathing (anaphylaxis).

Long-term use of Raloxifene (over several years) is generally considered safe for bone health and breast cancer risk reduction. However, the risk of blood clots remains elevated throughout the duration of therapy. Unlike estrogen therapy, Raloxifene does not appear to increase the risk of uterine (endometrial) cancer or heart disease, though it also does not provide cardiovascular protection.

The FDA has issued a "Black Box Warning" for Raloxifene, the highest level of alert for serious risks.

• Venous Thromboembolism: There is an increased risk of deep vein thrombosis (DVT) and pulmonary embolism (PE). The risk is highest during the first four months of treatment. Patients with a history of VTE should not take Raloxifene.
• Cardiovascular Disease: In a large clinical trial (the RUTH trial), women with documented coronary heart disease or those at high risk for major coronary events had an increased risk of death due to stroke when taking Raloxifene. The drug should be used with caution in women with stroke risk factors, such as smoking, hypertension, or atrial fibrillation.

Report any unusual symptoms to your healthcare provider immediately. Regular follow-ups are necessary to assess the ongoing risk-benefit ratio of the medication.

Raloxifene is a potent medication that requires careful screening before initiation. Patients must be aware that while it protects bones and reduces breast cancer risk, it does not provide the same benefits as estrogen for menopausal symptoms (like vaginal dryness or hot flashes) and carries significant vascular risks.

WARNING: INCREASED RISK OF VENOUS THROMBOEMBOLISM AND DEATH FROM STROKE

• Venous Thromboembolism: Increased risk of deep vein thrombosis and pulmonary embolism have been reported with Raloxifene. Women with a past or present history of venous thromboembolic events should not take Raloxifene.
• Stroke: Increased risk of death due to stroke occurred in a trial of postmenopausal women with documented coronary heart disease or at increased risk for major coronary events. Consider risk-benefit balance in women at risk for stroke.

Immobilization and Surgery

Raloxifene significantly increases the risk of blood clots during periods of prolonged immobility. You must stop taking Raloxifene at least 72 hours (3 days) before any scheduled surgery or any period where you will be confined to a bed or chair for a long time (such as a long flight). Do not restart the medication until you are fully mobile again. Discuss this with your surgeon well in advance of any procedure.

Cardiovascular Risk Factors

Before starting Raloxifene, your doctor should evaluate your risk for stroke. This includes checking for high blood pressure (hypertension), smoking status, history of a "mini-stroke" (TIA), or heart rhythm issues like atrial fibrillation. If you have a high risk of stroke, the risks of Raloxifene may outweigh the benefits.

Hepatic Impairment

Because the liver is the primary site of Raloxifene metabolism, patients with liver disease (cirrhosis, hepatitis) may experience dangerously high levels of the drug in their system. Raloxifene is generally avoided in these patients.

Triglyceride Levels

In women with a history of high triglycerides (fats in the blood) in response to oral estrogen therapy, Raloxifene may cause a further increase in triglyceride levels. Your doctor may need to monitor your lipid profile during treatment.

To ensure safety, the following monitoring is typically recommended:

• Bone Mineral Density (BMD): Periodic DEXA scans to ensure the medication is effectively maintaining bone mass.
• Lipid Profile: Monitoring of triglycerides, especially in those with pre-existing elevations.
• Clinical Breast Exams: Regular screenings and mammograms as recommended by your doctor, even though Raloxifene reduces the risk of invasive breast cancer.
• Liver Function Tests: If symptoms of liver dysfunction (jaundice, dark urine) appear.

Raloxifene does not typically cause drowsiness or cognitive impairment. However, if you experience dizziness or vision changes, you should avoid driving or operating heavy machinery until you know how the medication affects you.

There is no known direct interaction between alcohol and Raloxifene. However, excessive alcohol consumption is a risk factor for osteoporosis and can increase the risk of falls and fractures. It is generally advised to limit alcohol intake to support overall bone health.

There is no evidence of a withdrawal syndrome or a need to taper Raloxifene. If you stop taking it, the bone-protective effects will gradually wear off over time, and your bone loss rate will return to that of a postmenopausal woman not taking the drug. Always consult your doctor before stopping the medication to discuss alternative bone-protection strategies.

> Important: Discuss all your medical conditions, especially any history of blood clots or heart disease, with your healthcare provider before starting Raloxifene.

