Jun 13, 2009

Cancer Book-Chapter 8



The “Top 7 Stage IV” treatments detailed in Chapter 7 are the
ONLY treatments which I recommend for Stage IV cancer (except
for the “O.C.C.” detailed in Chapter 9). However, there are many
more alternative cancer treatments which are worth discussing. The
treatments addressed in this chapter are strong treatments for Stage
III cancers. They are in no particular order.
The Budwig Diet
A remarkable alternative cancer treatment was devised by a German
biochemist, Dr. Johanna Budwig, also a seven time Nobel nominee.
Her most important medical contributions involved her research
into the roles of essential fatty acids. In order to mass produce and
distribute foods high in oils, food manufacturers deliberately alter
the chemical composition of the oils, which gives them longer “shelf
lives.” In the 1950s, she proved that these chemically-altered,
hydrogenated fats (which she called “pseudo” fats) are rigid fats
“There is not one, but many cures for cancer available.
But they are all being systematically suppressed by the
ACS, the NCI and the major oncology centers. They
have too much of an interest in the status quo.”
Dr. Robert Atkins
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which stick to the cell membranes, thus causing them to
malfunction.
Dr. Budwig believed that these hydrogenated, processed fats and oils
shut down the electrical field of the cells and make us susceptible to
chronic and terminal diseases, since the beneficial oxidase ferments
are destroyed by heating or boiling. She also demonstrated that the
absence of healthy unsaturated fats (i.e. omega-3 and omega-6) is
responsible for the production of oxidase, which induces cancer
growth and is the cause of many other chronic disorders. She came
to believe that cancer was not the result of too much cell growth,
but defective cell growth (i.e. cell division), caused by the
combination of too much “pseudo” fats and too few healthy fats in
the cell membrane.
But exactly what happens to fats when they are processed? In
healthy fats there is a vital electron cloud which enables the fat to
bind with oxygen. Healthy, oxygenated fats are capable of binding
with protein and in the process become water-soluble. This water
solubility is vital to all growth processes, cell damage restoration,
cell renewal, brain and nerve functions, sensory nerve functions,
and energy development. In fact, the entire basis of our energy
production is based on lipid metabolism. Hydrogenation destroys the
vital electron cloud and as a result, these “pseudo” fats can no longer
bind with oxygen or with protein. These fats end up blocking
circulation, damaging the heart, inhibiting cell renewal, and
impeding the free flow of blood and lymph. Might want to
remember this fact the next time you want to buy some margarine
or fried foods, since both typically contain these harmful fats.
Dr. Budwig began to study fats in the 1950s, and she quickly
discovered much more about the metabolism of fats than had
previously been known. She began her research by analyzing the
blood samples of thousands of seriously ill patients, then she
compared these samples to the blood of healthy people. She soon
found that the blood of seriously ill cancer patients was deficient in
certain important essential ingredients, including phosphatides and
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lipoproteins, whereas the blood of a healthy person always
contained sufficient quantities of these ingredients.
She hypothesized that the lack of these ingredients resulted in the
proliferation of cancer cells. When she analyzed the blood of cancer
patients, instead of finding healthy, red, oxygen-rich hemoglobin,
she discovered a greenish-yellow substance. She found that when
these natural ingredients were replaced, that the cancerous tumors
began to shrink. The strange greenish elements in the blood were
replaced with healthy red blood cells as the lipoproteins and
phosphatides amazingly reappeared. She then discovered that eating
a combination of two foods would replace the lipoproteins and
phosphatides and turn the blood healthy again.
She discovered that these abnormalities were linked to a deficiency
in omega-3 and omega-6 essential fatty acids (EFAs), which are
essential to our health. Ocean fish (such as salmon, tuna, and
mackerel) are the highest in omega-3 fats, while seeds and nuts
(such as flax, linseed, and walnuts) are the highest in omega-6 fats.
When we take a closer look at our cells, we find that the cell walls
are made of fats, the most common being omega-3 fats and
cholesterol. The EFAs are full of electrons, which bind to oxygen
and proteins, and when they are absorbed into the cell wall, they
pull oxygen into the cell. And when bound to sulfur-based proteins,
they become water-soluble. This is the theory behind the Budwig
Diet: the use of oxygen in the organism can be stimulated by sulfurrich
proteins, which make oils water-soluble.
On page 85 of his book Oxygen Therapies, Ed McCabe discusses his
point of view on essential fatty acids: “The red blood cells in the
lungs give up carbon dioxide and take on oxygen. They are then
transported to the cell site via the blood vessels, where, they release
their oxygen into the plasma. This released oxygen is ‘attracted’ to
the cells by the ‘resonance’ of the … fatty acids. Otherwise, oxygen
cannot work its way into the cell. ‘Electron rich fatty acids’ play the
decisive role in respiratory enzymes, which are the basis of cell
oxidation.” Essential fatty acids combined with sulfur-rich proteins
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(such as those found in cottage cheese and yogurt) increases
oxygenation of the body, since the electrons are naturally protected
until the body requires the energy.
Of course, as you would expect, she was persecuted for her work.
Just think of the money generated each year from the fat and oil
industry. The hydrogenation process is central to both of these
industries, and Dr. Budwig’s theory was based upon the foundation
that hydrogenated fats contribute to the formation of cancer cells!
Eventually, she was prevented from doing further research and
prevented from publishing her findings.
In her own words, “I have the answer to cancer, but American
doctors won’t listen. They come here and observe my methods and
are impressed. Then they want to make a special deal so they can
take it home and make a lot of money. I won’t do it, so I’m
blackballed in every country.” Thank God, she endured and now her
work is available for us.
Several excellent sources of sulfur-rich proteins are nuts, onions,
chives, garlic, and especially cottage cheese and yogurt. The flaxseed
oil should optimally be virgin, cold-pressed, organic, liquid,
refrigerated, and unrefined. One of the best brands is Barlean’s High
Lignan Flaxseed Oil. The blend of flaxseed oil and cottage cheese
should be a part of every cancer patient’s diet. You simply mix one
cup of organic cottage cheese with 2-3 tablespoons of flaxseed oil. Be
sure to mix them together and let them sit for several minutes. This
will convert the oil-soluble omega-3 into water-soluble omega-3. It
is important to note that neither foods rich in EFAs nor sulfur-rich
proteins alone will accomplish these tasks. This is because the oils
must first bind to the proteins before oxygen can be bound and
before the body can assimilate the combination.
I also munch on dehydrated flax seed crackers that Charlene makes
along with cottage cheese, stevia, and strawberries. It’s an excellent
snack and boy is it healthy! I also like to add a couple of tablespoons
of Carlson’s Fish Oil, an excellent source of omega-3 fats. If you have
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cancer and use the Budwig Diet, be sure to stay away from sugar, all
animal fats, salad oils, and hydrogenated oils.
Thanks to the tireless work of Dr. Budwig we now know that
electron-rich fats interact with sulfur-rich proteins to bind oxygen
and promote aerobic metabolism which restores health. According
to Dr. Dan C. Roehm, M.D. (oncologist and former cardiologist),
“What she (Dr. Johanna Budwig) has demonstrated to my initial
disbelief but lately, to my complete satisfaction in my practice is:
CANCER IS EASILY CURABLE, the treatment is dietary/lifestyle,
the response is immediate; the cancer cell is weak and vulnerable;
the precise biochemical breakdown point was identified by her in
1951 and is specifically correctable, in vitro (test-tube) as well as in
vivo (real)... This diet is far and away the most successful anti-cancer
diet in the world.” (Townsend Letter for Doctors, July 1990)
Bill Henderson has worked with over a thousand “terminal” cancer
patients. The keystone to his treatment protocol is the Budwig Diet.
I read his book, Beating Cancer Gently, a couple of years ago. It is
an excellent book, and the neat thing is that he will work with you
over the phone. His protocol includes some very advanced
attributes that make it one of the most potent cancer treatments
available. He really focuses on a strict cancer diet, which is one of
the reasons that it is such a wonderful protocol. And as the name
says, it is also one of the most “gentle” treatments. Anyone who
chooses the Budwig protocol should use Bill Henderson’s protocol.
You can purchase his book here: www.beating-cancer-gently.com.
Dr. Kelley’s Enzyme/Metabolic Therapy
The primary basis of the enzyme/metabolic therapy for cancer
emanates from the recognition that cancer cells are virtually
indistinguishable from placental cells found in pregnancy. This
theory, called the “trophoblast” theory, was proposed by Scottish
embryologist, Dr. John Beard, around 1900. First he observed that
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the invading placental (trophoblast) cells were astonishingly similar
to cancer cells, and other observations led him to believe there was
an intimate correlation between these trophoblasts and cancer cells.
In early fetal development, the placental trophoblasts produce a
protective environment (placenta) and a source of nutrition
(umbilical cord), much in the same manner as cancer cells form a
protective environment (tumor) and a source of nutrition (new
blood supply). Another observation was that the placental
trophoblasts seem to take a downturn in activity around the 8th
week of pregnancy. It became clear to Beard that this downturn
coincided with the completion of the digestive system in the fetus,
and the activation of the fetal pancreas.
Modern medical research has also shown that these trophoblast cells
secrete a hormone called human chorionic gonadotropin (hCG), and
the quantities of this hormone rise until around the 8th week and
then begin to taper off. It is this very hormone that coats the
trophoblast cells and cancer cells and makes them impervious to our
immune system. It has been proven that hCG is found in all types of
cancers. Other than the trophoblast cell and the cancer, no other
human cells produce hCG. So, if you take an hCG urine test and get
a positive result, then you are either a pregnant woman or you have
cancer.
Trophoblasts are also surrounded by a coating of glycoprotein
including a molecule that give them a negative charge. This same
type of coating is found around the cancer cell. And in fact, it is one
of the chief reasons for classifying all cancer cells as “trophoblastic.”
Also negatively charged are the leukocytes (white blood cells) of the
immune system. And as we all know, like charges repel, while
opposites attract. This being so, both trophoblasts and cancer cells
are impermeable to the immune system’s natural defense
mechanism.
Remember that the placental trophoblasts produce hCG until the 8th
week of pregnancy, when they taper off. This is a direct result of the
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fact that the fetal pancreas begins to produce enzymes! And when
certain enzymes, namely trypsin and chymotrypsin and amylase,
encounter a trophoblast cell, they are able to break down its
negatively charged protein coating. This is why “morning sickness”
typically begins around the 8th week of pregnancy – the fetal
pancreas is not yet fully developed and does not yet produce
amylase, which is responsible for digesting glycogen (the “glyco”
part of the glycoprotein coating). As a result, the glycoproteins are
not broken down into their smallest units, and the mother’s kidneys
and pancreas are both forced to compensate and become overloaded.
The result is nausea, pain in the lower back, and low energy. Thus,
the pregnant mother can supplement her diet with amylase to
minimize morning sickness.
Interestingly, one of the rarest cancers is cancer of the duodenum,
which is the area of the intestines which is highest in pancreatic
enzymes. The reason that we do find cases of pancreatic cancer is
that the enzymes have not yet been “activated” in the small
intestine. This is also the reason that pancreatic cancer has such a
high mortality rate – the pancreas loses its ability to produce
enzymes, thus there is no control mechanism for the cancer!
In 1911, Dr. Beard published a paper entitled The Enzyme Therapy
of Cancer, which summarized his therapy and the supporting
evidence. After his death in 1923, the enzyme therapy was largely
forgotten, especially with the advent of Marie Curie and her
radiation work. The pioneer in the development of
Enzyme/Metabolic therapy was Dr. William Donald Kelley (a Texas
orthodontist). Around 1960, at the age of 35, his health began to
deteriorate. In 1964, a series of X-rays showed the signs of advancing
pancreatic cancer, including lesions in his lungs, hip and liver. The
surgeon said Kelley was too sick to operate on and told Mrs. Kelley
(his wife and the mother of his four children) that he had 4 to 8
weeks to live. Kelley was ready to give up, but his mother was not!
She threw out the junk food and meat and instructed him to eat only
fresh and raw fruits, vegetables, nuts, grains, and seeds. After several
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months, Kelley began to feel better, and he was even able to return
to work.
However, after 6 or 7 months, he stopped improving and developed
severe digestive problems, probably from the advancing cancer. He
therefore began taking pancreatic enzymes to aid his digestion, and
eventually increased the dose to 50 enzyme capsules per day. It was
at this point that he discovered the work of Dr. John Beard
concerning the relationship of pancreatic enzymes to cancer. He also
encountered the writings of Dr. Edward Howell, an early advocate
of the raw plant food diet. In time, Kelley fully recovered from his
cancer. Considering the fact that the Medical Big Medicine still
considers pancreatic cancer incurable, this was very impressive!
