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<html>
<head><title>Preventing and treating cancer with progesterone.</title></head>
<body>
<h1>
Preventing and treating cancer with progesterone.
</h1>
<em>"The energy of the mind is the essence of life." Aristotle</em>
<p></p>
<p>
All through the last century, as more and more resources were devoted to solving "the cancer problem," the
death rate from cancer increased every year. Something was clearly wrong with the way the problem was being
approached.
</p>
<p>
If you grind up a computer and dissolve it in acid, you can find out exactly what substances it was made of,
but you won't learn from that information how the computer worked. Twentieth century biologists became fond
of emulsifying cells and studying the soluble parts. By the end of the century, they had identified so many
parts that the government was financing projects to use supercomputers to try to understand how the parts
interacted.
</p>
<p>
If some essential information was lost in studying the parts, supercomputation isn't the way to find it.
Even with infinite computing capacity, a description of the electrons on carbon and hydrogen atoms on amino
acids in protein molecules won't lead to the reality of how those atoms would have functioned in the living
state.
</p>
<p>
The image of a cell as a watery solution contained in an elastic membrane bag is still having a radically
stupefying effect on biology and medicine. The idea that a cell can be understood by using a computer to
model a network of interactions between genes and gene products is nothing more than a technologizing of the
primitive understanding of life that was promulgated by the Weismann-Mendel-Morganist school. It was the
dogmatic insistence of that genetic determinist school that cancer originated with a genetic mutation.
</p>
<p>
By the middle of the 20th century, that dogma had excluded the most important parts of biology from the
schools and the journals. Ideas of a developmental field, cellular coherence, and holistic cooperativity
were denounced as unscientific vitalism. Returning to the idea of a "cancer field" is an essential first
step in thinking realistically about preventing and treating cancer, but that idea has hardly progressed
since the 1930s.
</p>
<p>
In the last few years, interest in cloning and stem cells and tissue regeneration has revived interest in
studying the factors that contribute to the spatial and temporal ordering of cell growth.
</p>
<p>
The idea of a developmental field was a fundamental part of embryology in the first half of the 20th
century. It was an empirical idea, supported most commonly by evidence that diffusing substances and
secreted materials governed the differentiation of cells and tissues, but the form-generating effects of
bioelectric fields were also often demonstrated, and there was some evidence that tissue radiations played a
role. The extracellular matrix secreted by cells served to transmit information between cells, but its form
was regulated by cells, and its structure was a factor governing the cells' differentiation.
</p>
<p>
Experiments in amphibians showed that regeneration of organs had a reciprocal relationship with the
development of cancer--a tumor could be turned into a tail, for example, if it was grafted onto the stump
following amputation of the tail, but factors that weakened regeneration could cause a tumor to develop. In
these experiments, the normal organism's morphogenetic or epimorphic field overrode the disordered
developmental field of the tumor.
</p>
<p>
In the absence of overriding external influences, the disordered system of the tumor, in which cells emitted
many products of their disordered metabolism, could interfere with the normal functions of the organism. All
of the products of the injured cells, including their altered extracellular matrix, constituted the cancer
field.
</p>
<p>
The recent recognition of the "bystander effect" of radiation exposure, in which cells that haven't been
irradiated undergo genetic changes or death when they are exposed to irradiated cells, has provided an
opportunity to return to the "field" idea in cancer, because the stress-induced factors emitted by
irradiated cells are the same toxic factors emitted by cells undergoing carcinogenesis from other causes,
such as over-exposure to estrogen.
</p>
<p>
H. J. Muller, one of T. H. Morgan's students and colleagues, studied the mutagenic effects of x-rays, and
the genetic determinists argued that the random changes produced in the genetic material by ionizing
radiation provided a model of the evolutionary process. Randomly altered genes and natural selection would
explain everything, including cancer. Every time cells divide, their genes supposedly become more
susceptible to random changes, so increased replication of cells would increase the risk of producing
genetic changes leading to cancer. This idea is so simple and so widely believed that many people focus only
on the rate of proliferation, and the random mutations that supposedly occur during proliferation, when they
try to explain carcinogenesis. They feel that it's reasonable to discuss cancer without bothering to
understand the physiology of the cell or the organism.
</p>
<p>
The organism can only be understood in its environments, and a cell can't be understood without reference to
the tissue and organism in which it lives. Although the geneticists were at first hostile to the idea that
nutrition and geography could have anything to do with cancer, they soon tried to dominate those fields,
insisting that mutagens and ethnicity would explain everything. But the evidence now makes it very clear
that environment and nutrition affect the risk of cancer in ways that are not primarily genetic.
</p>
<p>
Every tumor, like every person, has a uniqueness, but valid and practical empirical generalizations can be
made, if we understand some of their properties and the conditions that govern their development and
survival.
</p>
<p>
Percival Potts' observation of scrotal cancer in chimney sweeps eventually led to the study of soot
carcinogenesis, and then to the study of the properties of the polycyclic aromatic hydrocarbons in soot. The
similarities of those properties to estrogen's soon became apparent.
</p>
<p>
Over the decades, many studies have confirmed that prolonged, continuous exposure to estrogen is
carcinogenic, and that progesterone offsets those effects.
</p>
<p>
Following the animal studies that showed that carcinogenesis by estrogen could be prevented or reversed by
progesterone, studies of the endogenous hormones in women showed that those with a natural excess of
estrogen, and/or deficiency of progesterone, were the most likely to develop uterine or breast cancers.
</p>
<p>
The Morganist school of genetic determinism moved into endocrinology with a doctrine that hormones act only
through hormone receptors, proteins which activate certain genes.
</p>
<p>
Many researchers -- physical chemists, biochemists, cytologists, embryologists, reproductive and
developmental biologists, gerontologists, physiologists, neurologists, endocrinologists -- were
investigating estrogen's properties and actions, and had made great progress by the 1950s, despite the
medical frauds being perpetrated by the estrogen industry (Rothenberg, 2005).
</p>
<p>
All of this complex and subtle work was of no interest to a small group of people who wanted to impose their
genetic views onto biology.
</p>
<p>
The inventor of the estrogen receptor, Elwood Jensen, has written that the results of certain of his
experiments "caused the demise of the transhydrogenation hypothesis and convinced all but the most diehard
enzymologists that estradiol binds to a characteristic component of target cells to exert its physiological
effect without itself being chemically altered." The hypothesis he referred to was just part of a large
fairly systematic international effort.
</p>
<p>
How he did away with the opposition, who were studying the complex metabolic actions of estrogen, was by
synthesizing isotope-labeled estradiol and estrone, and claiming to observe that they weren't metabolically
altered, as they produced their hormonal effect. Since the experiment was extremely expensive, and required
the cooperation of the Atomic Energy Commission, it wasn't easily repeated. However, many experiments have
subsequently demonstrated that practically every tissue in the body (and plants and bacteria) metabolize the
estrogens, causing estradiol to change into estrone, and estrone, into estradiol. Jensen's decisive and
historically crucial experiment was false.
