Welcome to Journal of Tea Science,Today is

Journal of Tea Science >

2016 , Vol. 36 >Issue 6: 557 - 566

DOI: https://doi.org/10.13305/j.cnki.jts.2016.06.002

Inhibitory Effects of Tea and Tea Catechins on Breast Cancer

  • QIAO Ruying ,
  • LI Ming ,
  • ZHENG Xinqiang ,
  • LU Jianliang ,
  • YE Jianhui ,
  • WANG Kairong ,
  • LIANG Yuerong
Expand
  • 1. Tea Research Institute, Zhejiang University, Hangzhou 310058, China;
    2. General Station of Forestry Speciality Technology Extension of Yuyao City, Yuyao 315499, China;
    3. Ningbo Huangjinyun Tea Science and Technology Co., Ltd., Yuyao 315400, China

Received date: 2016-06-24

  Online published: 2019-08-26

Fold

Abstract

Tea with high catechin contents has various health benefits. There are more than ten catechins in tea, among which epigallocatechin gallate (EGCG) is the most abundant. The inhibitory effects of tea and its major catechin (EGCG) on breast cancer were reviewed in the present paper, which included their abilities of suppressing carcinogen-induced ROS elevation and DNA damages, decreasing the responsiveness of cells to tumor necrosis factors, blocking the binding of estrogen to estrogen receptor, inhibiting DNA methylation, protecting mitochondria from oxidative damages and inhibiting tumor angiogenesis. The anti-proliferation and anti-metastasis of cancer cells and their synergistic effects with anticancer drugs were also mentioned. The inconsistent results in previous studies and directions for future research were finally discussed.

Key words: tea; catechins; anticancer; antioxidant; estrogen receptor; anti-proliferation; metastasis

Cite this article

QIAO Ruying , LI Ming , ZHENG Xinqiang , LU Jianliang , YE Jianhui , WANG Kairong , LIANG Yuerong . Inhibitory Effects of Tea and Tea Catechins on Breast Cancer[J]. Journal of Tea Science, 2016 , 36(6) : 557 -566 . DOI: 10.13305/j.cnki.jts.2016.06.002