Kelley theorized that the formation of cancer was attributable to
excess female hormones which were responsible for changing a stem
cell into a trophoblast cell. Simply put, this means that cancer is the
growth of normal tissue, but at the wrong place at the wrong time.
He believed that cancer progresses due to a lack of pancreatic
enzymes that digest the cancer cells. Eventually, Kelley went on to
treat over 33,000 patients who had cancer. That’s right…33,000. Dr.
Kelly had a cure rate of 93% in patients that lived at least 1½ years
after starting his treatment.
Of course, the building blocks of his treatment protocol were
pancreatic enzymes. He also instructed patients to eliminate
pasteurized milk, peanuts, white flour and sugar, chlorinated water,
and all processed foods. Dr. Kelley developed a line of over 50
nutritional formulations for different types of cancers, and he always
individualized plans for patients according to their own metabolic
type. The typical Kelley diet restricts protein, is 70% to 80% raw,
and emphasizes whole grains, fruits, vegetables, raw juices, sprouts,
and pancreatic enzymes. Coffee enemas are taken to help the body
detoxify and to eliminate toxins secreted by tumors as they dissolve.
The Cancer Industry, in their pompous ignorance and diabolical
greed, didn’t like Dr. Kelley curing cancer with inexpensive
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enzymes! So, they sent a young medical intern, Dr. Nicholas
Gonzalez, to investigate Kelly’s claims and debunk him. Gonzalez
traveled to Dallas in 1981 to interview and investigate Dr. Kelley.
He was astonished to find case after case of appropriately diagnosed,
advanced cancer patients who were healthy and active 10 to 15
years after their diagnosis. Kelley made all his records available, of
over 10,000 patients, and encouraged Gonzales to contact any and all
of them. Eventually, the study sample was narrowed down to 50
cases which represented 25 different types of cancer. All 50 patients
were initially diagnosed as terminal. The median survival of this
group of 50 patients was 10 years!
As incredible as these results seemed, Dr. Gonzalez decided to go a
step further. He wanted to focus on pancreatic cancer, since the 5
year survival rate with orthodox treatments is virtually zero percent.
He searched and found 22 pancreatic cancer patients who had been
treated by Dr. Kelley between 1974 and 1982.
The 22 patients fell into three categories:
1. Ten patients consulted with Kelley only once and never
went on the protocol – All had died.
2. Seven patients followed the protocol only partially and
sporadically (as determined by interviews with family
members, doctors, and records) – All had died.
3. However, five patients followed the protocol completely –
All achieved long-term remission (although one had died of
Alzheimer’s disease after 11.5 years of survival). The median
survival rate of these five pancreatic cancer patients was 9
years!
Of course, as with other medical mavericks, Dr. Kelley had his share
of persecution from the Cancer Industry and its wolves. He was
issued a restraining order which prohibited him from treating
anything but dental disease. When he violated this order, he was
thrown in jail. A Texas court also made it illegal for him to distribute
his self-published booklet, entitled One Answer To Cancer. This
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makes Dr. Kelley the first (and only) doctor ever to be prohibited by
court decree from publishing!
Although he appealed the decision to the United States Supreme
Court, arguing that his First Amendment rights were being
flagrantly violated, the ruling was upheld. He eventually had to
move his clinic to Mexico. Not surprisingly, his enzyme/metabolic
therapy protocol was put on the American Cancer Society’s
Unproven Methods blacklist in 1971 where it remains today.
However, One Answer To Cancer can be found here:
www.drkelley.com/CANLIVER55.html. Check out Dr. Kelley’s
website here: www.drkelleycancerprogram.com.
Dr. Kelley died in 2005, but before he died, he wrote a book entitled
Cancer: Curing the Incurable Without Surgery, Chemotherapy or
Radiation. This book is even better than his first book and is
available on Amazon.com. His work is currently being continued by
Dr. Gonzalez, who runs a clinic in New York City. His phone
number is 212-213-3337 and his website is www.dr-gonzalez.com.
Vitamin B17 (Laetrile)
When dad died back in 1996, I began my cancer journey. The first
alternative cancer treatment which I discovered was Vitamin B17,
also known as Laetrile. I saw a video of a champion arm wrestler
named Jason Vale who had been cured of cancer by eating the seeds
from apples and apricots (which contain vitamin B17) and read lots of
good information on his website. The logic and science of how and
why vitamin B17 kills cancer cells was fascinating to me. Laetrile
therapy is based upon the theory that cancer is result of a nutritional
deficiency, and is based upon the trophoblast theory of cancer.
In the 1940s, Dr. Ernst T. Krebs, Sr. and his son (Dr. E.T. Krebs, Jr.)
and other doctors were involved in researching Beard’s thesis on the
trophoblast theory of cancer and they affirmed that he was correct.
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In 1949, the elder Krebs wrote a paper on the pregnancy toxemias
and the role of the pancreas and trophoblast in these disorders. The
following year, Dr. Krebs and his son published a paper The
Unitarian or Trophoblastic Thesis of Cancer, in the Medical Record,
New York.
In the following years, the Krebses investigated co-enzymes, and the
possibility that cancer results from a vitamin deficiency disease. In
the early 1950s, they theorized that cancer was caused by the lack of
an essential food compound in modern-man’s diet, identified as part
of the nitriloside family which is found in over 1200 edible plants.
Krebs learned of the kingdom of Hunza in the Himalayan Mountains
of Northern Pakistan, who were said to be “cancer-free.” Doctors
Krebs knew that they ate huge quantities of apricots, but they did
not believe that the fruit contained any cancer fighting substances.
Until they learned that the Hunzakuts also eat the pits of the apricot
seeds, which are one of the richest sources of nitrilosides!
Nitrilosides are especially prevalent in the seeds of apricots, peaches,
apples, millet, bean sprouts, buckwheat, and other fruits and nuts,
including bitter almonds. Dr. Krebs was able to extract certain
glycosides from plants which contained nitrolosides, and eventually
applied for a patent for the process of producing a metabolite form of
these glycosides for clinical use. He named it “Laetrile.” (LAE-vomandeloniTRILE-
beta-glucuronoside).
It took several years and actual clinical testing around the world
before a model was proposed rationalizing the utility of Laetrile in
the prevention as well as the treatment of cancer, when it received
the name “Vitamin B17.” Now, it is important to remember that a
vitamin is a co-enzyme, which basically means that it must be
associated with an enzyme in order for the enzyme to function
optimally. We know that the pancreatic and other enzymes are
reliant upon several essential co-factors and co-enzymes. Let’s
remember this “co-enzyme” information as we learn a little bit more
about the Hunzakuts.
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The Hunzakuts consume between 100-200 times more B17 in their
diet than the average American, due mainly to eating the seeds of
apricots and also lots of millet. Interestingly, there is no such thing
as money in Hunza. A man’s wealth is measured by the number of
apricot trees he owns. And the most coveted food is the pit of the
apricot seed, one of the highest sources of B17 on earth. Visiting
teams of doctors found the Hunzacuts to be cancer free. One of the
first medical teams to study the Hunza was headed by world-renown
British surgeon Dr. Robert McCarrison. Writing in the AMA Journal
January 7, 1922 he reported: “The Hunza has no known incidence of
cancer. They have an abundant crop of apricots. These they dry in
the sun and use largely in their food.”
But why haven’t you heard of vitamin B17? It seems so simple! Well,
the fact of the matter is that the Cancer Industry has suppressed this
information and has even made it illegal to sell B17. Big Medicine has
mounted highly successful “scare” campaigns based on the fact that
vitamin B17 contains quantities of “deadly” cyanide. This is patently
false. Studies show that vitamin B17 is harmless to healthy tissue.
Here’s why: each molecule of B17 contains one unit of hydrogen
cyanide, one unit of benzaldehyde and two of glucose (sugar) tightly
locked together. In order for the hydrogen cyanide to become
dangerous it is first necessary to unlock the molecule to release it, a
trick that can only be performed by an enzyme called betaglucosidase,
which is present all over the human body only in
minute quantities, but in huge quantities at only one place: cancer
cells. Thus the hydrogen cyanide is unlocked only at the cancer site
with drastic results, which become utterly devastating to the cancer
cells since the benzaldehyde unit unlocks at the same time. The
cancer cells get a double whammy of cyanide and benzaldeyhde!
Benzaldehyde is a deadly poison in its own right, but when it teams
up with cyanide, the result is a poison 100 times more deadly than
either in isolation. The cancer cells are literally obliterated!
But what about danger to the rest of the body’s cells? Another
enzyme, rhodanese, always present in far larger quantities than the
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unlocking enzyme beta-glucosidase in healthy tissues, has the ability
to completely break down both cyanide and benzaldehyde into a
silicate, which is much like aspirin. It contributes greatly to pain
control. Interestingly, malignant cancer cells contain no rhodanese
at all, leaving them completely at the mercy of the two deadly
poisons. This whole process is known as selective toxicity, since only
the cancer cells are specifically targeted and destroyed. Amazing,
huh?
Now remember that I earlier referred to vitamin B17 as a co-enzyme
and said that this therapy is based, in part, on the trophoblast theory
of cancer? The trophoblast theory focuses on the importance of
pancreatic enzymes (trypsin, chymotrypsin, and amylase) to digest
the protective coating around cancer cells. Here’s the connection
between this theory and vitamin B17: In the presence of certain
inhibitors in our blood, trypsin is inactivated and must be acted
upon by hydrogen cyanide to become active again. On this basis,
vitamin B17 acts as a co-enzyme to trypsin, since it provides
hydrogen cyanide, a harmless molecule, which reactivates the
trypsin which is necessary to digest the protective coating of cancer
cells. Fascinating, isn’t it?
The hundreds of clinical studies conducted by many competent
physicians around the world, including those directed by Dr. Emesto
Contreras at the Oasis of Hope Hospital in Mexico, give us complete
confidence that B17 therapy poses no threat to normal cells. This is
bad news for the Cancer Industry. Apricot seeds are cheap…real
cheap…not nearly as expensive as their latest chemotherapy drug
cocktail.
Believe it or not, the Cancer Industry outlawed vitamin B17 in the
1990s. That’s right...it is now illegal to sell apricot seeds in the U.S.
How absurd! Remember Jason Vale? Vale was diagnosed with
terminal cancer in 1986 and suffered from the disease for eight
years, enduring chemotherapy, radiation, and an operation to
remove a tumor. But in 1994, he saw a video touting apricot seeds as
a cure for cancer and began taking the seeds. He was cured of
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cancer! He began to sell the seeds on the internet. Big mistake!
Jason is now serving 5 years in prison for selling apricot seeds. As the
FDA Commissioner Mark McClellan stated, “The FDA takes
seriously its responsibility to protect patients from unproven
products being peddled on the internet by modern day snake oil
salesmen such as the defendant in this case. There is no scientific
evidence that Laetrile offers anything but false hope to cancer
patients.” What a crock!
The longest and most famous laetrile tests ever performed were run
for nearly 5 years at the United States’ most prestigious cancer
research center, Memorial Sloan-Kettering Cancer Center in New
York. Dr Kanematsu Suguira, the preeminent cancer researcher in
America, headed the team of researchers. At the conclusion of the
trials, on June 15, 1977, they released a press statement. The press
release read; “Laetrile was found to possess neither preventative, nor
tumor-regressent, nor anti-metastatic, nor curative anticancer
activity.”
So that is it then, right? Wrong. When a journalist asked Dr. Sugiura
“Do you stick by your belief that laetrile stops the spread of cancer”?
He replied, “I stick. ” He was then asked why Sloan-Kettering was
against using laetrile to fight cancer. Sugiura answered “I don’t
know. Maybe the medical profession doesn’t like it because they are
making too much money.”
Dr. Lloyd Schloen, a biochemist at Sloan-Kettering, also performed
test on laetrile, but he had also included proteolytic enzymes to his
injections and reported 100% cure rate among his albino mice. This
data had to be buried. Sloan-Kettering took action quickly. They
performed their own tests which were designed to contradict Dr.
Schloen’s findings. They then changed the protocols of the tests and
amounts of laetrile to make certain that they failed. Not surprisingly,
the tests failed, and that is what they reported. They couldn’t let the
word out that laetrile had been proven to be a natural, effective cure
for cancer. This would have spelled economic disaster for the
Cancer Industry.