</p>
<p>
But it served its purpose, and (with help from the pharmaceutical industry and government granting agencies)
marginalized the work of those "enzymologists" and everyone else who persisted in studying the complex
actions of estrogen.
</p>
<p>
The enzyme that converts the weaker estrone into the stronger estradiol is an important factor in
determining estrogen's effects on a particular tissue. Progesterone is able to regulate the cell's
metabolism, so that the oxidative pathway, forming estrone from estradiol, predominates. Estrogen-dominated
tissues are likely to have a balance in the direction of reduction rather than oxidation, increasing the
amount of the active estradiol.
</p>
<p>
The immediate effects of estrogen and progesterone on cells, that occur long before genes can be activated,
were simply ignored or denied by the promoters of the estrogen receptor doctrine. Some of these excitatory
or antiexcitatory effects are probably structural changes, that involve the mobilization of calcium inside
cells, and the activation or inhibition of reactions involving phosphoric acid. Although they have been
known for many years, they are always referred to as "novel" or "non-classical" effects, and are called
"membrane effects," because that's the only way the reductionists are able to identify changes that happen
immediately throughout the cell.
</p>
<p>
Cellular excitation involves an increase of intracellular calcium and the activation of phosphorylating
enzymes in cells. Some experiments suggest (Improta-Brears, et al., 1999) that the estrogen receptor
mediates estrogen's ability to mobilize calcium (leading to the activation of cell division, mitosis).
Whether or not it does, the recognition that estrogen activates calcium, leading to activation of the
phosphorylation system, should "cause the demise of" the "classical estrogen receptor" doctrine, because the
phosphorylation system alters the expression of genes, much as the estrogen receptor was supposed to do by
its direct actions. <strong>But before it alters the expression of genes, it alters the activities of
enzymes.</strong> When estrogen activates calcium and phosphorylation independently of the estrogen
receptor, the situation is even worse for the Jensen dogma.
</p>
<p>
Progesterone's opposition to those early excitatory effects of estrogen are so basic, that there shouldn't
be any difficulty in thinking of it as an antiestrogen, that stops cell division primarily by opposing the
excitatory effects of estrogen and other mitogens. Progesterone's opposition to the calcium-activating and
phosphorylating effects of estrogen affects everything in the cell, according to the cell's specific nature.
</p>
<p>
But the reductionists don't like "nongenomic" explanations of anything, even when they are triggered by the
estrogen receptor rather than by a membrane-event. So, to argue that progesterone's opposition to estrogen
is general, it's necessary to examine each of estrogen's actions, where those actions are clearly known, and
to evaluate progesterone's effects on the same events.
</p>
<p>
When a cell is stimulated or slightly stressed, homeostatic mechanisms are activated that help it to return
to its normal resting state. The mobilization of calcium and the phosphorylation system is followed by
increased synthesis of cholesterol and the formation of glucose from glycogen. Cholesterol itself is
protective, and in some cells it is massively converted into progesterone, which is even more effective in
restoring homeostasis.
</p>
<p>
In the ovary, the enzymes that synthesize cholesterol, along with the production of progesterone, are
activated by the pituitary hormone, FSH, but also by estrogen. In the liver and uterus and vascular
endothelium, which aren't specialized for the production of progesterone, stimulation by estrogen activates
the enzymes to increase the formation of cholesterol.
</p>
<p>
When cells are injured or seriously stressed, instead of being able to directly recover their normal
quiescence, they may instead mobilize their systems for growing and replicating, to replace damaged or
destroyed cells.
</p>
<p>
Prolonged exposure to estrogen, that can't be offset by the homeostatic factors, such as progesterone,
typically causes cells to enter a growth phase. (But so do other excitatory processes, such as ionizing
radiation.)
</p>
<p>
One of the basic reactions to injury is to shift the cell away from oxidative metabolism to glycolytic
metabolism, which is inefficient, but can support cell division. Chemical stains show that during cell
division cells are in a reduced state, with abundant sulfhydryl groups including reduced glutathione and
protein sulfhydryls. This shift in itself increases the formation of active estradiol from estrone.
</p>
<p>
In the inflamed or estrogen dominated cell, enzymes such as the cyclooxidases (COX), that convert
arachidonic acid into prostaglandins, are activated. Beta-glucuronidase and sulfatases are activated, and
these cause intracellular estrogen to increase, by removing the water soluble sulfate and glucuronate
portions from estrogens that had been inactivated. The detoxifying enzymes that attach those molecules to
estrogen are inactivated in the estrogen dominated cell. The prostaglandin formed from arachidonic acid
stimulates the formation of the enzyme aromatase or estrogen synthetase, that converts androgens into
estrogen.
</p>
<p>
Those processes, initiated by excitation or injury, increase the amount of estrogen in the cell, which
intensifies the excitation.
</p>
<p>
Progesterone opposes all of those processes, decreasing the amount of estrogen in the cell by modifying the
activities of those five types of enzyme.
</p>
<p>
Although many kinds of protein (including enzymes) bind estrogen, the protein that Jensen called "the
estrogen receptor" is largely responsible for the ability of the uterus and breasts to retain high
concentrations of estrogen. Various kinds of stimulation or stress (including heat and oxygen deprivation)
cause its appearance, and estrogen itself increases the amount of the estrogen receptor in a cell. The
estrogen receptor doesn't just "activate genes," as the Jensen dogma claimed. For example, the estrogen
receptor directly binds and inactivates the "tumor suppressor" p53 protein, which otherwise would restrain
the replication of damaged cells.
</p>
<p>
Progesterone causes the estrogen receptor to be eliminated. (Batra; Boling and Blandau; Resko, et al.)
</p>
<p>
Among the cell activating factors, other than estrogen, are proteins that are considered to be "oncogenes,"
because of their involvement in cancer. Several of these proteins are activated by estrogen, inhibited by
progesterone. The term "oncogene" refers to any gene that contributes to the development of cancer, but it
is so burdened by ideology that it shouldn't be used as if it had a simple clear meaning.
</p>
<p>
A variety of proteins promote cell activity and replication, under the influence of estrogen. The "composite
transcription factor activating protein 1," AP-1 which integrates the effects of other transcription
factors, is important in a variety of cell types, and its activity is increased by estrogen and decreased by
progesterone.
</p>
<p>
When the "progesterone receptor" <strong>lacks progesterone,</strong> it has the opposite effect of
progesterone, and this feature has been used propagandistically, by infecting cells with a virus carrying
the progesterone receptor protein, and then suggesting that the disturbed functions of the cell reflect a
potential effect of progesterone. The receptor, lacking progesterone, tells the cell that it has a
progesterone deficiency, but too many molecular endocrinologists are trying to say that the receptor protein
is the same as the progesterone.
</p>
<p>
The generality of the process of excitation/activation can be clearly seen in the effects of the
nerve-inhibiting GABA and the nerve-exciting glutamate or NMDA. In cultured breast cancer cells, GABA
inhibits growth, NMDA increases growth. As in the brain, progesterone supports the actions of GABA, and
opposes those of NMDA or the excitatory amino acids, while estrogen in general promotes the effects of the
excitatory amino acids, and opposes those of GABA.
