Toxic Additives in Your Food and Drink
Not Just Another Scare
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There are a growing number of clinicians and basic scientists who are
convinced that excitotoxins play a critical role in the development
of several neurological disorders, including migraines, seizures, infections,
abnormal neural development, certain endocrine disorders, specific types
of obesity, and especially the neurodegenerative diseases; a group of
diseases which includes: ALS, Parkinson’s disease, Alzheimer’s disease,
Huntington’s disease, and olivo-ponto-cerebellar degeneration.
An enormous amount of both clinical and experimental evidence has accumulated
over the past decade supporting this basic premise. Yet, the FDA still
refuses to recognize the immediate and long term danger to the public
caused by the practice of allowing various excitotoxins to be added
to the food supply, such as MSG, hydrolyzed vegetable protein, and aspartame.
The amount of these neurotoxins added to our food has increased enormously
since their first introduction. For example, since 1948 the amount of
MSG added to foods has doubled every decade. By 1972, 262,000 metric
tons were being added to foods. Over 800 million pounds of aspartame
have been consumed in various products since it was first approved.
Ironically, these food additives have nothing to do with preserving
food or protecting its integrity. They are all used to alter the taste
of food. MSG, hydrolyzed vegetable protein, and natural flavoring are
used to enhance the taste of food so that it tastes better. Aspartame
is an artificial sweetener.
The public must be made aware that these toxins (excitotoxins) are
not present in just a few foods but rather in almost all processed foods.
In many cases they are being added in disguised forms, such as natural
flavoring, spices, yeast extract, textured protein, soy protein extract,
etc. Experimentally, we know that when subtoxic (below toxic levels)
of excitotoxins are given to animals, they experience full toxicity.
Also, liquid forms of excitotoxins, as occurs in soups, gravies and
diet soft drinks are more toxic than that added to solid foods. This
is because they are more rapidly absorbed and reach higher blood levels.
So, what is an excitotoxin? These are substances, usually amino acids,
that react with specialized receptors in the brain in such a way as
to lead to destruction of certain types of brain cells. Glutamate is
one of the more commonly known excitotoxins. MSG is the sodium salt
of glutamate. This amino acid is a normal neurotransmitter in the brain.
In fact, it is the most commonly used neurotransmitter by the brain.
Defenders of MSG and aspartame use, usually say: How could a substance
that is used normally by the brain cause harm? This is because, glutamate,
as a neurotransmitter, is used by the brain only in very, very small
concentrations - no more than 8 to 12ug. When the concentration of this
transmitter rises above this level the neurons begin to fire abnormally.
At higher concentrations, the cells undergo a specialized process of
cell death.
The brain has several elaborate mechanisms to prevent accumulation
of MSG in the brain. First is the blood-brain barrier, a system that
impedes glutamate entry into the area of the brain cells. But, this
system was intended to protect the brain against occasional elevation
of glutamate of a moderate degree, as would be found with un-processed
food consumption. It was not designed to eliminate very high concentrations
of glutamate and aspartate consumed daily, several times a day, as we
see in modern society. Several experiments have demonstrated that under
such conditions, glutamate can by-pass this barrier system and enter
the brain in toxic concentrations. In fact, there is some evidence that
it may actually be concentrated within the brain with prolonged exposures.
There are also several conditions under which the blood-brain barrier
(BBB) is made incompetent. Before birth, the BBB is incompetent and
will allow glutamate to enter the brain. It may be that for a considerable
period after birth the barrier may also be incompletely developed as well.
Hypertension, diabetes, head trauma, brain tumors, strokes, certain
drugs, Alzheimer’s disease, vitamin and mineral deficiencies, severe
hypoglycemia, heat stroke, electromagnetic radiation, ionizing radiation,
multiple sclerosis, and certain infections can all cause the barrier
to fail. In fact, as we age the barrier system becomes more porous,
allowing excitotoxins in the blood to enter the brain. So there are
numerous instances under which excitotoxin food additives can enter
and damage the brain. Finally, recent experiments have shown that glutamate
and aspartate (as in aspartame) can open the barrier itself. Another
system used to protect the brain against environmental excitotoxins,
is a system within the brain that binds the glutamate molecule (called
the glutamate transporter) and transports it to a special storage cell
(the astrocyte) within a fraction of a second after it is used as a
neurotransmitter. This system can be overwhelmed by high intakes of
MSG, aspartame and other food excitotoxins. It is also known that excitotoxins
themselves can cause the generation of numerous amounts of free radicals
and that during the process of lipid peroxidation (oxidation of membrane
fats) a substance is produced called 4-hydroxynonenal. This chemical
inhibits the glutamate transporter, thus allowing glutamate to accumulate
in the brain.