References

[1] Stewart BW, Wild CP. World cancer report2014 [R]. French: World Health Organization, 2014: 16-53, 362-373.
[2] Kushi L H, Doyle C, McCullough M, et al. American Cancer Society guidelines on nutrition and physical activity for cancer prevention[J]. CA: a cancer journal for clinicians, 2012, 62(1): 30-67.
[3] Thomson C A.Diet and breast cancer understanding risks and benefits[J]. Nutrition in Clinical Practice, 2012, 27(5): 636-650.
[4] Liang Y R, Ye Q, Jin J, et al.Chemical and instrumental assessment of green tea sensory preference[J]. International Journal of Food Properties, 2008, 11(2): 258-272.
[5] Dong J J, Ye J H, Lu J L, et al.Isolation of antioxidant catechins from green tea and its decaffeination[J]. Food and Bioproducts Processing, 2011, 89(1): 62-66.
[6] Lin S Y, Chen Y L, Lee C L, et al.Monitoring volatile compound profiles and chemical compositions during the process of manufacturing semi-fermented Oolong tea[J]. Journal of Horticultural Science and Biotechnology, 2013, 88(2): 159-164.
[7] Liang Y, Lu J, Zhang L, et al.Estimation of black tea quality by analysis of chemical composition and colour difference of tea infusions[J]. Food Chemistry, 2003, 80(2): 283-290.
[8] Xu J Y, Wu L Y, Zheng X Q, et al.Green Tea polyphenols attenuating ultraviolet B-induced damage to human retinal pigment epithelial cells in vitro[J]. Investigative Ophthalmology and Visual Science, 2010, 51(12): 6665-6670.
[9] Chen X, Lu W, Zheng Y, et al.Exercise, tea consumption, and depression among breast cancer survivors[J]. Journal of Clinical Oncology, 2010, 28(6): 991-998.
[10] Li M, Tse L A, Chan W, et al.Evaluation of breast cancer risk associated with tea consumption by menopausal and estrogen receptor status among Chinese women in Hong Kong[J]. Cancer Epidemiology, 2016, 40: 73-78.
[11] Suzuki Y, Tsubono Y, Nakaya N, et al.Green tea and the risk of breast cancer: pooled analysis of two prospective studies in Japan[J]. British Journal of Cancer, 2004, 90(7): 1361-1363.
[12] Zhang M, Holman C D A J, Huang J, et al. Green tea and the prevention of breast cancer: a case-control study in Southeast China[J]. Carcinogenesis, 2007, 28(5): 1074-1078.
[13] Shrubsole M J, Lu W, Chen Z, et al.Drinking green tea modestly reduces breast cancer risk[J]. Journal of Nutrition, 2009, 139(2): 310-316.
[14] Dai Q, Shu X O, Li H, et al.Is green tea drinking associated with a later onset of breast cancer?[J]. Annals of Epidemiology, 2010, 20(1): 74-81.
[15] Wu A H, Yu M C, Tseng C C, et al.Green tea and risk of breast cancer in Asian Americans[J]. International journal of Cancer, 2003, 106(4): 574-579.
[16] Zhang M, Huang J, Xie X, et al.Dietary intakes of mushrooms and green tea combine to reduce the risk of breast cancer in Chinese women[J]. International Journal of Cancer, 2009, 124(6): 1404-1408.
[17] Yuan J M, Koh W P, Sun C L, et al. Green tea intake, ACE gene polymorphism and breast cancer risk among Chinese women in Singapore[J]. Carcinogenesis, 2005, 26(8): 1389-1394.
[18] Inoue M, Robien K, Wang R, et al.Green tea intake, MTHFR/TYMS genotype and breast cancer risk: the Singapore Chinese health study[J]. Carcinogenesis, 2008, 29(10): 1967-1972.
[19] Ganmaa D, Willett W C, Li T Y, et al.Coffee, tea, caffeine and risk of breast cancer: A 22-year follow-up[J]. International Journal of Cancer, 2008, 122(9): 2071-2076.
[20] Kumar N, Titus-Ernstoff L, Newcomb P A, et al.Tea consumption and risk of breast cancer[J]. Cancer Epidemiology Biomarkers and Prevention, 2009, 18(1): 341-345.
[21] Guyton K Z, Kensler T W.Oxidative mechanisms in carcinogenesis[J]. British Medical Bulletin, 1993, 49(3): 523-544.
[22] Birnboim H C, Sandhu J K.Levels of DNA strand breaks and superoxide in phorbol ester-treated human granulocytes[J]. Journal of Cellular Biochemistry, 1997, 66(2): 219-228.
[23] Ruch R J, Cheng S, Klaunig J E.Prevention of cytotoxicity and inhibition of intercellular communication by antioxidant catechins isolated from Chinese green tea[J]. Carcinogenesis, 1989, 10(6): 1003-1008.
