Side effects of bicalutamide
The side effects of bicalutamide, a nonsteroidal antiandrogen, including its frequent and rare side effects, have been well-studied and characterized. The most common side effects of bicalutamide monotherapy in men include breast tenderness, breast growth, feminization, demasculinization, and hot flashes. Less common side effects of bicalutamide monotherapy in men include sexual dysfunction, depression, fatigue, weakness, and anemia. Bicalutamide is well tolerated and has few side effects in women. General side effects of bicalutamide that may occur in either sex include diarrhea, constipation, abdominal pain, nausea, dry skin, itching, and rash.
In men with prostate cancer, bicalutamide monotherapy has been found to increase the likelihood of death due to causes other than prostate cancer. Bicalutamide has been found to cause unfavorable liver changes in around 3 to 11% of people, with such changes necessitating discontinuation in approximately 1%. Rarely, bicalutamide has been associated with serious liver toxicity and lung disease, as well as sensitivity to light. It has also uncommonly been associated with hypersensitivity reactions. Bicalutamide has a theoretical risk of birth defects in male fetuses.
Central nervous system
Hot flashes
In the Early Prostate Cancer clinical trial programme, at 7.4 years follow-up, the rate of hot flashes was 9.2% for bicalutamide monotherapy relative to 5.4% for placebo, which was regarded as relatively low. In the subgroup of the trial, the rate of hot flashes with bicalutamide monotherapy was 13.1%.Sexual dysfunction
Bicalutamide may cause sexual dysfunction, including decreased sex drive and erectile dysfunction. However, the rates of these side effects with bicalutamide monotherapy are very low. In the trial, at 7.4 years follow-up, the rates of decreased libido and impotence were only 3.6% and 9.3% in the 150 mg/day bicalutamide monotherapy group relative to 1.2% and 6.5% for placebo, respectively. Similarly, in the trials of 150 mg/day bicalutamide monotherapy for advanced prostate cancer, fewer than 10% of men reported decreased sex drive or reduced erectile function as a side effect. About two-thirds of men in these trials, who had advanced prostate cancer and were of almost invariably advanced age, maintained sexual interest, while sexual function was slightly reduced by 18%. Most men experience sexual dysfunction only moderately or not at all with bicalutamide monotherapy, and the same is true during monotherapy with other. Bicalutamide monotherapy at a dosage of 50 mg/day had no effect on nocturnal erections in men with prostate cancer. The preservation of sexual desire and function with monotherapy may be related to testosterone metabolites such as estradiol and the 3α-androstanediol maintaining these functions rather than the androgen receptor or to bicalutamide and other possibly incompletely blocking the androgen receptor in the brain.Similarly to in men, bicalutamide has been associated with minimal or no sexual dysfunction in women. A phase III clinical study of 50 mg/day bicalutamide in conjunction with a combined oral contraceptive in women with severe hirsutism due to polycystic ovary syndrome carefully assessed the side effect of decreased libido and found that the incidence with bicalutamide did not differ from the control group. Minimal rates of reduced sex drive have also been associated with the related NSAA flutamide. These findings are in accordance with the fact that women with complete androgen insensitivity syndrome show normal sexual function in spite of complete loss of androgen receptor signaling. They are also in accordance with a variety of findings concerning testosterone levels and sexual function in premenopausal women, in which no change in parameters of sexual function, including libido, have been observed in association with increases or decreases in testosterone levels. It appears that testosterone levels within the normal physiological range are not importantly involved in sexual desire or function in women.