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The most effective method of B17 treatment has been 6 grams,
intravenous once a day, usually given for three weeks. You should
also add zinc, since it is the transportation mechanism for B17 in the
body. Biochemists and researchers have found that you can give
massive doses of B17 to a patient, but if the patient was deficient in
zinc, none of the B17 would get into the tissues of the body. Also
important with B17 therapy are pancreatic enzymes, which form the
first layer of defense the body has against cancer. If you have a low
supply of these digestive enzymes then it will be difficult for B17 to
work. Also, emulsified vitamin A is usually used as an additional
supplement to B17 therapy. And laetrile therapy is best used in
conjunction with a very strict nutritional regimen, oftentimes with a
raw foods diet.
If you have cancer and are considering B17 therapy, I recommend
that you strongly consider visiting the Oasis of Hope in Tijuana,
Mexico. One of the principal proponents of laetrile was Dr. Ernesto
Contreras, who opened this clinic in 1963. Since that time, tens of
thousands of American citizens with cancer have traveled to the
Oasis of Hope, for treatments that have been outlawed by the
Cancer Industry in the United States. Dr. Ernesto Contreras passed
away of natural causes on October 14, 2003 at the age of 88. Today,
Oasis of Hope is directed by his son, Dr. Francisco Contreras. You
can visit their website at www.oasisofhope.com.
The Oasis of Hope is my most highly recommended cancer clinic, as
they employ strict nutritional regimen along with laetrile therapy,
all under the supervision of an oncologist. Oasis of Hope is a hightech
medical facility that employs cutting-edge technology, such as
digital CT scanners and state-of-the-art touch screen ventilators.
Doctors have access to electronic medical files through a wireless
LAN, which allows them to access patient records. Patients surf the
web on broadband workstations and keep in touch with loved ones
via digital telephone lines. The Oasis of Hope is comparable to the
top hospitals in the United States. If you have any questions about
admissions, please call 1-888-500-HOPE, Monday through Friday
between 8:00 AM and 5:00 PM Pacific time.
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If you want to take B17 as a preventative, Dr. Krebs suggested a
minimum level of fifty milligrams per day for normal, healthy adult.
Personally, I take one or two of the 100 milligram B17 pills every
evening before I go to bed. I also take two tablets of Intenzyme
Forte, a pancreatic enzyme. I purchase my B17 either from Medicina
Alternativa: www.tjsupply.com or CytoPharma: www.cytopharma.com.
Over the past decade, I have purchased B17 from both companies,
and both have proven to be reliable sources. A bottle of 100 pills
(100 milligrams per pill) is right around $20. A bit of trivia: the
bitter almond tree, a wonderful source of nitrilosides, was banned
from the United States in 1995.
Essiac Tea
My grandmother, Helen Cade, “Mama Helen” as we all
affectionately called her, was the church visitor for Castle Hills First
Baptist Church in San Antonio for over 40 years. She and my mom
had been 2 of the 18 charter members of the church way back in
1952. (The church now has over 10,000 members.) As the church
visitor, Mama Helen’s job was to travel to hospitals and visit sick
people … dying people … injured people. I remember traveling
with her and everywhere she went, to everyone she met, she would
say, “Honey, do you know Jesus?” And then she would proceed to
give them on of her “pet rocks” on which were painted “Jesus Loves
You,” then she would tell them about Jesus’ death and resurrection.
What a woman she was! I can only guess that there are literally
thousands of souls in heaven as a direct result of Mama Helen’s
witness for Jesus.
Mama Helen was diagnosed with terminal cancer in 1988. I’m not
sure where she learned of it, but almost immediately she began to
brew her own Essiac Tea. I remember going to her house in San
Antonio and helping her make the tea, fill those amber bottles, and
stick them in the fridge. She drank it faithfully, almost as faithfully
as she shared the gospel with everyone she met. I say almost as
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faithfully, because I honestly don’t know of anything that she did
more faithfully than share the gospel. Anyway, Mama Helen lived
another 10 years with her “terminal” cancer, largely as a result of
taking Essiac Tea, in my opinion. I’m not sure why, but she had
stopped drinking the tea about 2 years before she died.
Back in 1922, a Canadian nurse named Rene Caisse noticed some
scar tissue on the breast of an elderly woman. The woman told her
that doctors had diagnosed her with breast cancer years before.
However, the woman didn’t want to risk surgery nor did she have
the money for it. Providentially, she had met an old Indian medicine
man who told her that he could cure her cancer with an herbal tea.
The woman proceeded to tell Caisse about the ingredients in the tea.
About a year later, Caisse was walking beside a retired doctor who
pointed to a common weed and stated, “Nurse Caisse, if people
would use this weed there would be little or no cancer in the
world.” This “weed” (sheep sorrel) was one of the herbs in the
medicine man’s formula. The doctor had watched his horse cure
itself of cancer by repeatedly grazing in a particular part of the
pasture where sheep sorrel grew.
In 1924, Caisse wanted to test the tea on her aunt who had been
diagnosed with “terminal” stomach cancer and was given less than
six months to live. Caisse asked the physician, Dr. R. O. Fisher, for
permission to try the tea on her aunt, and he consented. Her aunt
drank the herbal tea daily for two months and recovered.
Amazingly, she lived for twenty more years! Caisse also tested the
tea on her mother who had been diagnosed with “terminal” liver
cancer and had been given less than two months to live.
Remarkably, her mother lived another 18 years!
Dr. Fisher and nurse Caisse immediately began treating cancer
patients with the magic tea, which she eventually named “Essiac,”
which is “Caisse” spelled backwards. She healed thousands of
terminal cancer victims with Essiac in her clinic between the mid
1920s and the late 1930s. At the height of her involvement, Caisse
saw up to 600 patients a week. The majority of those whom she
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treated came on referral with letters from their physicians certifying
they had incurable or terminal forms of cancer and that they had
been given up by the medical profession as untreatable. It was
typical for Nurse Caisse to give her patients the Essiac treatment at
no cost.
After word of her impressive results spread to the United States, a
leading diagnostician in Chicago introduced Caisse to Dr. John
Wolfer, director of the tumor clinic at Northwestern University
Medical School. In 1937, Wolfer arranged for Caisse to treat 30
“terminal” cancer patients under the direction of 5 doctors. She
commuted from Canada across the border to Chicago, carrying her
bottles of freshly prepared herbal brew. After supervising 18 months
of Essiac therapy, the Chicago doctors concluded that the herbal
mixture “prolonged life, shrank tumors, and relieved pain.” So
effective were her free treatments that in 1938 her supporters
gathered 55,000 signatures for a petition to present to the Ontario
legislature to make Essiac Tea an official cancer treatment. She fell
three votes short.
Caisse was not aware of the vast influence of Big Pharma and Big
Medicine, which were (and still are) more interested in making
money than in helping people. Essiac was cheap and non-toxic. It
could cut into the huge lucrative profits from the “Big 3.” Caisse
constantly played “cat and mouse” with Canadian federal health
officials. They demanded clinical tests, but she stubbornly refused to
divulge her formula unless she got official assurance that Essiac
would not be lost to the people who needed it, since her primary
loyalty was to the people who had come to depend on her. The
authorities couldn’t give her the assurance she needed, thus she
never divulged the formula.
Even the world’s largest cancer research center, Memorial Sloan-
Kettering Cancer Center in New York, could not convince Caisse to
divulge her formula. A steady stream of doctors visited her in
Canada, observing case files and talking to patients, pressuring her to
sell them the formula. She was offered huge sums of money to
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commercialize Essiac, but refused all but minimal amounts of
payment for her services. Not surprisingly, Caisse was heavily
persecuted and continually threatened with arrest. Finally, fearing
prosecution, she closed the clinic in 1942 and went into seclusion.
Rene Caisse died in 1978, at the age of 90. Before she died, she
signed over the rights to the Essiac formula to two parties: Resperin
Corporation of Toronto, to test, manufacture and distribute it, and to
a long-trusted friend, Dr. Charles Brusch of Cambridge,
Massachusetts, Director of the prestigious Brusch Clinic and
personal physician to former President John F. Kennedy. Dr. Brusch
himself had cancer of the lower bowel, which completely
disappeared after Essiac treatments. Brusch once stated “I know
Essiac has curing potential. It can lessen the condition of the
individual, control it, and it can cure it.”
On a side note, Dr. Frederick Banting, the co-discoverer of insulin,
became interested in Essiac and even offered Nurse Caisse research
facilities to test it. He believed that Essiac must somehow stimulate
the pancreas into functioning properly. Remember the trophoblast
theory of cancer and the pancreatic enzymes? Hmmmmmm…very
interesting…
BEWARE: Due to the increasing popularity of Essiac, numerous
“entrepreneurs” on the internet have jumped on the Essiac
bandwagon with their own four, six, or eight-herb products. But
Caisse never published her formula. The only person she trusted to
help her make Essiac was her best friend, Mary McPherson, who
knew the formula by heart. Dr. Gary Glum had also learned the
formula from one of Caisse’s patients and published it in 1988.
According to Dr. Glum, the original Indian formula contained only
four herbs. Every herbal formula has its own synergy and therefore
creates a specific effect. Essiac works. Why change it by adding
more herbs that may diminish its proven healing powers?
Anyone can verify, with a computer, the correct Essiac formula that
Caisse entrusted to Mary McPherson. Simply visit “The Rene M.
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Caisse Memorial Room” at www.octagonalhouse.com and click on
the “Essiac” hotlink. There you will see this formula:
􀂾 6 1/2 cups cut up Burdock Root (cut into pea-sized pieces)
o For centuries, burdock root has been regarded as an
effective blood purifier that neutralizes and
eliminates poisons from the body. Studies have
shown anti-tumor activity in burdock. Japanese
scientists have isolated an anti-mutation property in
burdock, which they call the “B factor.” A memo
from the WHO revealed that burdock is effective
against HIV.
􀂾 1 pound powdered Sheep Sorrel
o Caisse isolated sheep sorrel leaves as the main essiac
herb that dissolves cancerous tumors. Sheep sorrel
contains aloe emodin, a natural substance that shows
significant anti-leukemic activity. Sheep sorrel
contains antioxidants, is diuretic and has been used
to check hemorrhages.
􀂾 1/4 cup powdered Slippery Elm Bark
o Slippery elm is well-known for its soothing
properties. It reduces inflammations such as sore
throat, diarrhea, and urinary problems. It contains
beta-sitosterol, which has shown anti-cancer
activity.
􀂾 1 ounce powdered Turkish Rhubarb Root
o “Turkey Rhubarb” has been shown to have antitumor
activity. It is diuretic, anti-inflammatory, and
anti-bacterial.
IMPORTANT: As with all herbal teas, Essiac’s ability to work is
heavily dependent on the quality of the growing, processing, and
storage of the herbs. Herbs that have been dehydrated or frozen are
basically useless. It is best if you can grow your own fresh herbs.
The preparation of Essiac Tea is as important as the formula itself.
Essiac is a decoction, not an infusion. An infusion is what people do
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when they put a tea bag in a cup of hot water. Generally speaking,
an infusion tends to extract vitamins and volatile oils. A decoction is
used to extract minerals, etc. from roots, bark or seeds by boiling for
several minutes and then allowing the herbs to steep for several
hours. Entrepreneurs often sell Essiac imitations in tincture form
(herbs in alcohol) or in gelatin capsules; neither form is Essiac
because Essiac is a decoction.
1. Using a stainless steel pot and lid, boil 1/2 cup of herb mix in
one gallon of pure, unchlorinated water for ten minutes.
2. Turn off heat and allow herbs to steep for 12 hours.
3. Heat up tea to steaming, but not boiling. Allow herbs to
settle a couple minutes.
4. Strain off hot liquid into sterilized canning jars. The
remaining pulp can be used for healing poultices.
5. Refrigerate tea. For long-term storage use the boiling water
bath canning method and store in a cool, dark, dry place.
For preventive purposes, people take 1 to 2 oz. (1/8 to 1/4 cup) per
day diluted with about 1/2 cup hot water. Be sure to drink plenty of
water (at least half a gallon) each day to help flush the toxins out of
your system. If you have cancer, you should take Essiac three times
a day. Do not eat or drink anything (except water) one hour before
to one hour after taking Essiac. Essiac tea is compatible with other
alternative cancer treatments, except for Cancell. Do not take
ProtocelTM with Essiac tea, since they tend to neutralize each other.
Check out http://theherbs.info for more info on Essiac Tea,
including numerous quality vendors.
