Ultra-absorbable curcumin for whole-body health support containing ultra-potent patented BCM-95® Curcumin. Shown to aid in lowering systemic inflammation, brain/immune/digestive health as well as antioxidant support.
60 Servings
Trained By JP Cure Coming
€34.99
In stock
In stock
Description
Trained By JP Cure Coming
Trained by JP Cure-Coming – an ultra-absorbable curcumin for whole-body health support containing ultra-potent patented BCM-95® Curcumin. Shown to aid in lowering systemic inflammation, brain/immune/digestive health as well as antioxidant support.
Additionally Curcumin, the bioactive component of turmeric, Curcuma longa has an exceptionally wide spectrum of activities most notably its antioxidant and anti-inflammatory properties. Postulated to have anti-depressive properties in major depressive patients as well as positive cognitive outcomes in older populations.
Curcumin inhibits pro-inflammatory transcription factors such as nuclear factor-kappa beta (NFK- B) which can effect joint inflammation. It also activates peroxisome proliferator–activated receptor gamma (PPAR-γ) and Nrf2 cell signaling pathways, leading to the downregulation of tumor necrosis factor (TNF) and interleukin-6 (IL-6), and upregulates adiponectin (the hormone involved in blood glucose and fatty acid breakdown made by adipose fat tissue).
In simple terms, curcumin has the potential to lower C-Reactive Protein (CRP; a measure of inflammation in the body), induce autophagy through mTOR inhibition (the selective destruction of damaged cellular organelles), protect against cardiac hypertrophy, and potentially decrease artherosclerosis risk.
Despite the promising nutritional and pharmacological properties of curcumin, it exhibits low aqueous solubility, poor gastrointestinal absorption and poor bioavailability.
Its high rate of metabolism, metabolic inactivation and rapid elimination from the body makes it difficult to yield appreciable plasma concentrations. Because of its poor oral absorption, it is difficult for orally administered curcumin to reach blood levels sufficient to exert its bioactivities. Poor absorption from the gut and avid metabolism in the body is cited as reasons for the lack of systemic availability.
To overcome this problem, several curcumin preparations with drug-delivery systems (DDS) have been developed to increase the bioavailability of curcumin after oral administration.
Combinations with piperine have been most common. Piperine, an inhibitor of phase II liver metabolism and intestinal glucuronidation. In rats, the bioavailability of curcumin increased by 154% with piperine compared with a control group without piperine. In humans, piperine (20 mg/kg) co-administered with curcumin (2 g) and the bioavailability 20-times that of the control group. However, enhancing bioavailability by inhibiting phase II metabolism must be carefully carried out since many compounds are detoxified through this liver route which may be slowed by adminstering piperine.
BCM-95® is a novel bio-enhanced preparation of curcumin with the addition of phosphatidylcholine and turmeric essential oils. Leads to enhanced and sustained absorption. In a human study, 2g administration showed the bioavailability of BCM-95 to be almost 6.93-fold higher than that of a control curcumin formulation with no additive. The half life shown to be approx 4.96 h compared to 2.6 h for the control. 2 g/day dose levels well tolerated without even mild adverse reactions. However, the mechanisms of these enhancements are unknown.
Additionally Trained by JP are proud to produce Cure-Coming; a supplement which we believe supports the health of nearly every organ in your body.
Formulated alongside Dr Dean St Mart.
Additionally here are some references
Antony, B et al. A Pilot Cross-Over Study to Evaluate Human Oral Bioavailability of BCM-95®CG (Biocurcumax™), A Novel Bioenhanced Preparation of Curcumin. Indian J Pharm Sci. 2008. 70(4): 445–449.
Kurita, T. Novel Curcumin Oral Delivery Systems. Anticancer Research. 2013. 33(7): 2807-2821.
Tatti, M et al. BCM-95 and (2-hydroxypropyl)-β-cyclodextrin reverse autophagy dysfunction and deplete stored lipids in Sap C-deficient fibroblasts. Human Molecular Genetics. 2015. 24(15): 4198–4211.
Karawi, D et al. The Role of Curcumin Administration in Patients with Major Depressive Disorder: Mini Meta‐Analysis of Clinical Trials. Phytotherapy Research. 2015. 30 (2): 176-183.
Also Rainey-Smith, S R et al. Curcumin and cognition: a randomised, placebo-controlled, double-blind study of community-dwelling older adults. British Journal of Nutrition. 2016. 115 (12): 2106-2113.
Purpura M et al. Analysis of different innovative formulations of curcumin for improved relative oral bioavailability in human subjects. Eur J Nutr. 2018. 57(3): 929–938.
Hewlings, S et al. Curcumin: A Review of Its’ Effects on Human Health. Foods. 2017. 6(10): 92.
Also see https://examine.com/supplements/curcumin
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