Excitotoxins destroy neurons partly by stimulating the generation of
large numbers of free radicals. Recently, it has been shown that this
occurs not only within the brain, but also within other tissues and
organs as well (liver and red blood cells). This could, from all available
evidence, increase all sorts of degenerative diseases such as arthritis,
coronary heart disease, and atherosclerosis, as well as induce cancer
formation. Certainly, we would not want to do something that would significantly
increase free radical production in the body. It is known that all of
the neurodegenerative disease, such as Parkinson’s disease, Alzheimer’s
disease, and ALS, are associated with free radical injury of the nervous
system.
It should also be appreciated that the effects of excitotoxin food
additives generally is not dramatic. Some individuals may be especially
sensitive and develop severe symptoms and even sudden death from cardiac
irritability, but in most instances the effects are subtle and develop
over a long period of time. While MSG and aspartame are probably not
causes of the neurodegenerative diseases, such as Alzheimer’s dementia,
Parkinson’s disease, or amyotrophic lateral sclerosis, they may well
precipitate these disorders and certainly worsen their effects. It may
be that many people with a propensity for developing one of these diseases
would never develop a full blown disorder had it not been for their
exposure to high levels of food borne excitotoxin additives. Some may
have had a very mild form of the disease had it not been for the exposure.
In July, 1995 the Federation of American Societies for Experimental
Biology (FASEB) conducted a definitive study for the FDA on the question
of safety of MSG. The FDA wrote a very deceptive summary of the report
in which they implied that, except possibly for asthma patients, MSG
was found to be safe by the FASEB reviewers. But, in fact, that is not
what the report said at all. I summarized, in detail, my criticism of
this widely reported FDA deception in the revised paperback edition
of my book, Excitotoxins: The Taste That Kills, by analyzing exactly
what the report said, and failed to say. For example, it never said
that MSG did not aggravate neurodegenerative diseases. What they said
was, there were no studies indicating such a link. Specifically, that
no one has conducted any studies, positive or negative, to see if there
is a link. In other words it has not been looked at. A vital difference.
Unfortunately, for the consumer, the corporate food processors not
only continue to add MSG to our foods but they have gone to great links
to disguise these harmful additives. For example, they use such names
as hydrolyzed vegetable protein, vegetable protein, hydrolyzed plant
protein, caseinate, yeast extract, and natural flavoring. We know experimentally,
as stated, when these excitotoxin taste enhancers are added together
they become much more toxic. In fact, excitotoxins in subtoxic concentrations
can be fully toxic to specialized brain cells when used in combination.
Frequently, I see processed foods on supermarket shelves, especially
frozen or diet food, that contain two, three or even four types of excitotoxins.
We also know that excitotoxins in a liquid form are much more toxic
than solid forms because they are rapidly absorbed and attain high concentration
in the blood. This means that many of the commercial soups, sauces,
and gravies containing MSG are very dangerous to nervous system health,
and should especially be avoided by those either having one of the above
mentioned disorders, or are at a high risk of developing one of them.
They should also be avoided by cancer patients and those at high risk
for cancer.
In the case of ALS, amyotrophic lateral sclerosis, we know that consumption
of red meats and especially MSG itself, can significantly elevate blood
glutamate, much higher than is seen in the normal population. Similar
studies, as far as I am aware, have not been conducted in patients with
Alzheimer’s disease or Parkinson’s disease. But, as a general rule I
would certainly suggest that person’s with either of these diseases
avoid MSG containing foods as well as red meats, cheeses, and pureed
tomatoes, all of which are known to have high levels of glutamate.
