ANTICANCER-ONCOXIN cu Germaniu Organic (GE-132) in activitatea anticancer

Germaniu Organic, Garlic si I3C un anticancer inhiba carcinogeneza

1 Anticancer-Oncoxin cu Germaniu Organic (GE-132) in activitatea anticancer la activarea importanta de macrofage si celulele T.

2 Anticancer-Oncoxin cu Germaniu Organic (GE-132) induce productia de interferon, activarea celulelor NK si macrofage.

2 Anticancer-Oncoxin cu Germaniu Organic Alil sulfid din Garlic si I3C un anticancer inhiba carcinogeneza.

ANTICANCER-ONCOXIN cu Germaniu Organic (GE-132)

Germaniu Organic (GE-132) cu activitate anticancer

1 Anticancer-Oncoxin cu Germaniu Organic (GE-132) in activitatea anticancer la activarea importanta de macrofage si celulele T.

2 Anticancer-Oncoxin cu Germaniu Organic (GE-132) pentru imunitate induce productia de interferon si activarea celulelor NK si macrofage

Germaniu Organic (GE-132) pentru imunitate

Anticancer-Oncoxin: 1055 mg, 30 buc
Analiza Nutritiva: 8 Ingrediente 1 Fl. + 1 Fl. + 1 Fl. a 30 buc:1055 mg
Germaniu Organic (GE-132)	30 mg	/**
Garlic cu Alil sulfid	100 mg	/**
L-Arginina	200 mg	/**
N-Acetilcisteina	200 mg	/**
L-Lizina	200 mg	/**
Vitamina C	200 mg	333,00%
Ceai Verde extr.stand. EGCG 40%	100 mg	/**
Vitamina D 3 - 1000 UI	25 mg	250%

3 Anticancer-Oncoxin cu Germaniu Organic, Alil sulfid din Garlic si I3C (Indole-3-Carbinol) inhiba carcinogeneza.

Alicin este sintetizata in usturoi printr-o reactie enzimatica a enzimei alinaza (Allinase) care interfereaza conversia alinei (Alliin), in alicina.

4 Germaniu Organic (GE-132) cu activitate antivirala la infectia cu gripa aviara, influenta virus sau virusul gripal

5 Remisia completa de celulele de cancer pulmonar dupa tratamentul cu Germaniu Organic (GE-132)

6 Farmacocinetica la Germaniu Organic (GE-132) cura miraculoasa de Dr. Asai

7 Germaniu Organic (GE-132) este un imuno potentiator cu activitate biologica de imunitate, mecanismul antitumoral - reviu

8 Germaniu Organic (GE-132) inhiba cresterea de tumora prin celulele macrofage

9 Cu activitate anticancer noul Germaniu Organic (GE-132) compus prin functia de Limfocitele T si la macrofage

10 Germaniu Organic (GE-132) cu activitate antitumorala, coopereaza cu Limfocitele T si cu macrofagele

11 Germaniu Organic (GE-132) inhiba cresterea tumorala prin macrofagele peritoneale

12 Germaniu Organic (GE-132) un anticancer inhiba tumora si metastaza canceroasa, mediaza la celulele T si la macrofage.

13 Germaniu Organic (GE-132) cu efect antitumorala celulelor de cancer la plamin

14 Noul Germaniu Organic (GE-132) cu preventie de metastaza de cancer la plamin si activarea de macrofage celulelor de cancer la plamin

15 Germaniu Organic (GE-132) activareaza celulelor NK la limfocitele sangvine, pacientilor de cancer

16 L-Arginina inhiba cresterea de cancer mamar

17 L-Arginina stimuleaza reducerea cancerului mamar

18 L-Arginina la coma hepatica cu complicatie cu cancer si metastaza hepatica

19 L-Arginina cu efect metabolic si imunologic la cancer

20 Suplimente nutritive cu Vitamina C ca suport la boala de cancer si prelungirea supravietuirii umane

L-Lizina inhiba colagenaza care descompune colagenul si favorizeaza cresterea celulelor de cancer

L-Lizina inhiba colagenaza care descompune colagenul si favorizeaza metastaza canceroasa

21 Vitamina C cu doza inalta in tratamentul pacientilor de cancer unde nu are prioritate citostaticele, studiu randomizat dublu-orb placebo controlat

Ceai Verde (Camellia Sinensis) - foto

Nutraceutice - Nutraceuticele Anti Aging Systeme sint din plante naturale: Farmacia Naturala, care au efecte farmaceutice numite si fitofarmaceutice.

