- Research article
- Open Access
- Open Peer Review
Anticancer effect of berberine based on experimental animal models of various cancers: a systematic review and meta-analysis
BMC Cancer volume 19, Article number: 589 (2019)
Numerous studies have explored the anti-tumor effect of berberine (BBR), but little clinical evidence guides the use of BBR in cancer patients.
Our aim was to investigate the impact of BBR on various cancers in healthy animals to promote the transformation from bench to bed.
PubMed, Embase, Springer, and Cochrane databases were searched from January 2000 to October 2018 for relevant articles.
Only published studies focusing on the relationship between BBR and various cancers in vivo were qualified. Two review authors independently assessed the risk of bias for each study, and any disagreement was resolved by discussion or by involving a third assessor.
A total of 26 studies from 2000 to 2018, focusing on various cancer types, including breast cancer, liver cancer, colorectal cancer, nasopharyngeal carcinoma, lung cancer, gastric cancer, neuroepithelial cancer, endometrial carcinoma, esophageal cancer, tongue cancer, cholangiocarcinoma, and sarcoma were included. Overall, BBR reduced tumor volume (SMD =3.72, 95% CI: 2.89, 4.56, Z = 8.73, p < 0.00001) and tumor weight (SMD =2.35, 95% CI: 1.51, 3.19, Z = 5.50, p < 0.00001) in a linear The dose–response relationship (Pearson r = − 0.6717, p < 0.0001 in tumor volume analysis; Pearson r = − 0.7704, p < 0.0005 in tumor weight analysis). BBR inhibited angiogenesis in tumor tissues (SMD = 4.29, 95% CI: 2.14, 6.44, Z = 3.92, p < 0.00001), but it had no significant effect on the body weight of experimental animals (SMD = 0.11, 95% CI: − 0.70, 0.92, Z = 0.27, p = 0.78). Publication bias was not detected.
BBR exerted anti-tumor effects in a variety of tumors in vivo, especially breast cancer and lung cancer, and the evidence was still insufficient in colorectal cancer and gastric cancer.
Berberine (BBR) is a natural component purified from the species of the genus Berberis, which has long been used as an anti-diarrheal drug in gastrointestinal disorders in traditional Chinese medicine . At the same time, the anti-tumor effect of BBR has been a hot topic in experimental research in recent years. In the past 3 years, latest studies have shown the anticancer actions of BBR against several high-risk cancers, including lung cancer , breast cancer , prostate cancer , colorectal cancer , and gastric cancer .
However, little clinical evidence guides the use of BBR in cancer patients. Thus, systematic reviews and meta-analyses of animal studies may help to clarify whether cancer patients could benefit from this approach and promote the transformation of animal studies into humans at the same time .
Our aim was to investigate the impact of BBR on cancer growth and its adverse effects in randomized controlled trials in healthy animals.
Identification of studies
From January 2000 to October 2017, relevant literature from PubMed, Embase, Springer, and Cochrane databases was systematically screened. The following Mesh terms and textwords were used: “Neoplasms”[Mesh], “Neoplasia,” “Neoplasias,” “Neoplasm,” “Tumors,” “Tumor,” “Cancer,” “Cancers,” “Malignant Neoplasms,” “Malignant Neoplasm,” “Neoplasm, Malignant,” “Neoplasms, Malignant,” “Malignancy,” “Malignancies,” “Berberine”[Mesh]," “Berberine,” “Umbellatine,” and “BBR.” The “AND” or “OR” operator was used to combine these terms in varying combinations. At the same time, references in the articles were also included in the screening. We did not set a language limit during the process. Two authors (Jianhao Xu, Yuming Long) independently reviewed the titles and abstracts identified in the search. In this process, we discussed the articles to incorporate the differences. If problems still could not be resolved, a third assessor (Yusong Zhang) was invited to make a decision. Only published articles were included. No protocol was developed for this review.
The inclusion criteria were as follows: (1) participants: experimental animals including rodent, mouse, rat, rabbit, guinea pig, dog, horse, sheep, and monkey; (2) invention: BBR only; (3) outcomes: the effects of BBR in animal models after tumor implantation, including tumor volume, tumor weight, tumor vessel density, and body weight; and (4) study design: experiments should be prospectively controlled. The exclusion criteria were as follows: (a) literature published as letters, editorials, abstracts, reviews, and expert opinions; (b) non-animal-based studies; (c) articles with missing data information; (d) similar and repeated studies; and (e) outdated articles with little significance and credibility. Cohen’s kappa statistic was used to assess chance-corrected agreement between reviewers (SPSS version 18. 0, SPSS Inc. Chicago, IL) .