It must be remembered that it is the glutamate molecule that is toxic
in MSG (monosodium glutamate). Glutamate is a naturally occurring amino
acid found in varying concentrations in many foods. Defenders of MSG
safety allude to this fact in their defense. But, it is free glutamate
that is the culprit. Bound glutamate, found naturally in foods, is less
dangerous because it is slowly broken down and absorbed by the gut,
so that it can be utilized by the tissues, especially muscle, before
toxic concentrations can build up. Therefore, a whole tomato is safer
than a pureed tomato. The only exception to this, based on present knowledge,
is in the case of ALS. Also, in the case of tomatoes, the plant contains
several powerful antioxidants known to block glutamate toxicity.
Hydrolyzed vegetable protein should not be confused with hydrolyzed
vegetable oil. The oil does not contain an appreciable concentration of
glutamate, it is an oil. Hydrolyzed vegetable protein is made by a chemical
process that breaks down the vegetable’s protein structure to purposefully
free the glutamate, as well as aspartate, another excitotoxin. This
brown powdery substance is used to enhance the flavor of foods, especially
meat dishes, soups, and sauces. Despite the fact that some health food
manufacturers have attempted to sell the idea that this flavor enhancer
is " all natural" and "safe" because it is made
from vegetables, it is not. It is the same substance added to processed
foods. Experimentally, one can produce the same brain lesions using
hydrolyzed vegetable protein as by using MSG or aspartate.
A growing list of excitotoxins is being discovered, including several
that are found naturally. For example, L-cysteine is a very powerful
excitotoxin. Recently, it has been added to certain bread dough and
is sold in health food stores as a supplement. Homocysteine, a metabolic
derivative, is also an excitotoxin. Interestingly, elevated blood levels
of homocysteine has recently been shown to be a major, if not the major,
indicator of cardiovascular disease and stroke. Equally interesting,
is the finding that elevated levels have also been implicated in neurodevelopmental
disorders, especially anencephaly and spinal dysraphism (neural tube
defects). It is thought that this is the protective mechanism of action
of the prenatal vitamins B12, B6, and folate when used in combination.
It remains to be seen if the toxic effect is excitatory or by some other
mechanism. If it is excitatory, then unborn infants would be endangered
as well by glutamate, aspartate (part of the aspartame molecule), and
the other excitotoxins. Recently, several studies have been done in
which it was found that all Alzheimer’s patients examined had elevated
levels of homocysteine.
Recent studies have shown that persons affected by Alzheimer’s disease
also have widespread destruction of their retinal ganglion cells. Interestingly,
this is the area found to be affected when Lucas and Newhouse first
discovered the excitotoxicity of MSG. While this does not prove that
dietary glutamate and other excitotoxins cause or aggravate Alzheimer’s
disease, it makes one very suspicious. One could argue a common intrinsic
etiology for central nervous system neuronal damage and retinal ganglion
cell damage, but these findings are disconcerting enough to warrant
further investigations.
The Free Radical Connection
It is interesting to note that many of the same neurological diseases
associated with excitotoxic injury are also associated with accumulations
of toxic free radicals and destructive lipid enzymes. For example, the
brains of Alzheimer’s disease patients have been found to contain high
concentration of lipolytic enzymes, which seems to indicate accelerated
membrane lipid peroxidation, again caused by free radical generation.
In the case of Parkinson’s disease, we know that one of the early changes
is the loss of glutathione from the neurons of the striate system, especially
in a nucleus called the substantia nigra. It is this nucleus that is
primarily affected in this disorder. Accompanying this, is an accumulation
of free iron, which is one of the most powerful free radical generators
known. One of the highest concentrations of iron in the body is within
the globus pallidus and the substantia nigra. The neurons within the
latter are especially vulnerable to oxidant stress because the oxidant
metabolism of the transmitter-dopamine- can proceed to the creation
of very powerful free radicals. That is, it can auto- oxidize to peroxide,which
is normally detoxified by glutathione. As we have seen, glutathione
loss in the substantia nigra is one of the earliest deficiencies seen
in Parkinson’s disease. In the presence of high concentrations of free
iron, the peroxide is converted into the dangerous, and very powerful
free radical, hydroxide. As the hydroxide radical diffuses throughout
the cell, destruction of the lipid components of the cell takes place,
a process called lipid peroxidation.