Ceai Verde Supreme din: Farmacia Naturala

22Ceai Verde Supreme cu: Polifenoli 90%, Catechine 70% si EGCG - Galatul de epigalocatechina extr. stand. 50% previne cancerul, inhiba angiogeneza

23Ceai Verde Supreme cu: Polifenoli 90%, Catechine 70% si EGCG - Galatul de epigalocatechina extr. stand. 50% inhiba cresterea tumorala

24Ceai Verde Supreme cu: Polifenoli 90%, Catechine 70% si EGCG - Galatul de epigalocatechina extr. stand. 50% are capacitatea de inhibare de enzima metaloproteinaza matricial -9(MMP-9) (cunoscut ca Gelatinaza B) si (Gelatinaza A) aceasta enzima detine un rol important pentru invazia tumorala si metastazarea cancerului

25 Extractul EGCG - Galatul de epigalocatechina extr. stand. 50% inhiba si actioneaza regresia la celulele de cancer de prostata (PC-3) si cancerul mamar

26 Extractul EGCG - Galatul de epigalocatechina extr. stand. 50% inhiba celulele oncogene

27Ceai Verde Supreme cu: Polifenoli 90%, Catechine 70% si EGCG - Galatul de epigalocatechina extr. stand. 50% inhiba proteolitic enzima urokinaza si ornitin decarboxilaza, urokinaza este o enzima de care se foloseste celula de cancer pentru a intra in tesutul sanatos si a forma metastaze.

28Ceai Verde Supreme cu: Polifenoli 90%, Catechine 70% si EGCG - Galatul de epigalocatechina extr. stand. 50% reduce enzima 5-alfa reductaza este un agent citostatic natural, inhiba proliferarea celulelor canceroase de prostata

29Ceai Verde Supreme cu: Polifenoli 90%, Catechine 70% si EGCG - Galatul de epigalocatechina extr. stand. 50% inhiba glioblastoma

30 Ceai Verde Supreme cu: Polifenoli 90%, Catechine 70% si EGCG - Galatul de epigalocatechina extr. stand. 50% previne riscul de melanom malign (cancer de piele) reduce inflamatia razelor UVB

31 Teoria radicalilor liberi in procesul de imbatrinire

Procesul de imbatranire cu cauzele endogene si exogene

- Radicalii liberi considerati ca mediatori patologici.

- Formarea de radicali liberi prin: Factorii exogeni ca poluarea aerului, razele-UV, radiatii ionizante, etc., factorii endogeni pot fi stres, exercitiu fizic extenuant, inflamatii, fumat, etc.

- Tipuri de radicali liberi: Radicalii liberi ai oxigenului, Radicalii liberi ai azotului, Radicalul thiil,etc

Formarea de radicali liberi	Structura celulei este oxidata de actiunea agresiva a radicalilor liberi

- Inalta concentratie de oxigen reactiv - radicalii liberi si cantitatea insuficienta in organism de antioxidanti, genera in organite (centrale energetice celulare) eficacitatea scazuta a repararii ADN-ului, ca rezultat: Disfunctia mitocondriala, care este o caracteristica a celulelor maligne.

32 Chimia la catechine antioxidanti inhiba stresul oxidativ, reactia la EGCG galatul de epigalocatechina cu radicalul peroxil (ROO-)

Radicalii liberi produc stres oxidativ	Distrugerile ADN-ului de radicalii liberi care produc stres oxidativ

- Mutatiile ADN-ului de radicalii liberi afecteaza energia celulara ATP Administrarea de antioxidanti ca factor anti cancer determina reversia fenotipului malign prin inhibarea celulelor de cancer - Anti cancer: EGCG Galatul de epigalocatechina

Degradarea ADN-ului prin acumularea de 8-hidroxi-2’-deoxiguanozina	Reversia fenotipului malign prin inhibarea celulelor de cancer

Neutralizarea de radicali liberi - Densitatea antioxidativa

Despre antioxidanti: Antioxidantii sint molecule care apara organismul de efectele oxigenului reactiv - Radicalii liberi
Radicalii liberi produc stres oxidativ, iar antioxidantii apara celula de radicalii liberi care sint molecule instabile, contin electroni neimperecheati, adica un electron ocupa un singur orbital.

