Tamoxifeno Vir

Tamoxifeno Vir Uses, Dosage, Side Effects, Food Interaction and all others data.

Tamoxifeno Vir is a nonsteroidal agent that binds to estrogen receptors (ER), inducing a conformational change in the receptor. This results in a blockage or change in the expression of estrogen dependent genes. The prolonged binding of tamoxifen to the nuclear chromatin of these results in reduced DNA polymerase activity, impaired thymidine utilization, blockade of estradiol uptake, and decreased estrogen response. It is likely that tamoxifen interacts with other coactivators or corepressors in the tissue and binds with different estrogen receptors, ER-alpha or ER-beta, producing both estrogenic and antiestrogenic effects.

Tamoxifeno Vir is a selective estrogen receptor modulator that inhibits growth and promotes apoptosis in estrogen receptor positive tumors. It has a long duration of action as the active metabolite N-desmethyltamoxifen has a half life of approximately 2 weeks. It has a narrow therapeutic index as higher doses can lead to breathing difficulty or convulsions. Tamoxifeno Vir administration is also associated with an increased incidence of uterine malignancies.

Trade Name Tamoxifeno Vir
Availability Prescription only
Generic Tamoxifen
Tamoxifen Other Names Tamoxifen, Tamoxifène, Tamoxifene, Tamoxifeno, Tamoxifenum, trans-Tamoxifen
Related Drugs Supprelin LA, estradiol, anastrozole, letrozole, Premarin, testosterone, Lupron, Arimidex, megestrol, fluorouracil
Type
Formula C26H29NO
Weight Average: 371.5146
Monoisotopic: 371.224914555
Protein binding

The protein binding of tamoxifen in plasma is over 98% and mostly to serum albumin.

Groups Approved
Therapeutic Class Hormonal Chemotherapy
Manufacturer
Available Country Spain
Last Updated: September 19, 2023 at 7:00 am
Tamoxifeno Vir
Tamoxifeno Vir

Uses

Tamoxifeno Vir is used for the treatment of breast cancer.

Tamoxifeno Vir is a praparation of Tamoxifeno Vir which is a non-steroidal, triphenylene based drug and displays a complex spectrum of oestrogen antagonist and oestrogen agonist like pharmacological effects in different tissues. In breast cancer patients, at the tumour level, Tamoxifeno Vir acts primarily as an antioestrogen, preventing oestrogen binding to the oestrogen receptor. Additionally Tamoxifeno Vir has been reported to lead to maintenance of bone mineral density in post-menopausal women.

Tamoxifeno Vir is also used to associated treatment for these conditions: Breast Cancer, Desmoid Tumors, Endometrial Cancer, Gynecomastia, Invasive Breast Cancer, Invasive Breast Carcinoma, Metastatic Breast Cancer, Ovarian Cancer, Puberty, Precocious, Ovulation induction therapy

How Tamoxifeno Vir works

Tamoxifeno Vir competitively inhibits estrogen binding to its receptor, which is critical for it's activity in breast cancer cells. Tamoxifeno Vir leads to a decrease in tumor growth factor α and insulin-like growth factor 1, and an increase in sex hormone binding globulin. The increase in sex hormon binding globulin limits the amount of freely available estradiol. These changes reduce levels of factors that stimulate tumor growth.

Tamoxifeno Vir has also been shown to induce apoptosis in estrogen receptor positive cells. This action is thought to be the result of inhibition of protein kinase C, which prevents DNA synthesis. Alternate theories for the apoptotic effect of tamoxifen comes from the approximately 3 fold increase in intracellular and mitochondrial calcium ion levels after administration or the induction of tumor growth factor β.

Dosage

Tamoxifeno Vir dosage

Adults (including elderly): The dosage range is 20 to 40 mg daily, given either in divided doses twice daily or as a single dose once daily.

Side Effects

Side effects can be classified as either due to the pharmacological action of the drug, e.g., hot flushes, vaginal bleeding, vaginal discharge, pruritus vulvae and tumour flare or as more general side effects, e.g., gastrointestinal intolerance, headache, light-headedness and occasionally fluid retention and alopecia. When such side effects are severe, it may be possible to control them by a simple reduction of dosage (within the recommended dose range) without loss of control of the disease.

Skin rashes including isolated reports of erythema multiforme, Stevens Johnson syndrome and bullous pemphigoid and rare hypersensitivity reactions, including angio-oedema have been reported. A small number of patients with bony metastases have developed hypercalcaemia on initiation of therapy.