Psychiatric conditions
At 5.3 years follow-up, the incidence of depression was 5.5% for bicalutamide monotherapy relative to 3.0% for placebo in the trial, and the incidence of asthenia was 10.2% for bicalutamide monotherapy relative to 5.1% for placebo. Rarely, bicalutamide has been associated with hallucinations. This is thought to be secondary to AR antagonism.Breasts and reproductive system
Breast changes
The most common side effects of bicalutamide monotherapy in men are breast pain/tenderness and gynecomastia. These side effects may occur in as many as 90% of men treated with bicalutamide monotherapy, but gynecomastia is generally reported to occur in 70 to 80% of patients. In the trial, at a median follow-up of 7.4 years, breast pain and gynecomastia respectively occurred in 73.6% and 68.8% of men treated with 150 mg/day bicalutamide monotherapy.Rates of gynecomastia with bicalutamide monotherapy and monotherapy with other varies significantly across different trials, in reviews ranging from 38 to 85% with bicalutamide, 21 to 80% with flutamide, and 50 to 79% with nilutamide. This variation is presumably related to factors like duration of therapy, differing patient characteristics, and the specific methods of collection of adverse-event data. One review noted that rates of breast side effects were much lower with open questioning as opposed to direct questioning in studies of bicalutamide monotherapy for prostate cancer.
Gynecomastia associated with monotherapy usually develops within the first 6 to 9 months following initiation of treatment. In one study, 89% of those who developed gynecomastia and 98% of those who developed breast pain did so within the first 6months. Of those who developed gynecomastia, around 55% did so in the first 3months, around 35% between 3 and 6months, and 10% after more than 6months. For breast pain, rates were around 75% in the first 3months, 25% between 3 and 6months, and less than 5% after more than 6months. In the programme, 85% who developed breast pain did so in the first 6months and 80% who developed gynecomastia did so in the first 9months.
In more than 90% of affected men, bicalutamide-related breast changes are mild-to-moderate in severity. It is only rarely and in severe and extreme cases of gynecomastia that the proportions of the male breasts become so marked that they are comparable to those of women. In addition, bicalutamide-associated breast changes improve or resolve in most men upon discontinuation of therapy. In the trial, 16.8% of bicalutamide patients relative to 0.7% of controls withdrew from the study due to breast pain and/or gynecomastia. Gynecomastia and breast pain improved or resolved upon discontinuation in 70 and 90% of patients, respectively. Resolution of breast symptoms was dependent on duration of bicalutamide therapy, with resolution rates ranging from 29% with >18months of treatment to 64% for <6months of treatment.
Gynecomastia and breast pain/tenderness with monotherapy is due to increased estradiol levels and unopposed estrogen action in the breasts due to androgen receptor blockade.
The incidence and severity of gynecomastia are reportedly slightly higher with estrogens than with like bicalutamide in the treatment of men with prostate cancer.
Management of breast changes
Tamoxifen, a selective estrogen receptor modulator with antiestrogenic actions in breast tissue and estrogenic actions in bone, has been found to be highly effective in preventing and reversing bicalutamide-induced gynecomastia in men. Moreover, in contrast to analogues, tamoxifen poses minimal risk of accelerated bone loss and osteoporosis. For reasons that are unclear, anastrozole, an aromatase inhibitor, has been found to be much less effective in comparison to tamoxifen for treating bicalutamide-induced gynecomastia. A 2015 systematic review of -induced gynecomastia and breast tenderness concluded that tamoxifen and radiotherapy could effectively manage the side effect without relevant adverse effects, though with tamoxifen showing superior effectiveness. A 2019 network meta-analysis likewise concluded that tamoxifen was more effective than radiotherapy or anastrozole for preventing bicalutamide-induced gynecomastia. Surgical breast reduction may also be employed to correct bicalutamide-induced gynecomastia.Male breast cancer
A case report of male breast cancer subsequent to bicalutamide-induced gynecomastia has been published. According to the authors, "this is the second confirmed case of breast cancer in association with bicalutamide-induced gynaecomastia." It is notable, however, that gynecomastia does not seem to increase the risk of breast cancer in men. Moreover, the lifetime incidence of breast cancer in men is approximately 0.1%, the average age of diagnosis of prostate cancer and male breast cancer are similar, and millions of men have been treated with bicalutamide for prostate cancer, all of which are potentially in support of the notion of chance co-occurrences. In accordance, the authors concluded that "causality cannot be established" and that it was "probable that the association is entirely coincidental and sporadic."Lower reproductive system
