Naturopathic Medicine in Pain Management 4/11/2008
4/11/2008 Naturopathic Medicine in Pain Management Rick Marinelli, N.D., M.Ac.O.M. Clinical Professor NCNM 1600 SW Cedar Hills Blvd. Portland, Oregon, 97225 www.natural-healthmedicine.com Naturopathic Principles • • • • • • First do no harm Find the cause Treat the whole person Prevention is the best cure Let nature do the healing Physician as teacher Naturopathic Physicians in Oregon • • • • Are primary care yet focus on chronic conditions Order and utilize all types of diagnostic tests Have a Formulary Tend to emphasize healthy lifestyle changes, especially – – – – Diet Exercise Relaxation and stress reduction The use of herbal, homeopathic, and nutritional supplements 1 4/11/2008 First Intervention is Dietary and Individualized • Emphasis is initially on reducing refined carbohydrates, optimizing protein, fatty acid and micronutrient intake • Excess CHO intake has negative effect on insulin metabolism, weight gain, inflammation (perhaps 60%) • Insufficient protein limits repair and regeneration (~30% < RDA) • Excess (n-6 PUFAs) promote inflammation, cancer, poor circulation and contribute to decline Excess CHOs • Decreased tolerance to carbohydrates with aging • Epidemic of obesity, DM continuum, cardiovascular disease, hypertension • Need N d lless caloric l i intake i k with i h aging i andd less l calories decreases aging rate • Generally better to markedly increase vegetables (increased flavonoid and micronutrient intake) and fruit intake than to rely on grains for carbohydrates Protein Optimization • Protein synthesis is decreased with aging and therefore increased intake is usually necessary • Protein-energy malnutrition is associated with impaired muscle function, decreased bone mass, immune dysfunction, anemia, reduced cognitive function, poor wound healing, delayed recovery from surgery, and ultimately increased morbidity and mortality 2 4/11/2008 Protein Optimization • Common medical conditions such as gastrointestinal disease, malabsorption syndromes, acute and chronic infections, and hypermetabolism often cause anorexia, anorexia micronutrient deficiencies, and increased energy and protein requirements • Chronic pain patients are major users of prescription medications, which can cause malabsorption of nutrients, gastrointestinal symptoms, and loss of appetite Micronutrients for OA • A daily 12oz nutritional beverage containing milkbased micronutrients, vitamins, and minerals was beneficial in alleviating pain symptoms and dysfunction in subjects with osteoarthritis (n=31) Nutrition 2002 May;18(5):388-92 • Low intake of micronutrients (vitamins C, E, and D, and beta-carotene) may adversely influence the progression of knee OA and the incidence of hip OA Curr Rheumatol Rep. 1999 Oct;1(1):48-53 Fatty Acid Immune Modulation • Reduction in the amount of fat intake enhances several indices of immune response, including lymphocyte proliferation, natural-killer-cell activity cytokine production, activity, production and delayed delayed-type type hypersensitivity • Intake of omega-3 fatty acids reduced production of inflammatory eicosanoid mediators (prostaglandin E2 and leukotriene B4) by neutrophils, monocytes, and lymphocytes • Nutrition 2001 Jul-Aug;17(7-8):669-73 3 4/11/2008 Omega 6s as Agents of Inflammation and Decline • Omega-6 PUFAs , abundant in the Western diet, are precursors for a number of key mediators of inflammation including the 2series of prostaglandins and IL-6 IL 6 • PGE2 , a cyclooxygenase (COX) metabolite of arachidonic acid, an omega-6 PUFA, is a potent mediator of inflammation and cell proliferation • Omega 6s examples include safflower, corn, soybean, and cottonseed oils • Proc Natl Acad Sci U S A. 2003 Feb 18;100(4):1751-6 Omega-6s More Toxic Than You Think • Known to increase not only risk of cancer but metastatic invasion Br J Cancer 2006 Mar 7 • Soybean oil emulsion (TPN) decreased lymphocyte proliferation and provoked neutrophil and lymphocyte apoptosis and necrosis JPEN 2006 Mar-Apr;30(2):115-23. • Compared to omega-3s, impaired immune function and symptoms in Crohn’s and Sjogren’s Aliment Pharmacol Ther 2005 Dec;22(11-12):1121-8, Invest Opthalm Vis Sci 2005 Dec;46(12):4474-9. Fatty Acid Modulation Omega 3s (N-3) • N-3 Fatty acids favorably affect atherosclerosis, coronary heart disease, inflammatory disease, behavioral disorders • Docosahexaenoic acid, DHA (22:6n3), which is a vital component of the phospholipids of cellular membranes, especially in the brain and retina, is necessary for their proper functioning • Importance of n-3 fatty acids in health and disease, Connor WE Am J Clin Nutr 2000 Jan;71(1 Suppl):171S-5S 4 4/11/2008 Fish Oil as Solution • Increasing the omega-3 content of membrane phospholipid results in a decrease in mitogen-induced PGE(2) synthesis h i • Data suggest that replacement of omega6 PUFA with omega-3 PUFA in cell membranes can result in a decreased cellular response to mitogenic and inflammatory stimuli • Proc Natl Acad Sci U S A. 2003 Feb 18;100(4):1751-6 Fish Oil as Healer • Reduction in strokes • Decrease in arthritis pain • Decrease in collagen and bone degrading enzymes • Modulate inflammation in IBD, autoimmune disorders, RA, dermatitis, asthma, sickle cell pain episodes • Preliminary evidence of cancer prevention, (lung, breast, colon), treatment of cachexia N-3 FA in Arthritis • N-3 fatty acids specifically modulate catabolic factors involved in articular cartilage degradation • Dose related reduction in the expression and activity of proteoglycan degrading enzymes (aggrecanases) • Reduced expression of inflammation-inducible cytokines (interleukin (IL)-1alpha and tumor necrosis factor (TNF)-alpha) and cyclooxygenase (COX-2) – but not the constitutively expressed cyclooxygenase COX-1 • J Biol Chem 2000 Jan 14;275(2):721-4 5 4/11/2008 Fish Oil in Arthritis • Omega 3s reduced, in a dose-dependent manner, the endogenous and IL-1-induced release of proteoglycan metabolites from articular cartilage explants and specifically abolished endogenous aggrecanase and collagenase proteolytic activity • Omega 3s abolished the expression of mRNA for mediators of inflammation (cyclooxygenase 2, 5-lipoxygenase, 5-lipoxygenase-activating protein, TNF- alpha, IL-1alpha, and IL-1beta) without affecting the expression for other proteins involved in normal tissue homeostasis Arthritis Rheum. 2002 Jun;46(6):1544-53. Omega-3 in Cancer • Modulation of omega-3/omega-6 polyunsaturated ratios with dietary fish oils in men with prostate cancer. Urology. 