Hèhè, thanks. The joke issue is my problem, not yours. The thrust of my "joke" was 99% banality. Sorry.
A related issue is that what wonders me in this thread are the short-term observations that seem to prevail the long-term benefits. I'm taking 200mg TRES for about a week now. So I do not belong to the 500mg club. But my metabolism functions in such a way that I have comparable effects with half the supplement dosage than that is used in general for various substances. Anyway, taking 200mg also elevates my mood and "energy" big-time, as also has been reported by others. In the beginning, but still in the 100mg period, I did experience some GI effects that could be described as "explosive". Fortunately, they vanished completely. Individuals (e.g. Duke N. ) using the 99% pure form are stating that the otherwise mentioned short term beneficial effects do not occur on them. Mind raised the hypothesis that people who already have an optimal supplement regime might not experience much additional benefits of TRES on short notice. However, my concern is that the non-TRES part of the resveratrol capsules might be responsible for these short-time effects in stead of the prim airy contents. Which causes me to be cautious; (a) we do not have long-term data on human use of TRES and (b) we are lacking data on the non-TRES contents of the stuff we are taking and data on purity of non-synthetic resveratrol products in general.
Ok, why am I taking it when i'm that pedantic? I do have some auto-immune related issues with some of my joints. The issues are not severe, but tolerable to a certain level. Imuno-suppresive medication is out of order since the symptoms are not that severe to justify the side effects of these treatments. So, TRES is one of my current "experiments". I do not have current data yet on my blood markers for inflammation, but they will be updated in 2 months.
Resveratrol and curcumin suppress immune response through CD28/CTLA-4 and CD80 co-stimulatory pathway.Sharma S, Chopra K, Kulkarni SK, Agrewala JN.
Immunology Laboratory, Institute of Microbial Technology, Chandigarh, India.
The role of resveratrol and curcumin is well documented in cancer, inflammation, diabetes and various other diseases. However, their immunosuppressive action on T cells, B cells and macrophages is not well documented. In the present study, we have ascertained the effect of resveratrol and curcumin on T and B cells and macrophages. The most striking findings were that both resveratrol and curcumin suppressed the activity of T and B cells and macrophages, as evidenced by significant inhibition in proliferation, antibody production and lymphokine secretion. Interestingly, curcumin imparted immunosuppression by mainly down-regulating the expression of CD28 and CD80 and up-regulating CTLA-4. Resveratrol also functioned by decreasing the expression of CD28 and CD80, as well as by augmenting the production of interleukin (IL)-10.
PMID: 17177975
Effects of resveratrol in inflammatory arthritis.Elmali N, Baysal O, Harma A, Esenkaya I, Mizrak B.
Department of Orthopaedics and Traumatology, Inonu University Medical Faculty, 44069, Malatya, Turkey, nelmali@hotmail.com.
Nuclear factor kappa B (NF-kappaB), is a pivotal transcription factor involved in the activation of the TNF-alpha and IL-1beta genes. Activation of NF-kappaB in synovial cells is a feature seen in arthritis patients. Resveratrol, a polyphenolic, natural phytoalexin found with particularly high levels in grape skin and red wine is potent and specific inhibitor of TNF-alpha and IL-1beta induced NF-kappaB activation. We aimed to determine the in vivo effects of intra-articular injections of resveratrol on cartilage and synovium in an experimental rabbit inflammatory arthritis model. MATERIALS AND METHODS: Arthritis was induced by intra-articular injection of three times of 50 mug lipopolysaccharide (LPS) at day 0, 4 and 8 at 4-day intervals into the knee joints of rabbits. To the test group, 10 muMol/kg resveratrol in the DMSO was injected in the knees at day 0 and then it was continued once daily for 2 weeks. To the control group the same time and amount of DMSO was injected the knees of rabbits. All rabbits were killed 1 week after the last injection and cartilage tissue and synovium were evaluated with semiquantitative scoring histologically. RESULTS: According to control group in the resveratrol group, significantly decreased cartilage destruction was determined by H&E staining (p = 0.04). Loss of matrix proteoglycan content in the cartilage was much lower, as determined by safranin O staining (p = 0.03). We also observed marked synovial inflammation after intra-articular injection to control knees, but not in the resveratrol treated group knees (p = 0.01). CONCLUSION: This study suggests that intra-articular injection of resveratrol may protect cartilage against the development of experimentally induced IA.
PMID: 17115116
Effect of resveratrol in experimental osteoarthritis in rabbits.Elmali N, Esenkaya I, Harma A, Ertem K, Turkoz Y, Mizrak B.