• Systemic Estrogens: Raloxifene should not be used concurrently with estrogen replacement therapy (tablets, patches, or gels). Because Raloxifene is designed to block estrogen in some tissues, taking both can lead to unpredictable results and may increase the risk of side effects like blood clots without providing additional benefit.
• Cholestyramine: This bile acid sequestrant (used to lower cholesterol) significantly reduces the absorption and enterohepatic cycling of Raloxifene. Specifically, it can reduce Raloxifene levels by as much as 60%. These two drugs should never be taken together.

• Warfarin (Coumadin): Raloxifene can interfere with how the body processes warfarin, potentially leading to a decrease in prothrombin time (PT). If you are taking warfarin or other blood thinners, your doctor must monitor your INR (International Normalized Ratio) very closely when starting or stopping Raloxifene.
• Highly Protein-Bound Drugs: Since Raloxifene is 95% bound to plasma proteins, it may displace other highly bound drugs, or be displaced by them. Examples include clofibrate, indomethacin, naproxen, and diazepam. This could lead to increased levels and toxicity of either drug.

• Thyroid Hormones: Some studies suggest that Raloxifene may decrease the absorption of levothyroxine (Synthroid), potentially leading to hypothyroidism. It is recommended to separate the administration of these two drugs by several hours and monitor thyroid-stimulating hormone (TSH) levels.
• Ampicillin: This antibiotic can reduce the peak concentrations of Raloxifene, although the overall absorption is not significantly changed. No specific dose adjustment is usually required, but awareness is necessary.

• Grapefruit: Unlike many other medications, Raloxifene is not metabolized by the CYP3A4 enzyme, so grapefruit and grapefruit juice do not have a significant interaction with this drug.
• Calcium Supplements: While calcium is recommended for bone health, taking very large doses at the exact same time as Raloxifene might theoretically interfere with absorption. However, most clinical guidelines suggest they can be taken together without issue.

• Soy Isoflavones / Phytoestrogens: Supplements containing high doses of soy or red clover (which act like weak estrogens) may interfere with Raloxifene's ability to block estrogen receptors in the breast. Consult your doctor before using these supplements.
• St. John's Wort: While primarily known for interacting with CYP enzymes (which Raloxifene avoids), St. John's Wort can affect overall drug metabolism and should be used with caution.

Raloxifene does not typically interfere with standard laboratory tests. However, it can lower total cholesterol and LDL cholesterol levels (which is generally considered a positive side effect) and may slightly increase levels of certain clotting factors, though these are not usually measured in routine blood work.

Mechanism of Interaction Summary:

• Bile Acid Sequestrants: Interfere with enterohepatic circulation (the recycling of the drug between the liver and gut).
• Protein Binding Displacement: Competition for binding sites on albumin.
• Pharmacodynamic Interaction: Opposing or additive effects on blood clotting or hormonal pathways.

> Important: Tell your doctor about ALL medications, supplements, and herbal products you are taking, including over-the-counter pain relievers and vitamins.

In certain situations, the risks of Raloxifene are so high that the drug must NEVER be used. These include:

1. 1History of Venous Thromboembolism (VTE): This includes a past or current diagnosis of Deep Vein Thrombosis (DVT), Pulmonary Embolism (PE), or retinal vein thrombosis (blood clot in the eye). Raloxifene significantly increases the risk of forming new clots, which can be fatal.
2. 2Pregnancy: Raloxifene is classified as Pregnancy Category X. It can cause fetal harm, including skeletal abnormalities and developmental issues. It is strictly for postmenopausal women.
3. 3Breastfeeding: It is unknown if Raloxifene passes into breast milk, but because it interferes with estrogen (which is necessary for milk production and infant development), it is contraindicated.
4. 4Hypersensitivity: Any known allergy to Raloxifene or any of the inactive ingredients in the tablet (such as lactose or titanium dioxide).

These conditions require a careful risk-benefit analysis by a specialist:

• Active Liver Disease: Due to the risk of drug accumulation and toxicity.
• High Risk of Stroke: Women with a history of TIA, atrial fibrillation, or uncontrolled hypertension.
• Severe Renal Impairment: Due to lack of safety data in this specific population.
• Pre-menopausal Status: Raloxifene is not indicated for women who have not yet completed menopause, as it can interfere with normal ovarian function and has not been studied for safety in this group.
• Hypertriglyceridemia: If a patient has had a massive increase in triglycerides while on oral estrogen, they must be monitored closely on Raloxifene.

