The challenging role of antiandrogens in the management of polycystic ovary syndrome





Introduction (why to use antiandrogens)


Excessive androgen secretion, manifested as hirsutism, acne, and/or alopecia, constitutes one of the cardinal features in women and adolescents with polycystic ovary syndrome (PCOS) . Regardless of its severity, clinical hyperandrogenism may harm psychosocial well-being and reduce the quality of life, since it has been associated with both anxiety and depression . Therefore, lowering androgen concentrations or controlling their effect at the tissue level is a priority in the therapeutic strategy in women with PCOS. The “antiandrogens” act either as antagonists to the androgen receptor (AR) or gonadotropins or as inhibitors of the activity of 5α-reductase, the enzyme that catalyzes the transformation of testosterone to dihydrotestosterone . The available antiandrogens and their way of action are presented in Table 1 . Pharmacologic therapy with antiandrogens, although evidence-based, is used off-label. It is applied combined with other pharmacologic treatments and/or topical aesthetic therapies, alongside lifestyle modifications . Treatment should be individualized, aiming to improve quality of life and health outcomes .



Table 1

Antiandrogens in the treatment of women with PCOS.



















Antiandrogens Way of action


  • (A)

    Antiandrogenic progestins




  • Cyproterone acetate (CPA) a



  • Chlormadinone acetate (CMA) b



  • Drospirenone (DSP) b



  • Dienogest (DNG) b




  • Antagonist of the androgen receptor



  • Antigonadotropic activity



  • Inhibition of 5α-reductase activity c



  • (B)

    Spironolactone




  • Antagonist of androgen receptors



  • Inhibition of 5α-reductase activity and other enzymes involved in testosterone synthesis



  • (C)

    Flutamide/bicalutamide




  • Selective androgen receptor antagonist



  • (D)

    Finasteride/dutasteride




  • Inhibitor of 5α-reductase type II


a In an oral estrogen-progestin contraceptive or as CPA tablets.


b In an oral estrogen-progestin contraceptive.


c Only for CPA and CMA.



This chapter aims to provide a current understanding of the therapeutic role of antiandrogens in managing hyperandrogenism in women with PCOS, focusing on their way of action, efficacy, and associated adverse effects.


Antiandrogenic progestins


Combined oral contraceptives and antiandrogenic progestins


Combined oral (estrogen-progestin) contraceptives (COCs) are recommended for the treatment of clinical hyperandrogenism and/or menstrual irregularity in women and adolescents with PCOS . Various progestin preparations are contained in COCs with distinct pharmacologic characteristics and variable androgenicity ( Table 2 ). COCs containing an antiandrogenic progestin are the drugs of choice for hirsutism, alopecia, and acne . The antiandrogenic effect of COCs is achieved by suppressing the hypothalamus-pituitary-ovarian axis, as they reduce the pulse frequency of gonadotropin hormone-releasing hormone (GnRH). This mechanism inhibits the secretion of follicle-stimulating hormone (FSH) and luteinizing hormone (LH), and subsequently, ovarian androgen production . Furthermore, COCs reduce bioavailable androgen concentrations by stimulating the hepatic production of sex hormone-binding globulin (SHBG) and slightly suppress adrenal androgen secretion . Antiandrogenic progestins ( Table 2 ) exert additional antagonizing effects on the AR and inhibit 5α-reductase activity .



Table 2

Progestin preparations in COCs combined with ethinylestradiol (20–35 μg) .












































































Progestin Dose (mg) Generation Androgenicity Structural groups (derivate)
Norethindrone (NET) 0.5–1.5 1 Medium 19-Nortestosterone (Estranes)
Ethynodiol diacetate 1 1 Medium 19-Nortestosterone (Estranes)
Norgestrel (NG) 0.3 2 High 19-Nortestosterone (Gonanes)
Levonorgestrel (LNG) 0.1–0.15 2 High 19-Nortestosterone (Gonanes)
Norgestimate (NGM) 0.25 3 Low 19-Nortestosterone (Gonanes)
Gestodene 0.75 3 Low 19-Nortestosterone (Gonanes)
Desogestrel (DSG) 0.15 3 Low 19-Nortestosterone (Gonanes)
Dienogest (DNG) 2.3 4 a Antiandrogen 19-Nortestosterone (Estranes nonethinylated)
Drospirenone (DSP) 3 4 Antiandrogen Spironolactone
Chlormadinone acetate (CMA) 2 1 a Antiandrogen 17α-Hydroxyprogesterone
Cyproterone acetate (CPA) 2 1 a Antiandrogen 17α-Hydroxyprogesterone

a Not officially included in the generation categorization.



However, COC administration is associated with common adverse effects, such as headaches, mood changes, nausea, breast tenderness, which are usually palliated within the first months, and an increased risk of venous thromboembolism (VTE) . In general, the incidence of VTE associated with COC use is low [i.e., 9–10 events per 10,000 women-years of exposure for COCs containing levonorgestrel (LNG)], less than the respective in gestation, which varies between different COCs . Antiandrogenic progestins may present the highest effect on hyperandrogenism, but exert a higher risk of VTE comparing with progestins with androgenicity . A meta-analysis showed that the VTE risk for COCs containing 30-μg ethinylestradiol (EE) and antiandrogenic progestins, such as cyproterone acetate (CPA) or drospirenone (DSP), was higher compared with COCs containing LNG [pooled risk ratio (RR) 1.5–2.0]. However, there was no difference for dienogest (DNG) . In general, the use of COCs containing EE 35-μg and CPA is recommended only for cases with moderate-to-severe hirsutism or acne, since they confer a higher VTE risk compared with EE 30-μg . On the other hand, antiandrogenic progestins present a more favorable metabolic profile compared with LNG [the latter increase low-density lipoprotein cholesterol (LDL-C) concentrations by 6.8 mg/dL, p < 0.001) and decrease high-density lipoprotein cholesterol (HDL-C) concentrations by 4.4 mg/dL, p < 0.001)] .