33 Ceai Verde cu EGCG - Galatul de epigalocatechina extr. stand. 50% are activitate antioxidanta de neutralizare de radicali liberi: radicalul superoxid (O₂^-), radicalul peroxil (RO₂^-), radicalul peroxinitrit (OONO ^-), peroxid de hidrogen (H₂O₂) previne oxidarea LDL - biologia si medicina radicalilor liberi

34 Ceai Verde cu EGCG - Galatul de epigalocatechina extr. stand. 50% are activitate antioxidanta de neutralizare a radicalilor liberi, inhiba peroxidarea lipidelor, degradarea ADN-ului, in 8-hidroxi-2’-deoxiguanozina (8-OHdG), este un biomarker a stresului oxidativ, acumulata in ADN cauzeaza disfunctia mitocondriala si criza energetica

Disfunctia mitocondriala care este o caracteristica a celulelor maligne, datorat prin capacitatea scazuta antioxidativa.

Antioxidantii apara celula de efectele oxigenului reactiv	Antioxidantii cu neutralizarea de radicali liberi - Capacitate scazuta antioxidativa

- Antioxidanti se gasesc in orice celula, protejeaza organismul de distrugerile provocate la nivel celular de radicalii liberi.
- Antioxidantii pot neutraliza radicalii liberi limitind distrugerea provocata, daca suficienti antioxidanti sint involvati - Capacitate suficienta antioxidativa
- Acid Alfa Lipoic prin proprietati si functie regenereaza alti antioxidanti ca: Vitamina C, Vitamina E, Glutation, Coenzima Q10 ofera protectie antioxidativa de efectele radicalilor liberi.

Antioxidantii protejind celula de radicalii liberi - Capacitate suficienta

Sint o multime de antioxidanti in extracte de plante naturale, fitofarmaceutice, nutraceutice cu capacite de neutralizare a radicalilor liberi Antioxidanti cheie: Acid Alfa Lipoic, Coenzima Q10, Vitamine: Vitamina C, Vitamina E, Caretenoizi, (beta caroten,alfa caroten, licopen, luteina, zeaxantina) Compusi fenolici: Flavonoizi, polifenoli care confera protectie ridicata antoxidativa

- Suficienti antioxidanti de recomandat: Acid Alfa Lipoic, Ceai Verde EGCG, Vitamina C, Glutation, Vitamin E, Carotenoizi, Coenzima Q10 sau enzime antioxidante ca superoxid dismutaza (SOD) care detoxifica radicalul superoxid, peroxidul de hidrogen (H ₂O₂) si Glutation peroxidaza (GPx) care detoxifica peroxizii celulari

Spirulina contine superoxid dismutaza (SOD) un antioxidant puternic 110000 Unitati/100g

Suficienti antioxidanti de recomandat: Acid alfa lipoic, Ceai Verde, Vitamina C, Glutation, Vitamin E, Carotenoizi, Coenzima Q10 sau enzime antioxidante ca superoxid dismutaza (SOD) care detoxifica radicalul superoxid, peroxidul de hidrogen (H₂O₂) si Glutation peroxidaza (GPx) care detoxifica peroxizii celulari

EGCG cu capacitate de absorbtie a radicalului liber a oxigenului - ORAC, comparatia valorilor fata de Vitamina C

35 Vitamina D si analogi de Vitamina D sint agenti citostatici

36 Vitamina D3 - 800 UI/zi si Calciu 1800 mg/zi cu potential in preventia de cancer mamar si cancer de colon

37 Vitamina D3 1000 UI mediaza transcrierea genei prin receptorul Vitamina D (VDR) si transfoma celulele epiteliale de Cancer mamar in celule normale

38 Vitamina D3 un modulator in cresterea de cancer mamar

39 Vitamina D3 in preventia de cancer mamar

40 Vitamina D3 regleaza receptorul Vitamina D (VDR) care inhiba linia celulara HT29 si MCF-7 la cancerul mamar si cancerul de colon