Bicalutamide reduces the size of the prostate gland and seminal vesicles, though not of the testes. Slightly but significantly reduced penile length is also a recognized adverse effect of. Reversible hypospermia or aspermia may occur. However, bicalutamide does not appear to adversely affect spermatogenesis, and thus may not necessarily abolish the capacity/potential for fertility in men. Due to the induction of chronic overproduction of and testosterone, there was concern that long-term bicalutamide monotherapy might induce Leydig cell hyperplasia and tumors, but clinical studies indicate that Leydig cell hyperplasia does not occur to a clinically important extent.Male birth defects
Because bicalutamide blocks the, like all antiandrogens, it can interfere with the androgen-mediated sexual differentiation of the genitalia during prenatal development. In pregnant rats given bicalutamide at a dosage of 10 mg/kg/day and above, feminization of male offspring, such as reduced anogenital distance and hypospadias, as well as impotence, were observed. No other teratogenic effects were observed in rats or rabbits receiving up to very high dosages of bicalutamide, and no teratogenic effects of any sort were observed in female rat offspring at any dosage. As such, bicalutamide is a selective reproductive teratogen in males, and may have the potential to produce undervirilization/sexually ambiguous genitalia in male fetuses. Due to its teratogenic capacity, contraception should be used in women taking bicalutamide who are fertile and sexually active.Skin, fat, and bone
Skin changes
Antiandrogen therapy and estrogen therapy are known to produce demasculinizing and feminizing effects in the skin and on hair follicle distribution in people assigned male at birth. Androgens are involved in regulation of the skin, and antiandrogens are known to be associated with skin changes. Skin-related side effects, which included dry skin, itching, and rash, were reported at a rate of 2% in both monotherapy and clinical studies of bicalutamide in men.Sensitivity to light
A few cases of photosensitivity associated with bicalutamide have been reported. In one of the cases, bicalutamide was continued due to effectiveness in treating prostate cancer in the patient, and in combination with strict photoprotection. Eventually, the symptoms disappeared and did not recur. Flutamide is also associated with photosensitivity, but much more frequently in comparison to bicalutamide.Fat distribution
Antiandrogen therapy and estrogen therapy are known to produce demasculinizing and feminizing effects on fat distribution in people assigned male at birth.Bone density and fractures
Bicalutamide monotherapy preserves bone mineral density in men with prostate cancer relative to surgical or medical castration. This is considered to be due to preservation of gonadal estradiol production with bicalutamide monotherapy, in contrast to castration which greatly reduces estradiol levels. The risk of osteoporosis and serious bone fractures with bicalutamide monotherapy appears to be no different than with non-use in men with prostate cancer.Gastrointestinal system
The incidence of diarrhea with bicalutamide monotherapy in the trial was comparable to placebo. In phase III studies of bicalutamide monotherapy for, the rates of diarrhea for bicalutamide and castration were 6.4% and 12.5%, respectively, the rates of constipation were 13.7% and 14.4%, respectively, and the rates of abdominal pain were 10.5% and 5.6%, respectively.Heart, liver, kidneys, and lungs
Cardiovascular system
A study of high-dose bicalutamide monotherapy in 248men with or metastatic prostate cancer found that there were no effects of bicalutamide on heart rate, blood pressure, or electrocardiogram parameters. At the 5-year follow-up of the study, the incidence of cardiovascular events was low, with no differences between the bicalutamide group and the castration group. There were also no differences in the incidences of arrhythmia, myocardial infarction, or other ischemic cardiac or cerebrovascular conditions.In the group of the study, which compared 150mg/day bicalutamide monotherapy versus placebo/standard care, there were numerically more deaths from heart failure in the bicalutamide group. This contributed to a trend toward significantly increased mortality due to causes other than prostate cancer in the bicalutamide group. Cardiovascular morbidity, on the other hand, was similar between the bicalutamide and placebo groups. In the NRG/RTOG 9601 trial, bicalutamide monotherapy significantly increased the risk of grade 3 to 5 cardiovascular incidents after a median 13years of follow-up.