2001 Aug;58(2):283-8. • M Modulation d l i off experimental i l colon l tumorigenesis i i by types and amounts of dietary fatty acids. Cancer Res. 2001 Mar 1;61(5):1927-33. • Three percent dietary fish oil concentrate increased efficacy of doxorubicin against mda-mb 231 breast cancer xenografts. Clin Cancer Res. 2001 Jul;7(7):2041-9. Fish Oil as Stroke Prevention in Women • A significantly reduced risk of thrombotic infarction was found among women who ate fish 2 or more times per week (multivariate RR, 0.49; 95% CI, 0.26-0.93) • Women in the highest quintile of intake of long-chain omega-3 polyunsaturated fatty acids had reduced risk of total stroke and thrombotic infarction, with multivariate RRs of 0.72 (95% CI, 0.53-0.99) and 0.67 (95% CI, 0.42-1.07), respectively JAMA 2001 Jan 17;285(3):304-12 6 4/11/2008 Omega-3 In Other Disorders • The emerging role of omega-3 polyunsaturated fatty acids in the management of patients with IgA nephropathy • J Ren Nutr. 2001 Jul;11(3):122-8. • Prevention of sudden death in CAD • Am J Clin Nutr. 2003 Jul;78(1):65-71 • Lower risk of death (especially arrhythmic IHD death) in ischemic heart disease • Circulation 2003 Mar 18;107(10):1372-7 • Decreases perimenopausal bone loss • Prostaglandins Leukot Essent Fatty Acids. 2003 Jun;68(6):361-72 Exercise Improves Health, Vitality, Bodily Pain • General practitioners were prompted by the patient to give oral and written advice on physical activity during usual consultations • For every 10 green prescriptions written, one person achieved hi d andd sustained i d 150 minutes i off moderate d or vigorous leisure activity per week, at 12 months • Measures of self rated "general health," "role physical," "vitality," and "bodily pain" improved significantly • Trend (but not significant) in lowering BP • BMJ 2003 Apr 12;326(7393):793. 7 4/11/2008 EXERCISE Stretching and Strength Training • Increases muscle mass and vascularity thereby increasing oxygenation • Increases hGH, testosterone, and decreases insulin resistance • Increases ligamentous strength and mass • Increases TIMPs • Inhibits Myosin Heavy Chain degradation • A great anti-depressant as well Strength training in the elderly: effects on risk factors for age-related diseases • In addition to improved strength, function, endurance, muscle mass and power • Reduces insulin resistance • Decreases D bboth h totall andd intra-abdominal i bd i l fat f • Increases resting metabolic rate in older men • Prevents the loss of BMD with age • Reduces risk factors for falls • May reduce pain and improve function • Sports Med. 2000 Oct;30(4):249-68 Water, Nature Cure and Naturopathy • Central thesis: Fresh air, sunshine, a proper diet without overeating, exercise, scientific relaxation, constructive thinking and the right mental attitude, along with prayer and meditation create a sound mind in a sound body • Most people must be concomitantly treated with herbs, supplements or drugs till a healthier state is reached 8 4/11/2008 Herbal and Supplemental Approaches to Pain Management • Nutraceuticals – Common examples are the GAGs ( GS, CS, HA) MSM, DLPA, Amino acids, fish oils, antioxidants, vitamins, minerals,, and enzymes, y , pprobiotics • Herbal extracts – Vast pharmacopoeia from Western and Eastern traditions – Common examples include Hypericum, Gingko, Corydalis, Ginger, Capsicum, Willow, Feverfew, Bromelain, Kava, Turmeric, Valerian, Licorice, Boswellia, Hawthorne, Scutellaria, Noni, Mangosteen Glucosamine as a Collagen Type II Enhancing, Pain Relieving Supplement • Glucosamine sulfate is a Biological Response Modifier of chondrocytes under conditions of joint stress Osteoarthritis Ot th iti Cartilage. C til 2003 May;11(5):335-42 M 11(5) 335 42 • Reduces knee OA symptoms and progression – Lancet. 2001 Jan 27;357(9252):251-6. • Decreases MMP-3 and aggrecanase expression – Osteoarthritis Cartilage. 2003 Jun;11(6):424-32. Chondroitin Sulfate • While GS is extracted from crab, shrimp, or lobster shell and is a smaller molecule and easily absorbed, CS is extracted from trachea cartilage, is a larger proteoglycan and is not a easily absorbed orally • CS is probably more chondroprotective than chondroregenerative, inhibits bradykinin formation • Topical applications may be better than oral CS GAIT trial showed combination with Glucosamine helped those most severely affected New Engl J Med 2006 Feb 23;354(8):795-808 9 4/11/2008 Proteolytic Enzymes in Inflammation • • • • Bromelain B l i Plant Proteases Trypsin/Chymotrypsin Pancreatic enzymes Proteolytic Enzymes in Inflammation: Historical • Clinical application of plant protease (Kimotab) in the surgical field. Nippon Geka Hokan. 1966 Mar 1;35(2):395-40 • Clinical note on fluidifying activity on bronchial secretions by a plant proteolytic enzyme]. Gaza Int Med Chir. 1965 Sep 15;70(17):1455-67 • Enzyme therapy of pulpo-apical affections. The lysozyme]. Rev Fr Odontostomatol. 1968 Aug-Sep;15(7):947-50 Bromelain : Ananas comusus • Introduced in the U.S. 1957 ; was marketed as Ananase in the ’60s • Therapeutic applications – Aids digestion – Anti-inflammatory Anti inflammator – Prevents edema – Inhibition of platelet aggregation – Enhanced wound healing – Enhanced antibiotic absorption/antibiotic activity 10 4/11/2008 Bromelain : Ananas spp Anti-inflammatory and Wound Healing Activity • Several mechanisms of action – Activation of proteolysis at site of inflammation – Fibrinolysis Fib i l i via i plasminogen-plasmin l i l i system t – Depletion of kininogen – Inhibition of inflammatory prostaglandins and induction of PGE1 – Induction of the wound healing cytokine IL-6 Clin Exp Immunol 2006 Jan;143(1):85-92 Bromelain : Ananas spp • Studies in RA/OA with/without curcumin there was reduced need for corticosteroids • Significant reduction in swelling, bruising, pain, healing time post-surgery • Athletic injuries reduction of bruising , edema, healing time Bromelain : Ananas spp Clinical Applications • Thrombophlebitis - numerous studies • DBPC of 73 patients with acute thrombophlebitis reduced all symptoms of inflammation including pain edema, pain, edema redness, redness elevated skin temperature at dose of 400-800 mg (high-strength, >1800 mcu) • Seligman B: oral Bromelains as adjuncts in the treatment of acute thrombophlebitis. Angiology 20, 22-26, 1969 11 4/11/2008 Bromelain : Ananas spp Clinical Applications • Musculoskeletal injuries(contusions, muscle strains/sprains, ligament tears) – By decreasing fibrin, bromelain helps promote circulation and post-traumatic resorption of inflammatory by-products • Masson M. Bromelain in the treatment of blunt injuries to the musculoskeletal system. A case observation study by an orthopedic surgeon in private practice. Fortschr Med 113(19):303-306. 