While there is no direct cross-sensitivity with other SERMs (like tamoxifen or toremifene), patients who have had severe adverse reactions to other benzothiophene derivatives should use Raloxifene with caution. Always inform your pharmacist of any previous drug allergies.

> Important: Your healthcare provider will evaluate your complete medical history, including any history of smoking or vascular disease, before prescribing Raloxifene.

FDA Category X. Raloxifene is strictly contraindicated in women who are or may become pregnant. In animal studies, Raloxifene caused significant fetal abnormalities, including issues with bone development and delayed parturition (birth). Because Raloxifene is only indicated for postmenopausal women, pregnancy should not occur during its use. If a woman becomes pregnant while taking this drug, she must stop immediately and be apprised of the potential hazard to the fetus.

It is not known whether Raloxifene is excreted in human milk. However, many drugs are excreted in human milk, and the potential for serious adverse reactions in nursing infants is high. Furthermore, as an anti-estrogen, Raloxifene may interfere with the hormonal regulation of milk production (lactation). Use in nursing mothers is not recommended.

Raloxifene is not approved for use in children. The safety and effectiveness have not been established in any pediatric population. Estrogen receptors play a vital role in the closing of growth plates in bones; therefore, using a SERM in children could lead to stunted growth or other developmental skeletal issues.

In clinical trials, no overall differences in safety or effectiveness were observed between patients over 65 and younger postmenopausal women. However, the baseline risk for stroke and venous thromboembolism increases with age. Therefore, while no dose adjustment is needed, healthcare providers should perform regular vascular risk assessments in geriatric patients. The risk of falls and subsequent fractures should also be managed holistically alongside Raloxifene therapy.

Raloxifene is not significantly cleared by the kidneys (less than 0.2% in urine). However, the drug can influence systemic mineral metabolism. While no dose adjustment is required for mild to moderate impairment, the drug has not been sufficiently studied in patients with a GFR (Glomerular Filtration Rate) below 30 mL/min. Caution is advised.

Safety in patients with hepatic impairment has not been established. In a single-dose study, Raloxifene concentrations were 2.5 times higher in patients with child-pugh class A cirrhosis compared to healthy controls. Use is generally not recommended in patients with moderate to severe hepatic impairment.

> Important: Special populations require individualized medical assessment and frequent monitoring to ensure the safest possible outcomes.

Raloxifene is a Selective Estrogen Receptor Modulator (SERM). Its biological actions are mediated through binding to estrogen receptors alpha (ERα) and beta (ERβ). This binding induces a specific conformational change in the receptor, which then dictates how the receptor interacts with DNA and various co-regulatory proteins.

In the bone, Raloxifene acts as an agonist. It inhibits the activity of osteoclasts, the cells responsible for bone resorption. This leads to a decrease in the rate of bone turnover and an increase in bone mineral density. In the breast and uterus, it acts as an antagonist. It prevents the binding of natural estrogen to its receptors, thereby inhibiting the growth of estrogen-dependent tissues. This is why it can reduce the risk of ER-positive breast cancer without increasing the risk of uterine cancer.

Raloxifene decreases bone resorption, as evidenced by decreases in serum and urine markers of bone turnover (e.g., bone-specific alkaline phosphatase, osteocalcin). These markers typically decrease to levels seen in premenopausal women within 3 to 6 months of starting therapy. Raloxifene also has favorable effects on lipid metabolism, lowering total and LDL cholesterol without significantly affecting HDL or total triglycerides (unless a pre-existing sensitivity exists).

| Parameter | Value |

|---|---|

| Bioavailability | ~2% (due to extensive first-pass glucuronidation) |

| Protein Binding | ~95% (Albumin and α1-acid glycoprotein) |

| Half-life | 27.7 to 32.5 hours |

| Tmax | ~6 hours |

| Metabolism | Hepatic (Glucuronidation; non-CYP) |

| Excretion | Fecal (>95%), Renal (<0.2%) |

• Molecular Formula: C28H27NO4S • HCl
• Molecular Weight: 510.05 g/mol
• Solubility: Very slightly soluble in water; soluble in methanol.
• Description: Raloxifene hydrochloride is an off-white to pale-yellow solid. It is a non-steroidal benzothiophene derivative.

Raloxifene is the primary representative of the SERM class used for bone health. Other drugs in this class include Tamoxifen (used primarily for breast cancer treatment) and Bazedoxifene (used in combination with estrogens for menopause symptoms).