Falls in platelet count, usually only to 80,000-90,000 per/mm3 but occasionally lower, have been reported in patients taking Tamoxifeno Vir for breast cancer.

A number of cases of visual disturbances including infrequent reports of corneal changes and retinopathy have been described in patients receiving Tamoxifeno Vir therapy. An increased incidence of cataracts has been reported in association with the administration of the drug. Uterine fibroids and endometrial changes including hyperplasia and polyps have been reported. Cystic ovarian swellings have occasionally been observed in premenopausal women receiving Tamoxifeno Vir.

Leucopenia has been observed following the administration of Tamoxifeno Vir, sometimes in association with anaemia and/or thrombocytopenia. Neutropenia has been reported on rare occasions; this can sometimes be severe. There is evidence of an increased incidence of thromboembolic events including deep vein thrombosis and pulmonary embolism during Tamoxifeno Vir therapy.

Tamoxifeno Vir has been associated with changes in liver enzyme levels and on rare occasions with a spectrum of more severe liver abnormalities, including fatty liver, cholestasis and hepatitis. Rarely, elevation of serum triglyceride levels, in some cases with pancreatitis, may be associated with the use of Tamoxifeno Vir.

Toxicity

High doses of tamoxifen in animals lead to respiratory difficulty and convulsions. High doses in advanced metastatic cancer patients resulted in acute neurotoxicity seen by tremor, hyperreflexia, unsteady gait, and dizziness. Patients experiencing and overdose should be given supportive treatment as no specific treatment for overdose is suggested.

Precaution

Menstruation is suppressed in a proportion of premenopausal women receiving Tamoxifeno Vir for the treatment of breast cancer. An increased incidence of endometrial cancer has seen reported in association with Tamoxifeno Vir treatment. The underlying mechanism is unknown, but may be related to the oestrogen-like effect of Tamoxifeno Vir. Any patients receiving or having previously received Tamoxifeno Vir, who report abnormal gynaecological symptoms, especially vaginal bleeding, should be promptly investigated.

A number of second primary tumors, occurring at sites other than the endometrium and the opposite breast, have been reported in clinical trials, following the treatment of breast cancer patients with Tamoxifeno Vir. No causal link has been established and the clinical significance of these observations remains unclear.

Interaction

When Tamoxifeno Vir is used in combination with coumarin type anticoagulants, a significant increase in anticoagulant effect may occur. Where such co administration is initiated, careful monitoring of the patient is recommended. When Tamoxifeno Vir is used in combination with cytotoxic agents, there is an increased risk of thromboembolic events.

Food Interaction

  • Exercise caution with St. John's Wort. This herb induces CYP3A4 metabolism, which may reduce the serum concentration of tamoxifen.
  • Take with a full glass of water.
  • Take with or without food.

[Moderate] GENERALLY AVOID: Due to their estrogenic effect, isoflavones present in soy such as genistein and daidzein may stimulate breast tumor growth and antagonize the antiproliferative action of tamoxifen.

Supportive data are derived primarily from in vitro and animal studies.

In vitro, low concentrations of these phytoestrogens have been found to promote DNA synthesis and reverse the inhibitory effect of tamoxifen on estrogen-dependent breast cancer cell proliferation.

In contrast, high concentrations of genistein greater than 10 microM

It is not known if these high concentrations are normally achieved in humans.

Plasma concentrations below 4 microM

These concentrations are comparable to the low plasma concentrations associated with tumor stimulation reported in animals.

In a study of 155 female breast cancer survivors with substantially bothersome hot flashes, a product containing 50 mg of soy isoflavones (40% to 45% genistein; 40% to 45% daidzein; 10% to 20% glycitein) taken three times a day was found to be no more effective than placebo in reducing hot flashes.

No toxicity or recurrence of breast cancer was reported during the 9-week study period.

Green tea does not appear to have significant effects on the pharmacokinetics of tamoxifen or its primary active metabolite, endoxifen.

In a study consisting of 14 patients who have been receiving tamoxifen treatment at a stable dose of 20 mg (n=13) or 40 mg (n=1) once daily for at least 3 months, coadministration with green tea supplements twice daily for 14 days resulted in no significant differences in the pharmacokinetics of either tamoxifen or endoxifen with respect to peak plasma concentration (Cmax), systemic exposure (AUC), and trough plasma concentration (Cmin) compared to administration of tamoxifen alone.

