About 5–10% of pre-menopausal women are affected by Polycystic Ovary Syndrome (PCOS) [1,2,3,4] and its treatment could be very long, but always symptom-oriented, and also dynamic and adapted to the changing circumstances and personal needs of the individual patient. Ovarian dysfunction causes metabolic disorders and hyperandrogenism; these should be counteracted by all therapeutic approaches usually used in the management of PCOS [4].

In addition to pharmacological molecules, to improve the metabolic status of women with PCOS, it is highly recommended to suggest a modification of the lifestyle and weight reduction. The goal of all these interventions is the improving of ovulation regularity and the protection against cardiovascular diseases. The clinical treatment of PCOS is often a long-term therapy, and the most commonly used drugs are combined oral contraceptives (COCs), antiandrogenic progestins, and insulin-sensitizing drugs. Anyway, these drugs could treat the respective single sign of PCOS [5].

Because of the length of the therapy that can last for the whole fertile period of a woman and, therefore, could interfere with a hypothetical pregnancy, also botanicals have been considered against PCOS. In particular, berberine (BBR) is an alkaloid plant extract widely used in Chinese Herbal Medicine against infections, hypercholesterolemia, Diabetes type 2 and cancer [6].

Berberine is also shown to be effective against insulin resistance and obesity, particularly against visceral adipose tissue in vitro and in murine models [2, 7, 8].

Berberine is a very promising botanical compound because of the few minor side effects that could present and because its target is an AMP-activated protein kinase (AMPK) common to fatty acid oxidation, glucose generation and insulin resistance [9]. Zhang et al. explained the berberine mechanism of action and after that, scientists began to hypothesize and therefore to use berberine in clinical management of dyslipidemia, diabetes type 2 and obesity in order to counteract the cardiovascular risk derived from these metabolic disorders [9,10,11,12]. Moreover, thanks to the extreme tolerance and very minor side effects on long-term treatment, the berberine is the only botanical compound included in European guidelines for the management of dyslipidemia and it is used also in patients who do not tolerate statins [13,14,15].

Berberine, if associated with a healthy lifestyle, improves women’s body composition and causes androgen’s reduction as pointed out by Saleem et al. [3, 8].

PCOS is an endocrine–metabolic disorder very similar to the metabolic syndrome, indeed they have a common factor: insulin resistance. Ong et al. [6] explained that insuline resistance is the key factor that could cause obesity and anovulatory cycles and actually, that should be the target of therapeutic molecules against PCOS and also Metabolic Syndrome [2, 6].

Botanical compounds are always used in traditional Chinese medicine; among those, the berberine induces an amelioration of insulin resistance if administered at a dose of 500 mg per os twice a day for 6 months, and also improves the regularity of menstrual cycle [6].

Berberine is not only used in China, but also is being administered by English medical doctors dealing with women affected by PCOS to counteract PCOS’ symptoms and signs [16]. Rooney and Pendry in their survey among English clinicians pointed out the lack of scientific literature regarding the use of herbal medicine and consequently, the lack of uniformity in herbal prescription against PCOS [16].

Given this background, the aim of the present narrative review was to assess the state of the art about the use of berberine in the management of PCOS.


This narrative review was written after a PubMed and SCOPUS research performed with these keywords: “Berberine”, “PCOS” with the use of Boolean AND operator to establish the logical relation between them (Fig. 1). The research was conducted by skilled operators from July to September 2018 and following Egger’s criteria for systematic reviews [17, 18]. The research was time limited (from 2000 to 2018) and restricted for Human AND/OR Humans studies to know about the state of the art of the use of berberine in women affected by PCOS diagnosed by Rotterdam criteria.

Fig. 1
figure 1

Flow chart of literature research


Only five full-text papers were taken in analysis, and all of them mentioned the possible use of berberine in non-pharmacological treatment of the endocrine disorder. The results of these five studies have been shown in Table 1.

Table 1 Trials conducted on the effect of berberine on PCOS-premenopausal women

All studies conducted compared berberine with other PCOS pharmacological therapies such as combined oral contraceptives, anti-androgen drugs, metformin and monacolins to counteract cardiac risk in PCOS [19,20,21,22,23,24].

Authors found that berberine induced a redistribution of adipose tissue, reducing visceral fat mass even in the absence of weight loss, and insulin sensitivity was improved similar to metformin [19, 22]. The nutraceutical compound also improved the lipid pattern in subjects with PCOS against monacolins [21]. Berberine in women with PCOS also improved the insulin resistance in theca cells, thanks to an increase of the expression of Glut-4 in ovaries with an improvement of the ovulation rate per cycle; so, berberine is also effective on fertility and live birth rates in women affected by PCOS [23, 24].

Berberine is safe to use in premenopausal women who want to become pregnant and showed few side effects in all the cited studies, in particular constipation and nausea [23, 24]. Regarding specifically side effects, 3 out of 31 subjects (BBR group) complained of a bitter taste in their mouth versus 9 out of 30 subjects (MET group) suffered by nausea, vomiting, mild diarrhea and flatulence [19]. No adverse events were observed by Cicero et al. [21] and Orio et al. [25], while An et al. reported 1/50 subject (BBR group) transient gastrointestinal side effects including diarrhea vs. 2/50 subjects (Met group) gastrointestinal side effects including diarrhea [22]. Wu et al. reported that 1 subject out of 214 subject (BBR group) had constipation and nausea, no fetal abnormalities in BBR group versus 1 fetal abnormality in letrozole group resulting in termination of pregnancy [24]. All these observed side effects were transient and mild, underlining the good safety of the use of BBR in PCOS patients.

