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The majority of
people in the Western world have, through unwise monitoring of their
eating habits, developed a condition in their body wherein
inflammatory fatty acids such as omega-6 have free rein. For such
people it is imperative to increase the consumption of
anti-inflammatory fatty acids and antioxidants. The key supplements
that should be taken follow:
Fish is your key
source of two key omega-3 fatty acids – eicosapentaenoic (EPA) and
docosahexaenoic (DHA). These are major anti-inflammatories. EPA and
DHA are essential building blocks for the body's anti-inflammatory
prostaglandins (e.g., prostaglandin E1) and for turning off Cox-2 and
the body's pro-inflammatory cytokines (IL-1, IL-6, and TNFa). In
addition, omega-3 fatty acids block the activity of an enzyme that
breaks down joint cartilage. Mackerel, salmon, trout, sardines and
tuna are good sources of these fatty acids.
Curcumin is the
active ingredient of the Indian spice turmeric. Over the last few
decades hundreds of small scale studies have proven scientifically
what Indian people have known for centuries; that curcumin has the
ability to halt or prevent certain types of cancer, stop
inflammation, improve cardiovascular health, prevent cataracts and
kill or inhibit the toxic effects of certain microbes including fungi
and dangerous parasites.
(Arora RB, Basu
N, Kapoor V, Jain AP. Anti-inflammatory studies on Curcuma- longa
(turmeric). Ind J Med Res 1971 Aug;59(8):1289-95).
Curcumin is a
naturally occurring source of cyclooxygenase-2 (COX-2) inhibitors,
which can be artificially obtained through such drugs as Celebrex®
and Vioxx®. People who take COX-2 inhibitors as statistically
less likely to develop cancer than those who do not.
(Reddy BS, Rao
CV. Novel approaches for colon cancer prevention by cyclooxygenase-2
inhibitors. J Environ Pathol Toxicol Oncol
2002;21(2):155-64).
GLA
is actually an Omega-6 fatty acid. However, it has anti-inflammatory
properties, increasing production of the anti-inflammatory
prostaglandin E1. Evening Primrose Oil provides an excellent source
of GLA. Taken internally, the body converts GLA into prostaglandins.
These hormone like compounds help regulate various body functions,
controlling inflammation in some cases and promoting it in others.
The anti-inflammatory properties of evening primrose oil help people
suffering from pains, aches and cramps.
(Belch
JJ, Hill A. Evening primrose oil and borage oil in rheumatologic
conditions. Am
J Clin Nutr.
2000;71(1 Suppl):352S-356S).
Serrapeptase
is a proteolytic enzyme found naturally in the intestine of the
silkworm. It is widely used as an anti-inflammatory agent. Clinical
studies show that serrapeptase induces fibrinolytic,
anti-inflammatory and anti-edemic (prevents swelling and fluid
retention) activity in a number of tissues, and that its
anti-inflammatory effects are superior to other proteolytic
enzymes.
(Mazzone
A, Catalani M, Constanzo M, Drusian A, Mandoli A, Russo S, Guarini E,
Vesperini G. Evaluation of Serratia peptidase in acute or chronic
inflammation of otorhinolaryngolog pathology: a multicentre,
double-blind, randomized trial versus placebo. J Int Med Res
1990,18(5):379-88).
Bromelain
is a plant derived proteolytic enzyme. It is extracted from the flesh
and stem of the pineapple plant. It is most notable for its
effectiveness in the reduction of inflammation and the decreasing of
swelling. As a natural anti-inflammatory enzyme, bromelain has many
uses. Arthritis patients may reduce the swelling that causes joint
pain by taking bromelain. Bromelain may also be helpful for the pain,
numbness, tingling, aching and loss of motor and sensory function in
the fingers resulting from carpal tunnel syndrome (CTS).
(Kelly,
G.S. "Bromelain: A Literature Review and Discussion of Its
Therapeutic Applications." Alternative Medicine Review (November
1, 1996).