1995 Bromelain : Ananas spp Clinical Applications • May help post-operative ileus Life Sci 2006 Jan 25;78(9):995-1002 • May benefit chronic inflammatory, inflammatory malignant and autoimmune diseases via the innate as well as the adaptive immune system Eur J Med Res 2005 Aug 17;10(8):325-31 • Acute sinusitis in children In Vivo 2005 MarApr;19(2):417-21. Oral Enzyme Equivalence With NSAIDs in Arthritis • In patients suffering from painful osteoarthritis of the knee, periarthritis of shoulder, and painful vertebral syndromes there was a statistical equivalence of the pain-scores, comparing diclofenac and enzymes. The study demonstrated equivalence of the treatment with NSAIDs compared to therapy with enzymes. • Wien Med Wochenschr 1999;149(21-22):577-80 12 4/11/2008 NSAIDs vs. Oral Enzymes in Rheumatic Disease • Data of 3326 patients treated for rheumatic diseases between 1/93 and 3/95 were registered by 380 physicians • Joint diseases, spinal diseases, rheumatic soft tissue diseases • Treatment success (freedom from symptoms) with OE can be expected with a higher probability than with NSAID. OE were well tolerated showing much less adverse events when compared with conventional doses of NSAID. • Arzneimittelforschung 2000 Aug;50(8):728-38 Oral Enzymes vs. Diclofenac in Knee OA • • • • • Double blind prospective RCT N=103 Enzymes (ERC) = rutosid, trypsin, bromelain Tx for 6 wks Outcome = Lequesne’s Algofunctional Index, and a “complaint index”, physician assessment • Conclusion: Enzymes as safe and effective as NSAIDs in painful OA episodes Clin Rheum 2004 Oct;23(5):410-5 Oral Enzymes in Alzheimer’s Disease • Complexes with trypsin, alphachymotrypsin, and bromelain strongly degrade (1,25) I-Amyloid beta 1--42 • These results suggest that up-regulation of Amyloid beta catabolism could probably reduce the risk of developing AD by preventing Amyloid beta accumulation in brain and vasculature Exp Neurol 2001 Feb;167(2):385-92 13 4/11/2008 Oral Enzymes in Myocardial Infarction • Facilitates normalization of the atherogenic potential and has a positive action on the mediators of the i fl inflammatory process. The effect of Wobenzym on the atherogenic potential and inflammatory factors at the rehabilitation stage for patients who have had a myocardial infarct Lik Sprava 2000 Jul-Aug;(5):111-4 Oral Enzymes in Chronic Prostatitis • Urethrogenic prostatitis: 1) association with pancreatic pathology, 2) the presence of noninfectious agent, 3) autoimmune character h t • Treatment includes Wobenzyme as part of a pathogenetic therapy with positive results • Lik Sprava 1998 Aug;(6):118-20 Flavonoids • Are pigments in food and herbs • Tea, apples, wine, berries, fruits,vegetables and nuts are primary dietary sources • Inverse relationshipp of dietaryy flavonoids and cardiovascular disease, stroke, and cancer in multiple analyses from Zutphen Elderly Study • Common flavonoids are polyphenols such as resveratrol, catechins, quercitin, naringen, pro/anthocyanidins • Generally have antioxidant, circulation enhancing, collagen stabilizing effect. New evidence suggests may control aging through sirtuin activation. 14 4/11/2008 Flavonoids • Middleton et al. The effects of plant flavonoids on mammalian cells: implications for inflammation, heart disease, disease and cancer. cancer Pharmacol Rev 2000 Dec;52(4):673-751 • Reduces ROS that are pivotal in hypertension, atherosclerosis, Type II DM, cancer, Alzheimer’s, shortened lifespan, pain and disease. Activate sirtuins like caloric restriction J Hypertens 2005 Jul;23(7):1285-309 Grape Seed Extract Oligoproanthocyanidins(OPCs) Pharmacology • • • • Increase intracellular Vit. C Decrease capillary permeability Scavenge free radicals and oxidants Inhibit destruction of collagen by crosslinking collagen fibers • Inhibits the release and synthesis of histamine, PGs, leukotrienes, serine proteases Schwitters, Masquelier.OPC in Practice: Bioflavanols and their Application.Alfa Omega, Rome1993 Green Tea and Osteoarthritis • ECGC selectively inhibits IL-1β induced catabolism of chondrocytes • ECGC selectively inhibits IL-1β induced activity and expression of COX COX-22 and NO synthase synthase-22 in human chondrocytes • J Orthop Res. 2003 Jan;21(1):102-9 • Free Radic Biol Med. 2002 Oct 15;33(8):1097-105 • Arthritis Rheum. 2002 Aug;46(8):2079-86. 15 4/11/2008 Inhibiting Soft-tissue Inflammation and Collagen Degradation(GTP) • Green tea polyphenols(GTP) inhibit MMP-2, MMP-9 and MMP-12 in vitro (elastin,gelatin) and in vivo1 (human glioblastoma,pituitary tumors) • Most potent of these were the catechins ECG and EGCG but included resveratrol, genistein, and organosulfur compounds from garlic • 1Biochim Biophys Acta 2000 Mar 16;1478(1):51-60 Flavonoid Antioxidants and Sterols in Vegan Diet and Rheumatic disease • Uncooked vegan diet and consisting of berries, fruits, vegetables and roots, nuts, germinated seeds and sprouts resulted in a decrease of their joint stiffness and pain as well as an improvement of their self-experienced health in RA and FM pts. Toxicology 2000 Nov 30;155(1-3):45-53 • Ajoene, a natural product with non-steroidal antiinflammatory drug (NSAID)-like properties? Biochem Pharmacol 2001 Mar 1;61(5):587-93 Addressing Soft-tissue Inflammation and Collagen Degradation Serine Protease and MMP Inhibitors • • • • • • • • • OPCs/ Bioflavonoids/Antioxidants in general Catechins (green tea polyphenols) Boswellia Scutellaria, Triptyrigium, Angelica spp,Evodia GS,CS (Glycosaminoglycans,GAGs) Omega 3 oils NAC/MSM/Allicins (organosulfur compounds) Tetracyclines (Streptomyces spp) Statins (Aspergillis spp, Monascus purpureus) 16 4/11/2008 Antioxidants as Adjuvants in Rheumatic disease • Group I: Intramuscular methotrexate (CAS 59-05-2; 12.5 mg/week), oral sulphasalazine (CAS 599-79-1; 0.5 g b.i.d.) and indometacin (CAS 53-86-1; 100 mg suppository at bed-time). Groupp II: the patients received the standard treatment plus a combination of antioxidants. Group III:received a high dose of vitamin E (400 mg t.i.d.) in addition to the standard treatment. • With adjuvant therapy of either the antioxidant combination or a high dose of vitamin E the symptoms of arthritis were better controlled from the first month (n=30) • Arzneimittelforschung 2001;51(4):293-8 Antioxidants As Adjuvants in Alzheimer’s Disease • The products of inflammatory reactions such as prostaglandins (PGs; PGE1 and PGA1), free