</p>
<p>
Both the excitatory amino acids and a peptide that promotes inflammation, tumor necrosis factor (TNF),
activate the enzyme which makes estrogen, aromatase. Estrogen, by activating NF kappaB, increases the
formation of TNF, which in itself can promote the growth and metastasis of cancer. Various antiinflammatory
agents, including aspirin, progesterone, testosterone, saturated fats, and glycine, can inhibit the
production of NF kappaB.
</p>
<p>
An enzyme that has been thought of mainly in relation to the brain is catechol-O-methyl transferase, which
is inhibited by estrogen (producing effects similar to cocaine), leading to brain excitation.The enzyme
detoxifies catecholestrogen (Creveling, 2003), protecting cells from DNA damage (Lavigne, et al., 2001).
When the activity of this enzyme is low, there is increased risk of breast cancer (Matsui, et al., 2000).
Progesterone increases its activity (Inoue and Creveling, 1991, 1995).
</p>
<p>
Another enzyme system that affects the body's reactions to stress and modifies processes of inflammation and
growth, the monoamino-oxidases, is affected oppositely by estrogen and progesterone. Estrogen's effects are
partly mediated by increased formation of serotonin, progesterone's, by decreasing it. Histamine is another
promoter of inflammation that is increased by estrogen, decreased by progesterone.
</p>
<p>
Estrogen's effects in the nervous system go beyond the production of cocaine-like hypomania, or chorea, or
epilepsy, and include the activation of the basic stress hormones, increasing the formation in the
hypothalamus of pro-opiomelanocortin (POMC), which is a precursor of ACTH to activate the adrenals, and
endorphins ("endogenous opiates"), which stimulate growth processes. Both endorphins and ACTH can be found
in tumors such as breast cancer. The ACTH stimulates the production of cortisol, that protects against some
of the immediate causes of inflammation and growth, but that contributes to the loss of resistance, and
increases estrogen synthesis.
</p>
<p>
A protein called the sigma receptor, known for its role in cocaine's action, binds progesterone, and can
inhibit the growth of cancer. Some anesthetics have similar effects on tumors, acting through this protein.
The sigma receptor, in association with progesterone or pregnenolone, is protective against the excitatory
amino acids.
</p>
<p>
The extracellular medium changes during the development of a tumor. Irritated hypoxic cells, and
estrogen-stimulated cells, increase their production of collagen, and the increase of collagen interferes
with normal cell functions. Progesterone reduces the formation of collagen, and probably contributes to its
removal.
</p>
<p>
Naloxone or naltrexone, which blocks the actions of the endorphins and morphine, is being used to inhibit
the growth of various kinds of cancer, including breast cancer and prostate cancer. Leptin (which is
promoted by estrogen) is a hormone produced by fat cells, and it, like estrogen, activates the POMC-related
endorphin stress system. The endorphins activate histamine, another promoter of inflammation and cell
division.
</p>
<p>
Progesterone opposes those various biochemical effects of estrogen in multiple ways, for example by
inhibiting the ACTH stress response, by restraining cortisol's harmful actions, and by inhibiting leptin.
</p>
<p>
Mediators of the radiation bystander effect include NO, TNF, COX, and prostaglandins. These are produced by
other things that cause inflammation and injury, including estrogen.
</p>
<p>
Cell division, when it is part of the body's continuous renewal and adaptation, isn't a source of mutations
or degeneration, but when it is induced by the mediators of inflammation produced in response to injury, it
leads to inherited changes, loss of differentiated function, and eventually to genetic instability.
</p>
<p>
When cell division is so disturbed that the number of chromosomes becomes abnormal, the instability of these
cells decreases their ability to survive, but when the causes of the inflammation persist, they will
continue to be replaced by other abnormal cells. The toxic products of dying cells can reach a point at
which the debris can't be removed, adding to the injury and inflammation. The damaged bystander cells spread
their influence through a cancer field, injuring more cells.
</p>
<p>
One of the "field" effects of cancer is the stimulation of new blood vessel development, angiogenesis.
Lactic acid stimulates the formation of new blood vessels, the secretion of collagen, and tumor growth. Low
oxygen, nitric oxide, carbon monoxide, prostaglandins and other products of tissue stress can stimulate the
growth of new blood vessels, at the same time that they stimulate tumor growth and impair oxidative
metabolism. Several of these agents promote each other's activity.
</p>
<p>
Therapeutic thinking has been influenced by the doctrine of the mutant cell as the initiator of cancer,
leading to the idea that only things which kill the cancer cells can cure cancer. But when the body stops
activating the processes of inflammation and growth, normal processes of tissue repair have an opportunity
to eliminate the tumor. Even the fibroblasts which normally secrete collagen can participate in its removal
(Simoes, et al., 1984). Something as simple as eliminating lactate can change their functions.
</p>
<p>
Although the angiogenic action of lactate has been known for several decades, some researchers believed that
a specific anti-angiogenic peptide could be found which would stop the growth of cancer cells. The interest
in angiogenesis tacitly acknowledges that there is a cancer field, but the faith that cancer could be cured
only by killing the mutant cells seems to have guided the search for a single antiangiogenic substance. Such
a substance would be toxic to normal tissues, since blood vessels are constantly being renewed.
</p>
<p>
The more advanced a tumor is, the more numerous the growth-promoting factors are likely to be, and the
weaker the body's ability becomes to control them.
</p>
<p>
The search for toxic factors to kill the cancer cells is unlikely to lead to a generally effective
treatment. Even immunological approaches that think in terms of destroying a tumor might be misconceiving
the nature of the problem. For example, the protein called "tumor necrosis factor" (TNF) or cachectin was
discovered as a result of Lawrence Burton's work in the 1960s. He extracted proteins from the blood that
could shrink some tumors in mice with amazing speed. In the right setting, TNF is involved in the
destruction of tumors, but when other factors are missing, it can make them worse. Burton was focussing on
factors in the immune system that could destroy cancer, but he ignored the basic problem of tissue
degeneration that produces tumors which are complex and changing.
</p>
<p>
If the cancer-productive field is taken into account, all of the factors that promote and sustain that field
should be considered during therapy.
</p>
<p>
Two ubiquitous carcinogenic factors that can be manipulated without toxins are the polyunsaturated fatty
acids (PUFA) and estrogen. These closely interact with each other, and there are many ways in which they can
be modulated.
</p>
<p>
For example, keeping cells in a well oxygenated state with thyroid hormone and carbon dioxide will shift the
balance from estradiol toward the weaker estrone. The thyroid stimulation will cause the liver to excrete
estrogen more quickly, and will help to prevent the formation of aromatase in the tissues. Low temperature
is one of the factors that increases the formation of estrogen. Lactic acid, serotonin, nitric oxide,
prostaglandins, and the endorphins will be decreased by the shift toward efficient oxidative metabolism.