Study characteristics and data extraction
A detailed form was designed for data extraction: first author, publication year, country, cancer type, animals’ baseline characteristics, intervention, duration, and the data of specific outcomes (tumor volume, tumor weight, tumor vessel density, and body weight). Two review authors extracted the data by using the agreed form.
Quality of evidence and risk of bias
For risk of bias of individual studies, the ARRIVE checklist was used to assess pre-clinical animal studies . For risk of bias among studies, such as publication bias and selective reporting, funnel chart analysis, subgroup analysis, and sensitive analysis were all conducted. Two review authors (Jian−hao Xu, Yuming Long) independently assessed the risk of bias for each study.
Data synthesis and statistical analysis
We carried out statistical analysis by using the Review Manager software (RevMan 5.3) and STATA statistical software package version 12.0 (Stata Corporation, College Station, TX). The primary outcomes were tumor volume, tumor weight, and tumor vessel density of BBR group compared with the control group. The secondary outcome was the change of body weight. Mean value and standard difference (SD) were used as summary statistics. Standard mean difference (SMD) was measured for continuous data. Linear regression and Pearson’s correlation analysis were used to study the The dose–response relationship between BBR and the four outcomes. The heterogeneity among studies was measured by using the I2 test. The latent publication bias was assessed by using a funnel plot. All statistical tests were two-tailed, and p < 0.05 was considered statistically significant.
A total of 969 potential articles were identified from the literature search. After selection, 26 studies [10,11,12,13,14,15,16,17,18,19,20,21,22,23,24,25,26,27,28,29,30,31,32,33,34,35] matched the inclusion criteria and were suitable for our meta-analysis. The flow diagram in Fig. 1 showed the selection process. A review of the study selection and data extraction indicated excellent agreement between reviewers (k = 0.820).
Study characteristics and quality assessment
Study characteristics are summarized in Table 1. A total of 26 studies [10,11,12,13,14,15,16,17,18,19,20,21,22,23,24,25,26,27,28,29,30,31,32,33,34,35] from 2000 to 2018, focusing on various cancer types, including breast cancer [10,11,12,13,14,15,16], liver cancer [17,18,19], colorectal cancer [20,21,22], nasopharyngeal carcinoma [23, 24], lung cancer [25, 26], gastric cancer [27, 28], neuroepithelial tumor [29, 30], endometrial carcinoma , esophageal cancer , tongue cancer , cholangiocarcinoma , and sarcoma  were included. The studies used rats , hamsters , and mice [10,11,12,13, 15,16,17,18,19,20,21,22,23,24,25,26,27,28,29,30,31,32,33, 35] modeled via subcutaneous tumor implantation [10,11,12,13, 16,17,18,19,20,21,22,23,24,25,26,27,28,29,30,31,32,33,34,35] or induced tumor formation [14, 15]. BBR was administered in doses ranging between 2.5 mg/kg and 200 mg/kg body weight through intraperitoneal injection [10, 15,16,17, 19, 21, 23, 24, 30, 33, 35] and gavage [11,12,13,14, 18, 20, 22, 25,26,27,28,29, 31, 32, 34] or from 1000 ppm to 5400 ppm in drinking water [13, 20, 25]. The size of the study sample ranged from 6 to 20, while the follow-up ranged from 1 week to 32.5 weeks. Quality assessment based on the ARRIVE guideline is presented in Table 2. Overall, the studies included in our analysis were of moderate quality.
Of the 26 screened articles [10,11,12,13,14,15,16,17,18,19,20,21,22,23,24,25,26,27,28,29,30,31,32,33,34,35], 20 [11, 13, 14, 16,17,18,19, 21,22,23,24,25,26,27,28,29,30,31,32,33] reported the relationship between BBR and tumor volume in animals with breast cancer [11, 13, 14, 16], liver cancer [17,18,19], colorectal cancer [21, 22], nasopharyngeal carcinoma [23, 24], lung cancer [25, 26], gastric cancer [27, 28], neuroepithelial cancer [29, 30], endometrial carcinoma , esophageal cancer , and tongue cancer . The SMD and the 95%CI in each study are shown in Fig. 2. The pooled SMD remained statistically significant in breast cancer (SMD = 3.32, 95% CI: 1.29, 5.36; Z = 3.2, p = 0.001), liver cancer (SMD = 7.36, 95% CI: 3.45, 11.27; Z = 3.69, p = 0.0002), colorectal cancer (SMD = 0.70, 95% CI: 0.26, 1.15; Z = 3.10, p = 0.002), nasopharyngeal carcinoma (SMD = 3.85, 95% CI: 1.21, 6.49; Z = 2.86, p = 0.004), lung cancer (SMD = 7.18, 95% CI: 4.26, 10.10; Z = 4.82, p < 0.00001), neuroepithelial tumor (SMD = 1.66, 95% CI:0.41, 2.92; Z = 2.59, p = 0.010), and endometrial cancer (SMD = 4.65, 95% CI: 1.55, 7.74; Z = 2.94, P = 0.003). The pooled SMD remained statistically insignificant in gastric cancer (SMD = 1.47, 95% CI: − 1.01, 7.08; Z = 1.47, P = 0.14). For total studies, the pooled result suggested that the SMD was 3.72 (95% CI: 2.89, 4.56) with statistical significance (Z = 8.73, p < 0.00001).
