Coyne Healthcare

Bio-Curcumin (Curcumin)

R 298

Curcumin is one of the world’s most studied natural plant extracts, with over 10 000 published studies and counting. Modern science has validated many of the traditional claims and uses and has identified curcumin’s true potential. Today, millions of people across the world use curcumin as a part of their daily supplement routine to improve and maintain health.

Despite the remarkable benefits of curcumin, the major challenge of supplementation is poor oral bioavailability. This refers to the body’s ability to absorb curcumin and for it to become active,  allowing it to deliver its benefits.

    Indications
    • Provides antioxidant and cell-protective activity
    • Promotes a healthy inflammation response
    • Supports the health of organs and systems by modulating the production of cytokines and other signalling molecules
    • Supports joint health and helps relieve minor pain associated with physical activity
    • Supports the body’s efforts to promote healthy cell growth and inhibit unhealthy cell growth in certain cell lines
    • Supports brain/neuronal health and a healthy mood
    • Supports a healthy microbial environment
    COVID
    • Curcumin is useful in COVID during the following phases: 1. Prevention 3. Escalating inflammation 4. Recovery
    features
    • The Curcumin features BCM-95®, the most bioavailable form of curcumin in the world currently, a 100% pure turmeric extract standardized to curcumin, demethoxycurcumin, bisdemethoxycurcumin, and essential oils of turmeric rhizome.
    • This natural composition optimizes bioavailability and reflects true turmeric identity to deliver optimal health benefits.
    • BCM-95 has been extensively studied and shows broad efficacy without the use of phospholipids, excipients, additives, carriers, nanotechnology, or bio-enhancers.*
    • Curcumina longa 25:1 extract (root): Standard to 95% total curcuminoids complex with essential oils of turmeric rhizome by HPLC - 380mg

        Benefits
        • Bio-Curcumin® utilises BCM-95®, the world’s preferred bioavailable curcumin extract.
        • Delivers up to seven times more bioactive/free curcumin into the bloodstream
        • Active for over eight hours
        • Patented and synergistic combination of curcumin + Ar-Turmerone oil
        • 40 published studies, making it the most studied curcumin extract in the world
        • 100% natural, exclusively from the turmeric plant
        • Produced using green energy and is environmentally-friendly
        • Free from artificial additives
        • Bio-Curcumin® utilises a patented, clinically proven and synergistic combination of curcumin and Ar-Turmerone, exclusively sourced from the turmeric plant.
        • Bio-Curcumin® has been proven to deliver up to seven times more free and bioactive curcumin into the bloodstream than regular curcumin extracts and it remains active in the body for over eight hours.
        • Bio-Curcumin® is the most studied curcumin extract available today, trusted and recommended by health practitioners and used by millions of people across the world.
        Features
        • 100% natural
        • Made organically and free of any synthetics, pesticides or herbicides
        • No artificial additives, flavours or preservatives
        • GMO-free
        • Sugar-free
        • Gluten-free
        • Soy-free
        • Allergen Advice: contains no known allergens
        • Suitable for vegetarians and vegans
        • Eco-friendly packaging
        • Sustainable production and harvesting (powered by certified green solar energy)
        • Scientifically developed and validated through human clinical trials
        • State-of-the-art manufacturing under GMP standards
        • Tested purity and quality
            Recommended use
            • Adults and children over 12 years: Take one to two capsules daily with food, or as recommended by a healthcare practitioner.
               Ingredients
              • BCM95(R) Bio-CurcuminTM (400mg)
              • Curcumina longa25:1 extract (root) (std to 95% total curcuminoids complex with essential oils of turmeric rhizome by HPLC (380mg)
                Other ingredients 
                • Vegetable cellulose (capsule), vegetable stearate, silica

