CANCER SURVIVOR - PUNA WAI ORA MIND-BODY CENTER

Step 3 – Reducing Stress Hormone Cortisol Levels

Finding additional ways to remove / reduce stress inside your PHYSICAL body will help to calm the autonomic nervous system and lower stress Cortisol Levels that have been proven to suppress immune system function.  Those with cancer have abnormally high levels of the stress hormone Cortisol.  Regular aromatherapy massage, yoga, tai chi, meditation, relaxation techniques, and regular laughter, will all help to lower stress Cortisol levels.  Lowering stress Cortisol levels is an important part of your 11 Step Cancer Survivor Program.  A DAILY regime of one-two or more of these techniques should be a minimum requirement for those recovering from cancer.  See Lowering Cancer Stress for detailed research in this area. 

The use of Laughter should be strongly considered.  There are many instances of cancer patients who have used laughter therapy (i.e. Watched VERY funny movies/comedies everyday during their recovery) without using mainstream medicine and have fully recovered.  Laughter is found to lower bloodpressure, reduce stress hormones, and boost immune function by raising levels of infection-fighting T-cells, disease-fighting proteins called Gamma-interferon and B-cells, which produce disease-destroying antibodies. Laughter also triggers the release of endorphins, the body's natural painkillers, and produces a general sense of well-being.

Step 4 – Increasing Melatonin Levels

Those with cancer have abnormally low levels of Melatonin, a hormone produced by the pituitary gland of the brain during deep uninterrupted sleep.  This is important because 1) Melatonin is responsible for inhibiting cancer cell growth and 2) because Melatonin is the  hormone responsible for regulating the immune system.  Those with cancer have low Melatonin levels because the internal stress they feel means they have difficulty sleeping well.  Daily meditation has been shown in studies to significantly increase Melatonin levels and should be strongly considered as a key element of your 11 Step Cancer Survivor Program.  It has also been shown that those who meditate regularly, have very low incidence of cancer.  See Increasing Melatonin for detailed research in this area.

Step 5 – Boosting / Supporting The Immune System
 

Step 5 of your 11 Step Cancer Survivor Program is to boost / support your immune system.  High stress Cortisol levels, parasites, pathogenic microbes (viruses, bacteria, fungus), chemotherapy and radiation will all significantly weaken the immune system, whose job it is to keep the body healthy and to destroy cancer cells and other harmful pathogens in the body.  Therefore it is vitally important to support the immune system during recovery from cancer and during remission.  Intravenous Vitamin C Therapy can also be used for this purpose.  Consider the following:

Avemar (Wheat Germ Extract)

Avemar is the new wonder-alternative cancer treatment / adjuvant therapy for boosting the immune system and fighting cancer. "Research at UCLA has demonstrated that Avemar reduces glucose flow into the cancer cells.  Cancer cells can evade NK [natural killer] cells by masking their outer membrane with a special substance that the NK cells recognize as 'normal.'  Avemar suppresses the release of this masking substance -- allowing NK cells to better target and kill the cancer cells."  Avemar's immune-stimulating ability appears to be so powerful that it can be useful in helping to restore even the most severely compromised immune systems.