In view of the obvious heterogeneity (I2 = 80% for breast cancer; I2 = 81% for liver cancer; I2 = 63% for nasopharyngeal carcinoma; I2 = 89% for lung cancer; I2 = 61% for endometrial cancer), we conducted a subgroup analysis of different characteristics mainly on the following aspects: gender, animals, BBR dose, administration, duration, and cell lines (Fig. 3). In breast cancer, the BBR dose was a potential influencing factor (I2 decreased to 0% in one subgroup. Another two I2 were missing due to the limited study). In liver cancer, the cell line was a potential influencing factor (I2 decreased to 34% in one subgroup. Another two I2 were missing due to the limited study). In nasopharyngeal carcinoma, gender, duration, and cell line were potential influencing factors (I2 decreased to 0% in one subgroup. Another I2 was missing due to the limited study). In lung cancer, the BBR dose was a potential influencing factor (I2 decreased to 87, 86, and 0% in three subgroups respectively). In endometrial cancer, no potential influencing factor was filtered.
The dose–response relationship of different cancer types on the relationship between BBR and tumor volume of animals is shown in Fig. 4. For single cancer types, a statistically significant linear relationship in colorectal cancer (Pearson r = − 0.8785, p = 0.0499) and lung cancer (Pearson r = − 0.6718, p = 0.0459) was observed. For total studies, the SMD values of all studies showed a statistically significant decreasing trend with increasing concentration of BBR (Pearson r = − 0.6717, p < 0.0001).
Of the 26 screened articles [10,11,12,13,14,15,16,17,18,19,20,21,22,23,24,25,26,27,28,29,30,31,32,33,34,35], 12 [12, 14, 16, 20, 23, 26,27,28, 32,33,34,35] reported the relationship between BBR and tumor weight in animals with breast cancer [12, 14, 16], colorectal cancer , nasopharyngeal carcinoma , lung cancer , gastric cancer [27, 28], esophageal cancer , and tongue cancer . The SMD and the 95%CI in each study are shown in Fig. 5. The pooled SMD remained statistically significant in breast cancer(SMD = 3.71, 95% CI: 2.18, 5.25; Z = 4.74, p < 0.00001), lung cancer(SMD = 3.65, 95% CI: 1.86, 5.44; Z = 4.00, p < 0.0001), and gastric cancer(SMD = 1.90, 95% CI: 0.61, 3.20; Z = 2.88, p = 0.004). The pooled SMD remained statistically insignificant in colorectal cancer(SMD = − 0.17, 95% CI: − 0.71, 0.36; Z = 0.63, p = 0.53). For total studies, the pooled result suggested that the SMD was 2.35(95% CI: 1.51, 3.19) with statistical significance (Z = 5.50, p < 0.00001).
In view of the obvious heterogeneity(I2 = 89% for lung cancer), we conducted a subgroup analysis of different characteristics mainly on the following aspects: dose of BBR and cell lines(Fig. 6). In lung cancer, the dose of BBR was a potential influencing factor (I2 decreased to 0, 57, and 0% in three subgroups respectively).
The dose–response relationship of different cancer types on the relationship between BBR and tumor weight of animals is shown in Fig. 7. For single cancer types, a statistically significant linear relationship in lung cancer (Pearson r = − 0.9623, p = 0.0021) was observed. For total studies, the SMD values of all studies showed a statistically significant decreasing trend with increasing concentration of BBR (Pearson r = − 0.7704, p < 0.0005).
Tumor vessel density
Of the 26 screened articles [10,11,12,13,14,15,16,17,18,19,20,21,22,23,24,25,26,27,28,29,30,31,32,33,34,35], 3 [10, 15, 19] reported the relationship between BBR and tumor vessel density in animals with breast cancer [10, 15] and liver cancer . The SMD and the 95%CI in each study are shown in Fig. 8. The pooled SMD remained statistically significant in breast cancer(SMD = 1.09, 95% CI: 0.37, 1.81; Z = 2.96, p = 0.003). For total studies, the pooled result suggested that the SMD was 4.29(95% CI: 2.14, 6.44) with statistical significance(Z = 3.92, p < 0.00001).