COCs containing an antiandrogenic progestin are considered the drug of choice for clinical hyperandrogenism . A meta-analysis evaluated the effect of COCs containing similar estrogen (EE 30–35 μg) and different progestins [CPA, DSP, chlormadinone acetate (CMA), or desogestrel (DSG)] on hyperandrogenism in women with PCOS. Preparations with LNG and gestodene were excluded due to insufficient data . COC use was associated with a decline in Ferriman–Gallwey (FG) score and androgenic biochemical parameters [total (tT) and free testosterone (fT), androstenedione (Δ 4 A), and dehydroepiandrosterone sulfate (DHEAS)], as well as with an increase in SHBG concentrations . Both short-term and long-term use of all COCs decreased androgen concentrations; nevertheless, the prolonged use (6–12 months) was more effective on hirsutism and SHBG. The use of COCs containing CPA for 12 months presented the greatest impact on hirsutism . This meta-analysis confirmed that long-term treatment with COCs is needed to improve clinical hyperandrogenism (FG scores) and showed that neutral progestins could be as effective as antiandrogenic progestins in improving clinical and biochemical hyperandrogenism .


However, a network meta-analysis including hirsute women, COCs containing LNG, CPA, or DSP had similar effect on hirsutism scores . This study included women with both PCOS and non-PCOS . Moreover, a randomized-controlled trial (RCT) in women with PCOS ( n = 200) showed that COCs containing LNG had similar efficacy in clinical manifestations of hyperandrogenism after 3–6 months of therapy compared with COCs containing DSG, CPA, or DSP. However, COCs with LNG compound had a detrimental effect on lipid metabolism .


Dienogest (DNG)


DNG is a newer progestin used either as monotherapy or in combination with estrogens [EE or estradiol valerate (E 2 V)] . E 2 V/DNG was the first COC containing natural estrogen . Chemically, DNG belongs to estranes (19-nortestosterone derivatives), but it has a cyanomethyl instead of an ethinyl group at the C-17 position . As a result, DNG has fewer hepatic effects compared with other C-19 nortestosterone derivatives due to its low activity in the upregulation of mitochondrial cytochrome P450 (CYP) enzymes . Properties related to its C-19 derivative structure include its high oral bioavailability (> 90%) and short plasma half-life (~ 10 h) . DNG circulates bound to albumin by 90%, but not to other binding proteins . Regarding its receptor activities, DNG exhibits antiandrogenic activity and no glucocorticoid or estrogenic activity, in contrast to other ethylestranes. It also presents a very strong progestogenic effect on the endometrium, but no antiestrogen effect on the cardiovascular system and low gonadotropic activity . Data on DNG used alone for the treatment of endometriosis suggest a favorable safety (lipid metabolism, liver enzymes, hemostatic parameters, or thyroid gland metabolism) and tolerability profile even in a high dose (20 mg/day) . In studies conducted in women treated with COCs, the commonly reported adverse effects were comparable to other progestogens, such as headaches, nausea, mood changes, breast tenderness, and abdominal pain . In meta-analyses including COC users, DNG had a positive effect on LDL-C [− 7.7 mg/dL, p = 0.04 (data not available on other lipid parameters)] and comparable VTE risk with LNG, in contrast to the other antiandrogenic progestins [pooled RR 1.46, 95% confidence interval (CI), 0.57–5.41] .


Therefore, DNG may be considered in PCOS management due to its antiandrogenic effect, as an antagonist of the AR, and its favorable metabolic profile. In clinical practice, EE/DNG has a favorable impact on acne . The European Medicines Agency (EMA) has approved its use in the second-line treatment of moderate acne . However, there are limited clinical data concerning DNG’s efficacy in the treatment of women with PCOS. In a preliminary observational study of 36 women with PCOS and mild or moderate acne, E 2 V/DNG exerted a favorable effect on acne and SHBG concentrations after 12 months of treatment . Furthermore, this effect was also shown with EE/DNG in an RCT in women with PCOS ( n = 60), with a further decrease in fT, DHEAS, and Δ 4 A concentrations, although to a lesser extent compared with EE/DSP, but greater compared with EE/CMA . Further studies, RCTs and meta-analyses are needed to elucidate efficacy of DNG in improving hyperandrogenism in women with PCOS compared with the other antiandrogenic progestins.