                    • Read ingredients, dosages and cautions carefully.
                    • Do not exceed recommended dosages unless on the advice of a healthcare provider.
                    • If you are on medication, taking nutritional supplements, suffering from any medical condition, pregnant, or breastfeeding, consult your healthcare practitioner before starting any new food, supplement or remedy.
                    • Do not stop prescribed medication without consulting your healthcare practitioner.
                    • Report any new or strange symptoms to your healthcare practitioner to ensure appropriate medical care.
                    • Do not use this product if you are allergic to any of the ingredients.
                    • Due to the unique nature of each individual person’s health, specific results cannot be guaranteed and may vary from person to person.
                    • The product information provided is for educational purposes and is not intended as either diagnosis or treatment of any disease, nor does it replace professional medical advice.
                    • This medicine is not intended to diagnose, treat, cure of prevent any disease.
                    • Keep out of the reach of children. 
                    • Store in a cool (below 25°c), dry place.
                    Research
                    • Curcumin, the principal curcuminoid in turmeric, has been the subject of vast research in recent years. The pleiotropic nature of curcumin’s biological effects make it an interesting compound to researchers who study common chronic health concerns, such as those associated with joints, the cardiovascular system, glucose metabolism, brain function, mood, and cell-cycle regulation.*[1-6]
                    • The mechanisms underlying curcumin’s effects are diverse and have not been fully elucidated, but it is known that curcumin has powerful antioxidant activity and that it has multiple molecular targets, including transcription factors, cell cycle proteins, cytokines, chemokines, enzymes (e.g., COX-2), receptors, and adhesion molecules.[7] These effects make curcumin applicable to a wide array of clinical presentations.*
                    Patented Formulation: BCM-95®
                    • While the beneficial effects of curcumin are hardly arguable, an area of intense research is how to make curcumin more bioavailable. Poor absorption in the gastrointestinal (GI) tract, rapid metabolism, and rapid systemic elimination are characteristics of commercially available curcumin preparations. While investigating a way to overcome these challenges, scientists discovered they could take advantage of the synergism between the curcuminoids and the sesquiterpenoids (essential oils) naturally present in turmeric.[7] This discovery resulted in the development of BCM-95—a 100% natural whole turmeric extract composed of 86% curcuminoids (curcumin, demethoxycurcuminoid, and bisdemethoxycurcuminoid) and 7%-9% essential oils.*

                    • Essential oils are a natural component of the turmeric rhizome. Not only do they enhance absorption of curcuminoids, but they also impart health benefits.[8-10] The essential oils found in BCM-95 are extracted using double steam distillation. Essential oils comprise 7% to 9% of turmeric, with 50% of that being ar-turmerone, alpha-turmerone, and beta-turmerone. Some of the other essential oils present in BCM-95 include ar-curcumene, alpha-curcumene, zingiberene, beta-sesquiphellandrene, beta-atlantone, and germacrone.*

                    The Bioavailability of BCM-95
                    • Animal and human studies have demonstrated the superior bioavailability of the BCM-95 curcumin composition.[7,11,12] In a pilot crossover study, Antony et al compared the bioavailability of three forms of curcumin: BCM-95, normal curcumin, and a non-controlled release curcumin-piperine-lecithin formula. The data demonstrated that the absorption of curcumin from BCM-95 was fast, peaked at 4.5 hours with a gradual decline, and that curcumin was still detectable in the blood at eight hours. The other formulas showed slower curcumin absorption with an earlier peak and rapid disappearance from the blood after 4.5 hours. The relative bioavailability of BCM-95 was approximately 6.93- fold higher than normal curcumin and 6.3-fold higher than the non-controlled release curcumin-lecithin-piperine formula. According to the researchers, the results of this study indicate that the BCM-95 curcumin is “absorbed early and retained longer” compared to other forms.*[7]
                    • Unlike other bioavailability-enhanced curcumin formulas, BCM-95 does not contain any non-turmeric compounds; no phospholipids, excipients, additives, carriers, nanotechnology, or bioenhancers are used.
                    BCM-95 Studies
                    • To date, BCM-95 is backed by more than 21 published studies and over 12 years of research conducted around the world. Unlike many commercially available curcumin formulas, the bioavailability, safety, and efficacy of BCM-95 curcumin has been demonstrated in numerous preclinical and human studies. The following areas illustrate the massive body of research behind BCM-95 in relation to common health concerns: colon health[13-17], mood and stress[5,18-20], cognitive health[6], joint health[2,21], urinary health[22], cytokine modulation[23,24], prostate health[25-27], breast health[28], and cardiovascular health.*[29]
                    • As an example of the findings, in an eight-week randomized, double-blind, placebo-controlled trial (n=56), ingestion of 500 mg BCM-95 twice daily resulted in significant improvements in mood-related parameters during weeks four to eight.[20] These findings are supported by
                    Safety & Dosing
                    • Turmeric has been safely consumed for thousands of years, and its medicinal compound curcumin has an outstanding safety profile.
                    • Phase I clinical trials using up to 8 g/d for four months did not result in discernable toxicities.[30]
                    • Mild gastrointestinal distress can sometimes accompany curcumin supplementation, but this may be minimized by consuming the supplement with food.
                    • Current doses in clinical trials using BCM-95 range from 500 mg/d to 1000 mg/d.*
                    Warnings
                    • If you are taking anti-coagulant or anti-platelet medication, have a bleeding disorder or suffer from any other medical condition, consult your healthcare provider before taking Bio-Curcumin® BCM95®.
                    References