41 Vitamina D3 si Melatonina cresteTGF-beta-1 si induce inhibarea de cancer mamar

42 Suplimente nutritionale de Vitamina D in preventia de cancer mamar la femei in menopauza

43 Vitamina D3 1000 UI mediaza la regresia la tumora

44 Vitamina D atenueaza cresterea de tumora retinoblastoma tumorala cu inducerea apoptozei celulare de cancer

45 Vitamina D in preventia de cancer de prostata

Terapia Anti-Aging:

Anti-Aging-Systeme - Terapia Anti-Aging

 

Bibliografie-Referinte: ANTICANCER-ONCOXIN

Informatii din bibliografia electronica la tema: Nutritie si sanatate

1 Suzuki F, Brutkiewicz RR, Pollard RB. Importance ot T-cells and macrophages in the antitumor activity of carboxyethylgermanium sesquioxide (Ge-132). Anticancer Research 1985;5(5):479-483.
2 Aso H, Suzuki F, Yamaguchi T, Hayashi Y, Ebina T, Ishida N. Induction of interferon and activation of NK cells and macrophages in mice by oral administration of Ge-132, an organic germanium compound. Microbiology and Immunology 1985;29(1):65-74
3 Jang JJ, Cho KJ, Lee YS, Bae JH. Modifying responses of allyl sulfide, indole-3-carbinol and germanium in a rat multi-organ carcinogenesis model. Carcinogenesis 1991;4:691-695.
4 Aso H, Suzuki F, Ebina T, Ishida N. Antiviral activity of carboxyethylgermanium sesquioxide (Ge-132) in mice infected with influenza virus. Department of Bacteriology, Tohoku University School of Medicine, Sendai, Japan. J Biol Response Mod. 1989 Apr;8(2):180-9.
5 Mainwaring MG, Poor C, Zander DS, Harman E. Complete remission of pulmonary spindle cell carcinoma after treatment with oral germanium sesquioxide. Department of Medicine, Divisions of Hematology and Oncology, University of Florida College of Medicine and Veterinary Affairs Medical Center, Gainesville, FL 32610, USA. Chest. 2000 Feb;117(2):591-3.
6 Long QC, Zeng GX, Zhao XL. Pharmacokinetics of germanium after po beta-carboxyethylgermanium sesquioxide in 24 Chinese volunteers. Department of Clinical Pharmacology, Sun Yat-Sen University of Medical Sciences, Guangzhou, China. Zhongguo Yao Li Xue Bao. 1996 Sep;17(5):415-8
7 Brutkiewicz RR, Suzuki F. Biological activities and antitumor mechanism of an immunopotentiating organogermanium compound, Ge-132 (review). Department of Internal Medicine, University of Texas Medical Branch, Galveston 77550. In Vivo. 1987 Jul-Aug;1(4):189-203.
8 Suzuki F. Suppression of tumor growth by peritoneal macrophages isolated from mice treated with carboxyethylgermanium sesquioxide (Ge-132) Gan To Kagaku Ryoho. 1985 Nov;12(11):2122-8.
9 Suzuki F. Antitumor activity of Ge-132, a new organogermanium compound, in mice is expressed through the functions of macrophages and T lymphocytes Gan To Kagaku Ryoho. 1985 Jul;12(7):1445-52.
10 Suzuki F, Brutkiewicz RR, Pollard RB. Cooperation of lymphokine(s) and macrophages in expression of antitumor activity of carboxyethylgermanium sesquioxide (Ge-132). Anticancer Res. 1986 Mar-Apr;6(2):177-82.
11 Suzuki F. Suppression of tumor growth by peritoneal macrophages isolated from mice treated with carboxyethylgermanium sesquioxide (Ge-132) Gan To Kagaku Ryoho. 1985 Nov;12(11):2122-8.
12 Sato I, Yuan BD, Nishimura T, Tanaka N. Inhibition of tumor growth and metastasis in association with modification of immune response by novel organic germanium compounds. Journal of Biological Response Modifiers 1985;4(2):159-168.