Drospirenone (DSP)


DSP is a progestin, available either as a progestogen-only birth-control pill or in combination with estrogen (EE or E 2 ) . It is the only progestin whose chemical structure is similar to spironolactone, as it is a 17α-spironolactone derivative . DSP has a long half-life (~ 32 h) and oral bioavailability of ~ 76% . The vast majority (95–97%) of circulating DSP binds to albumin. Unlike other progestogens, it has neither binding affinity to SHBG nor corticosteroid-binding globulin (CBG) . DSP is extensively metabolized in the liver. There are two major metabolites in the plasma; M11, the open ring acid form and M14 (4,5 dihydro-drospirenone-3-sulfate), formed independently of the CYP450 and are pharmacologically inactive . DSP presents a moderate binding affinity to the progesterone receptor and a high binding affinity to the androgen and mineralocorticoid receptors (five times higher than that of aldosterone) . DSP progestogenic effect on the endometrium is relatively weak compared with other progestins . Owing to its high antimineralocorticoid property, DSP blocks aldosterone action in the kidneys and causes decreased sodium and water retention compared with other conventional progestins . As a result, DSP may additionally exert a mild antihypertensive effect .


EE/DSP has been used to treat moderate acne, premenstrual syndrome, premenstrual dysphoric disorder, and dysmenorrhea . However, COCs containing DSP are used off-label in women with PCOS, as DSP has a considerable antiandrogenic effect (~ 30% of CPA in in vivo rat models) by blocking testosterone binding to ARs and antigonadotropic activity . Furthermore, DSP does not bind to SHBG, and it does not increase fT . A meta-analysis showed a reduction in FG score in PCOS women with the EE/DSP (30 μg/3 mg) formulation, either after 6 [− 2.57 (− 3.94, − 1.20)] or 12 months of treatment [− 2.15 (− 3.05, − 1.24)] . Though CPA is considered a more potent antiandrogen, a meta-analysis including women with PCOS showed that the impact on clinical [FG score, body mass index (BMI)] and hormonal outcomes [(tT, SHBG, DHEAS, and free androgen index (FAI)] did not differ between DSP and CPA . No significant difference in these outcomes was found between DSP and DSG, a progestin with low androgenicity . Nonetheless, DSP exerts a more favorable effect on lipid and glucose metabolism compared with CPA, as it lowers total cholesterol (TC) concentrations and homeostatic model assessment for insulin resistance (HOMA-IR) index to a greater extent. It is also characterized by a more pronounced effect on HDL-C and LDL-C concentrations compared with DSG .


In addition, in another meta-analysis of patients with PCOS, COCs containing DSP reduced FG score after 6 months and Δ 4 A and tT concentrations after 3 months, to a greater extent compared with COCs antiandrogenic progestin CMA . On the other hand, EE/DSP monotherapy was more efficacious compared with metformin on biochemical hyperandrogenism (tT, FAI, and SHBG), whereas metformin showed a favorable metabolic profile [BMI, TC, LDL-C, and triglycerides (TGs)]. Moreover, the combination of EE/DSP with metformin was shown to be more effective in reducing BMI and LDL-C and LH concentrations compared with the use of EE/DSP alone .


The EE (20 or 30 μg)/DSP (3 mg) preparations are well-tolerated and present mostly nonspecific, mild-to-moderate, adverse events that do not require further intervention . However, DSP may potentially increase the risk of hyperkalemia, as DSP 3 mg is equivalent to a 25-mg dose of spironolactone . Although this adverse effect has not been proven in clinical practice, except for high-risk patients, package labeling recommends potassium monitoring in the first month for women under additional medications, which predispose to hyperkalemia and against DSP use in women with renal and adrenal insufficiency . In addition, DSP prescription is contraindicated in women with hepatic disease, as DSP is extensively metabolized in the liver . Regarding metabolic parameters, a meta-analysis showed that COCs containing DSP were associated with an increase in TG (32.0 mg/dL; 95% CI, 17.5 to 44.6) and HDL-C (9.26 mg/dL, 95% CI, 4.84 to 13.7), without any effect on LDL-C (3.44 mg/dL, 95% CI -4.29 to 11.2) concentrations, as well as BMI, insulin resistance or glycemia in women with PCOS . Furthermore, COCs containing DSP present higher VTE risk compared with those containing LNG (pooled RR 1.58, 95% CI 1.12–2.14), as shown in another meta-analysis .


In conclusion, DSP is an effective antiandrogenic progestin, with a relatively favorable or neutral profile, concerning the long-term cardiovascular and metabolic aspects of PCOS and higher antimineralocorticoid capacity compared with other progestins contained in COCs . In cases of increased VTE risk or contraindication to estrogens, DSP only pill may be an option, because it does not affect hemostatic mechanisms and presents no estrogenic action .


Cyproterone acetate (CPA)


CPA is the progestin with the highest antiandrogenic activity and is used to treat various androgen-dependent conditions . It is available either as a COC (1–2 mg CPA) in combination with EE and E 2 V or as monotherapy (at daily doses of 10 mg, 50 mg or 100 mg) or as a solution for injection (300 mg/3 mL) . After oral administration, the bioavailability of CPA is nearly 100% . It circulates bound to albumin by 93% and presents no binding affinity to SHBG and CBG . Since there is no binding of CPA to SHBG or CBG in the serum, 93% of the compound is bound to albumin . A single oral dose of 2 mg/day leads to peak serum concentrations of about 11 ng/mL, with half-lives of 2–8 h (t1/2a) and 60 h (t1/2b) . The major metabolic steps are hydroxylation and deacetylation. The metabolite 15b-hydroxy-CPA has an antiandrogenic activity similar to that of CPA, but only 10% of its progestogenic effect .


