Mineral Therapy and the Use of Gold
International Medical Veritas Association
The essay “The Age of Autism: Gold standards” by
Dan Olmstead of United Press International says, “A published scientific paper suggests
gold salts -- the treatment that may have prompted improvement in the first
child ever diagnosed with autism -- can affect mental conditions.” Before we
set off on a gold rush it would be helpful to see the name of this emerging
branch of medicine, mineral therapy,
brought into focus. Mineral therapy does offer a hope for autism children,
their families, as well as the entire human race threatened with plagues of
chronic and infectious diseases as well as chemical poisoning.
To focus on only one
of the minerals, and not on the entire
spectrum of minerals, will not serve the need of humanity.
Magnesium though is the
single most needed (in terms of quantity and strategic cellular importance) and
most helpful mineral (in a broad and specific sense). Selenium also takes on a
strategic importance living as we do in the age of a rising tide of mercury because it binds so strongly with mercury
before the mercury gets a chance to cause damage. Now we are hearing of the
possibility that gold salts[i][i] can pull mercury off
binding sites, something selenium and magnesium cannot do.
This is not a strange idea
when we consider the relationship between gold and mercury in gold mining.
There they use the mercury to harvest the gold. Unfortunately humanity has to
deal with hundreds of thousands of tons of environmental mercury pollution that
has accumulated through the last few centuries of gold mining.
Dr. Boyd Haley says,
"This does lend support to the possible removal of mercury from biological
proteins in individuals treated with gold salts." Gold, he thinks, might
pull mercury "off the enzyme it's inhibiting and reactivate that
enzyme." Dr. Haley though is adamant about the down side of using gold
salts. “This issue needs research as it has good possibilities for helping
the older autistics but it is also replete with danger if used
ignorantly. Also, consider the thiols that are part of the gold salts,
namely thioglucose and thiomalate, both analogs of natural compounds. It
might be that the delivery of these thiols to the appropriate areas of the body
is what reverses any possible mercury effect instead of the gold itself,” he
warns.
Selenium is a mineral that
binds with mercury in one way and gold in another. Using minerals as a medicine
is already very important in emergency medicine where magnesium chloride and
sulfate save lives. Now we have on the table the suggestion that minerals are
indicated for neurological disorders.
In mineral therapy we
understand that certain minerals are
both the cause (when deficient) and
cure of many diseases.
Mineral therapy with
magnesium is considered exceedingly safe because of its exceptionally low
toxicity. Selenium is more toxic and doses need to be regulated, gold breaches another level of toxicity that
preaches for extreme caution.[ii][ii] Side effects of gold salts
can occur any time during treatment or months after treatment has been
discontinued. The most common adverse reaction to aurothioglucose (gold salt)
is inflamed skin. An itching sensation can be an early warning sign of skin
reaction (dermatitis). Aurothioglucose is used in treating inflammatory
arthritis.
Exactly how gold salts work
is not well understood. In patients with inflammatory arthritis, such as adult
and juvenile rheumatoid arthritis, gold salts can decrease the inflammation of
the joint lining. This effect can prevent destruction of bone and cartilage.
Gold salts are called second-line drugs because they are often considered when
the arthritis progresses in spite of anti-inflammatory drugs (NSAIDs and
corticosteroids).
In seawater gold
occurs at 0.000004mg per liter.
Aurothioglucose can cause
grayish blue discoloration of the skin. It can also cause a metallic taste and
mouth sores. Because gold salts can cause serious kidney and bone marrow
problems, all patients require regular blood and urine test monitoring. An
unusual side effect of injectable gold is flushing, dizziness, and fainting
immediately after the injection. Patients starting injectable gold are observed
after the first dose for this problem. Rarely, patients can have severe
allergic reactions to aurothioglucose resulting in shock.
If we are going to use the
more toxic minerals we are going to want to set up the situation where we will
need to use the least amount possible. The mistake we commonly make in medicine
is to rely too heavily on one particular drug (with its list of side effects
and potential for collateral damages) and not supply foundation nutritional
support. In mineral therapy when we use minerals like magnesium we set the
stage for the “safer” use of a mineral like gold if we are going to try and use
it for mercury removal and neurological regeneration. Minerals are without
doubt effective medical agents that must be used with care. Minerals,
the building blocks of the universe itself, represent a revolution in
medicine, a hope for something beyond the exceptional toxicity of allopathic
medicine.
Mark Sircus Ac., OMD
Director International Medical Veritas Association
http://www.MagnesiumForLife.com
http://www.imva.info
http://www.detoxchelationclinic.com
http://www.worldpsychology.net
+55-83-3252-2195
www.skype.com
ID: marksircus
IMPORTANT DISCLAIMER: The communication
in this email is intended for informational purposes only. Nothing in this
email is intended to be a substitute for professional medical advice.
[iii][i] "Chrysotherapy"
or "aurotherapy" is the name used for treatment with gold
compounds. Use of gold compounds, take up to two months to reach a
"steady state" in the body....and have a fairly long half life.....in
10 days, only 70% is excreted .......this makes any gold toxicity problems that
might occur, more difficult to deal with, more difficult to overcome
rapidly. The rates of reaching steady state are faster when injectable
gold is used, than when oral gold is used. the effects of oral gold
are both slower and said to be less effective in rheumatoid
arthritis.:Pharmacokinetics: In 5 rheumatoid arthritic patients, the oral
administration of a single 6 mg (equivalent to 1.74 mg of gold) dose of a
solution of radiolabeled auranofin demonstrated that approximately 25% of the
oral dose was absorbed. Peak plasma radioactive gold concentrations of 0.039 to
0.11 µg 95u/mL were reached in 1.5 to 2.5 hours. The mean plasma terminal
half-life was 17 days, while the mean total body terminal half-life was 58
days. By day 10 post-administration, 77% of the initially administered labeled
gold had been excreted, 73% in the feces and 4% in the urine. Six months after
this single dose, approximately 99.6% of the initially administered labeled
gold had been excreted, with 0.4% retained in the body.
[iv][ii] The
potential benefits of using auranofin in patients with inflammatory bowel
disease, skin rash or history of bone marrow depression, should be weighed
against: 1) the potential risks of gold toxicity on organ systems previously
compromised or with decreased reserve, and 2) the difficulty in quickly
detecting and correctly attributing the toxic effect. Chrysotherapy is beneficial
in the treatment of rheumatoid arthritis, but gold-induced aplastic anemia may
be fatal. Absolute identification of patients at risk of having this
hematologic side effect is not possible, but dosage reduction and intense
monitoring of laboratory and clinical signs may prevent its occurrence.