13 Kumano N, Ishikawa T, Koinumaru S, Kikumoto T, Suzuki S, Nakai Y, Konno K. Antitumor effect of the organogermanium compound Ge-132 on the Lewis lung carcinoma (3LL) in C57BL/6 (B6) mice. Tohoku J Exp Med. 1985 May;146(1):97-104.
14 Sato I, Nishimura T, Kakimoto N, Suzuki H, Tanaka N. Prevention of pulmonary metastasis of Lewis lung carcinoma and activation of murine macrophages by a novel organic germanium compound, PCAGeS. Biological Response Modifiers 1988;7(1):1-5.
15 Tanaka N, Ohida J, Ono M, et al. Augmentation of NK activity in peripheral blood lymphocytes of cancer patients by intermittent Ge-132 administration. Gan To Kagaku Ryoho 1984;11(6):1303-1306.
16 Takeda Y, Tominga T, Tei N, et al. Inhibitory effect of L-arginine on growth of rat mammary tumors induced by 7,12-dimethlybenz(a)anthracine. Cancer Res 1975;35:2390-3.
17 Brittenden J, Park KGM, Heys SD, et al. L-arginine stimulates host defenses in patients with breast cancer. Surgery 1994;115:205-12.
18. Imler M, Ruscher H, Peter B et al: The effect of arginine in a case of recurrent hepatic coma complicating a feminizing cortico-adrenal tumor with hepatic metastasis. Sem Hop Paris 1973; 49:3183-3190.
19 Park KGM. The immunological and metabolic effects of L-arginine in human cancer. Proc Nutr Soc 1993;52:387–401.
20 Cameron E, Pauling L. Supplemental ascorbate in the supportive treatment of cancer: Prolongation of survival times in terminal human cancer. Proc Natl Acad Sci U S A. 1976 Oct;73(10):3685-9.
21 Moertel CG, Fleming TR, Creagan ET, Rubin J, O'Connell MJ, Ames MM. High-dose vitamin C versus placebo in the treatment of patients with advanced cancer who have had no prior chemotherapy. A randomized double-blind comparison. N Engl J Med. 1985 Jan 17;312(3):137-41.
22 Imai K, Suga K, Nagachi K. Cancer-preventive effects of drinking green tea among a Japanese population. Prev Med. 1997;26(6):769-775.
- Mukhtar H., Ahmad N. Tea polyphenols: prevention of cancer and optimizing health. Am. J. Clin. Nutr., 71: 1698S-702S, 2000.
- Cao Y., Cao R. Angiogenesis inhibited by drinking tea. Nature (Lond.), 398: 381 1999.
- Brown MD. Green tea (Camellia sinensis) extract and its possible role in the prevention of cancer. Alt Med Rev. 1999;4(5):360-370.
- Sazuka M, et al. Inhibitory effects of green tea infusion on in vitro invasion and in vivo metastasis of mouse lung carcinoma cells. Cancer Lett 1995;98:27-31.
23 Sugiyama T, Sadzuka Y. Enhancing effects of green tea components on the antitumor activity of adriamycin against M5076 ovarian sarcoma. Cancer letters 1998;133:19-26
- Fujiki H, Suganuma M, Okabe S, et al. Cancer inhibition by green tea. Mutation Research. 1998;307-310.
- Gao Yt, McLaughlin JK, Blot WJ Reduced risk of esophageal cancer associated with green tea consumption. J Natl Cancer Inst. 1994 Jun 1;86(11):855-8.
- Hirose M. Inhibition of mammary gland carcinogenesis by green tea catechins. Cancer Lett 1994;83:149-156.
- Inoue M, Tajima K, Mizutani M, et al. Regular consumption of green tea and the risk of breast cancer recurrence: follow-up study from the Hospital-based Epidemiologic Research Program at Aichi Cancer Center (HERPACC), Japan. Cancer Lett. 2001;167(2):175-182.
- Kaegi E. Unconventional therapies for cancer: 2. Green tea. [Review]. The Task Force on Alternative Therapies of the Canadian Breast Cancer Research Initiative. CMAJ. 1998;158(8):1033-1035.
- Nakachi K, Suemasu K, Suga K, Takeo T, Imai K, Higashi Y. Influence of drinking green tea on breast cancer malignancy among Japanese patients. Jpn J Cancer Res. 1998;89(3):254-261.