CPA is a highly potent progestogen (90% binding affinity for the progesterone receptor) and a moderately potent antiandrogen (6–21% binding affinity for the androgen). It also exhibits antigonadotropic, antiestrogenic, and glucocorticoid properties . The antiandrogenic effect of CPA results from its competitive inhibition of the binding of endogenous androgens to the AR and is dose-dependent . In addition, CMA blocks testosterone’s conversion to the more potent androgen, 5α-dihydrotestosterone (by inhibiting 5α-reductase in the skin) and reduces androgen production in the ovary . As it presents no binding affinity to SHBG, CPA does not affect fT .


EE (35 μg)/CPA (2 mg) has been widely used in the management of hyperandrogenism in women with PCOS . In a meta-analysis which evaluated the effect of COCs in women with PCOS, both short-term (3 months) and long-term (6–12 months) use of EE/CPA was associated with a decline in FG score [− 1.22, (96% CI − 1.62 to − 0.81) and − 7.96 (95% CI −8.65 to − 7.27) after 3 and 12 months, respectively]. EE/CPA also decreases androgen (tT, fT, and Δ 4 A) and increases SHBG concentrations at 3 and 12 months of continuous use . The greatest effect on hirsutism by EE/CPA was evident after 12 months of treatment [− 7.96 (95% CI − 8.65 to 7.27)] . EE/CPA may also improve co-existing acne and seborrhea in women with PCOS . However, after treatment cessation, it must be underlined that the antiandrogenic effect seems to vanish in a few months, indicating the need for long-term therapy .


EE/CPA use is generally well-tolerated with a safety profile similar to other COCs . However, it is contraindicated in women with a history of meningioma . From a metabolic point of view, the EE/CPA may negatively affect lipid metabolism, increasing TG concentrations . A meta-analysis of studies in premenopausal women with PCOS showed that EE/CPA increase plasma TG and HDL-C concentrations by 25.1 mg/dL (95% CI 13.8–36.4) and 6.09 mg/dL (95% CI 1.91–10.3), respectively . The effect of CPA on glucose homeostasis (fasting plasma glucose, HOMA-IR) and BMI is negligible . Nonetheless, EE/CPA use has been associated with increased VTE risk [pooled RR 2.04 (95% CI 1.55–2.49)] compared with LNG . Thus, its use is recommended only when treating moderate to severe hirsutism or acne .


Higher CPA dosages as monotherapy have also been used cyclically, in combination with a COC or estrogens, to treat hyperandrogenic states . CPA tablets are used internationally, but they are not available in the USA . The recommended dose of CPA is 50–100 mg/day for 10 days/cycle for the management of hirsutism . However, few pooled data about the use of CPA alone in treating women with PCOS are included in this context. In a Cochrane meta-analysis, no differences were found in FG score or serum androgen (tT, fT, Δ 4 A, and DHEAS) concentrations at 6 months between EE/CPA and CPA (at daily doses of 25–100 mg) in hirsute women with PCOS . Only one study on this concept was included, with a relatively small sample size ( n = 113) . Moreover, no clinical differences on hirsutism (except from FG score at 12 months favoring CPA) were observed when CPA was compared with other antiandrogens (spironolactone, flutamide, and finasteride), as well as GnRH-analogs in hirsute women with or without PCOS . A network meta-analysis on the treatment options for hirsutism in women (PCOS and non-PCOS) showed that the combination of a COC with CPA was equally effective compared with COC monotherapy [− 0.49 (− 1.41 to 0.43)], but the certainty of comparisons was low . CPA (50–100 mg/day) may also be beneficial in treating female pattern hair loss .


Adverse effects of higher doses (> 10 mg) of CPA include liver toxicity, irregular menstrual bleeding, nausea, decreased libido and mood, liver tumors and meningiomas . Furthermore, the CPA may increase the risk of undervirilization of male fetuses at higher doses, as proved in animal models . EMA’s safety committee has recommended that CPA daily doses of ≥ 10 mg should only be used for androgen-dependent conditions, when other treatment options (e.g., EE/CPA 2 mg) have failed. Furthermore, the dose should be gradually reduced to the lowest effective one, because of the increased risk for meningiomas, reported primarily at doses of ≥ 25 mg/day. In clinical practice, patients should be monitored for clinical signs and symptoms of meningioma .


Chlormadinone acetate (CMA)


CMA is a 17-acetoxyprogesterone derivative usually administered in combination with EE in a COC tablet (EE 30 μg/CMA 2 mg) to manage clinical hyperandrogenism in women with PCOS . It is also available as menopausal hormone therapy combined with estradiol . CMA use as a contraceptive pill has been licensed in over 40 countries , but it is not internationally available (e.g., in the USA). After oral administration, CMA bioavailability is almost 100%. It is stored in fatty tissues, but can also accumulate in the endometrium, myometrium, cervix, and fallopian tubes. Therefore, the clearance is relatively slow . CMA circulates bound to albumin (97–99%), with no binding affinity to SHBG and CBG. Its half-life is approximately 34–39 h. The main metabolites of CMA are 2α-, 3α-, and 3β-hydroxy derivatives, with the latter having 70% of the antiandrogenic action of CMA .