Using a laser microprobe mass analyzer, researchers have recently discovered
that iron accumulation in Parkinson’s disease is primarily localized
in the neuromelanin granules (which gives the nucleus its black color).
It has also been shown that there is dramatic accumulation of aluminum
within these granules. Most likely, the aluminum displaces the bound
iron, releasing highly reactive free iron. It is known that even low
concentrations of aluminum salts can enhance iron-induced lipid peroxidation
by almost an order of magnitude. Further, direct infusion of iron into
the substantia nigra nucleus in rodents can induce a Parkinsonian syndrome,
and a dose related decline in dopamine. Recent studies indicate that
individuals having Parkinson’s disease also have defective iron metabolism.
Another early finding in Parkinson’s disease is the reduction in complex
I enzymes within the mitochondria of this nucleus. It is well known
that the complex I enzymes are particularly sensitive to free radical
injury. These enzymes are critical to the production of cellular energy.
When cellular energy is decreased, the toxic effect of excitatory amino
acids increases dramatically, by as much as 200 fold. In fact, when
energy production is very low, even normal concentrations of extracellular
glutamate and aspartate can kill neurons.
One of the terribly debilitating effects of Parkinson’s disease is
a condition called " freezing up", a state where the muscle
are literally frozen in place. There is recent evidence that this effect
is due to the unopposed firing of a special nucleus in the brain (the
subthalamic nucleus). Interestingly, this nucleus uses glutamate for
its transmitter. Neuroscientist are exploring the use of glutamate blocking
drugs to prevent this disorder.
And finally, there is growing evidence that similar free radical damage,
most likely triggered by toxic concentrations of excitotoxins, causes
ALS. Several studies have demonstrated lipid peroxidation product accumulation
within the spinal cords of ALS victims. Iron accumulation has also been
seen in the spinal cords of ALS victims.
Besides the well known reactive oxygen species, such as super oxide,
hydroxyl ion, hydrogen peroxide, and singlet oxygen, there exist a whole
spectrum of reactive nitrogen species derived from nitric oxide, the
most important of which is peroxynitrate. These free radicals can attack
proteins, membrane lipids and DNA, both nuclear and mitochondrial, which
makes these radicals very dangerous.
It is now known that glutamate acts on its receptor via a nitric oxide
mechanism.Overstimulation of the glutamate receptor can result in accumulation
of reactive nitrogen species, resulting in the concentration of several
species of dangerous free radicals. There is growing evidence that,
at least in part, this is how excess glutamate damages nerve cells.
In a multitude of studies, a close link has been demonstrated between
excitotoxity and free radical generation. Others have shown that certain
free radical scavengers (anti-oxidants), have successfully blocked excitotoxic
destruction of neurons. For example, vitamin E is known to completely
block glutamate toxicity in vitro (in culture). Whether it will be as
efficient in vivo (in a living animal) is not known. But, it is interesting
in light of the recent observations that vitamin E slows the course
of Alzheimer’s disease, as had already been demonstrated in the case
of Parkinson’s disease. There is some clinical evidence, including my
own observations, that vitamin E also slows the course of ALS as well,
especially in the form of D- Alpha-tocopherol. I would caution that
anti-oxidants work best in combination and when use separately can have
opposite, harmful, effects. That is, when antioxidants, such as ascorbic
acid and alpha tocopherol, become oxidized themselves, such as in the
case of dehydroascorbic acid, they no longer protect, but rather act
as free radicals themselves. The same is true of alpha-tocopherol.
We know that there are four main endogenous sources of oxidants:
- Those produced naturally from aerobic metabolism of glucose.
- Those produced during phagocytic cell attack on bacteria, viruses,
and parasites, especially with chronic infections.
- Those produced during the degradation of fatty acids and other molecules
that produce H2O2 as a by-product. (This is important in stress, which
has been shown to significantly increase brain levels of free radicals.)
- Oxidants produced during the course of p450 degradation of natural
toxins.
And, as we have seen, one of the major endogenous sources of free radicals
is from exposure to free iron. Unfortunately, iron is one mineral heavily
promoted by the health industry, and is frequently added to many foods,
especially breads and pastas. Copper is also a powerful free radical
generator and has been shown to be elevated within the substantia nigra
nucleus of Parkinsonian brains.