</p>
<p>
Progesterone synthesis will be increased by the higher metabolic rate, and will tend to keep the temperature
higher.
</p>
<p>
Thyroid hormone, by causing a shift away from estrogen and serotonin, lowers prolactin, which is involved in
the promotion of several kinds of cancer.
</p>
<p>
Vitamin D and vitamin K have some antiestrogenic effects. Vitamin D and calcium lower the
inflammation-promoting parathyroid hormone (PTH).
</p>
<p>
Eliminating polyunsaturated fats from the diet is essential if the bystander effect is eventually to be
restrained. Aspirin and salicylic acid can block many of the carcinogenic effects of the PUFA. Saturated
fats have a variety of antiinflammatory and anticancer actions. Some of those effects are direct, others are
the result of blocking the toxic effects of the PUFA. Keeping the stored unsaturated fats from circulating
in the blood is helpful, since it takes years to eliminate them from the tissues after the diet has changed.
Niacinamide inhibits lipolysis. Avoiding over-production of lipolytic adrenaline requires adequate thyroid
hormone, and the adjustment of the diet to minimize fluctuations of blood sugar.
</p>
<p>
The endorphins are antagonistic to progesterone, and when they are minimized, progesterone tends to
increase, and to be more effective. The drugs naloxone and naltrexone, which block the effects of the
endorphins, have several remarkable effects that resemble progesterone's. Naltrexone has been successfully
used to treat prostate and breast cancer.
</p>
<p>
Opiates are still commonly used for pain relief in cancer patients, despite the evidence that has
accumulated for several decades indicating that they promote inflammation and cancer growth, while
suppressing immunity and causing tissue catabolism, exacerbating the wasting that commonly occurs with
cancer. Their use, rather than alternatives such as procaine, aspirin, and progesterone, is nothing but a
medical fetish.
</p>
<p>
Stress and estrogen tend to produce alkalosis, while thyroid, carbon dioxide, and adequate protein in the
diet help to prevent alkalosis.
</p>
<p>
Antihistamines and some of the antiserotonin drugs (including "dopaminergic" lisuride and bromocriptine) are
sometimes useful in cancer treatment, but the safe way to lower serotonin is to reduce the consumption of
tryptophan, and to avoid excessive cortisol production (which mobilizes tryptophan from the muscles).
Pregnenolone and sucrose tend to prevent over-production of cortisol.
</p>
<p>
In the breast, COX-2 converts arachidonic acid into prostaglandins, which activate the enzyme aromatase,
that forms estrogen from androgens. Until the tissues are free of PUFA, aspirin and salicylic acid can be
used to stop prostaglandin synthesis.
</p>
<p>
Thyroid is needed to keep the cell in an oxidative, rather than reductive state, and progesterone (which is
produced elsewhere only when cells are in a rapidly oxidizing state) activates the processes that remove
estrogen from the cell, and inactivates the processes that would form new estrogen in the cell.
</p>
<p>
Thyroid, and the carbon dioxide it produces, prevent the formation of the toxic lactic acid. When there is
enough carbon dioxide in the tissues, the cell is kept in an oxidative state, and the formation of toxic
free radicals is suppressed. Carbon dioxide therapy is extremely safe.
</p>
<p>
In the 1930s, primates as well as rodents had been used in experiments to show the carcinogenic effects of
estrogen, and the protective effects of progesterone.
</p>
<p>
By 1950, the results of animal studies of progesterone's anticancer effects were so clear that the National
Cancer Institute got involved. But the estrogen industry had already been conducting its campaign against
progesterone, and had convinced most doctors that it was inactive when taken orally, and so was inferior to
their proprietary drugs that they called "progestins." The result was that it was usually given by
injection, dissolved in vegetable oil or synthetic solvents such as benzyl benzoate or benzyl alcohol, which
are very toxic and inflammation-producing.
</p>
<p>
The NCI researchers (Hertz, et al., 1951) treated 17 women with visible cancers of the uterine cervix that
had been confirmed by biopsies. They were given daily intramuscular injections of 250 mg of progesterone in
vegetable oil. Although they described the treatment as "massive dosage with progesterone," it didn't
prevent menstruation in any of the women who had been menstruating before the treatment began. During a
healthy pregnancy, a woman produces more progesterone than that.
</p>
<p>
Their article includes some photographs of cervical tumors before treatment, and after 31 days, 50 days, and
65 days of progesterone treatment. The improvement is clear. The examining physicians described softening of
the tumor, and stopping of bleeding and pain.
</p>
<p>
"In eleven of the 17 treated patients visible and palpable evidence of regressive alteration of the tumor
mass could be demonstrated. This consisted of (a) distinct reduction in size of the visible portion of the
cancer as well as reduction of the palpable extent of the mass, (b) reduction in vascularity and friability
of the visible lesion with a clearly demonstrable epithelization of previously raw surfaces and (c) markedly
increased pliability of the previously rigid and infiltrated parametria."
</p>
<p>
"In 10 cases there was associated with this type of gross change a reduction in, or complete cessation of
vaginal bleeding and discharge."
</p>
<p>
"Only one of the 17 patients showed active progression of the carcinomatous process while under the
progesterone administration. The six patients whose lesions failed to show clearly demonstrable regressive
changes showed minor alterations in size and vascularity of insufficient degree to be convincing to all
clinical observers concerned. Nevertheless, none of the lesions under study appeared to be accelerated by
progesterone."
</p>
<p>
Observing very similar patients under similar conditions while they were waiting for surgery, but were not
receiving progesterone, they saw no such regressions of tumors.
</p>
<p>
The photographs and descriptions of the changes in the tumors were remarkable for any cancer study, but to
have been produced by a treatment that didn't even alter the patients' menstrual cycle, the reader might
expect the authors to discuss their plans for further studies of such a successful method.
</p>
<p>
But instead, they concluded "We do not consider the regressive changes observed to be sufficient to indicate
the use of progesterone as a therapeutic agent in carcinoma of the cervix."
</p>
<p>
(Their research was supported by a grant from the American Cancer Society.)
</p>
<p>
If the researchers had bothered to test progesterone on themselves or on animals, they would have discovered
that it is fully active when taken orally, dissolved in oil, and that nontoxic saturated fats could have
been used. Progesterone anesthesia was very well known at that time, so it would have been reasonable to use
doses that were at least equivalent to the concentrations present during pregnancy, even if they didn't want
to use doses that would approach the anesthetic level. The total daily doses could have been about ten times
higher, if they had been given orally as divided doses.
</p>
<p>
The solvent issue continues to impede research in the use of progesterone for treating cancer, but the main
problem is the continuing belief that "the cancer cell" is the problem, rather than the cancer field.
Substances are tested for their ability to kill cancer cells <em>in vitro</em>, because of the basic belief
that mutated genes are the cause of the disease. When progesterone is tested on cancer cells <em>in
vitro,</em>
the experimenter often sees nothing but the effects of the solvent, and doesn't realize that nearly all of
the progesterone has precipitated in the medium, before reaching the cancer cells.