radicals, cytokines, and complement proteins are neurotoxic and inhibited by antioxidants • NSAIDs inhibit the synthesis of PGs, reduce the rate of deterioration of cognitive functions in patients with advanced AD • Cholinergic drugs are routinely used in the treatment of AD to improve cognitive functions • Therefore a combination of all are more likely to be effective • Clin Neuropharmacol 2000 Jan-Feb;23(1):2-13 Antioxidants in Pancreatitis • Treatment with a complex containing Lmethionine, beta-carotene, vitamin C, vitamin E and organic selenium • Of 10 patients with chronic pancreatitis who completed treatment, the intensity of pain was reduced considerably in 9 (61.5 +/- 21.5 mm vs. 19.6 +/- 26.1 mm, p = 0.03), and pain was completely absent in 3 of these patients Rev Esp Enferm Dig 2000 Jun;92(6):375-85 17 4/11/2008 Antioxidants: Chronic Hepatitis C • Phase I Clinical Trial, n=50 • Treated with Glycyrrhizin, Schisandra, Silymarin, ascorbic acid, lipoic acid, L-glutathione, and alphatocopherol), along with four different intravenous tocopherol) preparations (Glycyrrhizin, ascorbic acid, L-glutathione, B-complex) • Results: A combination of antioxidants induced a favorable response in 48% of the patients, was well tolerated and “may have a beneficial effect on necro-inflammatory variables.“ J Clin Gastroenterolgy 2005 Sep;39(8):737-42. Inflammation in Type II Diabetes, PCOS • Elevated levels of CRP and IL-6 predict the development of type 2 DM. These data support a possible role for inflammation in diabetogenesis. JAMA 2001 Jul 18;286(3):327 18;286(3):327-34 34 • “Women with PCOS have significantly increased CRP concentrations relative to women with normal menstrual rhythm and normal androgen levels. We propose low grade chronic inflammation as a novel mechanism contributing to increased risk of CHD and type 2 diabetes in these women J Clin Endocrinol Metab 2001 Jun;86(6):2453-5 Inflammation in Diabetes • Flavonoids diosmin (90%) and hesperidin (10%), in a group of 28 Type 1 diabetic patients in a double blind placebo-controlled study. Parameters of glycation and oxidative stress were measured before and after the i t intervention ti • Decrease in glycation and HgbA1c unrelated to glycemic control was noted, with increased glutathione peroxidase activity • Diabetes Nutr Metab 1999 Aug;12(4):256-63 18 4/11/2008 Vit C in Inflammatory Atherosclerosis • Peripheral arterial disease (PAD) is a severe atherosclerotic condition frequently accompanied by inflammation and oxidative stress • Subclinical vitamin C deficiency (<11.4 micromol/L) confirmed by low serum alkaline micromol/L), phosphatase activity, was found in 14% of the PAD patients • Vitamin C concentrations are lower in intermittent claudication patients, is associated with higher CRP levels and severity of PAD • Circulation 2001 Apr 10;103(14):1863-8 Low DHEAS in Inflammatory Disorders • Mean DHEAS level was markedly lower in pemphigus (as with systemic lupus erythematosus, rheumatoid arthritis, polymyalgia rheumatica, giant cell arteritis) (n (n=46) 46) • DHEAS levels were independent of steroid treatment • “DHEAS deficiency is a permanent feature in these autoimmune diseases, and may contribute to their etiology and/or pathophysiology” • Clin Exp Rheumatol 1995 May-Jun;13(3):345-8 Low DHEAS in Inflammatory Arthritis/Synovitis • Serum DHEAS and its relation to clinical variables in RA, spondyloarthropathy, and inflammatory arthritis in 87 pts was performed • “Low Low DHEAS concentrations are commonly encountered in inflammatory arthritis, especially in women” • “DHEA replacement may be indicated in many patients with IA” • Arthritis Res 2001;3(3):183-8 19 4/11/2008 Physical Medicine Modalities in Naturopathic Medicine • • • • • Traditional hydrotherapy Manual therapy/Manipulation Electrotherapy Ultra/Infra-Sound Needling therapies – – – – Acupuncture/Dry-needling Myofascial trigger point injections Neural therapy/Mesotherapy Prolotherapy (aka Regenerative Injection Therapy, RIT)) Ligaments and Tendons at the Fibro-Osseous Junction • Hackett postulated in 1939 that the major cause of back pain was tendon and ligament relaxation • In his initial animal experiments he demonstrated a 30-40% 30 40% increase in tendon size after injection with Sylnasol, later with zinc sulfate, and silica oxide • Introduced the term prolotherapy in 1956, emphasized the postulates of Steindler, developed maps of pain referral patterns Newer Studies In Prolotherapy • Randomized prospective double-blind placebocontrolled study of dextrose prolotherapy for knee osteoarthritis with or without ACL laxity • CONCLUSION: Prolotherapy injection with 10% dextrose resulted in clinically and statistically significant f improvements in knee osteoarthritis. Preliminary blinded radiographic readings (1-year films, with 3-year total follow-up period planned) demonstrated improvement in several measures of osteoarthritis severity. ACL laxity, when present in these osteoarthritic patients, improved. N=110 Altern Ther Health Med 2000 Mar;6(2):68-74, 77-80 20 4/11/2008 Newer Studies In Prolotherapy • “Long-term effects of dextrose prolotherapy for anterior cruciate ligament laxity” – At the 3 year follow-up, pain at rest, pain with walking, and pain with stair use had improved by 45%, 43%, and 35% respectively • CONCLUSION: In patients with symptomatic anterior cruciate ligament laxity, intermittent dextrose injection resulted in clinically and statistically significant improvement in ACL laxity, pain, swelling, and knee range of motion • Altern Ther Health Med. 2003 May-Jun;9(3):58-62 Newer Studies In Prolotherapy • Randomized, prospective, placebo-controlled doubleblind study of dextrose prolotherapy for joints: evidence of clinical efficacy • CONCLUSION CONCLUSION: Dextrose D t prolotherapy l th was clinically effective and safe in the treatment of pain with joint movement and range limitation in osteoarthritic finger joints. N=150 joints in 27 patients J Altern Complement Med 2000 Aug;6(4):311-20 Newer Studies in Prolotherapy Prolotherapy can be an effective therapeutic modality that reduces TMJ pain and noise in a majority of patients Cranio 2005 Oct;23(4):283-8 Chronic groin pain that h preventedd full f ll sports participation in elite kicking athletes treated with dextrose prolotherapy. 