A systematic review and meta-analysis of randomized controlled trials of and risk of cardiovascular death in men with non-metastatic prostate cancer was published in 2011. It assessed in the form of a agonist or surgical castration alone or in combination with a and included over 4,000patients. The meta-analysis found no evidence of increased cardiovascular mortality or overall mortality. Non-prostate cancer mortality was not specifically assessed. A limitation of the meta-analysis was that of the trials included in the meta-analysis, only flutamide was employed and not bicalutamide. Subsequent reviews and meta-analyses, published between 2014 and 2022, have reported positive though inconsistent associations of with cardiovascular complications and death.
A case report in which bicalutamide was described as a probable cause of heart failure in a man with prostate cancer has been published.
Lipid profile
Bicalutamide has been found to increase total cholesterol and LDL cholesterol levels in women with polycystic ovary syndrome and hirsutism taking a combined birth control pill. There was also a non-significant trend toward increased triglyceride levels. Lipid changes with bicalutamide in men with prostate diseases have also been studied, but no significant changes have been found in studies in this population. Heightened LDL cholesterol and triglyceride levels are potential risk factors for atherosclerosis or coronary heart disease. Unfavorable blood lipid profile changes have also been seen with other antiandrogens in women, for instance cyproterone acetate and spironolactone, and with androgenic medications.Coagulation
monotherapy is associated with a greater risk of venous thromboembolism than non-use, although not to the same extent as surgical or medical castration or particularly high-dose estrogen therapy.Kidney function
Androgens and anabolic steroids, including testosterone, have trophic and anabolic effects in the kidneys. Androgen deprivation therapy, including with GnRH agonists and bicalutamide monotherapy, may increase the risk of kidney failure in men. A large randomized controlled trial in men with prostate cancer found that the incidence of kidney failure was 1 to 2% in men treated with combined androgen blockade using bicalutamide or flutamide, although this study had no placebo group. Several preclinical studies are suggestive that bicalutamide may have toxic effects on kidney cells. This may be secondary to androgen deprivation. Kidney toxicity with bicalutamide and has yet to be fully assessed clinically.Anemia
Androgens including testosterone are known to stimulate erythropoiesis and increase hematocrit. These effects are mediated by increasing production and secretion of erythropoietin from the kidneys. Erythropoietin in turn stimulates erythropoiesis in hematopoietic tissues such as bone marrow. The high levels of testosterone in males are why hematocrit and hemoglobin levels are higher in men than in women. Due to stimulation of erythropoiesis, anabolic–androgenic steroids such as oxymetholone and nandrolone decanoate are effective for and used in the treatment of severe anemia. High doses or levels of AAS, including testosterone, can cause polycythemia—high red blood cell and/or hemoglobin levels that increase the risk of stroke—as an adverse effect. Conversely, whether via castration, monotherapy, or, decreased erythropoiesis resulting in mild anemia is a common side effect of in men. The incidence of anemia with bicalutamide either as a monotherapy or with castration was about 7.3 to 7.5% in clinical trials, which was similar to the rate with castration of about 7.1%. A decrease of hemoglobin levels of 1 to 2 g/dL after about 6months of treatment may be observed.Greater decreases in hemoglobin levels and anemia incidences have been reported with flutamide relative to bicalutamide. Flutamide has been associated with cases of hemolytic anemia, macrocytic anemia, methemoglobinemia, sulfhemoglobinemia, leukopenia, neutropenia, and thrombocytopenia, whereas such complications may not be associated with bicalutamide.