The combination was well tolerated, with all reported adverse events categorized as mild (grade 1) and none categorized as serious or severe (grade 3 or higher) during the entire study.

Although some adverse events such as headache, polyuria, gastrointestinal side effects (e.g., constipation, dyspepsia), and minor liver biochemical disturbances were reported more often during concomitant treatment with green tea, most can be attributed to the high dose of green tea used or to the caffeine in green tea.

The green tea supplements used were 1000 mg in strength and contained 150 mg of epigallocatechin-3-gallate (EGCG), the most abundant and biologically active catechin in green tea.

According to the investigators, the total daily dose of EGCG taken by study participants is equivalent to the amount contained in approximately 5 to 6 cups of regular green tea.

However, it is not known to what extent the data from this study may be applicable to other preparations of green tea such as infusions, since the bioavailability of EGCG and other catechins may vary between preparations.

MANAGEMENT: Until more information is available, patients treated with tamoxifen may consider avoiding or limiting the consumption of soy-containing products.

Consumption of green tea and green tea extracts during tamoxifen therapy appears to be safe.

Volume of Distribution

The volume of distribution of tamoxifen is approximately 50-60L/kg.

Elimination Route

An oral dose of 20mg reaches a Cmax of 40ng/mL with a Tmax of 5 hours. The metabolite N-desmethyltamoxifen reaches a Cmax of 15ng/mL. 10mg of tamoxifen orally twice daily for 3 months results in a Css of 120ng/mL and a Css of 336ng/mL.

Half Life

The terminal elimination half-life of tamoxifen is 5 to 7 days, while the half-life of N-desmethyltamoxifen, the primary circulating metabolite, is approximately 14 days.

Clearance

The clearance of tamoxifen was 189mL/min in a study of six postmenopausal women.

Elimination Route

Tamoxifeno Vir is mainly eliminated in the feces. Animal studies have shown 75% of radiolabelled tamoxifen recovered in the feces, with negligible collection from urine. However, 1 human study showed 26.7% recovery in the urine and 24.7% in the feces.

Pregnancy & Breastfeeding use

Pregnancy: Tamoxifeno Vir must not be administered during pregnancy. There have been a small number of reports of spontaneous abortions, birth defects and foetal deaths after women have taken Tamoxifeno Vir, although no causal relationship has been established. Reproductive toxicology studies in rats, rabbits and monkeys have shown no teratogenic potential.

Women should be advised not to become pregnant whilst taking Tamoxifeno Vir and should use barrier or other nonhormonal contraceptive methods if sexually active. Premenopausal patients must be carefully examined before treatment to exclude pregnancy. Women should be informed of the potential risks to the foetus, if they want to become pregnant whilst taking Tamoxifeno Vir or within two months of cessation of therapy.

Lactation: It is not known if Tamoxifeno Vir is excreted in human milk and therefore the drug is not recommended during lactation. The decision to discontinue Tamoxifeno Vir should take into account in case of the importance of the drug to the lactating mother.

Contraindication

Tamoxifeno Vir must not be administered during pregnancy. Tamoxifeno Vir should not be given to patients who have experienced hypersensitivity to the product or any of its ingredients.

Storage Condition

Store between 20-25° C. Protect from light.

Innovators Monograph

You find simplified version here Tamoxifeno Vir

Tamoxifeno Vir contains Tamoxifen see full prescribing information from innovator Tamoxifeno Vir Monograph, Tamoxifeno Vir MSDS, Tamoxifeno Vir FDA label

FAQ

What is Tamoxifeno Vir used for?

Tamoxifeno Vir used to treat hormone receptor-positive breast cancer. It can greatly reduce the risk of cancer recurrence and invasive cancer.

How does Tamoxifeno Vir do to the body?

Tamoxifeno Vir attaches to the hormone receptors in the cancer cell, blocking estrogen from attaching to the receptors. This slows or stops the growth of the tumor by preventing the cancer cells from getting the hormones they need to grow.

What cancer does Tamoxifeno Vir treat?

Tamoxifeno Vir can be used to treat women with breast cancer who have or have not gone through menopause. It can be used in several ways: In women at high risk of breast cancer,Tamoxifeno Vir can be used to help lower the risk of developing breast cancer.

What are the side effects of Tamoxifeno Vir?