</p>
<p>
The cancer industry began a few years ago to combine chemicals for chemotherapy, for example adding caffeine
to paclitaxel or platinum (cisplatin), or histamine to doxorubicin, but they do it simply to increase the
toxicity of the chemical to the tumor, or to decrease its toxicity to the patient. Doctors sometimes refer
to combined chemotherapy as a "shotgun approach," meaning that it lacks the acumen of their ideal silver
bullet approach. If cancers were werewolves, the cancer industry's search for more refined killing
technologies might be going in the right direction. But the genetic doctrine of cancer's origin is just as
mythical as werewolves and vampires.
</p>
<p>
A safe physiological approach to cancer, based on the opposition of progesterone to estrogen, would be
applicable to every type of cancer promoted by estrogen, or by factors which produce the same effects as
estrogen, and that would include all of the known types of cancer. Estrogen acts even on cells that have no
"estrogen receptors," but estrogen receptors can be found in every organ.
</p>
<p>
As estrogen's non-feminizing actions are increasingly being recognized to include contributions to other
kinds of disease, including Alzheimer's disease, heart disease, and rheumatoid arthritis, the idea of the
bystander effect, and the field of cellular degeneration, will eventually clear the way for a rational use
of the therapeutic tools that already exist.
</p>
<p>
There are several types of drug---carbonic anhydrase inhibitors, to increase carbon dioxide in the tissues,
lysergic acid derivatives, to block serotonin and suppress prolactin, anti-opiates, antiexcitotoxic and
GABAergic agents, anesthetics, antihistamines, anticholinergics, salicylic acid derivatives---that could
probably be useful in a comprehensive therapy for cancer, but their combinations won't be explored as long
as treatments are designed only to kill.
</p>
<p>
Preventing or correcting disturbances in the morphogenetic field should be the focus of attention.
</p>
<p><h3>REFERENCES</h3></p>
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<p>
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epithelial cell cycles was evaluated in vivo. Results demonstrated that <strong>estradiol significantly
increases cell proliferation, while progesterone significantly decreases cell replication below that
observed with placebo.
</strong>
Transdermal progesterone was also shown to reduce estradiol-induced proliferation.
</p>
<p>
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indicate that the IGFR-I mRNA is up-regulated by two to threefold compared with untreated levels by 7 and 14
days E2 treatment. <strong>
In contrast, 7 or 14 days Pg treatment down-regulates the receptor mRNA to approximately half that of
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</p>
<p>
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</p>
<p>
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</p>
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<p>
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<p>
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<p>
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breast epithelial cells in vivo." Randomized Controlled Trial
</p>
<p>
Mol Cell Biochem 1999 Dec;202(1-2):53-61. <strong>Bcl-2, survivin and variant CD44 v7-v10 are downregulated
and p53 is upregulated in breast cancer cells by progesterone: inhibition of cell growth and induction
of apoptosis.
</strong>
Formby B, Wiley TS."This study sought to elucidate the <strong>mechanism by which progesterone inhibits the
proliferation of breast cancer cells."</strong>
"The results demonstrated that progesterone does produce a strong antiproliferative effect on breast cancer
cell lines containing progesterone receptors, and induced apoptosis. <strong>The relatively high levels of
progesterone utilized were similar to those seen during the third trimester of human pregnancy.</strong
>"
</p>
<p>
Ann Clin Lab Sci 1998 Nov-Dec;28(6):360-9. <strong>Progesterone inhibits growth and induces apoptosis in
breast cancer cells: inverse effects on Bcl-2 and p53.</strong> Formby B, Wiley TS.
</p>
<p>
Cancer Lett 1999 Jul 1;141(1-2):63-71.<strong>
Progestins suppress estrogen-induced expression of vascular endothelial growth factor (VEGF) subtypes in
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</p>
<p>
Mol Cell Biol. 2006 Oct;26(20):7632-44. <strong>TReP-132 Is a Novel Progesterone Receptor Coactivator
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Progesterone.
</strong>
Gizard F, Robillard R, Gross B, Barbier O, Revillion F, Peyrat JP, Torpier G, Hum DW, Staels B.
</p>
<p>
Am J Physiol. 1982 Oct;243(4):H619-27. <strong>NAD/NADH: redox state changes on cat brain cortex during
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</strong>
Gyulai L, Dora E, Kovach AG.
</p>
<p>
Drug Metab Dispos. 1995 Mar;23(3):430-2. <strong>Induction of catechol-O-methyltransferase in the luminal
epithelium of rat uterus by progesterone: inhibition by RU-486.</strong> Inoue K, Creveling CR.
</p>
<p>
Hertz R, Cromer J.K., Young J.P. and Westfall B.B., pages 366-374, in <strong><em>
Symposium on Steroids in Experimental and Clinical Practice,</em></strong>
Abraham White, Blakiston, 195.
</p>
<p>
Cancer Res. 2005 Jul 15;65(14):6450-8. <strong>Progesterone receptor in non-small cell lung cancer--a potent
prognostic factor and possible target for endocrine therapy.
</strong>Ishibashi H, Suzuki T, Suzuki S, Niikawa H, Lu L, Miki Y, Moriya T, Hayashi S, Handa M, Kondo T,
Sasano H. "Cell proliferation was inhibited by progesterone in these progesterone receptor-positive NSCLC
cells in a dose-dependent manner, which was inhibited by progesterone receptor blocker. Proliferation of
these tumor cells injected into nude mice was also dose-dependently inhibited by progesterone, with a
concomitant increase of p21 and p27 and a decrease of cyclin A, cyclin E, and Ki67. Results of our present
study suggested that progesterone receptor was a potent prognostic factor in NSCLCs and progesterone
inhibited growth of progesterone receptor-positive NSCLC cells. Therefore, progesterone therapy may be
clinically effective in suppressing development of progesterone receptor-positive NSCLC patients."
</p>
<p>
Naunyn Schmiedebergs Arch Pharmacol. 1986 Aug;333(4):368-76. <strong>Effect of progesterone on the
metabolism of noradrenaline in rabbit uterine endometrium and myometrium.</strong> Kennedy JA, de la
Lande IS.
</p>
<p>
Agressologie 1971;12(2):105-112. <strong>[The inhibiting effect of atmospheres oxygenated without CO2 on the
respiration of rat tissue slices (brain, liver). Physiopathological implications].</strong> Laborit H,
Lamothe C, Thuret F
</p>
<p>
Am J Respir Crit Care Med. 2004 Jan 1;169(1):46-56. <strong>Hypercapnic acidosis attenuates
endotoxin-induced acute lung injury.</strong> Laffey JG, Honan D, Hopkins N, Hyvelin JM, Boylan JF,
McLoughlin P.
</p>
<p>
<em>*Endocrinology. 1996 Apr;137(4):1505-6.