No statistical heterogeneity was observed (I2 = 0% for breast cancer).
The dose–response relationship of different cancer types on the relationship between BBR and tumor weight of animals is shown in Fig. 9. For single cancer types, no linear relationship was concluded because of the limited studies. For total studies, the SMD values of all studies showed no statistically significant trend(Pearson r = − 0.9866, p = 0.1044).
Of the 26 screened articles [10,11,12,13,14,15,16,17,18,19,20,21,22,23,24,25,26,27,28,29,30,31,32,33,34,35], 7 [11, 16, 17, 20, 22, 27, 35] reported the relationship between BBR and body weight in animals with breast cancer [11, 16], liver cancer , colorectal cancer [20, 22], gastric cancer , and sarcoma . The SMD and the 95%CI in each study are shown in Fig. 10. The pooled SMD remained statistically significant in liver cancer(SMD = − 2.18, 95% CI: − 4.00, − 0.36; Z = 2.35, p = 0.02). The pooled SMD remained statistically insignificant in breast cancer(SMD = 1.41, 95% CI: − 0.38, 3.20; Z = 1.54, p = 0.12) and colorectal cancer(SMD = − 0.14, 95% CI: − 1.03, 0.75; Z = 0.30, p = 0.76). For total studies, the pooled result suggested that the SMD was 0.11(95% CI: − 0.70, 0.92) with statistical significance(Z = 0.27, p = 0.78).
In view of the obvious heterogeneity(I2 = 73% for breast cancer; I2 = 80% for colorectal cancer; I2 = 52% for liver cancer), we conducted a subgroup analysis of different characteristics mainly on the following aspects: dose of BBR, administration, and cell lines(Fig. 11). I2 were missing in breast cancer group and liver cancer group due to limited studies. No potential influencing factor was found in colorectal cancer group.
The dose–response relationship of different cancer types on the relationship between BBR and body weight of animals is shown in Fig. 12. For single cancer types, no statistically significant linear relationship was found. For total studies, the SMD values of all studies showed no statistically significant trend(Pearson r = − 0.1440, p = 0.7116).
Publication bias and sensitivity analysis
The publication bias evaluation for the meta-analysis of tumor volume, tumor weight, tumor vessel density, and body weight is shown in Fig. 13. These funnel plots showed that most of the studies are in the upper part of the inverted funnel and approximately symmetrical, suggesting that the publication bias was unobvious.
A sensitivity analysis was performed to assess the stability of our results in terms of tumor volume, tumor weight, tumor vessel density, and body weight. The trim method was used, and the results did not show considerable changes between the previous and new SMDs (Fig. 14). Next, we deleted one individual study at a time, and the results of the rest of the studies were checked for any reversal. The statistical outcomes showed that the pooled SMDs were all still significant although one study was excluded (Fig. 15).
Molecular pathways and proteins
Among these included studies, a wide range of molecular targets, which are essential for the anti-cancer effect of BBR, was revealed. Except for three articles [15, 33, 35] that did not involve the discussion of molecular mechanisms, the remaining 23 articles [10,11,12,13,14, 16,17,18,19,20,21,22,23,24,25,26,27,28,29,30,31,32, 34] analyzed the anti-tumor mechanism of BBR. The pharmacological effects of BBR was summarized into five aspects: proliferation(including apoptosis, autophagy, cell cycle arrest, and others), intracellular oxidative stress, inflammation, angiogenesis, and migration. Table 3 shows how BBR works in different scenarios of multiple types of cancers. In addition, in order to understand the anticancer mechanism more clearly and deeply, Table 4 shows the clustering analysis of the common molecular pathways and target proteins between studies.
The most frequently studied pathways were on cell proliferation and 19 articles focused on this mechanism. Seven of these studies involved tumor cell apoptosis pathways (breast cancer [9, 12], liver cancer [17, 18], lung cancer , gastric cancer , esophageal cancer ), one involved autophagy pathways (neuroepithelial cancer ), and five involved cell cycle arrest pathways (colon cancer , lung cance , gastric cancer , esophageal cancer , cholangiocarcinoma ). The second most common frequently studied pathways were on cell migration. Four articles in three cancers studied the relationship between BBR and tumor cell migration (breast cancer [13, 16], liver cancer , endometrial carcinoma ). There was only one study reported the relationship between BBR and intracellular oxidative stress (breast cancer ), inflammation (breast cancer ), and angiogenesis (liver cancer ) respectively.
