Immune System Supplements
 

             
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    Immune System Supplements
Beta Glucan is a natural, branched polysaccharide (a molecule made up of many sugar units). It is composed of glucose molecules extracted and purified from the cell wall of common baker’s yeast. Beta Glucan enhances immunity by binding to macrophages and other phagocytic white blood cells at certain receptors and activating their anti-infection and anti-tumor activity by stimulating the production of free radicals. This stimulation signals the phagocytic immune cells to engulf and destroy foreign bodies, be they bacteria, viruses or tumor cells.

In a 2004 study, researchers tested the effects of oat beta glucan on respiratory infection, macrophage antiviral resistance, and NK cytotoxicity in mice. Results indicated that ingestion of beta glucan before infection prevented an increase in morbidity and mortality. Exercise stress was associated with a decrease in macrophage antiviral resistance, which was blocked by ingestion of beta glucan. (Effects of oat beta-glucan on innate immunity and infection after exercise stress. Med Sci Sports Exerc. 2004 Aug;36(8):1321-7).

In a 2003 study, the effect of beta-glucan on the enhancement of resistance to infections caused by Staphylococcus aureus and Eimeria vermiformis was studied in mice. An in vitro study using macrophages isolated from the peritoneal cavity showed that beta-glucan treatment significantly enhanced phagocytic activity. An in vivo study further demonstrated that beta-glucan treatment induced a significant protection against the challenge with S. aureus in mice.

(Beta-glucan, extracted from oat, enhances disease resistance against bacterial and parasitic infections. FEMS Immunol Med Microbiol. 2003 Jan 21;35(1):67-75.)

Echinacea is a plant native to the United States. The word Echinacea actually comes from a Greek word 'echinos,' which means sea urchin and refers to the plant's sea-urchin-shaped, flowering head. It was recognized over a century ago as a natural infection fighter. Echinacea is an immunostimulant in that it enhances the immune system. Evidence shows that it stimulates the body to produce more infection-fighting white blood cells, such as T-lymphocytes and killer white blood cells. It may also stimulate the release of interferons, one of the body's most potent infection-fighting weapons. Interferon kills germs and also infiltrates their genetic control center, preventing them from reproducing. Besides helping the body produce more infection- fighting cells, echinacea helps these cells to produce more germ-eating cells, called macrophages, and it helps these cells eat the germs more voraciously, a process called phagocytosis. Echinacea also prevents bacteria from secreting an enzyme called hyaluronidase, which enables them to break through protective membranes, such as the lining of the intestines and respiratory tract, and invade tissues. Echinacea also seems to search out and destroy some viruses, such as the common cold and flu viruses.

Many clinical studies demonstrate Echinacea’s efficacy as an immune system stimulant. According to the authors of a 1999 meta-analysis Echinacea is effective against respiratory infections, especially if taken as soon as the first symptoms appear.

(Barrett B, Vohmann M et Calabrese C. Echinacea for Upper respiratory infection. J Fam Pract 1999;48(8):628-35).

A double-blind placebo-controlled study was conducted in Sweden in 1999. 246 patients suffering from colds took either 6 Echinacea tablets daily, or a placebo. Echinacea was significantly more effective than the the placebo.]

(Brinkeborn RM, Shah DV, Degenring FH. Echinaforce® and other Echinacea fresh plant preparations in the treatment of the common cold. A randomized, placebo controlled, double-blind clinical trial. Phytomedicine 1999 Mar;6(1):1-6).

A 2002 study involving 48 volunteers showed that Echinacea significantly increases one of the markers of immune system stimulation: properdine.

Kim LS, Waters RF, Burkholder PM. Immunological activity of larch arabinogalactan and Echinacea: A preliminary, randomized, double-blind, placebo-controlled trial. Altern Med Rev  2002 Apr;7(2):138-149).

Zinc is an essential mineral that is necessary for the functioning of over 300 different enzymes. As well as it’s involvement in carbohydrate, protein, fat and energy metabolism, it has been shown to support the immune system. -lymphocytes are white blood cells that help fight infection and depend on zinc for their development and activation. In humans, zinc deficiency can result in a decreased number of T-lymphocytes and a diminished ability to fight infection and heal wounds. Because supplemental zinc may help fight infection and heal wounds, zinc status is especially important for patients with conditions such as HIV infection.

(Fraker PJ, King LE, Laakko T, Vollmer TL. The dynamic link between the integrity of the immune system and zinc status. J Nutr. 2000 May;130(5S Suppl):1399S-406S).

(Lim Y, Levy M, Bray TM. Dietary zinc alters early inflammatory responses during cutaneous wound healing in weanling CD-1 mice. J Nutr. 2004 Apr;134(4):811-6).

Iron is present in every cell. It is a component of hemoglobin in red blood cells, binding the oxygen that the blood circulates throughout the body. We need iron for strength and vigor, and the element plays a key role in DNA and enzyme synthesis and other basic life processes. Numerous studies indicate that a lack of iron lowers immunity. Adequate levels help maintain cellular immunity and help to protect against some infections. Cell-mediated immune response may be impaired when iron deficiency negatively impacts the iron-requiring enzyme called ribonculeotide reductase, an enzyme that appears to be essential for the proper function of the T-lymphocyte arm of immunity. Resistance to candida, herpes simplex virus and some other pathogens appears to be reduced in those with poor iron status. On the other hand, excess iron may predispose individuals to some infections.

(Immune function is impaired in iron-deficient, homebound, older women. N. Ahluwalia, J. Sun, D. Krause,  et al., Am J Clin Nutr, 2004, vol. 79, pp. 516—521).

(Dallman PR. Iron deficiency and the immune response. Am J Clin Nutr. 1987; 46:329-334).

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