</em>
</p>
<p>
<em>[Comment on: Laidlaw, et al., Endocrinology. 1995 Jan;136(1):164-71.]</em>
<strong><em>
Experiments on proliferation of normal human breast tissue in nude mice do not show that
progesterone does not stimulate breast cells.</em></strong>
<em>
Pike MC, Ursin G, Spicer DV. Letter</em>
</p>
<p>
*Endocrinology. 1995 Jan;136(1):164-71. <strong>The proliferation of normal human breast tissue implanted
into athymic nude mice is stimulated by estrogen but not progesterone.</strong> Laidlaw IJ, Clarke RB,
Howell A, Owen AW, Potten CS, Anderson E. "We conclude that E2 is sufficient to stimulate human breast
epithelial cell proliferation at physiologically relevant concentrations and that P does not affect
proliferation either alone or after E2 priming."
</p>
<p>
Agressologie 1971;12(2):105-112. <strong>[The inhibiting effect of atmospheres oxygenated without CO2 on the
respiration of rat tissue slices (brain, liver). Physiopathological implications].</strong> Laborit H,
Lamothe C, Thuret F
</p>
<p>
Endocrinology. 1995 Jan;136(1):164-71. <strong>The proliferation of normal human breast tissue implanted
into athymic nude mice is stimulated by estrogen but not progesterone.</strong> Laidlaw IJ, Clarke RB,
Howell A, Owen AW, Potten CS, Anderson E.
</p>
<p>
Int J Cancer. 2005 Nov 20;117(4):561-8. <strong>Gene regulation profile reveals consistent anticancer
properties of progesterone in hormone-independent breast cancer cells transfected with progesterone
receptor.</strong> Leo JC, Wang SM, Guo CH, Aw SE, Zhao Y, Li JM, Hui KM, Lin VC.<strong>"Progesterone
consistently suppressed the expression of genes required for cell proliferation and metastasis and
increased the expression of many tumor-suppressor genes.</strong>"
</p>
<p>
Fertil Steril. 2003 Jan;79(1):221-2. <strong>Topical progesterone cream has an antiproliferative effect on
estrogen-stimulated endometrium.</strong> Leonetti HB, Wilson KJ, Anasti JN. Randomized Controlled Trial
</p>
<p>
Prostate. 1995 Apr;26(4):194-204. <strong>Growth inhibition of androgen-insensitive human prostate carcinoma
cells by a 19-norsteroid derivative agent, mifepristone.</strong> Lin MF, Kawachi MH, Stallcup MR,
Grunberg SM, Lin FF. "Mifepristone, also known as RU 486, is a 19-norsteroid derivative. Currently,
mifepristone is being tested in clinical trials on meningioma and breast cancer.""<strong>The results
demonstrated that while both DHT and Dex alone had essentially no effect on cell growth, progesterone
alone resulted in a 20% growth inhibition, while mifepristone had more than 60% inhibition with a 16-day
exposure. At an equal concentration, the degree of growth inhibition of PC-3 cells by mifepristone or
progesterone was partially diminished by simultaneous exposure to Dex.</strong>"
</p>
<p>
Am J Pathol. 2003 Jun;162(6):1781-7. <strong>Progesterone induces cellular differentiation in MDA-MB-231
breast cancer cells transfected with progesterone receptor complementary DNA.
</strong>Lin VC, Jin R, Tan PH, Aw SE, Woon CT, Bay BH.
</p>
<p>
Endocrinology. 2003 Dec;144(12):5650-7. <strong>Distinct molecular pathways mediate progesterone-induced
growth inhibition and focal adhesion.</strong> Lin VC, Woon CT, Aw SE, Guo C.
</p>
<p>
Int J Cancer. 2005 Nov 20;117(4):561-8.<strong>
Gene regulation profile reveals consistent anticancer properties of progesterone in hormone-independent
breast cancer cells transfected with progesterone receptor.</strong> Leo JC, Wang SM, Guo CH, Aw SE,
Zhao Y, Li JM, Hui KM, Lin VC.
</p>
<p>
Int J Biometeorol. 1987 Sep;31(3):201-10. <strong>Effects of chronic normobaric hypoxic and hypercapnic
exposure in rats: prevention of experimental chronic mountain sickness by hypercapnia.</strong> Lincoln
B, Bonkovsky HL, Ou LC.
</p>
<p>
J Steroid Biochem Mol Biol. 2000 Jun;73(3-4):171-81. <strong>Progesterone effect on cell growth,
ultrastructural aspect and estradiol receptors of normal human breast epithelial (HBE) cells in
culture.</strong> Malet C, Spritzer P, Guillaumin D, Kuttenn F. "On a culture system of normal human
breast epithelial (HBE) cells, we observed an inhibitory effect on cell growth of a long-term P treatment (7
days) in the presence or absence of E2, using two methods...." "Cells exhibited a proliferative appearance
after E2 treatment, and returned to a quiescent appearance when P was added to E2." "Moreover, the
immunocytochemical study of E2 receptors indicated that <strong>E2 increases its own receptor level whereas
P and R5020 have the opposite effect, thus limiting the stimulatory effect of E2 on cell growth.</strong
> In the HBE cell culture system and in long-term treatment, P and R5020 appear predominantly to inhibit
cell growth, both in the presence and absence of E2."
</p>
<p>
Horm Res. 1987;28(2-4):212-8.<strong>
Antiestrogen action of progesterone in breast tissue.</strong> Mauvais-Jarvis P, Kuttenn F, Gompel A.
"Most data indicate that progesterone and progestins have a strong antiestrogen effect on breast cell
appreciated by the decrease of estradiol receptor content, the decrease of cell multiplication and the
stimulation of 17 beta-hydroxysteroid activity which may be considered as a marker of breast cell
differentiation dependent of progesterone receptor."
</p>
<p>
Biochem Biophys Res Commun 1982 Jan 29;104(2):570-6. <strong>Progesterone-induced inactivation of nuclear
estrogen receptor in the hamster uterus is mediated by acid phosphatase.</strong>
MacDonald RG, Okulicz WC, Leavitt WW.
</p>
<p>
Cancer Lett. 2005 Apr 18;221(1):49-53. <strong>Effects of progesterone on ovarian tumorigenesis in
xenografted mice.
</strong>
McDonnel AC, Van Kirk EA, Isaak DD, Murdoch WJ.
</p>
<p>
Int J Cancer. 2004 Nov 1;112(2):312-8. <strong>Endogenous sex hormones and subsequent breast cancer in
premenopausal women.</strong> Micheli A, Muti P, Secreto G, Krogh V, Meneghini E, Venturelli E, Sieri S,
Pala V, Berrino F.
</p>
<p>
J Clin Endocrinol Metab 2000 Sep;85(9):3442-52. <strong>Progesterone withdrawal up-regulates vascular
endothelial growth factor receptor type 2 in the superficial zone stroma of the human and macaque
endometrium: potential relevance to menstruation.</strong> Nayak NR, Critchley HO, Slayden OD, Menrad A,
Chwalisz K, Baird DT, Brenner RM.