[24] Abrahim N N, Kanthimathi M S, Abdul-Aziz A.Piper betle shows antioxidant activities, inhibits MCF-7 cell proliferation and increases activities of catalase and superoxide dismutase[J]. BMC Complementary and Alternative Medicine, 2012, 12(1): 220-230.
[25] Rathore K, Choudhary S, Wang H C R. Green tea catechin intervention of reactive oxygen species-mediated ERK pathway activation and chronically induced breast cell carcinogenesis[J]. Carcinogenesis, 2012, 33(1): 174-183.
[26] Saewong T, Ounjaijean S, Mundee Y, et al.Effects of Green Tea on iron accumulation and oxidative stress in livers of iron-challenged thalassemic mice[J]. Medicinal Chemistry, 2010, 6(2): 57-64.
[27] Rathore K, Wang H C R. Green tea catechin extract in intervention of chronic breast cell carcinogenesis induced by environmental carcinogens[J]. Molecular Carcinogenesis, 2012, 51(3): 280-289.
[28] Choudhary S, Sood S, Donnell R L, et al.Intervention of human breast cell carcinogenesis chronically induced by 2-amino-1-methyl-6-phenylimidazo [4,5-b] pyridine[J]. Carcinogenesis, 2012, 33(4): 876-885.
[29] Van Aller G S, Carson J D, Tang W, et al. Epigallocatechin gallate (EGCG), a major component of green tea, is a dual phosphoinositide-3-kinase/mTOR inhibitor[J]. Biochemical and Biophysical Research Communications, 2011, 406(2): 194-199.
[30] Farabegoli F, Barbi C, Lambertini E, et al.(-)-Epigallocatechin-3-gallate downregulates estrogen receptor alpha function in MCF-7 breast carcinoma cells[J]. Cancer Detection and Prevention, 2007, 31(6): 499-504.
[31] Curran S, Murray G I.Matrix metalloproteinases in tumour invasion and metastasis[J]. Journal of Pathology, 1999, 189(3): 300-308.
[32] Nelson A R, Fingleton B, Rothenberg M L, et al.Matrix metalloproteinases: biologic activity and clinical implications[J]. Journal of Clinical Oncology, 2000, 18(5): 1135-1149.
[33] Nakamura H, Ueno H, Yamashita K, et al.Enhanced production and activation of progelatinase A mediated by membrane-type 1 matrix metalloproteinase in human papillary thyroid carcinomas[J]. Cancer research, 1999, 59(2): 467-473.
[34] Sieg D J, Hauck C R, Ilic D, et al.FAK integrates growth-factor and integrin signals to promote cell migration[J]. Nature Cell Biology, 2000, 2(5): 249-256.
[35] Sen T, Moulik S, Dutta A, et al.Multifunctional effect of epigallocatechin-3-gallate (EGCG) in downregulation of gelatinase-A (MMP-2) in human breast cancer cell line MCF-7[J]. Life Sciences, 2009, 84(7): 194-204.
[36] Pike M C, Spicer D V, Dahmoush L, et al.Estrogens progestogens normal breast cell proliferation and breast cancer risk[J]. Epidemiologic Reviews, 1993, 15(1): 17-35.
[37] Haldosen LA, Zhao CY, Dahlman-Wright K.Estrogen receptor beta in breast cancer[J]. Molecular and Cellular Endocrinology, 2014, 382(1): 665-672.
[38] Yue W, Yager JD, Wang JP, et al.Estrogen receptor-dependent and independent mechanisms of breast cancer carcinogenesis[J]. Steroids, 2013, 78(2): 161-170.
[39] Paech K, Webb P, Kuiper GGJM, et al.Differential ligand activation of estrogen receptors ER alpha and ER beta at AP1 sites[J]. Science, 1997, 277(5331): 1508-1510.
[40] Pan XH, Zhao BW, Song Z, et al.Estrogen receptor-α 36 is involved in epigallocatechin-3-gallate induced growth inhibition of ER-negative breast cancer stem/progenitor cells[J]. Journal of Pharmacological Sciences, 2016, 130(2): 85-93.
[41] Kuruto-Niwa R, Inoue S, Ogawa S, et al.Effects of tea catechins on the ERE-regulated estrogenic activity[J]. Journal of Agricultural and Food Chemistry, 2000, 48(12): 6355-6361.
[42] Goodin MG, Fertuck KC, Zacharewski TR, et al.Estrogen receptor-mediated actions of polyphenolic catechins in vivo and in vitro[J]. Toxicological Sciences, 2002, 69(2): 354-361.
[43] Sartippour MR, Pietras R, Marquez-Garban DC, et al.The combination of green tea and tamoxifen is effective against breast cancer[J]. Carcinogenesis, 2006, 27(12): 2424-2433.