Regarding its receptor activities, CMA has a strong progestogenic effect (about one-third higher compared with that of progesterone), slight glucocorticoid activity, antiestrogenic activity, potent antiandrogenic and antigonadotropic effects, but no antimineralocorticoid activity . CMA has a good affinity for the AR at doses ≥ 0.5 mg, but lower than that of CPA, and blocks testosterone binding to ARs . Moreover, CMA inhibits (via competition) the conversion of testosterone to the more potent androgen, 5α-dihydrotestosterone, by skin 5α-reductase in sebaceous glands and hair follicles. CMA also has antigonadotropic activity, suppressing androgen production, without binding to SHBG . The in-vitro antiandrogenic activity of CMA is similar to CPA, at 10 − 8 M concentrations. At higher doses, both CMA and CPA demonstrate partial agonist activity instead of antagonistic effect .


EE/CMA (30 μg/2 mg) is generally well-tolerated, with adverse effects similar to the other low-dose COCs, with a low incidence of VTE (3.4 per 10,000 women-years for adolescents, 2.1 per 100,000 women-years for adults) . Like other COCs, it affects lipid metabolism. In a 2020 meta-analysis, CMA has been associated with the greatest increase in TG [56.7 mg/dL (95% CI 17.6–95.8)] and HDL-C [8.90 mg/dL (95% CI 3.22–14.6)] concentrations. No effect on BMI or glucose metabolism has been observed . At doses of CMA 2–4 mg/day, the body’s temperature may increase by 0.2–0.5 °C . CMA’s antiandrogenic properties may favor the use of EE/CMA for the treatment of hyperandrogenic conditions . In clinical studies, EE/CMA was effective in treating moderate acne and seborrhea . In women with PCOS, EE/CMA use was also associated with improvement in biochemical hyperandrogenism, but the effect on hirsutism was evident only after 6 months of treatment (nonsignificant results were seen after 3 or 12 months) . Furthermore, COCs containing CMA are less effective in the reduction of FG score and androgen (Δ 4 A and tT) concentrations, compared with COCs containing DSP .


Spironolactone


Spironolactone is synthetic aldosterone and androgen antagonist, structurally related to progestins . It is mainly used as a diuretic drug, and off-label, to treat androgen-mediated cutaneous disorders . Spironolactone is available as oral tablets, with a bioavailability of 60–90% and a short plasma half-life of 1–1.5 h . It undergoes extensive first-pass metabolism from the liver, acting as an inducer of CYP isoforms . Its active metabolites (7α-thiomethyl-spironolactone and canrenone) are responsible for most of its pharmacodynamics . Spironolactone binds to the mineralocorticoid receptor and results in a potassium-sparing diuretic effect in the kidney due to its antagonizing effect to the aldosterone receptor . It also binds with moderate affinity to androgen and progesterone receptors . Additionally to the competitive inhibition of androgen receptors, spironolactone increases SHBG and inhibits 5α-reductase activity and enzymes involved in testosterone synthesis .


Spironolactone is generally well-tolerated . Its dose-related antiandrogenic adverse effects include menstrual irregularities (minimized by concurrent COC use), breast tenderness, and decreased libido. Its mineralocorticoid adverse effects include diuresis, headache, and dizziness . In general, because of its diuretic effect, it is associated with an increased risk of hyperkalemia. Therefore, regular potassium monitoring is suggested . However in healthy young women with acne, the risk of clinically significant hyperkalemia has not been proven . Blood pressure and signs of hypotension should be monitored during spironolactone treatment . Moreover, due to the potential for male fetuses’ inadequate masculinization, spironolactone should be combined with contraception in women of reproductive age . The potential of a carcinogenic adverse effect seen in animal studies (increased risk of breast, uterine, cervical or ovarian cancer) has not been proven in human studies . Spironolactone is contraindicated in hyperkalemia, renal and adrenal insufficiency, concurrent use of potassium supplements or potassium-sparing diuretics .


In women with PCOS, spironolactone constitutes a second-line therapy combined with COC to treat hirsutism, following 6 months of therapy with COC and cosmetic means without adequate response. It is promoted to first-line treatment in cases of contraindication or poor tolerance of COCs . The antiandrogenic effect of spironolactone is thought to be dose-dependent, although there are no rigorous data . The starting dose is 25 mg/day in adolescent girls and 50 mg/day in adults . Doses may be increased as needed and range between 100 and 200 mg/day, divided into two doses . Spironolactone efficacy in treating hirsutism, as monotherapy or in combination with other therapies (COC or metformin) has been highlighted by studies in women with PCOS . Combination of COC (norgestimate-ethinyl estradiol) with spironolactone was more effective compared with COC monotherapy in improving hirsutism . Furthermore, spironolactone monotherapy at low doses (25–50 mg/day) improved menstrual irregularity and insulin resistance indices . Compared with metformin therapy alone, it is more effective in improving hirsutism . The addition of low-dose (25–50 mg/day) spironolactone to metformin reduces androgen concentrations and improves insulin sensitivity to a greater extent compared with metformin monotherapy . However, in a small RCT ( n = 37), including nonobese women, spironolactone (100 mg/day) monotherapy was as effective as combination with metformin in terms of BMI, FG score, androgen concentrations, and insulin resistance indices . Intermenstrual vaginal bleeding due to spironolactone was an important shortcoming in both groups . In a Cochrane review regarding hirsutism treatment, spironolactone 100 mg/day was effective and well tolerated, albeit the evidence was of low quality, and the analysis included both patients with PCOS and non-PCOS . Furthermore, a network meta-analysis including studies conducted in hirsute women with or without PCOS, showed antiandrogen monotherapy, either with flutamide, finasteride, or spironolactone, is superior to placebo in improving hirsutism scores, but of similar efficacy was shown among different compounds . The result was not significant for combining spironolactone with COC or metformin versus monotherapy . However, the certainty in comparisons with placebo was moderate, and for head-to-head comparisons was low. Except for hirsutism, spironolactone has been used to treat acne and androgen-dependent alopecia in women with PCOS, but the evidence on its efficacy is limited .


