Cesium and Cancer
The
High pH Therapy for Cancer
Tests on Mice and Humans
A. KEITH BREWER, Ph.D.
A.. Keith Brewer Science Library, 325 N. Central Ave., Richland
Center, WI 53581
BREWER,
A. K. The high pH therapy for cancer tests on mice and humans.
PHARMACOL BIOCHEM BEHAV 21: Suppl. 1, 1-5. 1984.---Mass
spectrographic and isotope studies have shown that potassium,
rubidium, and especially cesium are most efficiently taken
up by cancer cells. This uptake was enhanced by Vitamins
A and C as well as salts of zinc and selenium. The quantity
of cesium taken up was sufficient to raise the cell to the
8 pH range. Where cell mitosis ceases and the life of the
cell is short. Tests on mice fed cesium and rubidium showed
marked shrinkage in the tumor masses within 2 weeks. In
addition, the mice showed none of the side effects of cancer.
Tests have been carried out on over 30 humans. In each case
the tumor masses disappeared. Also all pains and effects
associated with cancer disappeared within 12 to 36 hr; the
more chemotherapy and morphine the patient had taken, the
longer the withdrawal period. Studies of the food intake
in areas where the incidences of cancer are very low showed
that it met the requirements for the high pH therapy.
Cancer
therapy.....Cesium.....High pH.....Pain.....Potassium.....Rubidium.....Tumor.....Vitamins
THE High pH Therapy for cancer was arrived at from an extensive
series of physical experiments. These involved the isotope
effect across membranes of many types, normal plant and
animal, embryonic, cancer, and synthetic. It also involved
mass spectrographic analyses of membranes and cells, as
well as fluorescence and phosphorescence decay studies of
many types of cells and parts thereof. It is the thesis
of this paper that the results obtained throw a direct light
upon the mechanism of carcinogenesis, and also indicate
a therapy. Tests on both mice and humans substantiate this
theoretical approach [1-8].
Angstrom Minerals Product And Price List
The information on this page has been extracted from http://www.cancer-coverup.com/brewer/default.html
A.
KEITH BREWER, Ph.D.
A.. Keith Brewer Science Library, 325 N. Central Ave., Richland
Center, WI 53581
BACKGROUND
The
isotope effect throws a very direct light on the mechanism
of carcinogenesis. In this study it was shown that the 39K/41K
ratio in ocean water down to 6000 ft was 14,20000 [9-11].
In normal matured cells, both plant and animal, the ratio
varied from 14.25 to 14.21. Embryonic and cancer cells all
gave a ratio of 14.35. In the case of all synthetic cells
across which there was a potential gradient, the ratio was
14.35. From these values it will be seen that the ratio
in normal living cells indicates that as many isotopes leave
the cell as enter.
In
the case of potassium for embryonic and cancer cells as
well as synthetic type cells with all types of membranes
even including liquid mercury films the observed isotope
ratio was given by equation 1.
(39K/41K)
o = (39K/41K) n (41 + m / 39 + m) 1/2 (1)
where
n refers to the normal ratio, o to the observed ratio, and
m is the associated mass for the ions.
All
cations in solution are associated. The attached mass for
Cs+ is 3 molecules of water, for Rb+ it is 5 molecules,
for K+ is 7 molecules. For cations below potassium in the
Electromotive Series all ions are highly associated. This
is to be expected from their position in the Hoffmeister
Series. In the case of Ca++ the association is 30 molecules,
while Na+ is 16. Equation (1) holds for all cations tested
from H+to U+. The value of m however will vary when polar
molecules are present in the solution. For example, K+ can
also attach glucose. In contrast, Ca++ can attach a wide
variety of molecules; it is this cation that transports
peroxides into the cell, as well as metabolic products out
of the cell.
The
results given in equation (1) are most significant in that
they show that transport is dependent entirely upon the
frequency with which the ions strike the membrane surface.
It is not a matter of capillary action, but one on which
the ion and its associated mass pass directly through the
bonding space between molecules which comprise the membrane.