[44] Li YY, Yuan YY, Meeran SM, et al.Synergistic epigenetic reactivation of estrogen receptor-alpha (ERα) by combined green tea polyphenol and histone deacetylase inhibitor in ER alpha-negative breast cancer cells[J]. Molecular Cancer, 2010, 9(1): 274-285.
[45] Lee W J, Shim J Y, Zhu B T.Mechanisms for the inhibition of DNA methyltransferases by tea catechins and bioflavonoids[J]. Molecular Pharmacology, 2005, 68(4): 1018-1030.
[46] Fang M Z, Wang Y, Ai N, et al.Tea polyphenol (-)-epigallocatechin-3-gallate inhibits DNA methyltransferase and reactivates methylation-silenced genes in cancer cell lines[J]. Cancer Research, 2003, 63(22): 7563-7570.
[47] Huo C, Yang H, Cui Q C, et al.Proteasome inhibition in human breast cancer cells with high catechol-O-methyltransferase activity by green tea polyphenol EGCG analog[J]. Bioorganic and Medicinal Chemistry, 2010, 18(3): 1252-1258.
[48] Landis-Piwowar K R, Wan S B, Wiegand R A, et al. Methylation suppresses the proteasome-inhibitory function of green tea polyphenols[J]. Journal of Cellular Physiology, 2007, 213(1): 252-260.
[49] Landis-Piwowar K, Chen D, Chan T H, et al.Inhibition of catechol-O-methyltransferase activity in human breast cancer cells enhances the biological effect of the green tea polyphenol (-)-EGCG[J]. Oncology Reports, 2010, 24(2): 563-569.
[50] Conklin K A.Dietary antioxidants during cancer chemotherapy: impact on chemotherapeutic effectiveness and development of side effects[J]. Nutrition and Cancer, 2000, 37(1): 1-18.
[51] Zaveri NT.Green tea and its polyphenolic catechins: Medicinal uses in cancer and noncancer applications[J]. Life Science, 2006, 78(18): 2073-2080.
[52] Stapleton AE, Walbot V.Flavonoids can protect maize DNA from the induction of ultraviolet radiation damage[J]. Plant Physiology, 1994, 105(3): 881-889.
[53] Landry LG, Chapple CCS, Last RL.Arabidopsis mutants lacking phenolic sunscreens exhibit enhanced ultraviolet-B injury and oxidative damage[J]. Plant Physiology, 1995, 109(4): 1159-1166.
[54] Vayalil PK, Elmets CA, Katiyar SK.Treatment of green tea polyphenols in hydrophilic cream prevents UVB-induced oxidation of lipids and proteins, depletion of antioxidant enzymes and phosphorylation of MAPK proteins in SKH-1 hairless mouse skin[J]. Carcinogenesis, 2003, 24(5): 927-936.
[55] Folkman J.Angiogenesis in cancer, vascular, rheumatoid and otherdisease[J]. Nature Medicine, 1995, 1(1): 27-31.
[56] Ferrara N, Davis-Smyth T.The biology of vascular endothelial growth factor[J]. Endocrine Reviews, 1997, 18(1): 4-25.
[57] Mukhtar H, Katiyar S K, Agarwal R.Green tea and skin—anticarcinogenic effects[J]. Journal of Investigative Dermatology, 1994, 102(1): 3-7.
[58] Stoner G D, Mukhtar H.Polyphenols as cancer chemopreventive agents[J]. Journal of Cellular Biochemistry, 1995, 59(S22): 169-180.
[59] Tang F Y, Meydani M.Green tea catechins and vitamin E inhibit angiogenesis of human microvascular endothelial cells through suppression of IL-8 production[J]. Nutrition and Cancer, 2001, 41(1/2): 119-125.
[60] Sartippour M R, Shao Z M, Heber D, et al.Green tea inhibits vascular endothelial growth factor (VEGF) induction in human breast cancer cells[J]. Journal of Nutrition, 2002, 132(8): 2307-2311.
[61] Seeram N P, Zhang Y, Nair M G.Inhibition of proliferation of human cancer cells and cyclooxygenase enzymes by anthocyanidins and catechins[J]. Nutrition and Cancer, 2003, 46(1): 101-106.
[62] Luo K W, Ko C H, Yue G G L, et al. Green tea (Camellia sinensis) extract inhibits both the metastasis and osteolytic components of mammary cancer 4T1 lesions in mice[J]. Journal of Nutritional Biochemistry, 2014, 25(4): 395-403.
[63] Slivova V, Zaloga G, DeMichele S, et al. Green tea polyphenols modulate secretion of urokinase plasminogen activator (uPA) and inhibit invasive behavior of breast cancer cells[J]. Nutrition And Cancer-An International Journal, 2005, 52(1): 66-73.
[64] Zhang Y, Wu H, Chen Y, et al.Green tea (-)-epigallocatechin-3-gallate down-regulates VASP expression and inhibits breast cancer cell migration and invasion by attenuating Rac1 activity[J]. European Journal of Pharmacology, 2009 , 606(1/2/3): 172-179.