Oleander Soup
In the early 1960s, a Turkish doctor named H. Zima Ozel discovered
a group of rural Turkish villagers who were amazingly healthy and
disease free, compared to other similar villagers. When he
investigated further, he found that the healthy villagers were all
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taking a folk remedy that had been used in the Middle East for over
2 millennia. This remedy was based on a common plant referred to
in the Bible as the “desert Rose,” or more commonly to most of us,
the oleander plant. This plant is a highly toxic plant when ingested
raw, but the source of a wonderful remedy when properly prepared.
The term “oleander” refers to two plant species, Nerium oleander
(common oleander) and Thevetia peruviana (yellow oleander). Both
species contain chemicals called “cardiac glycosides” that have
effects similar to the heart drug digoxin, which can be toxic.
However, virtually every substance a person puts in their mouth is
toxic if taken in high enough doses. Sugar is toxic if you eat too
much of it. So is processed salt.
Let’s get back to our “oleander” history lesson. After his discovery,
Dr. Ozel applied for a patent. In his patent application, he
mentioned several case studies as well as one study which included
494 patients. Here is a quote from the patent application: “Between
January 1981 and December, 1985, 494 patients with inoperable,
advanced malignant diseases were tested with NOI (injections of
oleander). All malignancy had previously been diagnosed at various
specialized medical institutions in Turkey and abroad. The
malignancies of these patients had progressed to a state where they
could no longer benefit from existing anti-tumor therapies. These
494 cases included examples of almost all varieties of malignancies
and were found in various organs.”
These 494 patients experienced improved quality of life as well as
regression of cancer, while reporting no notable side effects. The
best results were said to be in prostate, lung, and brain cancers. Even
sarcomas showed stabilization. Could it be that the oleander plant,
when prepared in the correct manner and administered correctly, is
preferentially toxic to cancer cells? If you remember, it is widely
accepted that there are numerous natural substances that are toxic to
cancer cells, but harmless to normal cells. In fact, there are many
natural substances that fit into this category. For example, purple
concord grapes have more than a dozen such substances. One of the
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goals of alternative cancer researchers is to find substances that are
toxic enough to kill cancer cells, but not so toxic that they kill
normal cells.
This is where oleander comes into the equation. As I have
mentioned, oleander is toxic. It should always be handled with
gloves. There are many other safety warnings when dealing with the
oleander plant. Rest assured, it is very toxic…to both cancer cells
and normal cells. But when we are able to dilute it in the
appropriate proportions, then it is still toxic to cancer cells but
harmless to normal cells! This level of dilution and toxicity is now
well-known.
Tony Isaacs has written what is, by far, the best ebook on oleander,
entitled Cancer’s Natural Enemy. If you plan on using this protocol,
please visit www.rose-laurel.com and purchase his ebook. It is very
inexpensive and very informative. In an email from Mr. Isaacs to
Webster Kehr, he stated, “I have heard nothing but good reports
from those who have been using oleander soup or the oleander
extract available now at Takesun do Brasil. Cancers gone, cancers in
remission, tumors shrinking, etc. And the reports out of South
Africa, where the government has embraced the mixture of oleander
plus agaricus blazei murrill, pau de arco and cat's claw extract combo
(80% oleander) is that every single patient is doing well. HIV-AIDS
halted and stabilized or even apparently reversed. And not one
single report to date of a serious side effect or adverse reaction to
oleander extract. It is a good feeling to be able to help someone.”
There is a chapter in the ebook titled “The Anti-Cancer and Disease
Protocol,” which details an extremely effective program for anyone
who wants to have the maximum chances of beating cancer and
disease. This chapter includes information on cleaning and
detoxification, diet, nutrition, building a strong immune system, and
cancer-fighting supplements.
The simple and honest truth is that oleander soup really works
incredibly well. The remedy can be used alone, with other immuneChapter
8 – Stage III Cancer Treatments Cancer – Step Outside the Box
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boosting supplements, and even with prescription medications and
conventional treatments such as the “Big 3.” From testimonials that
I have read, I have learned that combining oleander with chemo or
radiation will either eliminate or greatly lessen virtually all of the
deleterious side effects, including hair loss!
If you do not live in an area of the world where the oleander plant
grows wild, you should be able to purchase seeds on the internet.
However, if time is of the essence and you don’t want to wait for a
plant to grow, it is probably best to buy live plants at a local flower
shop or over the internet.
BEWARE: Even though the dilution factor is now well established,
you should read and re-read Cancer’s Natural Enemy several times
before you begin processing a real oleander plant, since the oleander
plant is toxic. Even a small amount of the raw material, if ingested,
can cause death.
Coral Calcium
In the October 13, 1998 issue of the New York Times published an
article entitled “Calcium Takes Its Place As a Superstar of Nutrients”
in which it reports that a study published in the Journal of the
American Medical Association reported that “increasing calcium
induced normal development of the epithelia cells and might also
prevent cancer in such organs as the breast, prostate and pancreas.”
An understanding of the tremendous cancer fighting benefits of
calcium was initially developed by Dr. Carl Reich. He theorized that
most diseases were a result of overly acidic bodies coupled with a
calcium deficiency. He worked several years with Dr. Otto Warburg
on this theory, and eventually determined that many people show
signs of calcium deficiency because they were also deficient in
vitamin D. It has been demonstrated that phosphates, found in red
meat and other foods, prevent calcium from being broken down.
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Once the calcium has been broken down, its absorption into the
body is totally dependent on the presence of vitamin D in the
intestine. Unfortunately, vitamin D is rare in most foods. The best
way to get vitamin-D is to expose your skin to at least 20 minutes of
ultra violet sunlight each day, take cod liver oil, or a supplement. In
any event, vitamin D is absolutely required so the body will absorb
the calcium.
Vitamin D also acts an effective regulator of cell growth and
differentiation in a number of different cell types, including cancer
cells. Laboratory, animal, and epidemiologic evidence suggest that
vitamin D may be protective against some cancers. Clinical studies
now show vitamin D deficiency to be associated with four of the
most common cancers (breast, colon, skin, and prostate).
Dr. Reich collaborated with Robert Barefoot, a chemist, and wrote a
book entitled The Calcium Factor: The Scientific Secret of Health
and Youth. In this tremendous book, the authors state that no other
mineral is capable of performing as many biological functions as is
calcium. This remarkable mineral provides the electrical energy for
the heart to beat and for all muscle movement. It is also the calcium
ion that is responsible for feeding every cell, a feat accomplished by
latching on to seven nutrient molecules and one water molecule,
pulling them through the nutrient channel, detaching the load, and
repeating the process. One common denominator which links all
people who live past 100 years is that they all get massive amounts
(over 5 grams) of calcium daily.
Another important biological job for calcium is DNA replication,
which is the basis for all body repair and is crucial for maintaining
health and preventing degenerative disease. As important as all
these and hundreds of other biological functions of calcium are to
human health, none is more important than the job of pH control. It
has been said that “Calcium to acid, is like water to a fire.” Calcium
quickly destroys oxygen robbing acid in the body fluids. It is
interesting to note that Reich and Barefoot recommend DMSO and
cesium chloride for “terminal” cancer patients (i.e. patients that have
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less than 6 months to live). I agree with them 100%, as DMCC is my
#1 recommended Stage IV cancer treatment protocol. They also
have a complete cesium chloride protocol which also includes coral
calcium.
Why coral calcium? As rain falls on the earth and runs down to the
oceans it brings with it all the elements from the soils and rocks.
Organisms that eventually form coral reefs take up these elements.
Over thousands of years they can build up into islands (like
Okinawa). The coral is bio-chemically altered to contain all of the
mineral nutrients of life. As Barefoot says, “the result is a
powerhouse of natural marine nutrients known around the world as
coral calcium.” It’s important to note that calcium must be ionized
(broken into component parts) before it can be absorbed into the
cell. The beautiful thing about coral calcium is that it is already
ionized, therefore when you have the proper supplements present
with the coral calcium, absorption and utilization is greater.
For a cancer treatment, a person should take between 1 and 2 grams
of coral calcium with each meal, every day. You should be sure to
eat plenty of fruits and vegetables with the calcium to assist with the
absorption. I recommend ionic coral calcium, which you can add to
your drinking water. I have already recommended the Wolfe Clinic
in Canada for the DMSO/Cesium Chloride protocol, and they also
are an excellent source for top quality ionic coral calcium.
www.thewolfeclinic.com/calcium.html

Jun 12, 2009

Cancer Book-Chapter 9



Within the last year, I have learned of a brand new treatment
protocol, called the Overnight Cure for Cancer (“O.C.C.”). This
book would not be complete unless I included a chapter on this
protocol. It is similar to my #1 recommended cancer protocol (the
“DMCC” protocol), but there are some distinct differences. This
entire chapter is taken from the research of Webster Kehr of the
Independent Cancer Research Foundation, Inc. (“ICRF”) in
conjunction with the research of Dr. Darrell Wolfe of the Wolfe
Clinic in British Columbia. It is reprinted in its entirety with the
express permission of Mr. Kehr and Dr. Wolfe.
Theories Behind the O.C.C.
What Causes Cancer? The past century has revealed extensive
research implicating a microbial origin as the cause of cancer. At
the leading edge, Dr. Royal Rife’s 1930s research identified evidence
of a human cancer virus by isolating and culturing the suspected
virus. After injecting numerous rats with the microbe, cancer
consistently developed in both live cells and tissue cultures.
Numerous other researchers also found evidence proving Rife’s
“If someone wanted to develop a cancer treatment that
could work fast, it would have to be a treatment that
reverted cancer cells into normal cells!”
R. Webster Kehr
Chapter 9 – The Overnight Cure for Cancer Cancer – Step Outside the Box
186
findings. Currently, Canadian biologist Gaston Naessens uses
ultraviolet microscopy that easily views what has now been
identified as the BX cancer virus in live blood samples of cancer
patients.
Dr. Rife was the first to prove beyond any doubt that the microbe
involved in cancer formation is pleomorphic, meaning the microbe
has multiple morphologies that change accordingly with particular
external stimulus. Dr. Robert O. Young, PhD., asserts that this
pleomorphic microbe is found in every human being and it is
irrefutably the inner terrain of the individual that enables the
microbe to morph into cancer. Rife proved that the BX cancer virus
has four distinct forms that can induce cancer formation within 36
hours of medium alteration.
According to Rife,“in reality, it is not the bacteria themselves that
produce the disease, but the chemical constituents of these
microorganisms enacting upon the unbalanced cell metabolism of
the human body that in actuality produces the disease. If the
metabolism of the human body is perfectly balanced, it is susceptible
to NO disease.”
Every human body contains extremely small microbes called
“somatids,” “microzyma,” “bion,” or “protits.” These are essentially
viruses in hibernation that capitalize on our inability to properly
detoxify, in which case they morphologically change. Under ideal
conditions, these somatids are inert. However, once an organism
mutates as a result of a change or stimulus in the environment and
the virus penetrates a healthy human cell, the microbe easily alters
metabolic functioning within the cell. This metabolic alteration is
the precursor to the formation of cancer as described below.
Metabolic Changes and Cancer Formation. A variety of cancer
causing agents or toxic carcinogens, enter the body stimulating their
transformation into yeast, fungus, mold and/or bacteria.
Independent cancer studies on these microbes have produced varied
perspectives on the pleomorphic microbe; some call it a virus, some
Chapter 9 – The Overnight Cure for Cancer Cancer – Step Outside the Box
187
a fungus, a mold, an acid-fast bacteria or mycobacterium, even an
amoeba. Which of these descriptions is correct? Most likely all
descriptions are valid.
Researchers have indicated that the primary cause of cancer of a cell
is the microbial interference with both the Krebs Cycle and the
Electron Transport Chain (ETC) in the mitochondria. These two
cycles are essential for proper cell functioning, as they are involved
in the production of ATP (adenosine triphosphate), the cells’ energy
source. During normal conditions the cell has an amazing ability to
restore the Krebs Cycle and ETC once they are broken. But what
interferes with the highly regulated production of ATP and how is it
able to continuously inhibit its production?
As previously described, environmental changes cause the alteration
of the BX virus into cancer causing pleomorphic forms. These same
environmental changes may result in damage or weakening of cell
membranes, enabling these pleomorphic microbes to enter the
normal cell, whether presenting as a fungus, mold or bacteria.
Once inside, the microbe intercepts the glucose that is entering the
cell and uses it as fuel resulting in microbial fermentation of glucose,
which causes excretion of acidic mycotoxins and dangerous
hormones. These highly acidic secretions cause a drop in the cells’
pH, a characteristic of cancer cells. With the continuous
interception of glucose entering the cell, the mitochondrion receives
very little glucose to produce ATP. This instigates a dramatic drop
in the cells energy levels.