Flutamide and bicalutamide


Flutamide is a potent nonsteroidal antiandrogen used primarily to treat prostate cancer, and off-label, for the treatment of androgen-dependent skin disorders in women . After oral administration, flutamide is absorbed from the gastrointestinal tract and undergoes extensive first-pass metabolism in the liver . Its major metabolites are 2-hydroxyflutamide (active metabolite) and the hydrolysis product 3-trifluoromethyl-4-nitroaniline, demonstrating a half-life of 4.3–21.9 h after a single dose of flutamide 250 mg . Flutamide’s antiandrogen effect is accomplished by a dose-response inhibition of ARs . Contrary to spironolactone and CPA, flutamide does not interact with estrogen, glucocorticoid, or progesterone receptors .


In women, flutamide has been used both at high (250–500 mg/day) and low doses (62.5–125 mg/day) with similar efficacy and fewer adverse effects with the latter doses . Most data come from studies in hirsutism (idiosyncratic or PCOS) treatment; the evidence was moderate-to-low quality, especially for the lower doses . In pooled analyses, flutamide 250 mg two times daily or 500 mg one time daily was more effective in improving hirsutism compared with placebo. Those analyses included women with or without PCOS; the quality of comparisons was not high .


Flutamide is relatively well-tolerated. The most common adverse effects are dry skin, gastrointestinal disorders, and headache . However, it is rarely used because of its hepatotoxicity and high cost . In most cases, hepatotoxicity occurs early after treatment initiation as an increase in transaminase concentrations, without further clinical impact. However, cases of fatal or fulminant hepatitis have been described . Although long-term use of low flutamide doses in young women with hyperandrogenemia is regarded as well tolerated , there are reports of hepatotoxicity even with ultra-low doses . In some cases, hepatotoxicity was life-threatening . In women treated with flutamide, liver tests are necessary before treatment and regularly after that . Treatment should be ceased in case of transaminasemia. Owing to the potential risk of undervirilization of a male fetus, flutamide should be combined with contraception .


Flutamide may be considered as second-line therapy in treating clinical hyperandrogenism in women with PCOS, in case of COC contraindication, or added to COC therapy after a minimum of 6 months without improvement . Its efficacy as a monotherapy or in combination with metformin or COC has been evaluated in women with PCOS. Flutamide monotherapy was effective in improving hyperandrogenism and lipid profile in nonobese (250 mg/day) and obese (500 mg/day) women, but it did not improve menstrual irregularities . Furthermore, flutamide monotherapy was beneficial to insulin sensitivity in nonobese women . Combination therapy of flutamide with metformin (1275–1700 mg/day) had a synergistic effect in increasing HDL-C and SHBG concentrations compared with flutamide monotherapy . Additionally, in young women with PCOS, flutamide (62.5 mg/day) combined with metformin (850 mg/day) plus either a DSP-containing or a transdermal COC had further metabolic, anti-inflammatory and adiposity-reducing benefits . However, these studies were of small sample size, and their results should be interpreted with caution. In a network meta-analysis, including women with or without PCOS, its efficacy on hirsutism was comparable to spironolactone and finasteride (low-certainty of comparison) . Flutamide may be effective on acne and androgen-dependent alopecia, but data in women with PCOS are limited .


Bicalutamide is a selective androgen-receptor antagonist similar to flutamide, widely used to treat prostate cancer . It does not have the risk of hepatotoxicity seen with flutamide; thus, it could be an alternative for managing women with androgen-dependent skin manifestations . Nonetheless, there is scarce data about its utilization in women, as its tolerability and pharmacokinetics have been assessed in patients with prostatic carcinoma . Bicalutamide’s efficacy in women with PCOS and severe hirsutism has been evaluated in phase III, randomized, double-blind, controlled study; its combination with a COC at a dose of 50 mg/day was well-tolerated and more effective compared with COC monotherapy in treating severe hirsutism after 12 months of treatment .


Finasteride and dutasteride


Finasteride is a synthetic steroidal antiandrogen, used in the treatment of benign prostatic hypertrophy and male androgenetic alopecia, and off-label, in the treatment of hirsutism and female pattern hair loss in women . It is a competitive inhibitor of 5-alpha-reductase type II, an enzyme that catalyzes testosterone conversion to dihydrotestosterone in the reproductive tissues, skin (hair follicle root sheath), and liver . It is available as an oral tablet or a topical gel . After oral administration, the bioavailability of finasteride is 80% with a mean plasma half-life of 5–7 h . Slow accumulation occurs with multiple doses: serum dihydrotestosterone concentrations are suppressed for up to 4 days after a single dose . Finasteride is extensively metabolized through oxidative pathways in the liver. Its major metabolites show an inhibitory potency on 5α-reductase of < 20% compared with finasteride . Finasteride in women is well-tolerated; usual adverse events include decreased libido, headache, gastrointestinal discomfort, menstrual disturbances, acne, and dizziness . Because of to the increased risk of congenital disabilities in male fetuses, finasteride should be combined with COCs .