We performed a systematic review and meta-analysis to systematically evaluate the efficacy and adverse effect of BBR on various cancers. The results showed that BBR could inhibit the growth of a variety of cancers in vivo, especially in breast cancer (SMD = 3.32, 95% CI: 1.29, 5.36 in tumor volume; SMD = 3.71, 95% CI: 2.18, 5.25 in tumor weight; SMD = 1.09, 95% CI: 0.37, 1.81 in tumor vessel density) and lung cancer (SMD = 7.36, 95% CI: 3.45, 11.27 in tumor volume; SMD = 3.65, 95% CI: 1.86, 5.44 in tumor weight). Evidence for the benefit of BBR was not sufficient for gastric cancer (SMD = 1.47, 95% CI: − 1.01, 7.08 in tumor volume) and colorectal cancer (SMD = − 0.17, 95% CI: − 0.71, 0.36 in tumor weight). BBR showed a dose–response relationship in tumor volume and weight (Pearson r = − 0.6717 and − 0.7704, with p < 0.0001 and p < 0.0005, respectively). At the same time, dose was an important influencing factor for heterogeneity from the subgroup analysis. The change in body weight of experimental animals was used as an indicator of the adverse effects of BBR. The above results indicated that no statistically significant difference was observed in terms of body weight under the effect of BBR (SMD =0.11, 95% CI: − 0.70, 0.92).
In the past 3 years, numerous studies have attempted to elucidate the relationship between BBR and breast/lung cancer. By using molecular modeling and in vitro studies, BBR significantly reduced EGFR and AKT phosphorylation and may be a useful alternative to lapatinib, an EGFR inhibitor which can cause acquired drug resistance in breast cancer patients . BBR lowers blood sugar, increases insulin sensitivity, and corrects lipid metabolism disorders; it may reduce the incidence of breast cancer . Single-drug BBR has an obvious inhibitory effect on lung cancer cells; BBR can inhibit doxorubicin (DOX)-mediated STAT3 activation and sensitize lung cancer cells to the cytotoxic effects of DOX treatment. Given the widespread clinical application of BBR and its low toxicity, our findings are important for the development of a new combination of BBR and DOX for the treatment of lung cancer . In addition to medical treatment, BBR has protective effects on radiation-induced lung injury via intercellular adhesion molecular-1 and transforming growth factor-beta-1 in patients with lung cancer .
Although, in the present study, the therapeutic effect of BBR in colorectal and gastric cancer required more evidence, numerous studies have confirmed the gain effect of BBR combined with chemotherapy in recent years. Latest research shows that the combination of the second generation Hsp90 inhibitor NVP-AUY922 and BBR therapy could inhibit a variety of oncogenic signaling pathways of colorectal cancer . Another study showed that BBR as an adjunctive therapeutic agent could attenuate chemical resistance during gastric cancer treatment. The combination of 5-FU and BBR showed synergistic inhibition of survivin and STAT3 levels, thereby enhancing the death of gastric cancer cells . In addition to the 5-FU-based chemotherapy regimen, BBR treatment reduced cisplatin resistance in gastric cancer cells by modulating the miR-203/Bcl-w apoptotic axis .
In the present study, body weight index was used to evaluate the growth of experimental animals to indirectly evaluate the adverse effects of BBR. However, studies have shown that BBR could induce weight loss in rodents [43, 44] and humans [45, 46]. In recent years, research has reported that BBR affected body weight by upregulating AMPK and UCP3 expression to control energy expenditure . Therefore, the toxic side effects of BBR cannot be objectively and accurately evaluated by the change of body weight alone.
There were some limitations to our analysis that deserve discussion. First, we observed considerable heterogeneity between the studies when analyzing tumor volume, tumor weight, and body weight. Although subgroup analysis (Figs. 3, 5, and 11) was performed, some I2 were missing because of the limited studies. Secondly, generally speaking, obviously significant publication bias was not found based on the funnel plot (Fig. 13). However, poor symmetry of the funnel plot on tumor volume suggested more high-quality researches should be included. Thirdly, although PubMed, Embase, Springer, and Cochrane databases had been carefully and comprehensively searched, articles selected for each cancer type were still small which could lead to bias. Fourthly, the anticancer effects of berberine in humans were not identified clearly and further studies in humans were needed to develop it as an anticancer agent.
BBR exerted anti-tumor effects in a variety of tumors in vivo, especially for breast cancer and lung cancer. However, evidence was still insufficient in colorectal cancer and gastric cancer. One of its anti-tumor mechanisms was anti-angiogenesis. There was a dose-response relationship in the anti-tumor effects.
Availability of data and materials
All data generated or analysed during this study are included in this published article.