Avemar Inhibits Breast Cancer Better than Tamoxifen

PRESS RELEASE: Wheat Germ Extract (AVEMAR) inhibits breast cancer in study published at ASCO 2007 (AMERICAL SOCIETY OF CLINICAL ONCOLOGY) CHICAGO, June 4 /PRNewswire/ -- A fermented wheat germ extract inhibits estrogen positive and estrogen negative breast cancer tumors better than the world's best selling cancer drug, Tamoxifen, according to research published this past weekend at the 2007 meeting of the American Society of Clinical Oncology, ASCO.  The compound, Avemar, has been extensively studied in many cell lines, animal tumor models, and several human clinical trials. In the current study, Andras Telekes, MD, Ph.D., head physician at the Hungarian National Institute of Oncology, and colleagues, implanted estrogen receptor-positive (ER+) and estrogen receptor-negative (ER-) breast tumors from humans and mouse cell lines into female mice and monitored tumor growth. They compared tumor growth in mice treated with Avemar alone, or treated with three of the most widely used and studied breast cancer drugs: Tamoxifen, Aromasin, or Arimidex, alone, and combinations of those drugs with Avemar. Against the mouse ER+ cell line, MXT, Avemar inhibited growth by 50%, Aromasin by 46.7%, Tamoxifen by 34% and Arimidex by 29.3%. Against the human ER+ cell line, T47T, Avemar inhibited growth by 49%, Tamoxifen 42%, Aromasin 25% and Arimidex 25%. Each agent was enhanced by 5 to 10% when combined with Avemar. Most effective was a combination of Aromasin and Avemar, inhibiting both the mouse and human derived ER+ breast tumors by 60%.  Effects against estrogen receptor-negative (ER-) breast cancer were measured with the human derived, MDA-MB-231 cell line. Estrogen-blocking drugs are not effective against ER- breast cancers, so they were not tested in this tumor model. However, Avemar did inhibit the growth of the ER-negative MDA-MB-231 breast tumors significantly (52%), suggesting to researchers that the mechanism by which the extract works is different from that of the anti- estrogen drugs, and is independent of a breast tumor's estrogen receptor status. Avemar's efficacy against both ER+ and ER- tumor types suggests the compound's mechanisms of action against breast cancer may be those that inhibited tumor growth in other cancers, including lung, pancreatic, colon, melanoma, leukemia, and other breast cancer lines, among others, against which the compound has also been tested. Chief among these mechanisms is its ability to interfere with the excess use of glucose by cancer cells (the Warburg effect), which interferes with the synthesis of DNA needed for (cancer) cell proliferation.

CONTRAINDICATIONS & DOSAGE

Avemar is not advised for pregnant womenor nursing mothers.  To boost the immune system / fight cancer,it is recommended those with cancer take 8.5 grams daily of Avemar.  Note:  Avemar costs around US$160 per month.  Visit www.avemar.com.au to order Avemar and for further background research information. 
  

DMG (N-DiMethylGlycine)

DMG is an important tool in restoring the body’s immune system for those with cancer and HIV.  What is so incredible about DMG is: how quickly it works (within weeks), how safe it is (there are no known side effects), and how affordable it is (less than US$70 for a 2 month high-dose supply).

DMG has been shown to consistently increase T cell / CD4 count in those with cancer and HIV by 50%-300% within 2 months of taking DMG.  DMG or N-Dimethylglycine is a non-protein amino acid found naturally in animal and plant cells.  It is a non-toxic, solid, water-soluble substance, and has been used as a nutritional supplement for 30-40 years.  

World Research Links DMG to Increased Immune Response

Researchers at Kazan Veterinary Institute (Soviet Union) first began using DMG to restore immune competence to guinea pigs and rabbits exposed to intense X-irradiation in the 1960s.

Charles Graber and his team of researchers at the Medical University of South Carolina found that DMG could significantly influence immune function in a number of in-vitro and in-vivo models, and published the following findings in the Journal of Infectious Diseases (1981): 1.  DMG invoked a humoral (increased antibody response) in rabbits given a typhoid vaccine, thus demonstrating enhanced B-cell activity.  2.  DMG increased T-lymphocyte population in an in-vitro lymphocyte blast transformation test on blood samples of 75 individuals.  3.  A double-blind study involving 20 human subjects showed DMG to be effective in stimulating both a humoral (antibody) as well as a cellular-mediated immune response when a Pneumovax vaccine was administered as an immune challenge.  Antibody's increased 4.5-fold compared to the control group and Leukocyte Inhibition Factor (LIF) also increased significantly in those given DMG.  The research demonstrated that DMG significantly stimulates B-cells to produce higher antibody responses (humoral branch) and to potentiate a greater activity of T-cells and macrophages (cellular immunity branch) - all-important cancer-fighting cells.