In PCOS, finasteride is considered a second-line therapy, added to a COC, to manage clinical hyperandrogenism (hirsutism and alopecia) . In clinical studies, including women with PCOS or androgen-dependent skin manifestations, oral finasteride doses ranged from 0.5 to 5 mg/day . Finasteride was usually administered continuously for 6–12 months . Intermittent (every 3 days) low-dose (2.5 mg/day) finasteride was effective for the treatment of hirsutism, idiosyncratic or secondary to PCOS, in women and adolescents, but the evidence comes from two small RCTs . At doses of 2.5–5 mg/day and 5–7.5 mg/day, finasteride was more effective compared with placebo in improving hirsutism in women with or without PCOS (low-to-moderate quality data) . According to a network meta-analysis, finasteride has comparable efficacy with flutamide and spironolactone in improving hirsutism in women (low certainty of comparison) . In this regard, the combination of finasteride with spironolactone or EE/CPA was more effective compared with monotherapy . Finasteride may mitigate female pattern hair loss (low-quality evidence) . Topical finasteride gel (0.25%–0.5%) may positively impact hirsutism and alopecia, but further research is needed .


The evidence from studies conducted on women with PCOS is limited. In an RCT comparing finasteride (5 mg/day) with metformin (1700 mg/day) or their combination in women with PCOS, finasteride monotherapy (5 mg/day) was effective in the treatment of hyperandrogenism and in improving insulin resistance after 12 months. Metformin monotherapy was not inferior to finasteride in reducing hyperandrogenemia and FG score. Their combination did not present additional benefit . However, the study was small and menstrual irregularities were not assessed . In another RCT, including hyperandrogenic anovulatory women with PCOS in which previous protocols with gonadotropin failed, administration of finasteride improved the ovulation rate during ovarian stimulation with recombinant FSH .


Dutasteride is a selective 5α-reductase type I and II inhibitor . It is a more potent inhibitor of 5α-reductase compared with finasteride, reducing plasma dihydrotestosterone concentrations by 90% and concomitantly raising plasma testosterone concentrations by 25% . It is indicated for benign prostatic hyperplasia treatment and is used, off-label, to treat female pattern hair loss (0.25–0.5 mg/day) . Although dutasteride may be a promising drug as a more potent antiandrogen compared with finasteride, there are scarce data regarding its use in women .


Topical antiandrogens


Topical antiandrogens may be a therapeutic choice for androgen-related skin disorders wishing to avoid systemic adverse effects . Topical finasteride gel (0.25%–0.5%) showed inconsistent efficacy in improving idiopathic hirsutism . There are promising results about its efficacy and safety regarding androgenic alopecia, but the studies include mostly male participants . Creams containing spironolactone 5% have been used with reported efficacy in mild-to-moderate acne , without benefit in hirsutism . Topical clascoterone cream 1% (cortexolone 17α-propionate) is a novel topical androgen-receptor inhibitor demonstrating safety and efficacy in reducing acne lesions in phase III trials . Concerning the management of hirsutism in women with PCOS, there are no recommendations for the use of topical antiandrogens .


Combination therapy


Antiandrogens are a second-line treatment for cutaneous disorders related to PCOS. They can be added to a COC, when a minimum of 6 months of therapy and cosmetic means did not achieve the desired response . In PCOS, antiandrogens have been combined with COC and/or insulin sensitizers . In a meta-analysis, no differences were found between COC plus antiandrogens and COC monotherapy, in terms of weight, FG score, FAI, tT, SHBG, fasting insulin, fasting glucose, TC, HDL C, TG, HOMA-IR, and C-reactive protein concentrations; the only differences were an improvement in BMI and a reduction in LDL-C favoring COC monotherapy (low to very-low certainty of comparisons) . When metformin plus diet versus metformin plus diet plus antiandrogen were compared, an improvement was found only in tT and fasting glucose concentrations, favoring the latter. No differences were found for weight, BMI, menstrual cyclicity, hirsutism, SHBG, FAI, fasting insulin, HOMA-IR, TC, HDL C, LDL-C, and TG (very-low certainty of comparisons) . In another meta-analysis, including women with PCOS, antiandrogens with or without COC were more effective in improving hirsutism compared with metformin monotherapy (− 2.04, 96% CI − 4.02 to − 0.07, low-quality evidence) . As mentioned above, in a network meta-analysis, including hirsute women with or without PCOS, COCs plus antiandrogen were superior to COC monotherapy in improving hirsutism scores (− 0.46, 95% CI − 0.91 to − 0.01)] . Furthermore, antiandrogen monotherapy, COC plus antiandrogen, and antiandrogen plus insulin sensitizer were superior to insulin sensitizer monotherapy (low-to-moderate quality data).


Personalized medicine


When and in whom to start an antiandrogen?


In general, the therapeutic approach to a woman with PCOS should be individualized, considering the patient’s medical history, demographic characteristics (e.g., age and BMI), family history, metabolic profile, malignancy potential, symptomatology (e.g., degree of hirsutism, other signs of hyperandrogenism, and oligo/amenorrhea), and pregnancy desire. An antiandrogen may be considered in cases of moderate-to-severe hirsutism with a negative impact on psychosocial well-being and no response to topical/cosmetic treatment (e.g., electrolysis, laser therapy, and eflornithine cream). When clinical hyperandrogenism co-exists with oligo/amenorrhea, COCs containing an antiandrogenic progestin, such as DSP, CPA, CMA, or DNG, constitute the treatment of choice. In more severe cases, it is prudent to add an antiandrogen (e.g., CPA for 10 days/cycle or continuous use of spironolactone or flutamide) to a COC . Antiandrogens should be added to a COC for the treatment of hirsutism after a minimum of 6 months of therapy with a COC and when cosmetic intervention did not achieve adequate response or in cases of androgen-related alopecia .