Epstein-Barr virus nuclear antigen 1
Reactive Oxygen Species
Standard Mean Difference
TNF-related apoptosis-inducing ligand
Chen C, Yu Z, Li Y, Fichna J, Storr M. Effects of Berberine in the gastrointestinal tract u2014 a review of actions and therapeutic implications. Am J Chinese Med. 2014;42:1450066.
Kim S, Song YL, Cho HJ. Berberine and zinc oxide-based nanoparticles for the chemo-photothermal therapy of lung adenocarcinoma. Biochemical & Biophysical Research Communications. 2018;501:765–70.
Cazzaniga M. Relationship between metabolic disorders and breast cancer incidence and outcomes. Is there a preventive and therapeutic role for Berberine? Anticancer Res. 2018;38:4393–402.
Yuantong T, Lijing Z, Wang H, Zhang X, Zhao J. Berberine inhibits androgen synthesis by interaction with aldo-keto reductase 1C3 in 22Rv1 prostate cancer cells. Asian J Androl. 2016;18:607–12.
Liu H, Huang C, Wu L, Wen B. Effect of evodiamine and berberine on miR-429 as an oncogene in human colorectal cancer. Oncotargets & Therapy. 2016;9:4121–7.
Hu Q, Li L, Zou X, Xu L, Yi P. Berberine attenuated proliferation, invasion and migration by targeting the AMPK/HNF4α/WNT5A pathway in gastric carcinoma. Front Pharmacol. 2018;9:1150.
Hui KK, Yu JL. Effects of protein kinase inhibitor, 1-(5-isoquinolinylsulfonyl)-2-methylpiperazine, on beta-2 adrenergic receptor activation and desensitization in intact human lymphocytes. Journal of Pharmacology & Experimental Therapeutics. 1989;249:492.
Cohen J. Weighted kappa: nominal scale agreement with provision for scaled disagreement or partial credit. Psychol Bull. 1968 1968-10-01;70:213–20.
Kilkenny C, Browne W, Cuthill IC, Emerson M, Altman DG. Animal research: reporting in vivo experiments--the ARRIVE guidelines. J Cereb Blood Flow Metab. 2011 2011-04-01;31:991–3.
Pierpaoli E, Damiani E, Orlando F, Lucarini G, Bartozzi B, Lombardi P, Salvatore C, Geroni C, Donati A, Provinciali M. Antiangiogenic and antitumor activities of berberine derivative NAX014 compound in a transgenic murine model of HER2/neu-positive mammary carcinoma. Carcinogenesis. 2015;36:1169.
Zhao Y, Jing Z, Lv J, Zhang Z, Lin J, Cao X, Zhao Z, Liu P, Mao W. Berberine activates caspase-9/cytochrome c-mediated apoptosis to suppress triple-negative breast cancer cells in vitro and in vivo. Biomed Pharmacother. 2017;95:18–24.
Refaat A, Abdelhamed S, Yagita H, Inoue H, Yokoyama S, Hayakawa Y, Saiki I. Berberine enhances tumor necrosis factor-related apoptosis-inducing ligand-mediated apoptosis in breast cancer. Oncol Lett. 2013;6:840–4.
Kim S, Lee J, You D, Jeong Y, Jeon M, Yu J, Kim SW, Nam SJ, Lee JE. Berberine suppresses cell motility through downregulation of TGF-beta1 in TripleNegative breast Cancer cells. Cell Physiol Biochem. 2018 2018-01-20;45:795–807.
Karnam KC, Ellutla M, Bodduluru LN, Kasala ER, Uppulapu SK, Kalyankumarraju M, Lahkar M. Preventive effect of berberine against DMBA-induced breast cancer in female Sprague Dawley rats. Biomed Pharmacother. 2017;92:207–14.
Elisa D, Elisa P, Fiorenza O, Abele D, Mauro P. Sidestream dark field videomicroscopy for in vivo evaluation of vascularization and perfusion of mammary tumours in HER2/neu transgenic mice. Clinical & Experimental Pharmacology & Physiology. 2015;42:225–9.
Su K, Hu P, Wang X, Kuang C, Xiang Q, Yang F, Xiang J, Zhu S, Wei L, Zhang J. Tumor suppressor berberine binds VASp to inhibit cell migration in basal-like breast cancer. Oncotarget. 2016;7:45849–62.
Guan-Yu W, Qing-Hua L, Qi D, Rong-Zhen X, Qing-Hua D. Berbamine induces Fas-mediated apoptosis in human hepatocellular carcinoma HepG2 cells and inhibits its tumor growth in nude mice. J Asian Nat Prod Res. 2009;11:219–28.