Signals are sent to the insulin and glucose receptors on the
membrane of the cells to become hyperactive and bind to more
glucose to facilitate cell entry. However, the microbe intercepts this
process and the mitochondrion is instead bathed in an increasingly
large sea of mycotoxins and hormones. Because there is a limit to
how high the activity of these two types of receptors can become, it
is impossible for the mitochondria to get enough glucose for energy
production. The cell is now officially cancerous due to the fact that
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its energy levels have drastically dropped and the cell switches to an
anaerobic state, as it is now fermenting glucose instead of breaking it
down.
The most important point is that a cancer cell consists of a very sick
human cell that is inhabited by a very healthy microbe.
Killing this microbe without killing the human cell is a tricky
process and most alternative cancer treatments kill the cancer cell
even if it is oxygen based.
There is one interesting thing about this process. Dr. Otto Heinrich
Warburg, a two-time Nobel Prize winner, discovered that cancer
cells receive their energy by fermenting glucose. In his own words,
Dr. Warburg said the following: “But, even for cancer there is only
one primary cause. Summarized in a few words, the cause of cancer
is the replacement of the respiration of oxygen in normal body cells
by a fermentation of sugar (glucose)” (Otto Warburg, The Prime
Cause and Prevention of Cancer, 1966).
Why is that important? Fermentation is impossible without yeast!
Yeast as a pleomorphic microbe now enters the cancer cell easily.
The microbe may enter the cell as a fungus, mold or bacteria, but
once inside the cell it ferments like yeast.
About the O.C.C.
The objective of this alternative treatment is to support the body
while effectively and efficiently turning cancer cells around. The
goals of the O.C.C. are to contribute to the successful treatment of
cancer by doing the following:
􀂾 To safely and quickly stop the spreading of cancer
􀂾 To reduce existing swelling, inflammation and congestion
thus increasing circulation
􀂾 To help the body revert as many cancer cells as possible into
normal cells
Chapter 9 – The Overnight Cure for Cancer Cancer – Step Outside the Box
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The main purpose of the treatment is to assist the body in
converting the maximum percentage of cancer cells back into
normal cells. Once reverted, these cells are subject to normal cell
death, known as apoptosis. Apoptosis does not cause swelling or
inflammation of tissue but instead may reduce it. This is the
opposite reaction to what the body may experience with other
alternative and conventional cancer treatments.
Because the O.C.C. requires a change in the metabolism of the
cancerous cell, it may take two or three weeks before it is fully
known what percentage of cancer cells have been reverted into
normal cells.
How the O.C.C. Supports the Body in Fighting Cancer
More than a dozen natural substances have been shown in vitro to
revert cancer cells back into normal, healthy cells. The most
successful of these substances is DMSO, which has been successfully
normalized several types of cancer cells. As such, DMSO and a
product known as MSM are the two key ingredients in the O.C.C.
DMSO (dimethyl sulfoxide) is a 100% natural substance which is
generally extracted from wood. A classic study using DMSO bound
to haematoxylon dye has proven that DMSO has the ability to
specifically target and enter cancer cells even with chemotherapy
treatment. More research has been done on DMSO, on more lines of
cancer, than on any other cancer fighting substance.
MSM (methyl sulfonyl methane), also known as DMSO2, is also an
important ingredient of the OCC treatment. It is generally made
from DMSO, but it is also ubiquitous in nature. MSM is completely
safe to use and is approximately 7 times less toxic than common
table salt.
Both DMSO and MSM are sulfur and methyl based molecules,
which have one (DMSO) or two (MSM) extra oxygen molecules. No
one knows for sure how DMSO and MSM work, but it is clear that
DMSO has the ability to enter cancer cells. One theory is that once
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190
inside the cancer cell, the DMSO and MSM molecules release their
extra oxygen atoms. These oxygen atoms are then used to kill the
microbes within the cancer cell without actually killing the cell
itself. Since the microbe is anaerobic, it has no immunity to an
oxygenated environment.
Emphasis should be placed on the vast differences between an
oxygen pair (O2) versus an oxygen singlet (O1). Most of the oxygen
in the body is the very stable oxygen pair, however, there is also
great need for oxygen singlets since they are used to kill microbes
and neutralize a number of dangerous molecules.
Most people have a significant shortage of oxygen singlets due to the
way food is processed. Both DMSO and MSM, among other
elements, provide oxygen singlets to the body without a high
amount of alkalinity; this allows the substances to be taken at much
higher doses. In addition, neither DMSO nor MSM are strong
enough to kill a cell, whether cancerous or non-cancerous. As such,
oxygen singlets and sulfur do not kill cells, but oxygen singlets can
kill microbes.
Once the microbe within the cancer cell is safely eradicated, the cell
begins the process of reverting the damage made by the microbe and
returning it to normal. Because the microbe is no longer
intercepting glucose, the mitochondria are able to produce ATP for
cellular use. Microbial death can occur overnight; however, the
process of reverting cellular metabolism to the normal state can take
several days or even weeks. It is possible for normal functioning
metabolism to be restored over time, although this is different in all
individuals.
There is much evidence that proves killing or halting the microbe’s
reproductive abilities, normalizes the cell allowing it to eventually
die a natural death through apoptosis. Dr. Rife, known for utilizing
electromagnetic waves based on the resonant frequency of the
microbe, supports this theory. This theory is similar to the Photon
Genie.
Chapter 9 – The Overnight Cure for Cancer Cancer – Step Outside the Box
191
How to Support the Body in Turning Cancer Around
There are a dozen alternative cancer treatments that currently have
a 50% success rate on advanced cancer patients. These treatments
work by directly eradicating the cancer cells and minimally take two
months to be affective.
When cancer cells die, the body needs time to remove it. As a
result, a rapid die-off of cancer cells and the associated debris can
overwhelm the body therefore an aggressive but cautious approach
is necessary.
The treatment targets the safe eradication of cancer cells, which
instigates an immune response by the body. The immune system
attacks the tissue causing painful and potentially dangerous swelling
and inflammation, which can be very dangerous particularly for
brain, lung and digestive cancers. For example, the targeting of a
mass of cancer cells within the brain can have detrimental affects
causing swelling that produces neurological problems, tissue damage
and even death.
However, treatment that reverts cancer cells into normal cells, with
no cell death and no detrimental symptoms, provides hope. As
previously discussed, the components of the O.C.C. treatment make
this possible by killing the cancer-causing microbe without killing
the cancer cell. This makes the O.C.C. unique when compared to
other alternative medicine treatments.
The O.C.C. Treatment
The O.C.C. treatment consists of dosages of DMSO and MSM every
half hour over a 12-hour period based on the age and weight of the
patient. During the treatment, no food is eaten for 12 hours before
and after the treatment. Also, no food is consumed during the
treatment, with only the topical application of DMSO, and ingestion
of MSM and the accompanying components of the therapy. This
results in a total of 36 hours of no food consumption.
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There are four premises behind the protocol during this therapy that
I will explain below:
1) Reverting Abnormal Cancer Cells into Normal Cells
This theory was explained above, with emphasis on this treatment’s
ability to convert cancer cells into normal functioning cells while
inhibiting negative symptom formation. DMSO and MSM have the
ability to target the cancer cell and initiate the conversion by
changing metabolic functioning within the cell with minimal
normal cell die-off.
2) The Fast
The O.C.C. protocol does not allow any food or drink and follows
the same theory as a “juice fast”. Eliminating the food supply to the
cancerous cells essentially starves the cancer-causing microbe. The
protocol involves the external application of DMSO, oral ingestion
of MSM and other supporting supplements only. The cells readily
absorb the abnormally high doses of DMSO and MSM provided by
the body, allowing for the direct targeting of the cancer cell and
eradication of the microbe.
The elimination of food ensures that no glucose is available for
microbe fermentation, although any lactic acid remaining can
potentially convert into glucose by the liver (known as the Lactic
Acid Cycle). Fortunately, MSM can bind to lactic acid and safely
remove it from the body, thereby reducing the availability of
glucose.
3) The Colon Cleanse
Although no food is entering the body, the colon still contains
putrefying waste from previous meals that must be eliminated.
Nutrients that have not yet entered the blood stream are still in the
digestive tract and potentially compete with and dilute the DMSO
and MSM.
It is essential for the colon to be cleansed prior to the
commencement of the treatment. This can be done using Royal Tea,
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a safe and gentle herbal colon cleanser and cell rejuvenator. Royal
Tea eliminates debris within the intestinal tract, in addition to
rejuvenating and toning the intestinal muscle. This promotes proper
elimination and efficient absorption of nutrients. This tea is used in
preparation for the protocol, during the therapy and after the
termination of the treatment. Royal Tea is safe to take on a
continual basis.
It is imperative to understand that the intestines are the main route
of nutrient absorption and detoxification. Without a proper
functioning intestinal tract, the effectiveness of any treatment is
compromised.
4) Consuming Small Quantities Several Times
The fourth key concept of O.C.C. is the consistent ingestion of small
doses of supplements over the course of the treatment. This ensures
a higher percentage of assimilation of nutrients than if only one or
two large doses were taken. This concept is comparable to the use of
IV’s in hospitals. IV doses are small and frequent therefore
effectively impacting the body because of efficient assimilation into
the cells.
A Final Comment on the Theory Behind the O.C.C.
After Dr. Rife identified and isolated the BX microbe within cancer
cells in the 1930s, he discovered the structural resonance frequency
of the virus. Based on this information, Rife developed an
electromagnetic machine that released resonance frequency waves
that could potentially be detrimental to the microbe. This particular
frequency, when applied to the microbe, eradicated the BX virus in
addition to other viruses, bacteria, mold, fungi, and yeast within the
body by lysing. Rife successfully utilized his technology on isolated
viruses and treat over 400 animals with tumors. Several frequency
machines have been produced since Rife’s initial findings.
The O.C.C. functions by starving the cancer cell of any glucose
source while subjecting it to the oxygen singlets of DMSO and MSM
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in order to eradicate the microbe within the cell. If the treatment is
unable to successfully kill all cancer causing microbes, at a
minimum, it has weakened the microbe within the cell. The
application of oscillations that vibrate at specific resonant
frequencies to the cancer cell will help eradicate the virus. Used in
44 different countries by holistic practitioners, the Photon Genie has
been shown to facilitate the regeneration of tissue and bone. The
use of a Photon Genie in conjunction with the O.C.C. treatment is a
superb combination.
In addition, research has also revealed that pulses released from a
magnetic field source, creates tiny electrical micro-currents in the
body. When these pulses are applied to human tissue they have the
ability to disable a wide range of microbes including viruses, fungi,
bacteria and parasites. The Sota Magnetic Pulser has shown to be
highly effective with all types of disease. When applied onto
infected areas of the body, this unit releases short bursts of a strong
magnetic field that travels through tissue layers and affectively
eradicates microorganisms within the tissue. I also suggest the use of
the Magnetic Pulser in conjunction with the O.C.C. treatment. Visit
www.thewolfeclinic.com for more information.
Supplements for the O.C.C.
The following products are necessary for the O.C.C. treatment and
are available at www.thewolfeclinic.com. The quantities indicated
are for the 3 day buildup and the 12 hour fast only. Some
individuals will extend or repeat the 12 hour fast and will require a
higher quantity of each product.
1. Four or more bottles of DMSO (16 fl.oz.) – 70% DMSO with
30% distilled water
􀀹 While perfectly safe, DMSO can legally be sold as a
“solvent”
􀀹 70% DMSO/30% distilled water penetrates the skin better
than 100% DMSO and is less irritating to the skin.
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􀀹 All doses in this article are based on 70% DMSO mixed
with 30% distilled water or 30% Aloe Vera
2. One pound of Lignisul Granular MSM Crystals
􀀹 MSM crystals should specifically state that there are “no
additives”
􀀹 We recommend the use of MSM cream or lotion in
addition to the granular crystals
􀀹 MSM cream and lotion are to be applied topically to
inhibit the formation of rashes from the application of
DMSO
3. One gallon of Theta Super Silver
􀀹 Super Silver is an antimicrobial product that specifically
targets any microbial, viral, and fungal infection within
the body.