Liver toxicity
Although rare, bicalutamide can be hepatotoxic. Symptoms may include elevated transaminases, jaundice, hepatitis, and liver failure. In the trial, in which bicalutamide monotherapy was evaluated for treatment of early prostate cancer in 8,113men, the incidence of abnormal liver function tests at 3-year median follow-up was 3.4% for bicalutamide plus standard care and 1.9% for standard care alone. However, in a phase 3 clinical trial of bicalutamide plus a GnRH agonist versus flutamide plus a GnRH agonist for metastatic prostate cancer, the rate of abnormal liver function tests was 7.5% with bicalutamide and 11.3% with flutamide. Markedly elevated liver enzymes occurred at rates of 0.5% with bicalutamide and 2.5% with flutamide in this trial, whereas rates of drug discontinuation due to elevated liver enzymes were 1.5% with bicalutamide and 2.0% with flutamide. In clinical trials, bicalutamide-induced liver changes have usually been transient and have rarely been severe. Bicalutamide was discontinued due to liver changes in clinical trials in 0.3% to 1.5% of patients, or approximately 1% overall. Aside from men with prostate cancer, liver changes have also been observed in women treated with low doses of bicalutamide for scalp hair loss. Rates of elevated liver enzymes have ranged from 2.9 to 11.4% in these studies, which spontaneously resolved in some women and necessitated discontinuation of treatment in others.No cases of liver failure or death due to liver toxicity were seen with bicalutamide in the initial clinical development programme for prostate cancer which included over 3,900men treated with bicalutamide. These trials employed bicalutamide alone and in combination with castration at doses ranging from 10 to 450mg/day. Fivecases of jaundice, including one man who died of prostate cancer, chronic renal failure, and jaundice, were recorded in the programme. Rates of jaundice with bicalutamide in the programme were similar to comparator therapies. No instances of fatal hepatotoxicity occurred with 150mg/day bicalutamide monotherapy in the substudy of the programme, in which 607men received bicalutamide. Following the initial clinical development programme of bicalutamide for prostate cancer and the programme, cases of grade 3 to 4 adverse liver changes have been reported with bicalutamide in subsequent individual trials of bicalutamide for treatment of various types of cancer.
The risk of liver changes with bicalutamide is considered to be small but significant, and monitoring of liver function is recommended. Elevation of transaminases above twice the normal range or jaundice may be an indication that bicalutamide should be discontinued. Liver changes with bicalutamide usually occur within the first 3 to 6 months of treatment, and it is recommended that liver function be monitored regularly for the first 4 months of treatment and periodically thereafter. Symptoms that may indicate liver dysfunction include nausea, vomiting, abdominal pain, fatigue, anorexia, "flu-like" symptoms, dark urine, and jaundice.
As of 2022, at least 10 case reports of bicalutamide-associated hepatotoxicity or liver failure, two of which were fatal, have been published in the literature. The dosages of bicalutamide in the cases ranged from 50 to 150 mg/day and the onsets were all within 6 months of therapy. One of the cases onset after only two doses of bicalutamide and may have been more related to prolonged prior exposure to flutamide and. Aside from published case reports, hundreds of additional cases of liver complications in people taking bicalutamide exist in the FDA Adverse Event Reporting System database. Similarly, additional cases exist in and have been described in published research for other pharmacovigilance systems, such as the Spanish pharmacovigilance system.
Liver toxicity is considered to be much more rare with bicalutamide than with flutamide, and bicalutamide is also regarded as having a lower risk than nilutamide. Rates of abnormal liver function tests have varied widely between studies, with reported ranges of 4 to 62% with flutamide and 2 to 33% with nilutamide. The risk of serious or fatal liver toxicity with flutamide has been estimated to be 3 in 10,000cases, and other studies suggest an even higher incidence. By 1996, 46 cases of severe cholestatic hepatitis associated with flutamide had been reported, with 20 of the cases resulting in death. A 2002 review reported that there were 18 reports of hepatotoxicity associated with in the medical literature, with 6 of the reported cases resulting in death. The review also cited a report of an additional 96 instances of hepatotoxicity that were attributed to, of which 33 resulted in death. However, clinically significant liver toxicity has almost exclusively been associated with high doses of in men with prostate cancer.
There is no evidence of greater liver function changes with higher doses of bicalutamide, and hence the liver toxicity of bicalutamide is not currently known to be dose-dependent across its clinically used dosage range. Older age, for a variety of reasons, appears to be an important risk factor for drug-induced hepatotoxicity. As such, the risk of liver changes with bicalutamide may be lower in younger individuals, for instance women with hirsutism and transgender women. However, it has been reported on the basis of very limited evidence that this may not be the case with flutamide.