Common side effects of Tamoxifeno Vir include:

  • Menopause-like symptoms, including hot flashes, night sweats and vaginal dryness.
  • Weight gain (more common) or fluid retention (edema).
  • Irregular or loss of menstrual periods.
  • Leg swelling.
  • Nausea.
  • Vaginal discharge.
  • Skin rash.
  • Erectile dysfunction .
  • Fatigue.
  • Headaches.



How long should I take Tamoxifeno Vir?

Most people take Tamoxifeno Vir or other hormone therapy for at least five years and sometimes up to 10 years. Treatment length depends on the features of your cancer diagnosis.

How do take I Tamoxifeno Vir?

You must take Tamoxifeno Vir daily by mouth, preferably at the same time each day.

Is it safe to take Tamoxifeno Vir during pregnancy?

Tamoxifeno Vir may cause birth defects. You shouldn’t take the medication if you’re pregnant or planning to become pregnant. To prevent pregnancy, talk to your healthcare provider about nonhormonal birth control options.

Is Tamoxifeno Vir safe during breasfeeding?

Tamoxifeno Vir and its active metabolites are detectable in milk and accumulate in milk over time. It can also suppress lactation. If a mother requires treatment with Tamoxifeno Vir, breastfeeding should be avoided.

Can I drink alcohol while taking Tamoxifeno Vir?

Alcohol can raise the risk of side effects with Tamoxifeno Vir, some of which can be serious. Alcohol makes it harder for Tamoxifeno Vir to work properly and should be limited or avoided while you're taking this medication. Alcohol can raise your risk of developing breast cancer.

How does Tamoxifeno Vir make me feel?

Some people go through mood swings or feel low or depressed while they are taking Tamoxifeno Vir. Or it may be harder to think clearly or concentrate.

Is Tamoxifeno Vir really necessary?

Tamoxifeno Vir is a highly effective breast cancer treatment. It may significantly lower your risk of breast cancer recurrence or invasive breast cancer. People who are at high risk for breast cancer may take Tamoxifeno Vir to reduce their chances of getting the disease.

Does Tamoxifeno Vir lower my immune system?

Taking hormone therapy does not affect your immune system.

Does Tamoxifeno Vir cause I to gain weight?

Tamoxifeno Vir has been loosely associated with weight gain. Studies have tracked weight gain and other side effects of the drug for years. Some resources even list weight gain as a possible side effect.

Can Tamoxifeno Vir raise blood pressure?

There was no effect of Tamoxifeno Vir on clinic BP.

Does Tamoxifeno Vir cause hair loss?

No one goes bald from Tamoxifeno Vir but some people do experience thinning hair. Like hair thinning, a lowered libido is common postmenopause and in the setting of reduce estrogen.

Is Tamoxifeno Vir an anti inflammatory?

Results suggest that the mechanism of action of Tamoxifeno Vir administration is to modulate anti-oxidant, anti-inflammatory and anti-gliotic responses.

Is Tamoxifeno Vir an anti inflammatory?

Results suggest that the mechanism of action of Tamoxifeno Vir administration is to modulate anti-oxidant, anti-inflammatory and anti-gliotic responses.

Does Tamoxifeno Vir make me tired?

When you start to take Tamoxifeno Vir, you may feel tired, drowsy, or feel like you have no energy.

Can Tamoxifeno Vir cause memory loss?

memory loss and concentration issues brought on by use of Tamoxifeno Vir or aromatase inhibitors.

Does Tamoxifeno Vir affect mood?

Tamoxifeno Vir does not affect mood or sexual functioning.

Can Tamoxifeno Vir cause anxiety?

Clinical evidence suggests the drug increases rates of anxiety and the incidence of hot flashes, both of which may result from reduced action of estrogen.

Can Tamoxifeno Vir cause hip pain?

The terrible groin and hip pain is pretty clearly a side effect of the Tamoxifeno Vir.

Is Tamoxifeno Vir good for my bones?

Taking Tamoxifeno Vir slows down bone loss and can reduce the risk of osteoporosis.

Does Tamoxifeno Vir make me itchy?

Dry, itchy skin is a common side effect of Tamoxifeno Vir.

Is it better to take Tamoxifeno Vir at night or morning?

Tamoxifeno Vir may be taken at any time of the day but should be taken at the same time each day. it is within 12 hours of the missed dose.

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*** Taking medicines without doctor's advice can cause long-term problems.
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