                    1. Yang F, Lim GP, Begum AN, et al. Curcumin inhibits formation of amyloid beta oligomers and fibrils, binds plaques, and reduces amyloid in vivo. J Biol Chem. 2005 Feb 18;280(7):5892- 901. [PMID: 15590663]

                    2. Chandran B, Goel A. A randomized, pilot study to assess the efficacy and safety of curcumin in patients with active rheumatoid arthritis. Phytother Res. 2012 Nov;26(11):1719-25. [PMID: 22407780]

                    3. Garcea G, Berry DP, Jones DJ, et al. Consumption of the putative chemopreventive agent curcumin by cancer patients: assessment of curcumin levels in the colorectum and their pharmacodynamic consequences. Cancer Epidemiol Biomarkers Prev. 2005 Jan;14(1):120-25. [PMID: 15668484]

                    4. Ghosh S, Banerjee S, Sil PC. The beneficial role of curcumin on inflammation, diabetes and neurodegenerative disease: A recent update. Food Chem Toxicol. 2015 Sep;83:111-24. [PMID: 26066364]

                    5. Sanmukhani J, Satodia V, Trivedi J, et al. Efficacy and safety of curcumin in major depressive disorder: a randomized controlled trial. Phytother Res. 2014 Apr;28(4):579-85. [PMID: 23832433]
                    6.Baum L, Lam CW, Cheung SK, et al. Six-month randomized, placebo-controlled, double-blind, pilot clinical trial of curcumin in patients with Alzheimer disease.
                    J Clin Psychopharmacol. 2008 Feb;28(1):110-13. [PMID: 18204357]

                    7. Antony B, Merina B, Iyer VS, et al. A pilot cross-over study to evaluate human oral bioavailability of BCM-95CG (Biocurcumax), a novel bioenhanced preparation of curcumin. Indian J Pharm Sci. 2008 Jul-Aug;70(4):445-9. [PMID: 20046768]

                    8. Honda S, Aoki F, Tanaka H, et al. Effects of ingested turmeric oleoresin on glucose and lipid metabolisms in obese diabetic mice: a DNA microarray study. J Agric Food Chem. 2006 Nov 29;54(24):9055-62. [PMID: 17117790]

                    9. Singh V, Jain M, Misra A, et al. Curcuma oil ameliorates insulin resistance & associated thrombotic complications in hamster & rat. Indian J Med Res. 2015 Jun;141(6):823-32. [PMID: 26205026]

                    10. Nishiyama T, Mae T, Kishida H, et al. Curcuminoids and sesquiterpenoids in turmeric (Curcuma longa L.) suppress an increase in blood glucose level in type 2 diabetic KK-Ay mice. J Agric Food Chem. 2005 Feb 23;53(4):959-63. [PMID: 15713005]

                    11. Shishu M. Comparative bioavailability of curcumin, turmeric and BiocurcumaxTM in traditional vehicles using non-everted rat intestinal sac model. J Funct Foods. 2010; 2(1):60-65. [on file]

                    12. Benny M, Antony B. Bioavailability of BiocurcumaxTM (BCM-095TM). Spice India. 2006; Sept:11-15. http://geronova.com/wp-content/uploads/2013/06/Spice_Board.pdf. Accessed September 22, 2015.

                    13. Buhrmann C, Kraehe P, Lueders C, et al. Curcumin suppresses crosstalk between colon cancer stem cells and stromal fibroblasts in the tumor microenvironment: potential role of EMT. PLoS One. 2014 Sep 19;9(9):e107514. [PMID: 25238234]

                    14. Shakibaei M, Buhrmann C, Kraehe P, et al. Curcumin chemosensitizes 5-fluorouracil resistant MMR-deficient human colon cancer cells in high density cultures. PLoS One. 2014 Jan 3;9(1):e85397. [PMID: 24404205]

                    15. Toden S, Okugawa Y, Jascur T, et al. Curcumin mediates chemosensitization to 5-fluorouracil through miRNA-induced suppression of epithelial-to-mesenchymal transition in chemoresistant colorectal cancer. Carcinogenesis. 2015 Mar;36(3):355-67. [PMID: 25653233]