The five studies analyzed showed some differences in the design of the study and in the results; in particular, Wei et al. An et al. and Wu et al. performed their research comparing BBR vs. ethynyl estradiol + cyproterone acetate/ metformin/letrozole, respectively (see details in Table 1). Studies have not been conducted comparing berberine with a real placebo, perhaps because of the studied target population: women of child-bearing age, so it would be probably unethical the administration of real placebo [19, 22, 24]. Only An and colleagues used a real placebo but the placebo group also underwent to ovarian stimulation like the interventions groups to become pregnant [22].

Women enrolled by Wei et al. and An et al. received lifestyle and nutritional counseling before the treatment with berberine, metformin or placebo [19, 22]; while in the study conducted by Orio et al., no lifestyle modifications were implemented [25] in spite of the fact that a good lifestyle has been demonstrated to be crucial to the amelioration of symptoms related to PCOS [3]. Only Cicero et al. before the beginning of the study gave a three-month lipid-lowering diet to enrolled women [21].

Only Wei et al. pointed out a statistically significant reduction of the waist circumference, the waist–hip ratio and the level of sex hormone-binding globulin in the berberine group vs. the metformin group (p > 0.05), and this result is not confirmed by other research groups [19]. An et al. showed a decreased BMI in the group of berberine vs. metformin (p < 0.05) [22].

Women affected by PCOS showed an impaired fasting glucose control and insulin resistance, and this aspect was investigated by all authors except Wu and colleagues [24]. Parameters taken into consideration from the authors were fasting glucose, fasting insulin, the HOMA index and the AUCINS; in all studies, berberine showed an improvement of the parameters with a reduction of insulin resistance in a statistically significant way only in berberine groups vs. placebo (p < 0.01 or p < 0.05), so berberine reduced insulin resistance but is not superior to metformin [19, 21, 22, 25]. All these authors also analyzed changes in the lipid profiles of PCOS women, and demonstrated that berberine improved, in all patients, HDL cholesterol and reduced total cholesterol and LDL cholesterol [19, 21, 22, 25].

Only Cicero and colleagues have studied the effect of berberine on the Protein C Reactive (PCR) and on inflammation [21]. Cicero et al. found out that berberine in obese PCOS women causes a reduction of PCR statistically relevant compared to obese subjects (p = 0.024) [21].

Only two research groups focused on the effect of berberine on pregnancy and live births in PCOS women [22, 24]. An et al. focused on live birth percentages and showed that the berberine group had a percentage of live births greater than the metformin group (p < 0.05) and the placebo group (p < 0.05) [22]. Wu et al. confirmed the positive association between berberine treatment and live births in PCOS women, with odds ratio higher than 1 in comparison between the berberine group vs. placebo (p = 0.004) and the berberine group vs. letrozole group (p = 0.001) [24].

All research groups had analyzed the effect of berberine on women affected by PCOS, but nutraceutical and drugs formulations used were quite different; in particular, Wei et al. and An et al. administered berberine hydrochloride 500 mg three times/day [19, 22], and Orio et al. administered a tablet twice a day, with 588 mg of Berberis aristata extract tittered as 85% of berberine [25]. Cicero et al. tested a nutraceutical compound tablet with 500 mg of berberine plus 3 mg of monacolins [21]; Wu et al. administered berberine in a daily dose of 1.5 g [24]. There was a great difference between the extracts of berberine used in these five studies, and only in one case, the extract of berberine was tittered, but not standardized. This paper pointed out the lack of literature about the use of berberine in the treatment of PCOS, and shows the need to conduct more clinical trials on this topic to create a consensus regarding the amount of berberine useful in creating positive effects in PCOS women in a long-term therapy.


Despite the number of studies taken into consideration in this review being low, the number of women considered in these 5 studies is high (1078), and the results of these studies are interesting.

Two authors found out that berberine induced a redistribution of adipose tissue, reducing visceral fat mass even in the absence of weight loss, and insulin sensitivity was improved similar to metformin. One author demonstrated that berberine improved the lipid pattern. Moreover, three authors demonstrated that berberine improved the insulin resistance in theca cells with an improvement of the ovulation rate per cycle; so berberine is also effective on fertility and live birth rates. Finally, berberine may be considered as a safe botanical compound to use in premenopausal women who want to become pregnant, because of the few side effects showed in the five reported studies. Furthermore, scientific literature provides a large number of studies which reported safety and tolerability on long-term treatment with berberine in humans. In conclusion, the use of berberine in women with PCOS is very promising, even if more clinical studies are needed to confirm the safety and the efficacy of the berberine associated with other pharmacological compounds used in long-term therapy of PCOS. Besides further studies are needed to create a consensus regarding the dosage of berberine useful to create positive effects in PCOS women, even in long-term therapy.