John W Lawson, PhD, of the Department of Microbiology and Molecular Medicine, Clemson University, found rabbits given DMG together with a typhoid or influenza antigen, produced a 4-fold increase in anti-body's compared to the control rabbits, and showed a 3 to 9 times greater increase in T-cell count, depending on the vaccine challenge used.  DMG was also found to cause a 2-fold increase in interferon (IFN) in these rabbits.  Interferon is a cytokine, a product of T-lymphocytes, which shows anti-viral and anti-tumor activity.  Lawson and his team also used DMG on a number of cells lines, and found as DMG concentrations increased, levels of cytokines, including TNF-a  (Tumor Necrosis Factor - Alpha), IL-1 and IL-2 (Interleukin-1 and 2), also increased for these cell lines.  This increase in cytokines greatly enhances immunity to infections as well as increased killing of cancer cells.  Dosages of DMG at even 10 times the recommended levels were found to be safe and did not lead to fever or inflammation. Clemson University also carried out a study on mice using DMG against the Melanoma antigen, a highly metastatic form of skin cancer.  Primary tumors developed in 70% of the mice in the control group given the melanoma antigen, but not given DMG.  None of the mice given DMG (who were also given the melanoma antigen) went on to develop primary tumors.

An immune study was carried out by the US Army to test the immune effectiveness of DMG.  Bruce Ivins, PhD, at the Medical Institute of Infectious Disease at Ft. Detrick, Maryland, evaluated the effects of DMG on guinea pigs given anthrax.  Both groups of guinea pigs were vaccinated against the anthrax virus, while one of these groups was given DMG in addition to the vaccine.  When the guinea pigs in both groups were challenged with a potentially lethal dose of virulent anthrax bacilli, 4 out of 9 (44%) of the vaccinated animals in the control group died.  Remarkably, 11 out of 11 (100%) of the vaccinated animals given DMG survived, demonstrating an enhanced immunity and enhanced cellular response.

The following is a reprint from the 4th edition of the AIDS Control Diet book by Mark Konlee (1992).  The AIDS Control Diet book is the forerunner of the current book on How To Reverse Immune Dysfunction:  "Early in July (1992), we talked to a man from California who had contacted us...He told us that 3 months earlier, he had doubled his T-cell (CD4) counts from 120 to 240 in one month by taking 800mg daily of DMG.  He had been on AZT for one year previous to this with his T-cell (CD4) counts holding steady at about 120.  He attributes the increase to DMG.  Then, he reportedly told four of his friends about his experiences with DMG.  They also tried it and used about 800mg per day (sublingually).  Everyone reported a signficant increase in T-cell (CD4) counts.  One man reportedly went from 45 to 170 in 2 months. Puna Wai Ora:  To test this claim, we chose a man infected with HIV at random who had a consistently low T-cell count that hovered between 180-240, that had remained between these levels for four years.  His last reading before taking DMG was 220.  This man took 750mg DMG daily (sublingually) for 6 weeks, then stopped.  Two months after he stopped taking DMG, his T-cell count was recorded at 360 by Auckland Hospital - Infectious Disease Unit, a 61% increase.

Hans Kugler, PhD, successfully treated his dog Foxie using DMG, who was diagnosed with a large abdominal tumor, possible carcinoma, in 1987.  An untrasound and blood tests revealed the tumor was very large and had spread to the liver and kidneys.  Kugler put Foxie on a daily regimen of 250mg of DMG daily, as the primary source of treatment.  After six weeks the tumor had shrunk to half its original size and continued to decrease until the twelfth week when it was barely noticeable.  Later examination revealed the tumor was completely gone, and Foxie had returned to normal health. [Preventative Medicine Up-Date 1990]

CONTRAINDICATIONS & DOSAGE

DMG is not advised for pregnant women or nursing mothers and should only be used in children under medical supervision.  There are no known reports of overdose with DMG.  DMG can lead to mild ulceration of the mouth and chalky teeth - these side effects pass after ceasing DMG intake. Rinse with warm salt water after meals and before bedtime to help heal broken areas, ulcers or sores in your mouth.

To boost the immune system, it is recommended those with active cancer or HIV take 750mg – 1000mg of DMG daily, sublingually (under the tongue), in between meals for 6-8 WEEKS. This should be taken as 2-3 capsules / tablets three times a day.  Those in remission should consider taking 250mg – 500mg DMG daily.  DMG can be purchased from Physicians Formulas (60 tablets at US$9. 95).  You will need to purchase seven (7) bottles ($69.65) for a 2 month supply on a higher dose of 750mg.