Li J, Li O, Kan M, Zhang M, Shao D, Pan Y, Zheng H, Zhang X, Chen L, Liu S. Berberine induces apoptosis by suppressing the arachidonic acid metabolic pathway in hepatocellular carcinoma. Mol Med Rep. 2015;12:4572.
Chi MT, Cheung KCP, Cheung YC, Man K, Lui WY, Tsao SW, Feng Y. Berberine suppresses Id-1 expression and inhibits the growth and development of lung metastases in hepatocellular carcinoma. BBA - Molecular Basis of Disease. 2015;1852:541–51.
Norio I, Shoichi H, Kiyoshi Y, Shigefumi Y, Akira T, Koji M, Kiwamu O, Masaaki O. Anticachectic effects of the natural herb Coptidis rhizoma and berberine on mice bearing colon 26/clone 20 adenocarcinoma. Int J Cancer. 2010;99:286–91.
Ruan H, Zhan YY, Hou J, Xu B, Chen B, Tian Y, Wu D, Zhao Y, Zhang Y, Chen X. Berberine binds RXRÎ± to suppress Î2-catenin signaling in colon cancer cells. Oncogene. 2017;36:6906.
Cai Y, Xia Q, Luo R, Huang P, Sun Y, Shi Y, Jiang W. Berberine inhibits the growth of human colorectal adenocarcinoma in vitro and in vivo. J Nat Med-Tokyo. 2014;68:53–62.
Wang C, Wang H, Zhang Y, Guo W, Long C, Wang J, Liu L, Sun X. Berberine inhibits the proliferation of human nasopharyngeal carcinoma cells via an Epstein-Barr virus nuclear antigen 1-dependent mechanism. Oncol Rep. 2017;37(4):2109–20.
Chi MT, Cheung YC, Lui WY, Yip YL, Zhang G, Lin VW, Cheung CP, Feng Y, Tsao SW. Berberine suppresses tumorigenicity and growth of nasopharyngeal carcinoma cells by inhibiting STAT3 activation induced by tumor associated fibroblasts. BMC Cancer(2013-12-31. 2013;13:619.
James MA, Fu H, Liu Y, Chen DR, You M. Dietary administration of berberine or Phellodendron amurense extract inhibits cell cycle progression and lung tumorigenesis. Mol Carcinog. 2011 2011-01-01;50:1–7.
Katiyar SK, Meeran SM, Katiyar N, Akhtar S. p53 cooperates berberine-induced growth inhibition and apoptosis of non-small cell human lung cancer cells in vitro and tumor xenograft growth in vivo. Mol Carcinogen. 2010;48:24–37.
Wang J, Yang S, Cai X, Dong J, Chen Z, Wang R, Zhang S, Cao H, Lu D, Jin T. Berberine inhibits EGFR signaling and enhances the antitumor effects of EGFR inhibitors in gastric cancer. Oncotarget. 2016;7:76076–86.
Li HL, Wu H, Zhang BB, Shi HL, Wu XJ. MAPK pathways are involved in the inhibitory effect of berberine hydrochloride on gastric cancer MGC 803 cell proliferation and IL-8 secretion in vitro and in vivo. Mol Med Rep. 2016;14:1430.
Wang J, Peng Y, Liu Y, Yang J, Ding N, Tan W. Berberine, a natural compound, suppresses hedgehog signaling pathway activity and cancer growth. BMC Cancer. 2015;15:595.
Sun Y, Yu J, Liu X, Zhang C, Cao J, Li G, Liu X, Chen Y, Huang H. Oncosis-like cell death is induced by berberine through ERK1/2-mediated impairment of mitochondrial aerobic respiration in gliomas. Biomedicine & pharmacotherapy = Biomedecine & pharmacotherapie. 2018;102:699.
Wang Y, Zhang S. Berberine suppresses growth and metastasis of endometrial cancer cells via miR-101/COX-2. Biomed Pharmacother. 2018 2018-07-01;103:1287–93.
Ren K, Zhang W, Wu G, Ren J, Lu H, Li Z, Han X. Synergistic anti-cancer effects of galangin and berberine through apoptosis induction and proliferation inhibition in oesophageal carcinoma cells. Biomed Pharmacother. 2016 2016-12-01;84:1748–59.
Ho YT, Yang JS, Lu CC, Chiang JH, Li TC, Lin JJ, Lai KC, Liao CL, Lin JG, Chung JG. Berberine inhibits human tongue squamous carcinoma cancer tumor growth in a murine xenograft model. Phytomedicine. 2009;16:887–90.
Nattapong P, Kulthida V, Wunchana S, Orasa W, Worasak K, Amornrat J, Somchai P, Chawalit P, Chaisiri W, Seiji O. Establishment of an Allo-transplantable hamster cholangiocarcinoma cell line and its application for in vivo screening of anti-cancer drugs. Korean J Parasitol. 2013;51:711–7.