22/24 had no pain and had returned to full competition after a mean of 2.8 treatments. Conclusions: “Dextrose prolotherapy showed marked efficacy for chronic groin pain in this group of elite rugby and soccer athletes.” Arch Phys Med Rehab 2005 Apr;86(4):697-702 21 4/11/2008 Categories of Herbs for Pain Control • Analgesics • Anti Anti-convulsants convulsants • Anti-depressants • Antiinflammatories • Anxiolytics i • Narcotics • Sedatives • Alteratives/Adapto gen Materia Medica • • • • • • • • Bromelain Cayenne Feverfew Ginger Gingko Boswellia Corydalis Guggulipid • • • • • • • • Kava St. John’s wort Turmeric Valerian Griffonia (5-HTP) Hawthorne Licorice Grape Seed Extract Ginger : Zingiber officianalis Therapeutic Applications • • • • • • N/V Motion sickness Arthritis Analgesic Migraine HA Cardiotonic 22 4/11/2008 Ginger : Zingiber officianalis Pharmacology • Analgesic, antioxidant • Inhibition of inflammatory prostaglandins, thromboxane and leukotriene synthesis • Inhibition of platelet aggregation • Cholesterol-lowering, choleretic effect • Cardiotonic, GI protective actions, thermogenic properties, antibiotic activity • Vanilloid (VRI) receptor agonist Kiuchi F et al.: Inhibition of prostaglandin and leukotriene biosynthesis by gingerols and diarylhepatanoid. Chem Pharm bull 40, 387-391, 1992 Neuropharmacology 31, 1165-1169, 1992 Br J Pharmacol 2002 Nov;137(6):793-8. Ginger : Zingiber officianalis Anti-inflammatory • Several studies have shown efficacy in RA and OA, muscle discomfort • Recommended dosage 500-1,000mg 500 1 000mg a day. day Many patients took 3-4x this dose with quicker and better relief • Srivastava et al.: Ginger in rheumatic disorders. Med Hypothesis 29, 25-28, 1989 • Srivastava et al.: Ginger in rheumatism and musculoskeletal disorders. Med Hypothesis 39,342-348, 1992 Ginger : Zingiber officianalis Knee Osteoarthritis • Statistically significant effect on reducing symptoms of OA of the knee • RCT (n=247), multicenter trial, parallel, 6 wk trial • Less L knee k pain i with ith standing, t di after ft walking lki • Reduction in the Western Ontario and McMaster Universities osteoarthritis composite index • Good safety profile, with mostly mild GI adverse events in the ginger extract group. • Arthritis Rheum. 2001 Nov;44(11):2531-8 23 4/11/2008 Ginger: Zingiber officianalis Historically used to treat cardiovascular problems now shown to be effective in problems, hypertension, arrhythmia and increasing cardiac output Vascul Phamacol 2005 Oct;43(4):234-41 Ginger : Zingiber officianalis Analgesic • Analgesic effects in animals is thought to be the result of shagaol inhibiting the release of Substance P • Onogi T, et al.: Capsaicin-like effect of (6) shogoal on substance P-containing primary afferents rats; A possible mechanism of its analgesic action. Neuropharmacology 31, 11651169, 1992 Ginger : Zingiber officianalis Antioxidant • Potent inhibitor of oxidation of LDL, lowers cholesterol, attenuates atherosclerotic change1 • Potent antioxidant in lipid peroxidation generally, including linoleic acid2 1Furhman et al. Ginger extract consumption reduces plasma cholesterol, inhibits LDL oxidation and attenuates development of atherosclerosis in atherosclerotic, apolipoprotein E-deficient mice. J Nutr 2000 May;130(5):1124-31 • 2Shobana S, Naidu KA, Antioxidant activity of selected Indian spices. Prostaglandins Leukot Essent Fatty Acids 2000 Feb;62(2):107-10 • 24 4/11/2008 Ginger : Zingiber officianalis Cardiotonic • Gingerol has shown potent cardiotonic activity in animal models (positive inotropic and chronotropic action) • Shoji N, et al.: Cardiotonic principles of ginger (Z. officianalis). J Pharm Sci 10, 1174-1175, 1982 • Kobayashi M, et al.: Cardiotonic action of (8) gingerol, an activator of the Ca++-pumping ATPase of sarcoplasmic reticulum of guinea pig arterial muscle. J Pharmacol Exp Ther 246, 667-673, 1988 Gingko biloba (yin kuo) Traditional/Modern Use • Chinese used fruits/seeds since 2800 B.C. to “benefit the brain”, relieve symptoms of cough and asthma, to eliminate filaria • Last survivor of the 150M yr old order of Gingkoacea • Now used primarily as GBE in Europe for circulatory system disorders, cerebrovascular insufficiency,as an anti-asthmatic, and as a nootropic (mild-moderate dementia) • 1988 in Germany there were more Rxs for GBE than any other drug(5.4M) “Active Constituents” of Gingko • Active constituents: used as a standardized extract of 24% flavonoid glycosides (gingkoheterosides), 6% terpenes (gingkolide (gingkolide, bilobalide). bilobalide) Also contains proanthocyanidin flavonoids • Impressive literature for improving cerebral/peripheral blood flow, free-radical scavenging, reduction of clotting , as nootropic, anti-asthmatic, nerve regeneration 25 4/11/2008 Gingko: Gingko biloba Pharmacology • Membrane-stabilizing effect by activating Na+ pump • Effects on vascular endothelium by stimulating EDRF and prostacyclin • Effects are greatest in areas of poor perfusion • Fungfeld EW (ed.):Rokan (Gingko biloba). Recent Results in Pharmacology and Clinic. Springer-Verlag, NY, 1988 • DeFeudis FV(ed.): Gingko biloba Extract (Egb 761); Pharmacological Activities and Clinical Applications. Elsevier, Paris, 1991 Gingko: Gingko biloba Pharmacology • • • • Inhibits platelet activating factor (PAF) Increases synthesis of prostacyclin Competes with binding sites for PAF PAF induces inflammatory and allergic processes, including neutrophil activation, increases in vascular permeability, smooth muscle contraction (bronchconstriction, coronary artery spasm) • Koltai M et al. PAF. Drugs 42(1),9-29,1991 • Koltai M et al. PAF. Drugs 42(2),174-204, 1991 Gingko ~ CNS activity • Neuroprotective effect in ischemia and traumatic brain injury1 • Enhanced neurotrophic p and neuritogenic g effect post-injury2 • 1Advances in Gingko biloba Extract Research on the CNS, Elsevier, 1992 • 2Advances in Gingko biloba Extract Research on Neuronal Plasticity, Elsevier, 1996 26 4/11/2008 Gingko biloba Clinical Applications • Chronic cerebrovascular insufficiency • Peripheral vascular insufficiency • Age-related g memory/cognitive y g impairment. p Mildmoderate dementia of Alzheimer’s type • Vertigo /tinnitus, cochlear deafness • Retinopathy/macular degeneration • Neuralgia/neuropathy • Depression • Sexual dysfunction due to SSRIs Gingko biloba Retinal Effects • Improvement in long-distance visual acuity in macular degeneration and DM retinopathy • Protective effects against free-radical damage to retina • Shown to prevent DM retinopathy in diabetic rats • DeFeudis FV(ed.): Gingko biloba Extract (Egb 761); Pharmacological Activities and Clinical Applications. Elsevier, Paris, 1991 • Lanthony et al, Gingko biloba. J Fr Ophtalmol 11, 671-674, 1988 Gingko in Ischemic Heart Disease, Cerebral Infarction, Chronic Inflammation, and Aging • GBLE has