</p>
<p>
Endocrinology 1981 Dec;109(6):2273-5. <strong>
Progesterone-induced estrogen receptor-regulatory factor in hamster uterine nuclei: preliminary
characterization in a cell-free system.</strong>
Okulicz WC, MacDonald RG, Leavitt WW<strong>
In vitro studies have demonstrated a progesterone-induced activity associated with the uterine nuclear
fraction which resulted in the loss of nuclear estrogen receptor.</strong>
</p>
<p>
Mol Endocrinol. 1991 May;5(5):709-17. <strong>Progestins induce down-regulation of insulin-like growth
factor-I (IGF-I) receptors in human breast cancer cells: potential autocrine role of IGF-II.
</strong>
Papa V, Hartmann KK, Rosenthal SM, Maddux BA, Siiteri PK, Goldfine ID.
</p>
<p>
Gynecol Endocrinol. 1999 Jun;13 Suppl 4:11-9. <strong>Biological effects of progestins in breast cancer.
</strong>Pasqualini JR, Ebert C.
</p>
<p>
Gynecol Endocrinol. 2001 Dec;15 Suppl 6:44-52. <strong>Biological effects of progestins in breast
cancer.</strong> Pasqualini JR, Ebert C, Chetrite GS.
</p>
<p>
J Steroid Biochem Mol Biol. 2005 Feb;93(2-5):221-36. <strong>Recent insight on the control of enzymes
involved in estrogen formation and transformation in human breast cancer.</strong> Pasqualini JR,
Chetrite GS.
</p>
<p>
Cancer Epidemiol Biomarkers Prev. 2002 Apr;11(4):361-8. <strong>Steroid hormone levels during pregnancy and
incidence of maternal breast cancer.</strong>
Peck JD, Hulka BS, Poole C, Savitz DA, Baird D, Richardson BE. "<strong>When estrogen-to-progesterone ratios
were evaluated, there was an indication of a modest increased incidence of breast cancer for those with
high total estrogens and high estrone levels relative to progesterone.</strong>"
</p>
<p>
Br J Urol. 1990 Mar;65(3):268-70. <strong>Erythrocyte stearic to oleic acid ratio in prostatic
carcinoma.</strong> Persad RA, Gillatt DA, Heinemann D, Habib NA, Smith PJ.
</p>
<p>
Int J Cancer. 2006 Nov 9; <strong>Inflammation and IGF-I activate the Akt pathway in breast cancer.</strong>
Prueitt RL, Boersma BJ, Howe TM, Goodman JE, Thomas DD, Ying L, Pfiester CM, Yfantis HG, Cottrell JR, Lee
DH, Remaley AT, Hofseth LJ, Wink DA, Ambs S.
</p>
<p>
Biology of reproduction 15, 153-157, 1976, <strong>Sex steroids in reproductive tract tissues: Regulation of
estradiol concentrations by progesterone</strong>. Resko JA, Boling JL, Brenner RM and Blandau RJ.
</p>
<p>
Carla Rothenberg, <strong>History of hormone therapy,</strong> http:<a
href="http://leda.law.harvard.edu/leda/data/711/Rothenberg05"
target="_blank"
>leda.law.harvard.edu/leda/data/711/Rothenberg05</a>. pdf. <strong> </strong>2005.
</p>
<p>
J Clin Endocrinol Metab 1996 Apr;81(4):1495-501. <strong>Characterization of reproductive hormonal dynamics
in the perimenopause.</strong>
<hr />
<strong>altered ovarian function in the perimenopause can be observed as early as age 43 yr and include
hyperestrogenism, hypergonadotropism, and decreased luteal phase progesterone excretion.</strong> These
hormonal alterations may well be responsible for the increased gynecological morbidity that characterizes
this period of life."
</p>
<p>
Cancer Res. 1984 Feb;44(2):841-4. <strong>High testosterone and low progesterone circulating levels in
premenopausal patients with hyperplasia and cancer of the breast.</strong> Secreto G, Recchione C,
Fariselli G, Di Pietro S.
</p>
<p>
Gen Comp Endocrinol. 1988 Dec;72(3):443-52. <strong>Progesterone down-regulation of nuclear estrogen
receptor: a fundamental mechanism in birds and mammals.</strong>
Selcer KW, Leavitt WW.
</p>
<p>
Clin Exp Obstet Gynecol 2000;27(1):54-6. <strong>
Hormonal reproductive status of women at menopausal transition compared to that observed in a group of
midreproductive-aged women.</strong> Sengos C, Iatrakis G, Andreakos C, Xygakis A, Papapetrou P.
"<strong>CONCLUSION: The reproductive hormonal patterns in</strong>
<strong>perimenopausal women favor a relatively hypergonadotropic hyper-estrogenic milieu.</strong>"
</p>
<p>
J Natl Cancer Inst Monogr. 1994;(16):85-90. <strong>Menstrual timing of treatment for breast cancer.
</strong>
Senie RT, Kinne DW.
</p>
<p>
J Neurosci. 2001 Aug 1;21(15):5723-9. <strong>Progesterone blockade of estrogen activation of mu-opioid
receptors regulates reproductive behavior.</strong>
Sinchak K, Micevych PE.
</p>
<p>
J Clin Pathol. 2005 Oct;58(10):1033-8. <strong>Proliferating fibroblasts at the invading tumour edge of
colorectal adenocarcinomas are associated with endogenous markers of hypoxia, acidity, and oxidative
stress.</strong>
Sivridis E, Giatromanolaki A, Koukourakis MI.
</p>
<p>
Neuroscience. 1991;42(2):309-20. <strong>Progesterone administration attenuates excitatory amino acid
responses of cerebellar Purkinje cells.</strong> Smith SS.
</p>
<p>
Cancer Causes Control. 2004 Feb;15(1):45-53. <strong>Serum levels of sex hormones and breast cancer risk in
premenopausal women: a case-control study (USA).</strong> Sturgeon SR, Potischman N, Malone KE, Dorgan
JF, Daling J, Schairer C, Brinton LA. <strong>"For luteal progesterone, the RR for the highest versus lowest
tertile was 0.55 (0.2-1.4)."</strong>
</p>
<p>
Biomed Pharmacother 1984;38(8):371-9. <strong>Breast cancer and oral contraceptives: critique of the
proposition that high potency progestogen products confer excess risk.
</strong>Sturtevant FM A recent report by Pike et al. from the U. S. A. concluded on the basis of
epidemiologic evidence that an increased risk of breast cancer was manifested by young women who had used
combination oral contraceptives (OC) with a high "potency" of progestogen over a prolonged period. This
conclusion is criticized in the present article, centering on three cardinal defects in the Pike study: (1)
The assigned potencies of OC's are fiction and were derived from out-dated delay-of-menses data; (2)
Well-known risk factors for breast cancer were ignored; (3) The method assumed no error of recall of OC
brand, dose and duration of use occurring many years before telephone interviews. Noting that others have
not been able to confirm these findings, it is concluded that there is no scientific basis for accepting the
suggestion of Pike et al.
</p>
<p>
Cancer Res. 2004 Nov 1;64(21):7886-92. <strong>Reduction of human metastatic breast cancer cell
aggressiveness on introduction of either form a or B of the progesterone receptor and then treatment
with progestins.</strong> Sumida T, Itahana Y, Hamakawa H, Desprez PY.