Although it is
better known for it’s anti-depressant effect, St. John’s Wort has
also been shown to have anti-inflammatory properties. In a laboratory
experiment, researchers from the University of Frieburg, Germany
found that hypericin, one of the constituents of St. John's Wort,
inhibited NF-kB, which activates pro-inflammatory genes.
Researchers at
Case Western Reserve University, Cleveland, recently reported that
the antioxidant polyphenols in green tea had anti-inflammatory
properties by inhibiting Cox-2 and TNFa. Genistein inhibits
prostaglandin E2 and Cox-2, and quercetin inhibits the activity of
inflammation-promoting "adhesion" molecules. It's likely
that Pycnogenol, grape seed extract, and other flavonoids work
through similar mechanisms.
(School of Public
Health, University of California, Los Angeles
American
Journal of
Clinical Nutrition, Vol. 80, No. 6, 1558-1564, December
2004).
The popular herb
ginger contains over 500 different compounds, many of which have
anti-inflammatory properties. Suppression of inflammation is
attributed to suppression of pro-inflammatory cytokines and
chemokines produced by synoviocytes, chondrocytes, and leukocytes.
Ginger suppresses prostaglandin synthesis through inhibition of
cyclooxygenase-1 and cyclooxygenase-2. A ginger extract (EV.EXT.77)
derived from Zingiber officinale and Alpina galanga inhibits the
induction of several genes involved in the inflammatory response.
(Setty AR, Sigal
LH. Semin. Arthritis Rheum. 2005 Jun;34(6):773-84. Herbal
medications commonly used in the practice of rheumatology: mechanisms
of action, efficacy, and side effects).
Vitamin
C has long been recognized for its anti-inflammatory properties. In a
study published in the March, 2006 American Journal of Clinical
Nutrition, High
blood levels of Vitamin C reduced signs of inflammation by 45
percent. The study was conducted at a London university and involved
over 3200 men between 60 and 69. Researchers looked at C-reactive
protein and t-PA, both markers for inflammation levels in the body.
High blood levels of Vitamin C were also predictive of lower risk of
blood clots, as indicated by factors such as blood viscosity.
(American
Journal of Clinical Nutrition
(Vol. 83, pp. 567-574),
Vitamin
E plays a major role in reducing inflammation as well as cleansing
the body of free radicals. Ishwarlal
Jialal and Sridevi Devaraj of the University of Texas Southwestern
Medical Center at Dallas, Texas studied 47 men and women with
adult-onset, or type II, diabetes and 25 healthy volunteers. The
researchers sampled people's blood before and after each received
1,200 international units of vitamin E daily for 3 months. The
vitamin E cut production of a cytokine, an immune system signaling
molecule. In test-tube experiments, white blood cells were stimulated
to provoke an immune response. Cells from volunteers after treatment
responded by producing about one-third as much interleukin-6--a
cytokine that tells the liver to make CRP--as was generated by cells
from blood drawn before people took vitamin E.
Before
treatment, the 23 people with major diabetes complications such as
kidney failure produced roughly twice as much C-reactive protein
(CRP), a marker of inflammation, as the healthy group did.
Concentrations of CRP were about 33 percent higher in blood from the
24 people with mild diabetes than in the healthy volunteers.
Vitamin
E supplements lowered CRP concentrations dramatically in all three
groups. CRP measurements in people with mild disease fell to the
healthy group's starting concentration, and those in people with
advanced diabetes fell to the concentrations detected in the other
diabetic people before treatment
(Jialal
I, Devaraj S. Effect of vitamin E on acute chronic inflammation in
Type 2 Diabetes Patients: FREE
RADICAL BIOLOGY & MEDICINE
Oct. 2000).
(Upritchard
JE, Sutherland WHF, Mann JI. Effect of supplementation with tomato
juice, vitamin E, and vitamin C on LDL oxidation and products of
inflammatory activity in type 2 diabetes. Diabetes Care, 2000,
23:733-738).
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