                    16. Toden S, Okugawa Y, Buhrmann C, et al. Novel evidence for curcumin and boswellic acid-induced chemoprevention through regulation of mir-34a and mir-27a in colorectal cancer. Cancer Prev Res (Phila). 2015 May;8(5):431-43. [PMID: 25712055]

                    17. Shakibaei M, Buhrmann C, Kraehe P, et al. Curcumin chemosensitizes 5-fluorouracil resistant MMR-deficient human colon cancer cells in high density cultures. PLoS One. 2014 Jan 3;9(1):e85397. [PMID: 24404205]

                    18. Sanmukhani J, Anovadiya A, Tripathi CB. Evaluation of antidepressant like activity of curcumin and its combination with fluoxetine and imipramine: an acute and chronic study. Acta Pol Pharm. 2011 Sep-Oct;68(5):769-75. [PMID: 21928724]

                    19. Lopresti AL, Maes M, Meddens MJ, et al. Curcumin and major depression: a randomised, double-blind, placebo-controlled trial investigating the potential of peripheral biomarkers to predict treatment response and antidepressant mechanisms of change. Eur Neuropsychopharmacol. 2015 Jan;25(1):38-50. [PMID: 25523883]

                    20. Lopresti AL, Maes M, Maker GL, et al. Curcumin for the treatment of major depression: a randomised, double-blind, placebo controlled study. J Affect Disord. 2014;167:368-75. [PMID: 25046624]

                    21. Kizhakkedath R. Clinical evaluation of a formulation containing Curcuma longa and Boswellia serrata extracts in the management of knee osteoarthritis. Mol Med Rep. 2013 Nov;8(5):1542-48. [PMID: 24002213]

                    22. Hejazi J, Rastmanesh R, Forough-Azam T, et al. A pilot clinical trial of radioprotective effects of curcumin supplementation in patients with prostate cancer. J Cancer Sci Ther. 2013;5(10):320-24. http://www.omicsonline.org/a-pilot-clinical-trial-of-radioprotective-effects-of-curcumin-supplementation-in-patients-with-prostate-cancer-1948-5956.1000222. php?aid=19259. Accessed September 22, 2015.

                    23. Leray V, Freuchet B, Le Bloc’h J, et al. Effect of citrus polyphenol- and curcumin-supplemented diet on inflammatory state in obese cats. Br J Nutr. 2011 Oct;106 Suppl 1:S198-201. [PMID: 22005428]

                    24. Horohov D, Sinatra S, Chopra R, et al. The effect of exercise and nutritional supplementation on proinflammatory cytokine expression in young racehorses during training. J Equine Vet Sci. 2012; 32:805-15. http://www.equinenutriceuticals.com/pdf/Exercise-inflammation-paper-with-back.pdf. Accessed September 22, 2015.

                    25. Yan J, Katz AE. ProstaCaid induces G2/M cell cycle arrest and apoptosis in human and mouse androgen-dependent and-independent prostate cancer cells. Integr Cancer Ther. 2010 Jun;9(2):186-96. [PMID: 20587444]

                    26. Jiang J, Eliaz I, Sliva D. Suppression of growth and invasive behavior of human prostate cancer cells by ProstaCaidTM: mechanism of activity. Int J Oncol. 2011 Jun;38(6):1675-82. [PMID: 21468543]

                    27. Jiang J, Loganathan J, Eliaz I, et al. ProstaCaid inhibits tumor growth in a xenograft model of human prostate cancer. Int J Oncol. 2012 May;40(5):1339-44. [PMID: 22293856]
                    28. Jiang J, Wojnowski R, Jedinak A, et al. Suppression of proliferation and invasive behavior of human metastatic breast cancer cells by dietary supplement BreastDefend.
                    Integr Cancer

                    Ther. 2011 Jun;10(2):192-200. [PMID: 20926736]
                    29. Baum L, Cheung SK, Mok VC, et al. Curcumin effects on blood lipid profile in a 6-month human study.
                    Pharmacol Res. 2007 Dec;56(6):509-14. [PMID: 17951067]

                    30. Cheng AL, Hsu CH, Lin JK, et al. Phase I clinical trial of curcumin, a chemopreventive agent, in patients with high-risk or pre-malignant lesions. Anticancer Res. 2001 Jul- Aug;21(4B):2895-900. [PMID: 11712783]

                    Recently viewed