</p>
<p>
Endocr Relat Cancer 1999 Jun;6(2):307-14.<strong>
Aromatase overexpression and breast hyperplasia, an in vivo model--continued overexpression of aromatase
is sufficient to maintain hyperplasia without circulating estrogens, and aromatase inhibitors abrogate
these preneoplastic changes in mammary glands.</strong> Tekmal RR, Kirma N, Gill K, Fowler K "To test
directly the role of breast-tissue estrogen in initiation of breast cancer, we have developed the
aromatase-transgenic mouse model and demonstrated for the first time that increased mammary estrogens
resulting from the overexpression of aromatase in mammary glands lead to the induction of various
preneoplastic and neoplastic changes that are similar to early breast cancer." "Our current studies show
aromatase overexpression is sufficient to induce and maintain early preneoplastic and neoplastic changes in
female mice without circulating ovarian estrogen. Preneoplastic and neoplastic changes induced in mammary
glands as a result of aromatase overexpression can be completely abrogated with the administration of the
aromatase inhibitor, letrozole. Consistent with complete reduction in hyperplasia,<strong>
we have also seen downregulation of estrogen receptor and a decrease in cell proliferation</strong>
markers, suggesting aromatase-induced hyperplasia can be treated with aromatase inhibitors. Our studies
demonstrate that <strong>aromatase overexpression alone, without circulating estrogen, is responsible for
the induction of breast hyperplasia and these changes can be abrogated using aromatase
inhibitors."</strong>
</p>
<p>
Ann N Y Acad Sci 1986;464:106-16. <strong>
Uptake and concentration of steroid hormones in mammary tissues.</strong>
Thijssen JH, van Landeghem AA, Poortman J "For estradiol the highest tissue levels were found in the
malignant samples<strong>. No differences were seen in these levels between pre- and postmenopausal women
despite the largely different peripheral blood levels."</strong> "Striking differences were seen between
the breast and uterine tissues for the total tissue concentration of estradiol, the ratio between estradiol
and estrone, and the subcellular distribution of both estrogens. <strong>
At similar receptor concentrations in the tissues these differences cannot easily be explained.</strong
>" "<strong>Lower concentrations of DHEAS and DHEA were observed in the malignant tissues compared with the
normal ones and the benign lesions.</strong>"
</p>
<p>
Cancer. 1983 Jun 1;51(11):2100-4. <strong>Elevated serum acute phase protein levels as predictors of
disseminated breast cancer.</strong> Thompson DK, Haddow JE, Smith DE, Ritchie RF.
</p>
<p>
Crit Care Med. 2003 Nov;31(11):2705-7. <strong>Carbon dioxide: a "waste product" with potential therapeutic
utilities in critical care.</strong>
Torbati D.
</p>
<p>
J Steroid Biochem Mol Biol 2000 Jun;73(3-4):141-5. <strong>Elevated steroid sulfatase expression in breast
cancers.</strong> Utsumi T, Yoshimura N, Takeuchi S, Maruta M, Maeda K, Harada N. In situ estrogen
synthesis makes an important contribution to the high estrogen concentration found in breast cancer tissues.
Steroid sulfatase which hydrolyzes several sulfated steroids such as estrone sulfate, dehydroepiandrosterone
sulfate, and cholesterol sulfate may be involved. In the present study, we therefore, assessed steroid
sulfatase mRNA levels in breast malignancies and background tissues from 38 patients by reverse
transcription and polymerase chain reaction. The levels in breast cancer tissues were significantly
increased at 1458.4+/-2119.7 attomoles/mg RNA (mean +/- SD) as compared with 535.6+/-663.4 attomoles/mg RNA
for non-malignant tissues (P&lt;0.001). Thus, increased steroid sulfatase expression may be partly
responsible for local overproduction of estrogen and provide a growth advantage for tumor cells.
</p>
<p>
Fed Proc. 1980 Jun;39(8):2533-8. <strong>Influence of endogenous opiates on anterior pituitary
function.</strong> Van Vugt DA, Meites J.
</p>
<p>
Clin Endocrinol (Oxf) 1978 Jul;9(1):59-66. <strong>Sex hormone concentrations in post-menopausal
women.</strong>
Vermeulen A, Verdonck L. "Plasma sex hormone concentrations (testosterone, (T), androstenedione (A),
oestrone (E1) and oestradiol (E2) were measured in forty post-menopausal women more than 4 years post-normal
menopause." <strong>"Sex hormone concentrations in this group of postmenopausal women (greater than 4YPM)
did not show any variation as a function of age,</strong> with the possible exception of E2 which showed
a tendency to decrease in the late post-menopause."
</p>
<p>
J Steroid Biochem 1984 Nov;21(5):607-12. <strong>
The endogenous concentration of estradiol and estrone in normal human postmenopausal
endometrium.</strong> Vermeulen-Meiners C, Jaszmann LJ, Haspels AA, Poortman J, Thijssen JH The
endogenous estrone (E1) and estradiol (E2) levels (pg/g tissue) were measured in 54 postmenopausal, atrophic
endometria and compared with the E1 and E2 levels in plasma (pg/ml). The results from the tissue levels of
both steroids<strong>
showed large variations and there was no significant correlation with their plasma levels. The mean E2
concentration in tissue was 420 pg/g, 50 times higher than in plasma and the E1 concentration of 270
pg/g was 9 times higher.
</strong>
The E2/E1 ratio in tissue of 1.6, was higher than the corresponding E2/E1 ratio in plasma, being 0.3.
<strong>We conclude that normal postmenopausal atrophic endometria contain relatively high concentrations of
estradiol and somewhat lower estrone levels.</strong> These tissue levels do not lead to histological
effects.
</p>
<p>
J Natl Cancer Inst Monogr. 2000;(27):67-73. <strong>Endogenous estrogens as carcinogens through metabolic
activation.</strong> Yager JD.
</p>
<p>
Regul Pept. 2003 Jul 15;114(2-3):101-7. <strong>Inhibition of cytosolic phospholipase A2 mRNA expression: a
novel mechanism for acetylsalicylic acid-mediated growth inhibition and apoptosis in colon cancer
cells.</strong> Yu HG, Huang JA, Yang YN, Luo HS, Yu JP, Meier JJ, Schrader H, Bastian A, Schmidt WE,
Schmitz.
</p>
<p>
Brain Res. 1999 Aug 28;839(2):313-22. <strong>Opioid growth factor and organ development in rat and human
embryos.</strong> Zagon IS, Wu Y, McLaughlin PJ.
</p>
<p>
J Biol Chem. 2005 Apr 29;280(17):17480-7. Epub 2005 Feb 22. <strong>A novel antiestrogenic mechanism in
progesterone receptor-transfected breast cancer cells.
</strong>Zheng ZY, Bay BH, Aw SE, Lin VC.
</p>
© Ray Peat Ph.D. 2007. All Rights Reserved. www.RayPeat.com
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