􀀹 Made up of a nano sized vegetable mineral, Theta Super
Silver is readily absorbed into cells
􀀹 There is no toxic dose
􀀹 Ionic and colloidal silver do not compare to Theta Super
Silver in delivery and effectiveness
􀀹 Silver readily binds to DMSO and is transported by the
DMSO to the target cancer cell, where it helps attack any
microbial presence within the cell
4. One bottle of Vitälzym (450 capsules)
􀀹 Vitälzym is a systemic enzyme that:
o Facilitates metabolic functions within the body
o Cleanses tissue
o Increases circulation by relieving toxins and
delivering nutrients faster and efficiently
o Aids the immune system
5. One bottle of Green Supreme Barley Power (400 capsules)
􀀹 Green Supreme contains 1400 live digestive enzymes in
every capsule that benefits any health protocol
􀀹 Green Supreme contains:
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o VITAMINS – A broad spectrum of vitamins to help
the body operate at peak efficiency, fight disease and
maintain good health
o MINERALS – Principle minerals and numerous trace
elements which work hand-in-hand with vitamins for
balanced body performance
o ENZYMES – Hundreds of essential live enzymes to
facilitate vital body functions
o AMINO ACIDS – Essential building and maintaining
of body tissues
o FIBER – To aid digestion and elimination of debris
o ALKALINE pH – Boosts alkalinity to balance the
bodies pH; high acid levels is characteristically
common with cancer patients
6. Two gallons of purified, structured, Vitalized Water
􀀹 Do not used chlorinated or fluoridated water as these are
both known carcinogens
7. One pack of Royal Tea
􀀹 Contains herbal extracts high in antioxidants and enzymes
specifically for cleansing and rejuvenating the intestinal
tract at the cellular level
8. One bottle of Super Z-Lite (60 mL) & one pack of Super ZLite
capsules
􀀹 Contains Zeolite, humic fulvic acid, and ocean & plant
derived minerals
􀀹 Liquid crosses the blood brain barrier
􀀹 Capsules specifically targets cells within the intestinal tract
(works well with Royal Tea to eliminate toxins)
􀀹 Effective against harsh microorganisms; functions as a
broad spectrum anti-viral agent
􀀹 Supports a healthy immune system
􀀹 Balances pH levels
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Below is a list of additional products that you will need for this
treatment. These products can be purchased locally.
􀂾 A container of sea salt
􀂾 An empty eye dropper bottle (available at The Wolfe Clinic)
􀂾 Skin brush
Prior to the O.C.C. Treatment Protocol
Preparing the body for detox.
It is important to cleanse the colon prior to commencing this
treatment. This will ensure that food within the intestinal tract does
not “compete” with the DMSO and MSM in entering the cancer
cells. The colon cleanse should be done during the build up (see
below). We suggest using the Royal Tea and Super Z-Lite.
Structured, vitalized water can be taken at any time during the build
up and treatment. Stay away from chlorinated and fluoridated
water, as they are known carcinogens. Distilled water is not
hydrating for the body and exhibits a pH of 5.5. Water that will aid
in the delivery of nutrients and the elimination of toxins at a cellular
level is much more desirable.
The 3 Day Buildup Prior to the O.C.C.
The “official treatment” will consist of 25 “one dose” treatments over
a twelve hour period. Each dose is administered every half hour.
However, it is generally wise to take three days to build up to this
dose because of the following reasons:
􀂾 The three day buildup functions as an early-warning system
to catch the appearance of inflammation, swelling, or
congestion caused by the treatment. These symptoms can
include flu-like symptoms, increased swelling, inflammation
and congestion in the cancer area, and/or a rise in body
temperature.
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􀂾 Allows the patient to become accustomed to working with
the products, most importantly the DMSO.
􀂾 To allow the digestive tract to become accustomed to the
administered levels of MSM.
􀂾 To become confident in the safety of this treatment.
If for any reason during the buildup or the actual treatment, the
patient experiences increased inflammation, swelling or congestion,
terminate the entire treatment. Start again once the patient has
detoxified efficiently or an alternative treatment may have to be
started after a two- day wait.
Use Royal Tea and Super Z-Lite during the buildup to ensure proper
elimination is occurring. This is essential to success. No food or
drink should be ingested during the specified hours of the buildup
(high quality water is allowed)
A typical buildup is 3 days long and is administered as follows:
Day 1 Buildup
Treatment is taken for 3 hours; a total of 7 doses of DMSO and MSM
are taken at half hour intervals. Super Silver doses (both orally and
topically) will be maintained with each DMSO dose. Also, Vitalzym
and Green Supreme Barley Power doses should be started and
maintained during this time.
Day 2 Buildup
Treatment is taken for 6 hours; a total of 13 doses of DMSO and
MSM are taken at half hour intervals. Super Silver doses (both
orally and topically) will be maintained with each DMSO dose.
Also, Vitalzym and Green Supreme Barley Power doses should be
maintained during this time.
Day 3 Buildup
Treatment is taken for 9 hours; a total of 19 doses of DMSO and
MSM are taken at half hour intervals. Super Silver doses (both
orally and topically) will be maintained with each DMSO dose.
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Also, Vitalzym and Green Supreme Barley Power doses should be
maintained during this time.
Day 4 – 12 Hour Treatment
The twelve-hour O.C.C. treatment is administered on day 4.
When possible and if time is not an issue, it would be advisable to
start with a 7 day primer that consists of a thorough detoxification
program prior to starting the build up. This will help to create a
strong foundation for the treatment.
Tables 1 through 4 provide detailed instructions on the
administration of DMSO and MSM on the buildup days.
Table 1 – Three Day DMSO Buildup Schedule
Weight DMSO Build Up Day 1 DMSO Build Up Day 2 DMSO Build Up Day 3
200 lbs
1 tbsp every half hour for 3
hours
1 tbsp every half hour for 6
hours
2 tbsp every half hour for 9
hours
175 lbs
7/8ths tbsp every half hour
for 3 hours
7/8ths tbsp every half hour
for 6 hours
7/8ths tbsp every half hour
for 9 hours
150 lbs
3/4th tbsp every half hour
for 3 hours
3/4ths tbsp every half hour
for 6 hours
3/4ths tbsp every half hour
for 9 hours
125 lbs
5/8ths tbsp every half hour
for 3 hours
5/8ths tbsp every half hour
for 6 hours
5/8ths tbsp every half hour
for 9 hours
100 lbs
1/2 tbsp every half hour for
3 hours
1/2 tbsp every half hour for
6 hours
1/2 tbsp every half hour
for 9 hours
***Adult schedule
Table 2 – Three-Day MSM Water Buildup Schedule
Weight
MSM Water Mixture Build
Up Day 1
MSM Water Mixture
Build Up Day 2
MSM Water Mixture
Build Up Day 3
200 lbs
9 tbsp every half hour for 3
hours
9 tbsp every half hour for 6
hours
9 tbsp every half hour for 9
hours
175 lbs
9 tbsp every half hour for 3
hours
9 tbsp every half hour for 6
hours
9 tbsp every half hour for 9
hours
150 lbs
9 tbsp every half hour for 3
hours
9 tbsp every half hour for 6
hours
9 tbsp every half hour for 9
hours
125 lbs
9 tbsp every half hour for 3
hours
9 tbsp every half hour for 6
hours
9 tbsp every half hour for 9
hours
100 lbs
9 tbsp every half hour for 3
hours
9 tbsp every half hour for 6
hours
9 tbsp every half hour for 9
hours
***Adult schedule
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Table 3 – Child Three-Day DMSO Buildup Schedule
Weight DMSO Build Up Day 1 DMSO Build Up Day 2 DMSO Build Up Day 3
75 lbs
3/16ths tbsp every half
hour for 3 hours
3/16ths tbsp every half
hour for 6 hours
3/16ths tbsp every half
hour for 9 hours
50 lbs
1/8ths tbsp every half hour
for 3 hours
1/8ths tbsp every half hour
for 6 hours
1/8ths tbsp every half hour
for 9 hours
25 lbs
1/16th tbsp every half hour
for 3 hours
1/16th tbsp every half hour
for 6 hours
1/16th tbsp every half hour
for 9 hours
*** Doses for children ages 12 and under
Table 4 – Child Three-Day MSM Water Buildup Schedule
Weight
MSM Water Mixture Build
Up Day 1
MSM Water Mixture
Build Up Day 2
MSM Water Mixture
Build Up Day 3
75 lbs
9 tbsp every half hour for 3
hours
9 tbsp every half hour for 6
hours
9 tbsp every half hour for 9
hours
50 lbs
9 tbsp every half hour for 3
hours
9 tbsp every half hour for 6
hours
9 tbsp every half hour for 9
hours
25 lbs
9 tbsp every half hour for 3
hours
9 tbsp every half hour for 6
hours
9 tbsp every half hour for 9
hours
*** Doses for children ages 12 and under
Please Note (For Brain, Colon and Lung Cancer):
Because the formation of swelling, inflammation and congestion are
particularly dangerous for cancer patients, the buildup program will
trouble shoot these potentials. Some types of cancers, including
brain, colon and lung require a modified approach to avoid any
detrimental results if the above symptoms occur. A slower buildup
is necessary. The buildup is administered as follows:
Day 1 Buildup
Treatment is taken for 2 hours; a total of 5 doses of DMSO and MSM
are taken at half hour intervals. Super Silver, Vitalzym, and Green
Supreme Barley Power are maintained.
Day 2 Buildup
Treatment is taken for 4 hours; a total of 9 doses of DMSO and MSM
are taken at half hour intervals. Super Silver, Vitalzym, and Green
Supreme Barley Power are maintained.
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Day 3 Buildup
Treatment is taken for 6 hours; a total of 13 doses of DMSO and
MSM are taken at half hour intervals. Super Silver, Vitalzym, and
Green Supreme Barley Power are maintained.
Day 4 – 12 Hour Treatment
The twelve-hour O.C.C. treatment is administered on day four.
MSM water doses may have to be halved depending on the
individual. See “How To Make MSM Water”
In addition, cancer patients who have blockage anywhere in the
digestive tract should not use this treatment or any other alternative
cancer treatment until the blockage is cleared. As previously
mentioned, Royal Tea can be used to relieve any blockage.
As above, if there is any unexpected inflammation, swelling or
congestion during this buildup, the treatment should be
immediately terminated and alternative treatments will be assessed.
A seven-day primer (detox program) should be started to prepare the
body for the O.C.C. or an alternative treatment should be started
after a 2-day wait.
The Official 12 Hour O.C.C. Treatment Protocol
The colon should be clean by 8:00 p.m. on the night BEFORE the
12-hour O.C.C. treatment is started. Eat and drink absolutely
nothing after the 8:00 p.m. starting point - drink only water
(preferably Vitalized or Wellness water).
Beginning at 8:00 a.m. on the first day of the 12-hour O.C.C.
treatment, the patient should take their first dose of the
supplements. Subsequent doses are administered every half hour for
12 hours. Dosages for DMSO, MSM, Super Silver, Vitalzym, Green
Supreme, Royal Tea and Super Z-Lite will be described in the
sections to follow.
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For 12 hours AFTER the last dose administered, eat and drink
nothing (patient can drink only Vitalized or Wellness water).
In summary:
􀂾 The O.C.C. protocol begins with a 3-day buildup including
the administration of low doses of DMSO and MSM to the
patient.
􀂾 A 12 hour fast must occur on the third day of the build up,
BEFORE the 12 hour O.C.C. treatment can begin. This will
ensure that all food particles are removed from the body and
will not interfere with the supplements.
􀂾 DMSO and MSM administration commences 12 hours after
the initial fast begins. Doses are administered every half
hour. Additional supplementation is also administered at
this time.
􀂾 An additional 12 hour fast commences after the last O.C.C.
dose is administered (ie. 8 p.m. to 8 a.m.).
How To Take the DMSO
DMSO must be topically administered for this treatment (external
application). This is done to avoid any stomach issues that may arise
and inhibits the passage of DMSO through the liver before it reaches
the blood stream.
Prior to administration, at least 6 different sections of the body
should be identified for the application of DMSO. For example, the
right and left forearm, the right and left thigh, and the right and left
calf can be used as areas for the DMSO to be applied. Every half
hour, rotate among the chosen sections for DMSO application. It
takes only a matter of minutes for the DMSO to absorb into the skin,
but the rotation inhibits the development of a rash. DMSO, when
repeatedly applied in the same area, tends to dehydrate and irritate
the skin.
An eyedropper is needed for the application of DMSO. Since each
eye-dropper is sized differently, please experiment to determine
how many drops of DMSO are proportional to your dose.
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IMPORTANT: The external application of DMSO should also be
mixed with Theta Super Silver. As soon as the DMSO and Super
Silver has been absorbed through the skin and the skin is dry
(approximately 15 minutes), follow by applying MSM cream onto
the area. Also, be sure to follow the application of DMSO by orally
taking Theta Super Silver (Silver is taken both externally and
internally). This is important, as it will help to prevent the
development of a rash prior to the application of the next DMSO
administration. If a rash develops anyways, simply choose another
area of the body to apply the DMSO.