an antioxidant action as a free radical scavenger • GBLE exerts an anti-inflammatory anti inflammatory effect on inflammatory cells by suppressing the production of active oxygen and nitrogen species • Beneficial effects on neuronal degenerative diseases by preventing chronic oxidative damage • Antioxid Redox Signal 1999 winter;1(4):469-80 27 4/11/2008 Gingko biloba Effects on Peripheral Vasculature • Marked improvement in intermittent claudication DM PVD, Raynaud’s, acrocyanosis, postphlebitis syndrome • Shown to be superior p to exercise,, pentoxifylline p y (Trental) ( ) in pain-free walking distance, plethysmographic/doppler US findings, blood lactate levels Angiology 45, 339-345, 1994 • RCT (n=111) of EGb 761 (40mg tid) in peripheral occlusive arterial disease patients with Fontaine stage II b is very safe and causes a significant and therapeutically relevant prolongation of the patients' walking distance Vasa 1998 May;27(2):106-10 Gingko biloba Nerve cell effects • Membrane-stabilizing and free-radical scavenging are most evident in brain and nerve cells • GBE promotes ↑ in nerve transmission rate, synthesis h i andd turn-over off bbrain i NTs, NT normalizes li ACh receptors in the hippocampus • Normalizes circulation in areas most affected by microembolization (hippocampus and striatum) • Fungfeld EW (ed.):Rokan (Gingko biloba). Recent Results in Pharmacology and Clinic. Springer-Verlag, NY, 1988 Gingko biloba Nerve cell effects • Exerts protective effect on neurodegenerative, sensory, and vascular diseases • EGb 761-induced inhibition of glucocorticoid production is due to specific transcriptional suppression of the adrenal PBR (peripheral-type benzodiazepine receptor) gene • Seven genes were identified whose expression was strongly modified by the EGb 761 treatment and likely linked to neuroprotective action including genes involved in antioxidant defenses and in stress response • Cell Mol Biol (Noisy-le-grand). 2002 Sep;48(6):641-6 • Cell Mol Biol (Noisy-le-grand). 2002 Sep;48(6):633-9. • Cell Mol Biol (Noisy-le-grand). 2002 Sep;48(6):601-11. 28 4/11/2008 Gingko biloba Memory Effects • In DBPC study of post menopausal women taking 120mg of gingko qd: • Significantly better than the placebo group in a matching-to-sample hi l test off nonverbal b l memory • Test of frontal lobe function (rule shifting) and in the Paced Auditory Serial Addition Test (PASAT) (which measures sustained attention but also involves frontal lobe function), the group treated with Ginkgo performed significantly better than the placebo group • Pharmacol Biochem Behav. 2003 Jun;75(3):711-20 Gingko biloba Memory Effects • AGAINST: Trial results do not support the view that Ginkgo is beneficial for patients with dementia or ageassociated memory impairment J Clin Epidemiol. 2003 Apr;56(4):367-76 • FOR:These results suggest that C4A(Egb761) treatment may reduce the risk of developing Alzheimer's dementia in elderly women (n=1462 women, age > 75) J Gerontol A Biol Sci Med Sci. 2003 Apr;58(4):372-7 • Overall, the results from both objective, standardized, neuropsychological tests and a subjective, follow-up self-report questionnaire provided complementary evidence of the potential efficacy of Ginkgo biloba EGb 761 in enhancing certain neuropsychological/memory processes of cognitively intact older adults, 60 years of age and over Hum Psychopharmacol. 2002 Aug;17(6):267-77 Gingko biloba Memory Effects:AGAINST • 6-week study, RCT • N=203, age >60, normal cognitive function (mini mental state exam, score >26), dose 40mg tid • Indicate that ginkgo did not facilitate performance on standard neuropsychological tests of learning, memory, attention, and concentration or naming and verbal fluency in elderly adults without cognitive impairment when taken as manufacturers suggest • JAMA 2002 Aug 21;288(7):835-40 29 4/11/2008 Gingko biloba Dosage/side-effects • 80 mg capsules of SE, dose from 80mg to 240mg in divided doses • In 9,772 taking GBE (leaf-extract) side-effects uncommon ; 21 cases of GI discomfort,, 7 cases of HA, 6 cases of dizziness • Contact with fruit-pulp can cause Rhus-like reaction • Exercise caution if patient is on anti-coagulant or ASA therapy • EGb 761 is a standardized extract(SE) of dried leaves of Ginkgo biloba containing 24% ginkgo-flavonol glycosides, 6% terpene lactones such as ginkgolides A, B, C, J and bilobalide St. John’s Wort : Hypericum perforatum Therapeutic Actions • • • • • Anti-depressant/SAD A ti i l Anti-viral Antioxidant Sleep disorders Topical as wound-healing agent St. John’s Wort : Hypericum perforatum Pharmacology • Hypericin and psuedohypericin exhibit strong anti-viral activity against HSV1,2, influenza A/B, EBV vesicular stomatitis virus EBV, • Meruelo et al. Therapeutic agents with dramatic antiretroviral activity and little toxicity at effective doses: Aromatic polycyclic diones hypericin and psuedohypericin.Proc Natl Acad Sci USA 1988; 85:5230-5234 30 4/11/2008 St. John’s Wort : Hypericum perforatum Pharmacology • Constituent hyperforin has significant serotonergic activity and inhibits synaptosomal uptake of dopamine norepinephrine dopamine, norepinephrine, GABA and L Lglutamate • Chatterjee et al. Hyperforin as a possible antidepressant component of hypericum extracts. Life Sci 1998 63:6 499-510 CNS Sensitization With Wind-up Phenomena And….. Depression, Sleep Disturbance, Fatigue • “PGE2, acting via an EP2-like receptor, directly depolarizes spinal neurons. Moreover, these findings imply an involvement of spinal cord-generated prostanoids in modulating sensory processing through an alteration lt ti in i dorsal d l horn h neuronall excitability” it bilit ” • J Neurosci 2001 Mar 1;21(5):1750-6 CNS Sensitization With Wind-up Phenomena And….. Depression, Sleep Disturbance, Fatigue • Hypericum has demonstrated action as an p p restoringg agent g 2, anti-depressant 1, sleep anti-nociceptive3 independent of endogenous opioid enhancement • Clin Ther 2000;22:411-419 • German Comm E Monographs • J Ethnopharmacol 1999; 67:307-312 31 4/11/2008 St. John’s Wort : Hypericum perforatum Antidepressant • Official German Comm E Monograph lists psychovegetative h i disturbances, di b depressive d i states, fear, nervous disturbance as indications for use • Many studies have shown as effective as standard anti-depressants but better tolerated with fewer side-effects St. John’s Wort : Hypericum perforatum Antidepressant • In multiple studies hypericum has been shown to be equipotent to SSRIs in relieving depression with greater safety profile and better tolerance • European