When free radicals are generated, the first site of damage is to the
cell membranes, since they are composed of polyunsaturated fatty acid
molecules known to be highly susceptible to such attack. The process
of membrane lipid oxidation is known as lipid peroxidation and is usually
initiated by the hydroxal radical. We know that one’s diet can significantly
alter this susceptibility. For example, diets high in omega 3-polyunsaturated
fatty acids (fish oils and flax seed oils) can increase the risk of
lipid peroxidation experimentally. Contrariwise, diets high in olive
oil, a monounsaturtated oil, significantly lowers lipid peroxidation
risk. From the available research. The beneficial effects of omega 3-fatty
acid oils in the case of strokes and heart attacks probably arises from
the anticoagulant effect of these oils and possibly the inhibition of
release of arachidonic acid from the cell membrane. But, olive oil has
the same antithrombosis effect and anticancer effect but also significantly
lowers lipid peroxidation.
The Blood-Brain Barrier
One of the MSG industry’s chief arguments for the safety of their product
is that glutamate in the blood cannot enter the brain because of the
blood-brain barrier (BBB), a system of specialized capillary structures
designed to exclude toxic substance from entering the brain. There are
several criticisms of their defense. For example, it is known that the
brain, even in the adult, has several areas that normally do not have
a barrier system, called the circumventricular organs. These include
the hypothalamus, the subfornical organ, organium vasculosum, area postrema,
pineal gland, and the subcommisural organ. Of these, the most important
is the hypothalamus, since it is the controlling center for all neuroendocrine
regulation, sleep wake cycles, emotional control, caloric intake regulation,
immune system regulation and regulation of the autonomic nervous system.
Interestingly, it has recently been found that glutamate is the most
important neurotransmitter in the hypothalamus. Therefore, careful regulation
of blood levels of glutamate is very important, since high blood concentrations
of glutamate can easily increase hypothalamic levels as well. One of
the earliest and most consistent findings with exposure to MSG is damage
to an area known as the arcuate nucleus. This small hypothalamic nucleus
controls a multitude of neuroendocrine functions, as well as being intimately
connected to several other hypothalamic nuclei. It has also been demonstrated
that high concentrations of blood glutamate and aspartate (from foods)
can enter the so-called "protected brain" by seeping through
the unprotected areas, such as the hypothalamus or circumventricular
organs.
Another interesting observation is that chronic elevations of blood
glutamate can even seep through the normal blood-brain barrier when
these high concentrations are maintained over a long period of time.
This, naturally, would be the situation seen when individuals consume,
on a daily basis, foods high in the excitotoxins - MSG, aspartame and
cysteine. Most experiments cited by the defenders of MSG safety were
conducted to test the efficiency of the BBB acutely. In nature, except
in the case of metabolic dysfunction (Such as with ALS), glutamate and
aspartate levels are not normally elevated on a daily basis. Sustained
elevations of these excitotoxins are peculiar to the modern diet. (And
in the ancient diets of the Orientals, but not in as high a concentration.)
An additional critical factor ignored by the defenders of excitotoxin
food safety is the fact that many people in a large population have
disorders known to alter the permeability of the blood-brain barrier.
The list of condition associated with barrier disruption include: hypertension,
diabetes, ministrokes, major strokes, head trauma, multiple sclerosis,
brain tumors, chemotherapy, radiation treatments to the nervous system,
collagen-vascular diseases (lupus), AIDS, brain infections, certain
drugs, Alzheimer’s disease, and as a consequence of natural aging. There
may be many other conditions also associated with barrier disruption
that are as yet not known.
When the barrier is dysfunctional due to one of these conditions, brain
levels of glutamate and aspartate reflect blood levels. That is, foods
containing high concentrations of these excitotoxins will increase brain
concentrations to toxic levels as well. Take for example, multiple sclerosis.
We know that when a person with MS has an exacerbation of symptoms,
the blood-brain barrier near the lesions breaks down, leaving the surrounding
brain vulnerable to excitotoxin entry from the blood, i.e. the diet.
But, not only is the adjacent brain vulnerable, but the openings act
as a points of entry, eventually exposing the entire brain to potentially
toxic levels of glutamate. Several clinicians have remarked on seeing
MS patients who were made worse following exposure to dietary excitotoxins.