In summary:
􀂾 Rotate the area of DMSO administration between 6 or more
areas.
􀂾 Spread the DMSO over the skin in a thin layer that covers a
wide area.
􀂾 Add Theta Super Silver over the area for external absorption
􀂾 Spray copious amounts of water (if needed) and apply MSM
cream over the area of DMSO application. (Wait 15 minutes
for the DMSO to absorb and the skin to dry)
Table 5 and 6 provides the DMSO doses for both Adults and
Children based on weight:
Table 5 – DMSO Dosage For Adults
Weight DMSO (tbsp) [25 doses]
200 lbs 1 tbsp every half hour
175 lbs 7/8ths of tbsp every half hour
150 lbs 3/4ths of a tbsp every half hour
125 lbs 5/8ths of a tbsp every half hour
100 lbs 1/2 tbsp every half hour
Table 6 – DMSO Dosage for Children
Weight Child DMSO (tbsp) [25 doses]
75 lbs 3/16th of a tbsp every half hour
50 lbs 1/8ths of tbsp every half hour
25 lbs 1/16ths of a tbsp every half hour
*** Doses for children ages 12 and under
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Safety Precautions for Handling DMSO. Do not panic at these
warnings, DMSO is not dangerous, there are just some simple
precautions that must be taken.
DMSO has a tendency to bind or attach to different substances and
carries them through the skin. As a result, precautions must be
taken when administering DMSO:
􀂾 DMSO should NOT touch gloves made of rubber, latex or
other synthetic materials.
􀂾 No Q-Tips should be used due to the composition of glue
found in the tip.
􀂾 Patient or caregiver should use their bare hands or fingers to
administer the DMSO and then wash their hands with water
(or use MSM cream or MSM lotion) immediately after
applying the DMSO. This will prevent wrinkles and rashes.
􀂾 DMSO can safely touch: metal, glass, wood, ceramic and
rigid plastics (including rigid plastic bottles).
What To Do If DMSO Is Not Quickly Absorbed.
Most DMSO sold in the United States is 99.9% pure DMSO mixed
with water in the ratio of 70% DMSO to 30% of water. This is the
ideal ratio of pure DMSO to water that promotes absorption into the
skin within 5 to 10 minutes.
DMSO may not absorb well if the ratio of DMSO to water is not
around 70% to 30%. Water may need to be added if too much
DMSO is present. If your ratio is less the 70% DMSO, unfortunately
nothing can be done. This is why it is important to try and avoid
mixing the DMSO with other liquids. Also, when purchasing the
DMSO, try to purchase one that is already composed of the ideal
ratio. The Wolfe Clinic has the requested DMSO available for
purchase.
If the ideal ratio is being used, but the DMSO is not absorbing, try
applying the DMSO onto a different location of the body. Any part
of your body is acceptable except for areas that contain a significant
amount of hair. It is not advisable to apply DMSO onto your head.
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How to make “MSM Water.” MSM crystals must be dissolved in
water for internal ingestion. MSM crystals should be dissolved in
water as follows:
􀂾 Add 1 gallon of purified Vitalized or Wellness water to a one
gallon jug
􀀹 The bottle should be full with a little bit of empty
space on top of the bottle to allow it to be shaken.
􀂾 One teaspoon is equivalent to 4 grams of MSM crystals (the
dosages are calculated according to a patient’s weight).
Follow the dosages shown in the chart (Table 7):
􀀹 Example: For a 200 pound individual 2 gram should
be taken every half hour for twelve consecutive
hours, therefore a total of 25 grams will be
administered (2 gram 25 times). 2 gram of MSM is
equivalent to ¼ of a teaspoon. The chart shows that
50 grams should be added to the 1 gallon of water.
􀀹 Children ages 12 and under should be administered a
lower proportion of the MSM and water mixture.
Please refer to the chart for child dosages (Table 8).
􀂾 Add 1 teaspoon of sea salt to the one gallon of water. This
will aid the entrance of water into the cells.
􀂾 During this treatment, the entire gallon will be consumed.
This amounts to approximately 9 tablespoons of the MSM
water every half hour.
􀂾 The proportional amounts of MSM required for half hour
dosages corresponding to your weight have been added to
the water, therefore, no matter what weight you are, take 9
tablespoons of MSM water every half hour.
Tables 7 and 8 (next page) provide the MSM doses for both Adults
and Children based on weight:
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Table 7 – Adult MSM Dosage
Weight Dose of MSM (g) per Half Hour Instructions for MSM + 1 Gallon Water Mixture
200 lbs 2 gram every half hour 50 grams added to 1 gallon of water
175 lbs 1.75 grams every half hour 43.75 grams added to 1 gallon of water
150 lbs 1.5 grams every half hour 37.5 grams added to 1 gallon of water
125 lbs 1.25 grams every half hour 31.25 grams added to 1 gallon of water
100 lbs 1 grams every half hour 25 grams added to 1 gallon of water
*** 9 tablespoons of MSM water mixture should be taken every half hour regardless of weight
􀂾 For a child or some adult cancer patients, drinking a gallon
of water over a 12 hour period may be too much water for
them. If so, use a half-gallon, but put the same amount of
MSM in the water as you would if it were a full gallon
(according to weight).
􀀹 Also add only ½ a teaspoon of salt to the half
gallon MSM mixture.
􀀹 Half as much MSM water will be ingested,
therefore, for half a gallon, drink 4 ½ tablespoons
each half hour.
Table 8 – MSM Dosage for Children Age 12 & Under
Weight Dose of MSM (g) per Half Hour Instructions for MSM + 1/2 Gallon Water Mixture
75 lbs 0.75 grams gram every half hour 18.75 grams added to 1 gallon of water
50 lbs 0.5 grams every half hour 12.5 grams added to 1 gallon of water
25 lbs 0.25 grams every half hour 6.25 grams added to 1 gallon of water
*** 9 tablespoons of MSM water mixture should be taken every half hour regardless of weight
*** Doses for children ages 12 and under
Dealing With Stomach Problems Caused by MSM
For some individuals, the administration of oral MSM can cause
stomach discomfort. In most cases the development of stomach
problems is due to the fact that individuals have not cleansed the
digestive tract properly. In this case there are two options:
􀂾 Delaying treatment for another day will allow the build up
to the dosages of MSM that the stomach can handle.
(Adding days to the buildup)
􀂾 Discontinuing the use of MSM for the rest of the day, while
continuing to administer the external application of DMSO
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can also be done. This option is acceptable because MSM is
only an appendage of the DMSO treatment. DMSO is the
main ingredient.
Keep in mind that MSM enables your cells and tissues to release
toxins that have built up over the years. Sulfur is a vital part of our
waste management system, and if we have not had enough of it, our
bodies are not able to release the waste substances. If too much
MSM is taken, a patient’s body will release too much waste at one
time for the kidneys and liver to handle. This waste in the blood
stream can cause all kinds of problems ranging from flu-like
symptoms to re-experiencing the effects of drugs taken in the past.
The key to reducing or eliminating detox symptoms is to start on
MSM slowly so that the waste in tissues is released slowly and to
drink lots of water so that the released toxins will be flushed out of
the body quickly.
Administering Theta Super Silver
Silver has been used for thousands of years as a systemic disinfectant
that functions like a secondary immune system. Our Theta Super
Silver is made up of nano sized vegetable silver minerals and is
readily available for absorption into cells. Since silver readily binds
to DMSO, its oral application will help the DMSO and MSM attack
any microbial infection within the cancer cell.
One ounce of Super Silver should be taken orally every half hour,
immediately after the external application of DMSO. Children ages
12 and under should be given half of the dose. In addition, Super
Silver should be mixed directly on the skin with DMSO (Please refer
to Tables 9 and 10).
Administering Super Z-Lite
Super Z-Lite liquid tincture and capsules are important supplements
during the O.C.C. treatment. Composed of purified volcanic ash
known as Zeolite, Super Z-Lite resembles a sieve and enters the
body with a negative charge. This negatively charged particle binds
to unwanted and potentially dangerous positively charged particles
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and safely removes them from the body. These particles include free
radicals, heavy metals, acid and viral fragments.
Super Z-Lite is especially important during the O.C.C. protocol
because it removes acid waste produced by cancer cells and
effectively attacks viruses and other microorganisms within the
body. At the same time, this fortified blend also delivers ocean and
plant derived minerals, in addition to humic fulvic acid, into the
cells.
Super Z-Lite tincture and capsules are both recommended as they
help to synergize and boost each other to fulfill zeolite’s highest
known capabilities. The capsule form can reach the intestines
where they chelate heavy metals and toxins much more thoroughly,
whereas the tincture has the ability to cross the blood-brain barrier
and reach vital organs.
Adult doses for Super Z-Lite tincture are 25 drops 4 times per day,
with the additional supplementation of Super Z-Lite capsules of 1
capsule 4 times a day. Children 12 years and younger should be
taking 10 drops of the liquid tincture 4 times per day and 1 Super ZLite
capsules.
Administering Vitalzym and Green Supreme Barley Power
Tables 9 and 10 summarize Vitalzym and Green Supreme Barley
Power doses based on the patient’s weight and age. Please keep in
mind that no more than 12 capsules should be taken a day because
some enzymes act as blood thinners and high doses can cause health
problems.
The purpose of these products is to assist the conversion of the
cancer cells back into normal cells, while providing the key enzymes
necessary for the metabolic production of ATP. These supplements
can and should be continued after the completion of the O.C.C.
protocol.
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Tables 9 and 10 provide the doses for Super Silver, Vitälzym, and
Green Supreme Barley Powder.
Table 9
Adult Administration of Super Silver, Vitalzym & Green Supreme Barley Power
Weight Super Silver Vitalzym Green Supreme Barley Power
1 ounce (orally) 1 cap every hour for 12
200 lbs 1 tsp (topically) hours (max 12 caps) 1 capsule every hour for 12 hours
1 ounce (orally) 1 cap every hour for 12
175 lbs ¾ tsp (topically) hours (max 12 caps) 1 capsule every hour for 12 hours
1 ounce (orally) 1 cap every hour for 12
150 lbs ¾ tsp (topically) hours (max 12 caps) 1 capsule every hour for 12 hours
1 ounce (orally) 1 cap every hour for 12
125 lbs ¾ tsp (topically) hours (max 12 caps) 1 capsule every hour for 12 hours
1 ounce (orally) 1 cap every hour for 12
100 lbs ½ tsp (topically) hours (max 6 caps) 1 capsule every hour for 12 hours
Table 10
Child Administration of Super Silver, Vitalzym & Green Supreme Barley Power
Weight Super Silver Vitalzym Green Supreme Barley Power
½ ounce (orally) 1 cap every 3 hours for
75 lbs ½ tsp (topically) 12 hours 1 cap every hour for 12 hours
½ ounce (orally) 1 cap every 3 hours for
50 lbs ½ tsp (topically) 12 hours 1 cap every hour for 12 hours
½ ounce (orally) 1 cap every 3 hours for
25 lbs ¼ tsp (topically) 12 hours 1 cap every hour for 12 hours
*** Doses for children age 12 and under
Administering Royal Tea (aka Wholly Tea)
The use of Royal Tea before, during and after the O.C.C. treatment
will help to promote proper evacuation of intestinal debris from the
body. This ensures that the intestinal tract is absorbing nutrients
and supplements during the therapy. As previously described, the
Royal Tea should be started immediately and taken during the
buildup, 12 hour treatment and continued after the treatment ends.
Below are instructions on how to take the tea:
Two tea bags will make one gallon and will last approximately one
week for one person.
􀂾 Bring a gallon of enhanced water (Wellness Water or
Vitalized Water) to a full boil
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􀂾 Turn off the stove and add two Royal Tea bags (three bags
for extra strength) into the boiling water while the pot
remains on the stove
􀂾 Cover and let STEEP for eight hours – this will bring the
herbs to full potency
􀂾 Refrigerate
􀂾 Drink (these doses are to be taken prior to the
commencement of the treatment):
􀀹 One 8 oz. glass in the morning
􀀹 One 8 oz. glass in the evening
􀀹 Two 4 oz. glasses during the day
􀂾 For children (these doses are to be taken prior to the
commencement of the treatment):
􀀹 75 pounds and greater – give ½ the dose
􀀹 Under 75 pounds – give 1/3 the dose
􀂾 Royal Tea is good for all ages
The following may be experience while using Royal Tea:
􀂾 Slight cramping may occur and can last from 3 to 14 days.