- Pianetti S, Guo S, Kavanagh KT, Sonenshein GE. Green tea polyphenol epigallocatechin-3 gallate inhibits Her-2/neu signaling, proliferation, and transformed phenotype of breast cancer cells. Cancer Res. 2002;62(3):652-655.
- Setiawan VW, Zhang ZF, Yu GP, et al. Protective effect of green tea on the risks of chronic gastritis and stomach cancer. Int J Cancer. 2001;92(4):600-604.
- Sano T, Sasako M. Green tea and gastric cancer. N Engl J Med. 2001;344(9):675-676.
- Tsubono Y, Nishino Y, Komatsu S, et al. Green tea and the risk of gastric cancer in Japan. N Engl J Med. 2001;344(9):632-636.
- Yu GP, Hsieh CC, Wang LY, Yu SZ, Li XL, Jin TH. Green-tea consumption and risk of stomach cancer: a population-based case-control study in Shanghai, China. Cancer Causes Control. 1995;6(6):532-538.
- Sugiyama T, Sadzuka Y. Enhancing effects of green tea components on the antitumor activity of adriamycin against M5076 ovarian sarcoma. Cancer Lett. 1998;133(1):19–26.
- Ji B-T, Chow W-H, Hsing AW, et al. Green tea consumption and the risk of pancreatic and colorectal cancers. Int J Cancer. 1997;70:255-258.
- Fujiki H, Suganuma M, Okabe S, et al. Mechanistic findings of green tea as cancer preventive for humans. Proc Soc Exp Biol Med. 1999;220(4):225–228.
- Ahmad N, Mukhtar H. Green tea polyphenols and cancer: biologic mechanisms and practical implications. Nutr Rev. 1999; 57:78-83.
- Ahmad N, et al. Green tea constituent epigallocathechin-3-gallate and induction of apoptosis and cell cycle arrest in human carcinoma cells. H Natl Cancer Inst 1997;89:1881-86.
- Wang Z, et al. Antimutagenic activity of green tea polyphenols. Mutation Research. 1989;223:273-285.
- Jankun J, et al. Why drinking green tea could prevent cancer. Nature 1997;387:561
- Taniguchi S, et al. Effect of (-)-epigallocatechin gallate, the main constituent of green tea, on lung metastasis with mouse B16 melanoma cells lines. Cancer Lett 1992;65:51-4.
-Kaegi E, on behalf of the Task Force on Alternative Therapies of the Canadian Breast Cancer Research Initiative. Unconventional therapies for cancer: 2. Green tea. Canadian Medical Association 1998;158:1033-1035.
24 Demeule M, Brossard M, Pagé, M, et al. Matrix metalloproteinase inhibition by green tea catechins. Biochim Biophys Acta. 2000; 1478:51-60.
25 Liao S, Umekita Y, Guo J, Kokontis JM, Hiipakka RA. Growth inhibition and regression of human prostate and breast tumors in athymic mice by tea epigallocatechin gallate. Cancer Lett. 1995;96:239-243.
- Carlin BI, Pretlow TG, Pretlow TP, et al. Green tea polyphenols inhibit growth of PC xenograft cwr-22 and decrease ornithine decarboxylase activity: implications for PC chemoprevention. J Urol 155: 510A, 1996.
26 Hu G, Han C, Chen J.Inhibition of oncogene expression by green tea and (-)-epigallocatechin gallate in mice. Institute of Nutrition and Food Hygiene, Chinese Academy of Preventive Medicine, Beijing, China. Nutr Cancer. 1995;24(2):203-9.
27 Carlin BI, Pretlow TG, Pretlow TP, et al. Green tea polyphenols inhibit growth of PC xenograft cwr-22 and decrease ornithine decarboxylase activity: implications for PC chemoprevention. J Urol 155: 510A, 1996.
28 Liao S, Hipakka, RA. Selective inhibition of steroid 5-alfa-reductase [5AR] by tea epicatechin-3-gallate and epigallocatechin-3-gallate. Biochemical and Biophysical Research Communications; 214(3), 833-838,1995).