From a theoretical standpoint, it has been suggested that flutamide, bicalutamide, and nilutamide, to varying extents, all have the potential to cause liver toxicity. However, in contrast to flutamide, hydroxyflutamide, and nilutamide, bicalutamide exhibits less or no mitochondrial toxicity and inhibition of enzymes in the electron transport chain such as respiratory complex I, and this may be the reason for its lower risk of hepatotoxicity in comparison. The activity difference may be related to the fact that flutamide, hydroxyflutamide, and nilutamide all possess a nitroaromatic group, whereas in bicalutamide, a cyano group is present in place of this nitro group, potentially reducing toxicity. A potential biological target mediating hepatotoxicity with antiandrogens, such as flutamide and cyproterone acetate, is the aryl hydrocarbon receptor.
Lung toxicity
Case reports of interstitial pneumonitis associated with bicalutamide treatment have been published in the medical literature. Hundreds of additional cases of interstitial lung disease in people taking bicalutamide exist in the FDA Adverse Event Reporting System database. Interstitial pneumonitis can progress to pulmonary fibrosis and can be fatal. Interstitial pneumonitis with bicalutamide is said to be a very rare event. The risk is much lower than that with nilutamide. In a large cohort of prostate cancer patients, the incidence of interstitial pneumonitis with was 0.77% for nilutamide, 0.04% for flutamide, and 0.01% for bicalutamide. An assessment done prior to the publication of the aforementioned study estimated the rates of pulmonary toxicity with flutamide, bicalutamide, and nilutamide as 1 case, 5 cases, and 303 cases per million, respectively. Strong safety signals of bicalutamide with interstitial lung disease have been observed in pharmacovigilance databases such as the FAERS and Japanese Adverse Drug Event Report databases. Similar safety signals have been observed for certain other antiandrogens, like nilutamide and flutamide. In addition to interstitial pneumonitis, there is a smaller number of published case reports of eosinophilic lung disease associated with bicalutamide. Side effects associated with the rare lung toxicity of bicalutamide may include dyspnea, cough, and pharyngitis.Risk of death
In men with early prostate cancer, bicalutamide has been shown to increase the likelihood of death due to causes other than prostate cancer. This was shown in the substudy of the programme, in which overall survival was significantly worse in the 150mg/day bicalutamide monotherapy group compared to the placebo/standard care group. There was also a near-significant trend toward increased overall mortality in the combined programme . At 5.4years of follow-up for the programme, the overall incidence of death was 25.2% in the bicalutamide group and 20.5% in the placebo/standard care group. This was because more bicalutamide than placebo/standard care recipients had died due to causes unrelated to prostate cancer. Bicalutamide reduced mortality due to prostate cancer, but this was not sufficient to overcome the increase in mortality due to non-prostate-cancer causes. Other trials, such as NRG/RTOG 9601, have also reported increased mortality with bicalutamide. Consequent to the programme findings, authorization of bicalutamide for the treatment of was revoked, and use of bicalutamide for this indication was discontinued. Bicalutamide continues to be authorized and used in the treatment of and, where the benefits of bicalutamide against prostate cancer outweigh any influence on non-prostate-cancer mortality.The reasons for the increased overall mortality with bicalutamide seen in the programme have not been fully elucidated. In any case, at 7.4-year follow-up, there were numerically more deaths from heart failure and gastrointestinal cancer in the bicalutamide group relative to placebo/standard care recipients. It has been said that there was no consistent pattern suggestive of drug-related toxicity for bicalutamide and that the causes were likely a consequence of androgen deprivation:
Low testosterone levels in men have been associated in epidemiological studies with cardiovascular disease as well as with a variety of other disease states. These include hypertension, hypercholesterolemia, diabetes, obesity, Alzheimer's disease, osteoporosis, and frailty. In any case, although bicalutamide monotherapy blocks the actions of androgens, it simultaneously preserves relatively high estradiol levels in men. This would potentially be expected to reduce or offset many of the risks of sex hormone deprivation. Yet increased mortality has still been seen with bicalutamide monotherapy in men in clinical trials.