Neuropsychopharmacology 1999, 9: 461-468 • Clinical therapy 2000, 22: 411-419 • International clinical psychopharmacology 2000, 15: 6168 • Compr psychiatry 2000, 41: 133-137 St. John’s Wort : Hypericum perforatum Antidepressant • In severe depression Hypericum(LI 160) @600mg tid vs. imipramine 50mg tid • Both B h drugs d gave similar i il reductions d i in i HAMD, HAMD CGI and D-S and considered effective while Hypericum had less side-effects • Vorbach EU, et al. Pharmacopsychiatry 1997;30(Suppl):81-5 32 4/11/2008 St. John’s Wort : Hypericum perforatum Antidepressant • Recent study compared once a day Hypericum dosing (900mg) to Citalopram (20mg) in a randomized placebo controlled multi-center trial (n=388) in moderate depression • Findings: Citalopram and Hypericum were superior to placebo but Hypericum was better tolerated than citalopram or placebo Pharmacopsychiatry 2006 Mar;39(2):66-75 St. John’s Wort : Hypericum perforatum Dosage • Anti-depressant dosage of standardized extract (0.3% hypericin) is 300mg tid cc for mildmoderate depression • Better effects will be obtained by higher doses • Anti-viral optimal dosage unknown but studies in HIV have shown encouraging results with 1mg hypericin qd • As topical usually in combination with Arnica, Bellis, Eupatorium, Belladonna (Traumeel) St. John’s Wort : Hypericum perforatum Potential Adverse Effects Induction of Cytochrome P450 (CYP 3A4) resulting in serum reduction of theophylline, digoxin cyclosporine, digoxin, cyclosporine coumarin, coumarin OCPs, OCPs indinavir and xenobiotics National Academy of Science USA 2000, 97,7500-7502 Lancet 2000, 355, 134-138 Also amitriptyline, irinotecan, alprazolam, simvastatin, dextromethorphan Eur J Clin Pharmacol 2006 Mar;62(3):225-33 33 4/11/2008 St. John’s Wort : Hypericum perforatum Adverse Effects • Can cause severe photosensitivity in animals (h (hypericism) i i ) • Reports of photosensitivity in humans is rare up to 11.25mg of total hypericin (tanning improved) • The usual cautions with MAO inhibitors may apply (avoid tyramine foods, l-dopa, 5-HTP, Tyr) • May cause mild gastric upset in sensitive individuals Valerian: Valeriana officianalis • Dioscorides et al described as Phu • Traditionally used for muscle spasms, emotional tension, insomnia, hysteria, fatigue, menstrual cramps, climacteric complaints • >120 chemical components from root/essential oil Valerian : Valeriana officianalis Therapeutic uses • Sedative • Anxiolytic • Spasmolytic • Anti-stress 34 4/11/2008 Valerian : Valeriana officianalis Pharmacology • Active constituents valeric a. isovaleric a. (sesquiterpenes), valepotriates, iridoids, hydroxypinoresinol which vary according to source • Normalizes CNS (sedative in agitation, stimulant in extreme fatigue) • Binds BZ receptors and enhances GABA • Smooth muscle relaxant, choleretic, anti-tumor and antibiotic activity J Pharm Pharmacol 1999 May;51(5):505-12 Valerian : Valeriana officianalis Clinical applications • Primarily as sedative in the treatment of insomnia p sleep p qquality, y deeper p stage g 3 and 4 • Improves with less morning sleepiness • Mild muscle relaxant activity due to CNS depression • Aid in benzodiazepine, barbituate withdrawal Valerian : Valeriana officianalis Clinical applications • Several RCT have demonstrated improvement in slow wave sleepp latency y1,2, increased REM vs. NREM1,2, equivalency with oxazepam 2 in sleep induction with markedly fewer adverse effects • • 1Pharmacopsychiatry 2000 Mar;33(2):47-53 Komplementarmed Klass Naturheilkd 2000 Apr;7(2):79-84 2Forsch 35 4/11/2008 Valerian : Valeriana officianalis Dosage • • • • Dried root (or as tea): 1-2g Tincture (10-20%) : 1-1.5 tsp (4-6ml) Fluid extract (1:1) : 0.5-1 tsp (1-2ml) Valerian extract (0.8% valeric acid) :150300mg • The above 30-45’ h.s. or up to qid Valerian : Valeriana officianalis Toxicity • GRAS approved for food use by FDA – Safety of valepotriates questioned, best to use watersoluble extracts standardized for valeric acid content • Recently shown to have neuroprotective effects by decreasing neuronal hyperexcitability, decreasing membrane peroxidation in hippocampal synaptosomes exposed to amyloid beta peptide Neurotox Res 2004;6(2):131-40 Griffonia simplicifolia ~ 5-HTP • 5-HTP readily crosses blood-brain barrier • Approximately 70% absorption • Increases serotonin in the CNS • Also increases melatonin, dopamine, norepinephrine, and beta endorphin in the CNS • Van Praag et al. Nutrition and the Brain. NewYork. Raven press;1986:89-139 36 4/11/2008 Serotonin Pharmacology Serotonin Deficiency has been implicated in • Mood disorders • Premenstrual syndrome • Autism • Eating disorders • Fibromyalgia • • • • • • Migraine Pain in general, Insomnia Sleep disorders Appetite control Alcohol abuse Clinical Studies ~ Depression • 5-HTP vs. Conventional Anti-Depressants • Compared p with fluvoxamine 150mgg tid and 5-HTP 100mg tid had similar effects (5-HTP considered superior but not statistically) • 5- HTP was better tolerated • Poldinger et al. Psychopathology 1991;24:53-81 Clinical Studies ~ Depression • 5-HTP vs. Conventional Anti-Depressants – In severe depression vs. chlorimipramine/imipramine, p p , 5-HTP shown to be as effective with doses up to 1200mg qd – fewer side effects were noted • Angst J et al. Arch Psychiatr Nervenkr 1977;224:175-186 37 4/11/2008 Migraine Headaches ~ 5-HTP • 124 subjects with 5-HTP 600mg qd vs. methysergide for 6 mos – 75% had prevented or substantially decreased # of migraines – not considered statistically significant – Titus et al. Eur Neurol 1986;25:327-329 Fibromyalgia • Three trials report improvement with 5-HTP • DBPC with 5-HTP 100mg tid for 30d in 50 pts. – Significant improvement in #s of TPs, TPs subjective pain severity, AM stiffness, anxiety, fatigue – low incidence of side-effects – Caruso, et al. J Int Med Res. 1990;18:201-209 Cautions with 5-HTP • Serotonin syndrome possible if taken with SSRI or MAOI such as Nardil or Parnate • Reported R d with i h L-Tryptophan@1200mg LT h @1200 qd d plus l MAOI • Not reported with 5-HTP@200mg qd plus MAOI • Beginning dose 5-HTP@50mg tid suggested • Can increase 5-HTP to 100mg tid if response after two weeks is inadequate 38 4/11/2008 Cautions with 5-HTP • Serotonin syndrome has agitation, confusion, delirium, tachycardia, diaphoresis, BP fluctuation • If suspect, di discontinue i 5-HTP, 5 HTP SSRI SSRI, MAOI • 5-HTP should not be used or used cautiously with SSRI or MAOI • When changing over consider washout period (314d) or possibility of serotonin syndrome symptoms exist Boswellia serrata ~ Salai guggul Frankincense/Indian Olibanum • Traditional gum resin exudate uses have been for arthritis, h i i abdominal bd i l pain, i diarrhea, di h hepatic h i disorders,neurologic disorders,and as a topical for sores • Used in Ayurvedic, Unani and Chinese herbal medicine, commonly used with Ginger, Turmeric, Commiphora, Corydalis in formulae Boswellia serrata ~ Salai guggul Pharmacology • Studies show that β-boswellic acids are p inhibitors of leukotriene specific,non-redox synthesis either interacting directly with 5lipoxygenase or blocking its translocation (but did not affect the 12-lipoxygenase and the cyclooxygenase activities) • Ammon HP, Safayhi H, Mack T, Sabieraj J Ethnopharmacol 1993 Mar 38:2-3 113-9 • Ammon HP Eur J Med Res 1996 May 24 1:8 369-70 39 4/11/2008 Boswellia serrata ~ Salai guggul Pharmacology • Inhibits Human Leukocyte Elastase (HLE) a serine protease which initiates injury that triggers i the h inflammatory i fl process • Safayhi H, et al. Inhibition by boswellic acids of human leukocyte elastase. J Pharmacol Exp Ther 281;460-463 Boswellia serrata ~ Salai guggul Pharmacology • Boswellic acids and triterpene constituents have been shown to inhibit leukemia cells in vitro and induce apoptosis p p and differentiation • Jing Y, et al Chin Med Sci J 1992 Mar 7:1 12-5 • Shao Y,et al. Planta Med 1998 May 64:4 328-31 • Jing Y, et al. Leuk Res 1999 Jan 23:1 43-50 Boswellia serrata ~ Salai guggul Clinical Applications • Recent studies have demonstrated efficacy in models of inflammation and as an analgesic • Reddy GK et al. Studies on the metabolism of glcosaminoglycans under the influence of new herbal antiinflammatory agents. Biochemical Pharmacology, Vol 38(20), 3527-3534, 1989 • Ammon et al. Mechanism of antiinflammatory actions or curcumin and boswellic acids.J Ethnopharmacol 1991 May-Jun 33:1-2 91-5 40 4/11/2008 Boswellia serrata ~ Salai guggul Clinical Applications • Ulcerative colitis(Grade II,III) • (350 mg tid for 6 weeks) on stool properties, histolopathology and scan microscopy of rectal biopsies, blood parameters including Hb, serum iron, calcium, phosphorus, proteins, total leukocytes and eosinophils was studied. Patients receiving sulfasalazine (1 g thrice daily) served as controls. All parameters tested improved after treatment with Boswellia serrata gum resin, the results being similar compared to controls: 82% out of treated patients went into remission; in case of sulfasalazine remission rate was 75%. • Eur J Med Res 1997 Jan 2:1 37-43 Boswellia serrata ~ Salai guggul Clinical Applications • Knee Osteoarthritis, DBPC trial, n=30 • Given BSE or placebo for 8 wks, after the first intervention, then washed out and crossed over • ALL patients i receiving i i BSE reportedd decreased d d knee pain, increased knee flexion, and increased walking distance • BSE was generally well-tolerated except for minor GI ADRs Phytomedicine 2003 Jan;10(1):3-7. Boswellia serrata ~ Salai guggul Dosage and Side-Effects • Anti-inflammatory: – 200mg TID • as Boswellia serrata extract containingg 60-70% organic acids or • 50mg TID if standardized to boswellic acids( 100%) • Free of typical NSAID toxicity, welltolerated, no GI or kidney complaints 41 4/11/2008 Boswellia serrata ~ Salai guggul Clinical Applications • In veterinary medicine has been used for disabling OA ,chronic post-operative knee arthritis general stifle problems arthritis, problems, sore backs, backs bowed tendons and bone spurs • McCrea B. Ancient Indian Herb proving itself a winner for modern day equine athletes. J Am Hol Vet Med Assoc 12(1),19 Boswellia serrata ~ Salai guggul Clinical Applications • Bronchial asthma – In a double-blind, placebo-controlled study forty patients, 23 males and 17 females in the age range of 18 - 75 years having mean duration of illness, bronchial asthma, of 9.58 +/- 6.07 years were treated with a preparation of gum resin of 300 mg thrice daily for a period of 6 weeks weeks. 70% of patients showed improvement of disease as evident by disappearance of physical symptoms and signs such as dyspnoea, rhonchi, number of attacks, increase in FEV subset1, FVC and PEFR as well as decrease in eosinophilic count and ESR. In the control group of 40 patients 16 males and 24 females in the age range of 14-58 years with mean of 32.95 +/12.68 were treated with lactose 300 mg thrice daily for 6 weeks. Only 27% of patients in the control group showed improvement. The data show a definite role of gum resin of Boswellia serrata in the treatment of bronchial asthma. • Eur J Med Res 1998 Nov 17 3:11 511-4 Herbal Medicines for Fibromyalgia • Hypericum : standardized to hypericin and hyperforin content; 600mg BID PC • Magnesium: 200-300mg BID to tolerance • Malic M li acid: id 200-300mg 200 300 BID • If insufficient response add 5-HTP 100mg QDTID • If sleep problems are still present after 2 weeks consider sleep aids such as melatonin, kava, zizyphus, valerian 42 4/11/2008 Migraine Strategies • Address the musculoskeletal dysfunction in the neck and jaw (if applicable) • Normalize hormonal triggers • Find and avoid dietary and environmental triggers • Mg taurate, B vitamins, antioxidants in individually optimized doses • 5-HTP 50-150mg h.s., or during the day not to exceed 300mg. Neuralgia Approaches • If impingement or local hypoxia is present it must be addressed first • Magnesium, Gingko, Hypericum, Kava, Valerian may be particularly helpful • B vitamin deficiencies often contribute • GABA or gabapentin is often specific • Needling therapies (acupuncture , neural therapy, mesotherapy) is generally most helpful • Undiagnosed DM or continuum should be strongly suspected Magnesium New mechanisms to consider • • • • Essential for production of ATP and Glutathione Lowers Il-6 which leads to lower MMP-1 Inhibits MMP-1----Angiology 1999 Jul;50 Inhibits MMP-2 in cardiac fibroblasts in a dose dependant fashion--- Basic Res. Cardiology 2004 July ‘99 • Magnesium is a N-methyl-D-asparate (NMDA) receptor antagonist---Masui. 1998 Sep;47(9):1109-13. 43 4/11/2008 Magnesium and MMPs cont. • A magnesium deficient diet feed to mice for 42 days lead to aortic wall thinning and severely damaged collagen and elastin via increased expression of MMP-2 MMP 2 and MMP MMP-9---9 Magnes Magnes. Res. 2003 Mar;16 • In a dose dependant manner, rat VSMC’s produced more MMP-2 with and without PDGF and were not influenced by verapamil and nifedipine in the context of a magnesium deficient diet.---Atherosclerosis 2003 Feb;166 Thank You! Rick Marinelli, ND, MAcOM 44
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