That the associated molecules are not lost in this transport
is due to the fact that the attraction between the molecules
and the ion is far greater than their attraction by the
material of the membrane.
In
the case of potassium an exact similarity exists between
embryonic and cancer cells. The isotope ratio indicates
that the K+ ions are taken up by the most efficient process
possible. The same held true for Cs+ and Rb+.
In
contrast to the above, a vast difference exists for cations
below potassium in the EMS. In the case of embryonic cells
all cations tested obeyed equation (1). In the case of cancer
cells cations below potassium were taken up sparingly, if
at all. For example the amount of calcium in cancer cells
is only about one percent of that in normal cells [18].
The
above isotope effect for potassium which transports glucose
into the cell, and for calcium which transports oxygen are
most significant with respect to cancer. They mean that
glucose can readily enter cancer cells but that oxygen cannot
enter. This accounts for the anaerobic state of cancer cells
pointed out by Warburg as early as 1925 [26].
The
mechanism responsible for the similarity in the isotope
effect for potassium and rubidium in cancer and embryonic
cells and for their marked difference in case of calcium
was investigated in some detail using mass spectrographic
analyses, and also fluorescence and phosphorescence decay
patterns.
The
phosphorescence decay patterns were found to be peculiar
to and specific for all cell types or parts thereof [12-15].
It should be mentioned that the decay spectra is due entirely
to the light emitted from the energized double bonds. All
double bonds are capable of being raised to the energized
state. While the fluorescence spectra and the phosphorescence
decay patterns are both specific for each double bond they
can be influenced by adjacent strong polar radicals. Again,
both can be completely depressed by molecules absorbed over
the surface; thus morphine, as well as attached polycyclic
type molecules, will completely depress the excitation of
the P=O radicals which characterize all cell membrane surfaces.
It
was observed that the membranes tested gave a phosphorescence
decay pattern due almost entirely to the P=O radicals which
are composed of phospholipids. These radicals are specifically
oriented over each type of membrane. This is most significant
from the point of view of membrane action, since the P=O
radicals are moderately strong electron donors in the ground
state and strong to powerful donors in the energized state.
This is due to the fact that the ionization potentials,
1st to 5th, are appreciably higher for the 0 than the P
atom. This means that the 4 bonding electron orbitals will
be displaced nearer the 0 atom thus surrounding this atom
with a pronounced negative field. The P atom is thus positive
in nature.
The
above results are most important with respect to membrane
action. They show that the strong electron acceptors Cs+,
Rb+, and K+ can be attracted into the membrane so that they
will enter the negative potential gradient which exists
across all living membranes. In contrast to these cations,
the highly associated cations farther down in the EMS are
not sufficiently strong electron acceptors to be drawn into
this gradient except when the P=O radicals are in the energized
state. This means that K+ cations which transport glucose
into the cell can readily enter cancer cells, but that Ca++
ions which transport oxygen into the cell cannot enter.
In the normal cell the glucose, upon entering the cell,
reacts with the oxygen in the cell and is burned to carbon
dioxide and water with the liberation of heat. This heat
in turn is absorbed on the membrane surface and raises the
P=O radicals to an energized state which permits them to
attach more Ca++ ions. Thus it will be seen that the amount
of oxygen entering the cell is determined by oxidation within
the cell, primarily that of glucose. This action is responsible
for the pH control mechanism of the cell which maintains
a value near 7.35.
The
reactivity of the double bond has been studied in some detail
using both light absorption and electron impact. It was
found that energy states of the order of those produced
by metabolic processes were not reactive. In contrast, high
energy states such as those that are induced by radioactivity.
are very reactive. Intermediate energy states in the ultra
violet range were not reactive. Intermediate energy states
in the ultra violet range were not reactive by electron
impact, but slightly with light quanta. Here however the
reactivity increased with a high power of the energy intensity
per unit area [16]. This suggests that the reactivity may
be due to the multiple absorption of light quanta, thus
raising the energy of the bond to the sum of the quanta
absorbed
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