Lei Z, Jingjing L, Fei M, Shining Y, Naisan L, Jing W, Yongbin W, Xiuzhen W, Qizheng Y. Synthesis and cytotoxicity evaluation of 13-n-alkyl berberine and palmatine analogues as anticancer agents. Molecules. 2012;17:11294–302.
Jabbarzadeh KP, Leong MP, Ismail P, Ling KH. Antitumor effects of berberine against EGFR, ERK1/2, P38 and AKT in MDA-MB231 and MCF-7 breast cancer cells using molecular modelling and in vitro study. Pharmacol Rep. 2018 2018-08-01;71:13–23.
Cazzaniga M, Bonanni B. Relationship Between Metabolic Disorders and Breast Cancer Incidence and Outcomes. Is There a Preventive and Therapeutic Role for Berberine? Anticancer Res. 2018 2018-08-01;38:4393–402.
Zhu T, Li LL, Xiao GF, Luo QZ, Liu QZ, Yao KT, Xiao GH. Berberine increases doxorubicin sensitivity by suppressing STAT3 in lung Cancer. Am J Chinese Med. 2015;43:1550084.
Yunfang L, Huiming Y, Cheng Z, Yufeng C, Likuan H, Xiaohui M, Yuxia Z. Protective effects of berberine on radiation-induced lung injury via intercellular adhesion molecular-1 and transforming growth factor-beta-1 in patients with lung cancer. Eur J Cancer. 2008;44:2425–32.
Su YH, Tang WC, Cheng YW, Sia P, Huang CC, Lee YC, Jiang HY, Wu MH, Lai IL, Lee JW. Targeting of multiple oncogenic signaling pathways by Hsp90 inhibitor alone or in combination with Berberine for treatment of colorectal Cancer. BBA - Molecular Cell Research. 2015;1853:2261–72.
Pandey A, Vishnoi K, Mahata S, Tripathi SC, Misra SP, Misra V, Mehrotra R, Dwivedi M, Bharti AC. Berberine and curcumin target Survivin and STAT3 in gastric Cancer cells and synergize actions of standard chemotherapeutic 5-fluorouracil. Nutrition & Cancer-an International Journal. 2015;67:1293–304.
You HY, Xie XM, Zhang WJ, Zhu HL, Jiang FZ. Berberine modulates cisplatin sensitivity of human gastric cancer cells by upregulation of miR-203. In Vitro Cellular & Developmental Biology - Animal. 2016;52:1–7.
Hu Y, Davies GE. Berberine inhibits adipogenesis in high-fat diet-induced obesity mice. Fitoterapia. 2010 2010-07-01;81:358–66.
Xu Z, Yufeng Z, Menghui Z, Xiaoyan P, Jia X, Chaoying K, Meng L, Chenhong Z, Zhiguo Z, Yifei Z. Structural changes of gut microbiota during berberine-mediated prevention of obesity and insulin resistance in high-fat diet-fed rats. PLoS One. 2012;7:e42529.
Zhang Y, Li X, Zou D, Liu W, Yang J, Zhu N, Huo L, Wang M, Hong J, et al. Treatment of type 2 diabetes and dyslipidemia with the natural plant alkaloid berberine. J Clin Endocrinol Metab. 2008 2008-07-01;93:2559–65.
Hu Y, Ehli EA, Kittelsrud J, Ronan PJ, Munger K, Downey T, Bohlen K, Callahan L, Munson V, et al. Lipid-lowering effect of berberine in human subjects and rats. Phytomedicine. 2012 2012-07-15;19:861–7.
Hu Y, Young AJ, Ehli EA, Nowotny D, Davies PS, Droke EA, Soundy TJ, Davies GE. Metformin and berberine prevent olanzapine-induced weight gain in rats. PLoS One. 2014;9:e93310.
The current study was funded by the Kunshan first people s hospital affiliated to Jiangsu University, and the second affiliated hospital of Soochow University.
The current study was supported by grants from the second affiliated hospital of Soochow university pre-research project (SDFEYGJ1609), the second affiliated hospital of Soochow university clinical discipline group project funding (XKQ 2015008), the international team of gastrointestinal tumor project funding (SZYJTD201804) and the project from national key laboratory of radiation medicine (GZK1201820). The funder had no role in the design of the study and collection, analysis, and interpretation of data and in writing the manuscript.
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Xu, J., Long, Y., Ni, L. et al. Anticancer effect of berberine based on experimental animal models of various cancers: a systematic review and meta-analysis. BMC Cancer 19, 589 (2019) doi:10.1186/s12885-019-5791-1
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