- Gupta S, Ahmad N, Mukhtar H. Prostate cancer chemoprevention by green tea. Semin Urol Oncol. 1999; 17:70-76.
- Suganuma M, Okabe S, Sueoka N, et al. Green tea and cancer chemoprevention. Mutation Res. 1999; 428:339-344.
- Suganuma M, Okabe S, Kai Y, et al. Synergistic effects of (-)-epigallocatechin gallate with (-)-epicatechin, sulindac or tamoxifen on cancer-preventive activity in the human lung cancer cell line PC-9. Cancer Research 1999; 59: 44-47.
29 Sachinidis A, Seul C, Seewald S, et al. Green tea compounds inhibit tyrosine phosphorylation of PDGF beta-receptor and transformation of A172 human glioblastoma. FEBS Lett. 2000; 471:51-55.
30 Katiyar SK, Matsui MS, Elmets CA, Mukhtar H. Polyphenolic antioxidant (-)-epigallocatechin-3-gallate from green tea reduces UVB-induced inflammatory responses and infiltration of leukocytes in human skin. Photochem Photobiol 1999;69:148-153.
- Mukhtar H., Katiyar S. K. et al. Green tea and skin: anticarcinogenic effects. J. Investig. Dermatol. 102: 3-7,
31 Beckman, K. & Ames, B. (1998) "The free radical theory of aging matures" Physiol Rev 78: 548-81
32 Valcic S, Muders A, Jacobsen NE, Liebler DC, Timmermann BN. Antioxidant chemistry of green tea catechins. Identification of products of the reaction of (-)-epigallocatechin gallate with peroxyl radicals. Department of Pharmacology & Toxicology, College of Pharmacy, The University of Arizona, Tucson, Arizona 85721, USA. Chem Res Toxicol. 1999 Apr;12(4):382-6.
33 Luo M, Kannar K, Wahlqvist ML, O'Brien RC. Inhibition of LDL oxidation by green tea extract. Lancet. 1997 Feb 1;349(9048):360-361.
- Miura Y, Chiba T, Miura S, et al. Green tea polyphenols (flavan 3-ols) prevent oxidative modification of low density lipoproteins: an ex vivo study in humans. J Nutr Biochem. 2000; 11:216-222.
- Yang TTC, Koo MWL. Inhibitory effect of Chinese green tea on endothelial cell-induced LDL oxidation. Atherosclerosis. 2000; 148:67-73.
- Shi X, Ye J, Leonard SS, et al. Antioxidant properties of epicatechin gallate (ECG) and its inhibition of Cr (VI)-induced DNA damage and Cr (IV)- or TPA-stimulated NF-Kappa B activation. Mol Cell Biochem. 2000; 206:125-132.
- Ketsawatsakul U., Whiteman M., Halliwell B. A reevaluation of the peroxynitrite scavenging activity of some dietary phenolics. Biochem. Biophys. Res. Commun., 279: 692-699, 2000.
- Nakagawa K, Ninomiya M, Okubo T, Aoi N, Juneja LR, Kim M, Yamanaka K, Miyazawa T. Tea catechin supplementation increases antioxidant capacity and prevents phospholipid hydroperoxidation in plasma of humans. Laboratory of Biodynamic Chemistry, Tohoku University Graduate School of Life Science and Agriculture, Sendai 981-8555, Japan. J Agric Food Chem. 1999 Oct;47(10):3967-73.
- Wei H, Zhang X, Zhao JF, Wang ZY, Bickers D, Lebwohl M. Scavenging of hydrogen peroxide and inhibition of ultraviolet light-induced oxidative DNA damage by aqueous extracts from green tea. Free Radic Biol Med. 1999;26(11-12):1427-1435.
- Miyazawa T.Absorption, metabolism and antioxidative effects of tea catechin in humans. Biodynamics Chemistry, Lab., Tohoku University Graduate School of Life Science & Agriculture, Sendai, Japan. Biofactors. 2000;13(1-4):55-9.
- Yang TTC, Koo MWI. Chinese green tea lowers cholesterol level through an increase in fecal lipid excreiton. Life Sciences. 1999:66:5:411-423.
- M.K. Shigenaga and B.N. Ames. Free Radical Biology and Medicine 10:211-6,1991.