Department of Orthopaedics and Traumatology, Inonu University Medical Faculty, 44069, Malatya, Turkey. nelmali@hotmail.com
OBJECTIVE: Resveratrol (trans-3,4',5-trihydroxystilbene) is a phytoalexin found in high concentration in the skins of grapes and red wines which has been shown to have antiinflammatory, anticancerogen and antioxidant properties. Resveratrol is a potent and specific inhibitor of nuclear factor kappa B (NF-kappaB). Resveratrol also inhibits COX-2 gene expression and enzyme activity. We aimed to determine the in vivo effects of intra-articular injections of resveratrol on cartilage and synovium in an experimental osteoarthritis (OA) model in rabbits. METHODS: As OA model, rabbits underwent unilateral anterior cruciate ligament transection (ACLT). Five weeks after test group was injected with 10 microMol/kg resveratrol in dimethylsulphoxide (DMSO) in the knees once daily for two weeks and as the control group at the same time DMSO was injected into the knees. All rabbits were killed one week after the last injection. Cartilage tissue and synovium were evaluated with a histological scoring system. RESULTS: Histological evaluation of cartilage tissue by H&E staining revealed a significantly reduced average cartilage tissue destruction score of 1.7 in the resveratrol group versus 2.8 in the control group (p = 0.016). Loss of matrix proteoglycan content in cartilage was also much lower, as determined by safranin O staining. Scores of synovial inflammation didn't show difference between groups (1.3 vs 2.2; p = 0.057). CONCLUSION: A characteristic parameter in arthritis is the progressive loss of articular cartilage. This study suggests that intraarticular injections of resveratrol starting at the onset of disease may protect cartilage against the development of experimentally induced OA.
PMID: 15883738
Inhibition of COX isoforms by nutraceuticals.Seaver B, Smith JR.
University of Montana, 441 S. 6th E., Missoula, MT 59812, USA.
Humans have two isoforms of Prostaglandin H Synthase or cyclooxygenase: COX-1 and COX-2. COX-1 is cytoprotective. COX-2 inhibitors reduce inflammation without the risk of ulceration and kidney damage. The ideal nutraceutical would inhibit COX-2 synthesis while preserving COX-1 synthesis. The hypothesis for this research was that COX inhibitors would fall primarily into three categories: COX-2 specific inhibition, non-specific inhibition (COX-1 and COX-2), and minimal inhibition. The human Cayman COX inhibitor screening assay was used to determine the inhibitory concentration 50 (IC50) of COX-1/ COX-2 activity of each nutraceutical. The assay was run, in duplicate, with three concentrations of a suspected inhibitor, a standard curve of eight concentrations, a non-specific binding sample, and a maximum binding sample. The inhibition and concentration of each sample was then put on a multiple regression best-fit line and the IC50 determined. For comparison, ibuprofen, rofecoxib, naproxen, and indomethacin were used. Positive results were seen for ipriflavone, resveratrol, MSV-60, amentoflavone, ruscus extract and notoginseng. Glucosamine, nexrutine, and berberine did not inhibit either isoform.
PMID: 15364641
Worrying (just a bit):
Potential pro-inflammatory action of resveratrol in vascular smooth muscle cells from normal and diabetic rats.Cignarella A, Minici C, Bolego C, Pinna C, Sanvito P, Gaion RM, Puglisi L.
Department of Pharmacological Sciences, University of Milan, via G. Balzaretti 9, I-20133 Milan, Italy. andrea.cignarella@unimi.it
BACKGROUND AND AIM: Based on the reported cardioprotective effects of resveratrol, a polyphenolic antioxidant abundant in grapes that binds to estrogen receptors, and the well-characterized anti-inflammatory properties of 17beta-estradiol, the effects of resveratrol on the functional expression of inflammatory enzymes were assessed in vascular smooth muscle cells (SMC) from normoglycaemic and streptozotocin-diabetic rats. METHODS AND RESULTS: SMC were isolated from the aorta four weeks after treating rats with streptozotocin or its vehicle. In SMC exposed to a cytokine mixture for 24h, unexpectedly, treatment with resveratrol (0.1-100microM) as well as the structurally related isoflavone genistein (1nM-1microM) enhanced expression of inducible NO synthase (iNOS). Genistein failed to mimic the elevated iNOS activity induced by resveratrol. Inhibition of estrogen receptors by the pure antiestrogen ICI 182,780 reversed the action of resveratrol on iNOS. In addition, resveratrol failed to alter cyclooxygenase-2 protein levels but reduced the accumulation of prostaglandin E(2) in the culture medium of SMC from normoglycaemic, but not diabetic rats. CONCLUSIONS: These results indicate that resveratrol, at concentrations approaching putative peak plasma levels in vivo, exhibited no anti-inflammatory properties in vascular SMC from normal and diabetic rats. By contrast, resveratrol displayed a potential pro-inflammatory activity in settings of vascular inflammation.
PMID: 16829340
Many more of this kind of data available. Insight on the matter would be very much appreciated!
Edited by alterego, 25 March 2007 - 01:34 AM.
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