[65] Annabi B, Lachambre M P, Bousquet-Gagnon N, et al.Green tea polyphenol (-)-epigallocatechin 3-gallate inhibits MMP-2 secretion and MT1-MMP-driven migration in glioblastoma cells[J]. Biochimica et Biophysica Acta (BBA)-Molecular Cell Research, 2002, 1542(1): 209-220.
[66] Sen T, Chatterjee A.Epigallocatechin-3-gallate (EGCG) downregulates EGF-induced MMP-9 in breast cancer cells: involvement of integrin receptor alpha 5 beta 1 in the process[J]. European Journal of Nutrition, 2011, 50(6): 465-478.
[67] Xiaokaiti Y, Wu H M, Chen Y.et al.EGCG reverses human neutrophil elastase-induced migration in A549 cells by directly binding to HNE and by regulating alpha1-AT[J]. Scientific Report, 2015, 7: 1-14.
[68] Farabegoli F, Papi A, Orlandi M.(-)-Epigallocatechin- 3-gallate down-regulates EGFR, MMP-2, MMP-9 and EMMPRIN and inhibits the invasion of MCF-7 tamoxifen-resistant cells[J]. Bioscience Report, 2010, 31(2): 99-108.
[69] Parvez S, Tabassum H, Rehman H, et al.Catechin prevents tamoxifen-induced oxidative stress and biochemical perturbations in mice[J]. Toxicology, 2006, 225(2): 109-118.
[70] Harris R E, Chlebowski R T, Jackson R D, et al.Breast cancer and nonsteroidal anti-inflammatory drugs prospective results from the women’s health initiative[J]. Cancer Research, 2003, 63(18): 6096-6101.
[71] McFadden D W, Riggs D R, Jackson B J, et al. Additive effects of Cox-1 and Cox-2 inhibition on breast cancer in vitro[J]. International Journal of Oncology, 2006, 29(4): 1019-1024.
[72] Schlachterman A, Valle F, Wall K M, et al.Combined resveratrol, quercetin, and catechin treatment reduces breast tumor growth in a nude mouse model[J]. Translational Oncology, 2008, 1(1): 19-27.
[73] Baker J A, Beehler G P, Sawant A C, et al.Consumption of coffee, but not black tea, is associated with decreased risk of premenopausal breast cancer[J]. Journal of Nutrition, 2006, 136(1): 166-171.
[74] Rosenblatt K A, Thomas D B, Jimenez L M, et al.The relationship between diet and breast cancer in men (United States)[J]. Cancer Causes and Control, 1999, 10(2): 107-113.
[75] Suganuma M, Okabe S, Sueoka N, et al.Green tea and cancer chemoprevention[J]. Mutation Research, 1999, 428(1): 339-344.
[76] Forester S C, Lambert J D.The catechol-O-methyltransferase inhibitor, tolcapone, increases the bioavailability of unmethylated (-)-epigallocatechin-3-gallate in mice[J]. Journal of Functional Foods, 2015, 17: 183-188.
[77] Dube A, Nicolazzo J A, Larson I.Chitosan nanoparticles enhance the intestinal absorption of the green tea catechins (+)-catechin and (-)-epigallocatechin gallate[J]. European Journal of Pharmaceutical Sciences, 2010, 41(2): 219-225.
[78] Yadav R, Kumar D, Kumari A, et al.Encapsulation of catechin and epicatechin on BSA NPs improved their stability and antioxidant potential[J]. Excli Journal, 2014, 13: 331-346.
[79] Tagashira T, Choshi T, Hibino S, et al.Influence of gallate and pyrogallol moieties on the intestinal absorption of (-)‐epicatechin and (-)‐epicatechin gallate[J]. Journal of Food Science, 2012, 77(10): H208-H215.
[80] Naumovski N, Blades B L, Roach P D.Food inhibits the oral bioavailability of the major green tea antioxidant epigallocatechin gallate in humans[J]. Antioxidants, 2015, 4(2): 373-393.
[81] Son Y R, Chung J H, Ko S, et al.Combinational enhancing effects of formulation and encapsulation on digestive stability and intestinal transport of green tea catechins[J]. Journal of Microencapsulation, 2016, 33(2): 183-190.
[82] Garcia J P D, Hsieh M F, Doma B T, et al. Synthesis of gelatin-γ-polyglutamic acid-based hydrogel for the in vitro controlled release of epigallocatechin gallate (EGCG) from Camellia sinensis[J]. Polymers, 2013, 6(1): 39-58.
Options
Outlines

/

浙ICP备14034295号
浙公网安备 33019902000101号
Copyright © 2019 Journal of Tea Science, All Rights Reserved.
Tel: 0571-86651482 Powered by Beijing Magtech Co. Ltd