34 Shigenaga MK, Ames BN. Assays for 8-hydroxy-2'-deoxyguanosine, a biomarker of in vivo oxidative DNA damage. Free Radic. Biol. Med., 1991; 10: 211-6.
- H. Kasai, P.F. Crain, Y. Kuchino, S. Nishimura, A.Ootsuyama and H. Tanooka. Carcinogenesis 7:1849-51, 1986.
35 Guyton KZ, Kensler TW, Posner GH. Vitamin D and vitamin D analogs as cancer chemopreventive agents. CCS Associates, 2005 Landings Drive, Mountain View, CA 94043, USA. Nutr Rev. 2003 Jul;61(7):227-38.
36 Garland CF, Garland FC, Gorham ED. Calcium and vitamin D. Their potential roles in colon and breast cancer prevention. Department of Family and Preventive Medicine, University of California, San Diego 92093, USA. Ann N Y Acad Sci. 1999;889:107-19.
37 Wietzke JA, Ward EC, Schneider J, Welsh J. Regulation of the human vitamin D3 receptor promoter in breast cancer cells is mediated through Sp1 sites. Department of Biological Sciences, University of Notre Dame, 214 Galvin Life Science Building, Notre Dame, IN 46556, USA. Mol Cell Endocrinol. 2005 Jan 31;230(1-2):59-68.
38 Welsh J, Wietzke JA, Zinser GM, Smyczek S, Romu S, Tribble E, Welsh JC, Byrne B, Narvaez CJ. Impact of the Vitamin D3 receptor on growth-regulatory pathways in mammary gland and breast cancer. Department of Biological Sciences, University of Notre Dame, Notre Dame, IN 46556, USA. J Steroid Biochem Mol Biol. 2002 Dec;83(1-5):85-92.
39 Welsh J, Wietzke JA, Zinser GM, Byrne B, Smith K, Narvaez CJ. Vitamin D-3 receptor as a target for breast cancer prevention. Department of Biological Sciences, University of Notre Dame, Notre Dame, IN 46556, USA. J Nutr. 2003 Jul;133(7 Suppl):2425S-2433S.
40 Gilad LA, Bresler T, Gnainsky J, Smirnoff P, Schwartz B. Regulation of vitamin D receptor expression via estrogen-induced activation of the ERK 1/2 signaling pathway in colon and breast cancer cells. Institute of Biochemistry, Food Science and Nutrition, Faculty of Agricultural, Food and Environmental Quality Sciences, The Hebrew University of Jerusalem, P.O. Box 12, Rehovot 76100, Israel. J Endocrinol. 2005 Jun;185(3):577-92.
41 M . Bizzarri Melatonin and vitamin D3 increase TGF-ß1 release and induce growth inhibition in breast cancer cell cultures . Journal of Surgical Research , Volume 110 , Issue 2 , Pages 332 - 337
42 McCullough ML, Rodriguez C, Diver WR, Feigelson HS, Stevens VL, Thun MJ, Calle EE. Dairy, calcium, and vitamin D intake and postmenopausal breast cancer risk in the Cancer Prevention Study II Nutrition Cohort. Epidemiology and Surveillance Research, American Cancer Society, 1599 Clifton Road Northeast, Atlanta, GA 30329-4251, USA. Cancer Epidemiol Biomarkers Prev. 2005 Dec;14(12):2898-904.
43 W Alton Jones Cell Science Center Lake Placid NY Vitamin D3 Mediated Tumor Regression Kathryn Van Weelden; Annual rept. 1 Jul 97-30 Jun 98
44 Audo I, Darjatmoko SR, Schlamp CL, Lokken JM, Lindstrom MJ, Albert DM, Nickells RW. Vitamin D analogues increase p53, p21, and apoptosis in a xenograft model of human retinoblastoma. Department of Ophthalmology, University of Wisconsin-Madison Medical School, Madison, WI 53706, USA. Invest Ophthalmol Vis Sci. 2003 Oct;44(10):4192-9.
45 Tuohimaa P, Lyakhovich A, Aksenov N, Pennanen P, Syvälä H, Lou YR, Ahonen M, Hasan T, Pasanen P, Bläuer M, Manninen T, Miettinen S, Vilja P, Ylikomi T. Vitamin D and prostate cancer. Medical School, University of Tampere, 33014, Tampere, Finland. J Steroid Biochem Mol Biol. 2001 Jan-Mar;76(1-5):125-34.

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