This is a normal occurrence for intestinal rejuvenation. The
body is cleansing old mucus, fungus, viruses, and bad
bacteria, which causes gas and abdominal cramping.
􀂾 If extreme cramping occurs, decrease the amount of the tea
taken, but do not stop the cleanse. This is due to the
breakdown of scar tissue in the colon or adhesions.
􀂾 Gas and cramping are symptoms of loosening of old mucus,
bacteria, fungus and fecal waste off of the intestinal walls.
This is a normal occurrence.
􀂾 Loose stool is normal
􀂾 If the stool is watery, decrease the amount of tea taken, but
do not stop the cleanse. You should maintain 2-3 bowel
movements per day, slightly on the loose side but of good
volume, NOT watery. Keep in mind that the 2-3 bowel
movements per day should only be occurring prior to the
12-hour O.C.C. treatment. Once the treatment is started the
patient should take as much Royal Tea necessary to maintain
evacuation.
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􀂾 Your rectum may feel warm. This is due to the acidity that
is being dumped from your tissues.
􀂾 Feces that are extremely dark in color (black) is very old
waste that is being expelled.
􀂾 Weight loss will occur only if the body needs it. Royal Tea
acts as a body balancer.
When using Royal Tea be sure to eat a healthy diet that includes
plenty of fresh and raw salads and whole grains. Reduce or avoid
animal protein, dairy, bread, sugar and processed foods. (Before,
during build up, and after treatment).
Possible Side Effects of the O.C.C.
One of the main side effects of this treatment is harmless, but could
be embarrassing….very severe body odor. DMSO and MSM are
sulfur-containing elements; as a result, sulfur is emitted from the
patient resulting in a distinctly unpleasant smell. A chemical
breakdown of these elements produces a molecule called DMS or
dimethyl sulfide. When high doses of either DMSO or MSM are
taken, enough DMS is chemically created in the body to cause body
odor. DMS does not contain any extra oxygen atoms, which is why
it causes the odor. The cancer patient will not be able to smell this
severe odor, but others will.
The odor will last for at least 5 days after terminating the treatment.
During the buildup, 12-hour treatment, and for 5 days after, it is
often best to avoid public areas.
Doing the following can dilute the odor:
􀂾 Bathing twice a day (but not within 2 hours before or after
the treatment)
􀂾 Changing and washing clothes daily
􀂾 Airing out the house twice a day
􀂾 Going for outdoor walks (but staying away from others)
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Unfortunately, there is no known way to shorten the length of time
that the odor remains after the treatment is terminated. If a
caregiver does not want to smell the DMSO, the caregiver can take 1
or 2 tablespoons of DMSO. By taking the DMSO, the caregiver will
no longer be able to distinctly smell the DMSO because it is now in
their blood.
Additional side effects include:
􀂾 DMSO can cause vertigo, a side-effect resulting dizziness.
􀂾 Nausea can also occur if the MSM buildup in the treatment
is too fast or DMSO is orally taken.
􀂾 Headaches are also possible, not as a result of the treatment,
but as a consequence to the sudden change in diet that
accompanies the protocol (ie. sudden drops in glucose
levels).
Repeating the Twelve Hour O.C.C. Protocol for Consecutive Days
The complete 12-hour O.C.C. protocol (not counting the buildup
days) can be administered from 1 to 4 consecutive days. The amount
of time that an individual continues with the protocol depends on
the amount of inflammation, swelling, congestion and/or the type of
cancer that the patient is dealing with. The treatment should be
administered for a longer period of time when the situation is more
serious.
When the treatment is continued for more than one day, the most
significant issue that must be dealt with is how well the areas of skin
that the DMSO treatments are being applied to are holding up.
Additional areas for repeated applications of DMSO may be needed.
For continual use, it is important for the patient to take a bath or
shower every night and every morning. Please keep in mind that
the showers or baths should not be taken within 2 hours of the
actual treatment. This is because the pores in the skin should not be
opened during treatment times; this will insure that too much
DMSO does not pass through the skin. The bathing and showering
in between the 12 hour treatments will ensure that the areas of skin
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that DMSO is being applied to will be hydrated. Remember that
DMSO tends to dehydrate the skin, thereby causing rashes.
Some individuals may want to use the O.C.C. treatment once a week
instead of for consecutive days (ex. for two consecutive Sundays).
Just remember that the odor lasts for several days after each
treatment. In such a case the odor may last for consecutive weeks.
In addition, when undertaking the O.C.C. treatment for more than
one day, the effect of the fasting will be enhanced, as this protocol is
quite potent.
Dealing With the Intensity of the Treatment
If the patient requires a break from the treatment during the hours
that DMSO and MSM are applied, a break can be taken for half an
hour to one hour. This does NOT mean that an application can be
skipped. If a break is needed, the patient must continue with the 25
applications but over a longer period of time. For example, instead
of taking 25 doses over a 12-hour period, patients can take 25 doses
over a 14 or 15-hour period, or longer if needed.
If the protocol is applied over a longer period of time, a 12-hour fast
will still need to be started after the last application. This is very
important because the length of the fasting is an imperative part of
the protocol.
Is the O.C.C. Dangerous?
On occasion, killing certain types of cancer cells can be dangerous.
As previously discussed, as cancer cells die, the immune system is
stimulated to attack these cells, thereby causing the appearance of
inflammation, swelling, and/or congestion. In addition, the death of
the cancer cells creates debris that the body needs time to dispose of.
Since none of the supplements in this treatment, individually or
collectively kill any of the cells whether healthy or cancerous, it is
not expected that the O.C.C. will cause any of the problems
mentioned above. Please keep in mind that part of the reason for
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the buildup prior to the 12-hour protocol is to catch any problems
early if they should happen.
The O.C.C. should not be combined with any other alternative
cancer treatments because virtually all other alternative cancer
treatments kill cancer cells and create unwanted and dangerous
reactions within the body. In combination with alternative
treatments the O.C.C. could greatly enhance the number of cancer
cells the other treatment kills, thereby creating a dangerous amount
of inflammation, swelling, congestion and/or debris.
In addition, the medical establishment has convinced cancer patients
that it is critical to shrink tumors. In some cases it is, but in vast
majority of cases the shrinking of tumors is not necessary as long as
the cancer cells in the tumor are killed or converted back into
normal cells. Only a small percentage of the tumor cells are
cancerous, as a result, the conversion of these cells back into healthy
cells will not shrink the tumor.
If the size of the tumor is important to the cancer patient (i.e. a
tumor that is pressing against an organ or is blocking the flow of
some fluid), the size of the tumor can be dealt with at a later time by
other treatment methods. However, if the tumor is creating a lifethreatening
situation, such as blocking the passage of vital fluids, it
should be dealt with immediately by orthodox medicine.
A Warning Against Making Changes or Additions to the O.C.C.
As previously mentioned, the eradication of too many cancer cells
can create a dangerous situation within the body. Do not tamper
with this protocol. The ramifications of ignoring these warnings
could result in the O.C.C. protocol enhancing the effectiveness of
the cancer cell eradication, thereby producing dangerous amounts of
inflammation, swelling, congestion and debris.
Overall, during the buildup time and the O.C.C. 12 hour treatment
and for 7-10 days after, refrain from undergoing any other cancer
treatment or aggressive detoxification programs that may kill cancer
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cells. Detoxification is important but not to the point of causing
exhaustion to the patient.
If the patient has been on a Cesium Chloride treatment, they should
wait for a period of three weeks before commencing the O.C.C.
buildup.
Enhancements to the O.C.C.
Dry Skin Brushing Massage Therapy, Salt Glow & Aesta
Supreme Far Infrared Therapy.
Dry skin brushing and salt glow therapies are important therapies
that will help enhance the benefits of the O.C.C. These therapies
aid the body by increasing blood circulation and lymphatic
cleansing, directly supporting the O.C.C. protocol in delivering
DMSO and MSM promptly to the cancerous site and facilitating the
elimination of toxins and debris from the body.
Dry Skin-Brushing Massage Therapy
This routine is done morning and night throughout the program
(prior to and during buildup and O.C.C. treatment) and once a day
after the program is completed.
Benefits of Dry Skin-Brushing:
􀂾 Opens pores, removes toxins and dead skin
􀂾 Increases blood circulation
􀂾 Helps to stimulate hormone and oil producing glands
􀂾 Helps to take the load off other organs by helping the
eliminative system
􀂾 Helps rejuvenate the nervous system
􀂾 Helps improve muscle tone and prevent fat deposits
􀂾 Improves complexion
􀂾 Improves overall health, which helps against premature
aging
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Skin-Brushing Tips:
􀂾 Every two weeks, wash your brush with natural soap and let
it dry in the sun
􀂾 Never share your brush
􀂾 Never brush irritated or infected areas of the body
􀂾 Brush scalp regularly to remove dead skin and to help
promote hair growth
􀂾 If you brush facial skin, be very gentle, better still, use a
facial skin brush
Below are directions on how to skin-brush:
􀂾 A long-handled natural bristle brush is best. Never use a
synthetic brush.
􀂾 Brush skin lightly to start. As the skin becomes more toned
you may brush more heavily.
􀂾 Start at the bottom of the feet using a rotary or circular
motion and then proceed to the legs, arms, back, abdomen
and chest. Women should avoid doing the breasts. Never
we-brush and always brush towards the heart. Continue
until your skin acquires a red glow. Skin brushing should
take about 10 minutes.
􀂾 Skin-brush as soon as you wake up and before retiring. This
will refresh the body in the morning and relax it before bed.
􀂾 A shower should always follow skin brushing. This will
remove uric acid crystals along with any dead skin that has
been loosened.
􀂾 Always start your shower with warm water and end with
cold. When the water turns cold, let it hit your legs first.
Do not let it hit your heart or head first as this can cause a
slight shock to the body. Once the water is cold, do not
linger.
􀂾 Baths can be unsanitary. When the pores open, they allow
the toxins to be reabsorbed. Avoid hot showers; when
showering in high temperatures; toxic chemicals are carried
in the stream. Warm showers are best if you do not have a
shower filter.
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􀂾 Soaps should always be used but do not soap the entire body.
Areas to be soaped are the underarms and groin region.
Rinse soap off thoroughly to avoid clogging of pores.
Skin-Brushing should be started a day before day 1 of the buildup.
This will remove dead skin cells and enhances the delivery of DMSO
and Theta Super Silver.
Salt Glow Therapy
A salt glow should be done after skin brushing. Below are directions
on how to administer a salt glow:
􀂾 Oil a large soap bowl
􀂾 Fill with Epson salts
􀂾 Wet it down with water
􀂾 Salt should have the texture of wet sand (granular, not
soupy)
􀂾 Undress and stand or sit in bathtub. Make sure that you are
secure so you do not slip
􀂾 Take a handful of salt and rub vigorously in circular motion
towards the heart (same routine as skin-brushing)
􀂾 Do not skimp on salt
􀂾 After doing the whole body, repeat, rubbing off the salt from
the first application
􀂾 Now shower with lukewarm water; going from hot to cold.
When the water turns cold, let it hit your legs first. Do not
let it hit your heart or head first as this can cause a slight
shock to the body
Regular salt glows will help ease constipation, swelling, skin
conditions, poor circulation, fatigue, stiffness, headaches and
arthritis.
A salt glow should be started a day before day 1 of the buildup. This
will remove dead skin cells and enhances the delivery of DMSO and
Theta Super Silver.
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Aesta Far Infrared Therapy
Aesta Far Infrared Therapy (FIR) has been used for over two
thousand years as a source of natural healing for many illnesses and
discomfort. Activated by heat, the natural earth minerals in Aesta’s
Sauna Dome and Ion Mats emit FIR radiant energy that is absorbed
by human cells, causing a physical phenomenon called resonance.
The cellular activities are instantly invigorated, resulting in a better
circulation and an overall improved metabolism.
The use of both an Aesta Dome and Mat provides 360 degrees of far
infrared heat and the release of negative ions that penetrate 2-3
inches into body tissues. Research has shown that in a 25-45 minute
fever sweat, the toxins that are released from the body are
equivalent to the release of toxins after 10 days of undergoing
regular metabolism. The creation of a false fever has been shown in
studies to be the most effective therapy for the human body. FIR
therapy would be an immense addition to the O.C.C., as its
therapeutic benefits would be greatly enhanced.
After the last administered dose of MSM and DMSO, skin-brushing
should be done each day (during buildup and 12 hour fast). A fever
sweat in the Aesta Supreme, Mat or Dome should be done one hour
after skin-brushing, followed by a shower in non-chlorinated water.
This will prepare the skin for maximum absorption of DMSO and
Super Silver.