In cases of contraindications to COCs, antiandrogen monotherapy may be considered, provided effective contraception is ensured due to its potentially teratogenic action. Such contraindications include < 6 weeks postpartum if breastfeeding, smoking in women > 35 years old, uncontrolled arterial hypertension, history of VTE, prolonged immobilization after surgery, known thrombogenic mutations, established cardiovascular disease, systemic lupus erythematosus, migraine with focal neurological symptoms, breast cancer, diabetic microvascular and macrovascular complications, and liver disease .


Which antiandrogen is suitable for a specific patient?


The selection of the most appropriate antiandrogen should be based on the severity of hirsutism, its cost-effectiveness and adverse effects, and the individual’s distinct clinical and metabolic characteristics . Since no superiority of high over low antiandrogen doses has been proven, the lowest effective dose is recommended to avoid dose-related adverse effects and reduce costs . However, specific antiandrogen types or doses cannot be recommended due to inadequate evidence in women with PCOS .


Considering the data mentioned above, in cases of metabolic disorders, such as dyslipidemia, obesity, and increased insulin resistance, DSP is preferred to CPA. The addition of metformin to EE/DSP is more beneficial compared with the use of EE/DSP alone . On the other hand, DSP and CPA should not be considered in renal or adrenal insufficiency, liver disease, and increased VTE risk. In the latter cases, especially in moderate clinical hyperandrogenism (hirsutism, acne, and seborrhea), CMA may be preferred to DSP and CPA .


In cases of hirsutism and contraindication or intolerance to COCs, either spironolactone, flutamide, or finasteride may be considered. Contraindications to spironolactone include hyperkalemia, renal and adrenal insufficiency, concurrent use of potassium supplements or potassium-spsaring diuretics. Liver disease is a contraindication to flutamide. In acne or androgen-dependent alopecia cases, spironolactone is preferred to flutamide due to lack of evidence regarding the efficacy of the latter. Finasteride, either per os or topically, can be considered in male and female pattern hair loss. Effective contraception in sexually active women is a prerequisite for monotherapy with spironolactone, flutamide, and finasteride .


Data regarding the antiandrogen therapy in adolescents with PCOS are limited. Antiandrogens may be considered in cases of severe clinical hyperandrogenemia, not successfully managed with COCs . Evidence exists mostly for spironolactone, [especially for the triple combination of spironolactone (50 mg/day)/pioglitazone (7.5 mg/day)/metformin (850 mg/day)], and flutamide . Regarding the former, it is beneficial for ovulation rates and metabolic profile, whereas the latter, at the dose of 250 mg/day, is efficacious in clinical and biochemical hyperandrogenemia, with no impact on menstrual disturbances .


When to stop an antiandrogen?


In general, the decision to stop an antiandrogen should be individualized, based on the response to therapy, adverse effects, and pregnancy potential. No RCTs exist concerning the optimal duration and time of cessation as the primary endpoint. Although improvement in both hirsutism and acne is observed within 3–6 months of treatment, a longer period (9–12 months) is often required for achieving the maximum benefit . This is the case especially for CPA, which exerts its greatest effect on hirsutism at 12 months of treatment . An RCT comparing the clinical efficacy of COCs containing DSG, CPA, and DSP, showed that the greatest efficacy in treating hirsutism achieved a pill containing CPA after 12 months of treatment. There was no difference among groups at 6 months .


Except for adverse effects necessitating antiandrogen cessation, there is no consensus on the optimal time for this decision. Regarding CPA, its daily dose can be gradually decreased to the lowest effective one after 6–12 months to reduce the risk of meningiomas. Clinicians should be aware that after treatment discontinuation, the antiandrogenic effect vanishes in a few months .


Conclusions


Antiandrogens constitute an effective choice in the therapeutic armamentarium for clinical hyperandrogenism in women with PCOS. Their use should be well-balanced after considering their efficacy and adverse effects, based on the patient’s clinical and metabolic characteristics, and desire for pregnancy. Combination of an antiandrogenic progestin (DSP, CPA, CMA, and DNG) with EE in a COC is the first-line therapy in moderate-to-severe cases of hirsutism, especially when oligo/amenorrhea co-exists. After 6–12 months of continuous use without clinical signs of improvement, the addition of an antiandrogen to COCs may be considered. Theoretically, this may include any of the agents mentioned above (CPA, spironolactone, flutamide, and finasteride) after considering their pros and cons. Antiandrogen monotherapy can be proposed in cases of contraindication or intolerance to COCs, provided that contraception with other means is ensured because of antiandrogens’ teratogenic effect. Further research is needed to elucidate issues, such as antiandrogens’ comparative efficacy as monotherapy, the optimal duration of use, and safety in adolescents with PCOS.


Conflicts of interest


The authors have no conflicts of interest.



References

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Nov 27, 2021 | Posted by in GYNECOLOGY | Comments Off on The challenging role of antiandrogens in the management of polycystic ovary syndrome

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