I have seen this myself.
It is logical to assume that patients with the other neurodegenerative
disorders, such as Alzheimer’s disease, Parkinson’s disease, and ALS
will be made worse on diets high in excitotoxins. Barrier disruption
has been demonstrated in the case of Alzheimer’s disease.
Recently, it has been shown that not only can free radicals open the
blood-brain barrier, but excitotoxins can as well. In fact, glutamate
receptors have been demonstrated on the barrier itself. In a carefully
designed experiment, researchers produced opening of the blood-brain
barrier using injected iron as a free radical generator. When a powerful
free radical scavenger (U-74006F) was used in this model, opening of
the barrier was significantly blocked. But, the glutamate blocker MK-801
acted even more effectively to protect the barrier. The authors of this
study concluded that glutamate appears to be an important regulator
of brain capillary transport and stability, and that overstimulation
of NMDA (glutamate) receptors on the blood-brain barrier appears to
play an important role in breakdown of the barrier system. What this
also means is that high levels of dietary glutamate or aspartate may
very well disrupt the normal blood-brain barrier, thus allowing more
glutamate to enter the brain, sort of a vicious cycle.
Relation to Cellular Energy Production
Excitotoxin damage is heavily dependent on the energy state of the
cell. Cells with a normal energy generation systems that are efficiently
producing adequate amounts of cellular energy, are very resistant to
such toxicity. When cells are energy deficient, no matter the cause
- hypoxia, starvation, metabolic poisons, hypoglycemia - they become
infinitely more susceptible to excitotoxic injury or death. In fact,
even normal concentrations of glutamate are toxic to energy deficient
cells.
It is known that in many of the neurodegenerative disorders, neuron
energy deficiency often precedes the clinical onset of the disease by
years, if not decades. This has been demonstrated in the case of Huntington
disease and Alzheimer’s disease using the PET scanner, which measures
brain metabolism. In the case of Parkinson’s disease, several groups
have demonstrated that one of the early deficits of the disorder is
an impaired energy production by the complex I group of enzymes from
the mitochondria of the substantia nigra. (Part of the Electron Transport
System.) Interestingly, it is known that the complex I system is very
sensitive to free radical damage.
Recently, it has been shown that when striatal neurons (Those involved
in Parkinson’s and Huntington’s diseases.) are exposed to microinjected
excitotoxins there is a dramatic, and rapid fall in energy production
by these neurons. CoEnzyme Q10 has been shown, in this model, to restore
energy production but not to prevent cellular death. But when combined
with niacinamide, both cellular energy production and neuron protection
is seen. I would recommend for those with neurodegenerative disorders,
a combination of CoQ10, acetyl-L carnitine, niacinamide, riboflavin,
methylcobalamin, and thiamine.
One of the newer revelation of modern molecular biology, is the discovery
of mitochondrial diseases, of which cellular energy deficiency is a
hallmark. In many of these disorders, significant clinical improvement
has been seen following a similar regimen of vitamins combined with
CoQ10 and L-carnitine. Acetyl L-carnitine enters the brain in higher
concentrations and also increases brain acetylcholine, necessary for
normal memory function. While these particular substances have been
found to significantly boost brain energy function they are not alone
in this important property. Phosphotidyl serine, Ginkgo Biloba, vitamin
B12, folate, magnesium, Vitamin K and several others are also being
shown to be important.
While mitochrondial dysfunction is important in explaining why some
are more vulnerable to excitotoxin damage than others, it does not explain
injury in those with normal cellular metabolism. There are several conditions
under which energy metabolism is impaired. For example, approximately
one third of Americans suffer from what is known as reactive hypoglycemia.
That is, they respond to a meal composed of either simple sugars or
carbohydrates that are quickly broken down into simple sugars (a high
glycemic index.) by secreting excessive amounts of insulin. This causes
a dramatic lowering of the blood sugar.
When the blood sugar falls, the body responds by releasing a burst
of epinephrine from the adrenal glands, in an effort to raise the blood
sugar. We feel this release as nervousness, palpitations of our heart,
tremulousness, and profuse sweating. Occasionally, one can have a slower
fall in the blood sugar that will not produce a reactive release of
epinephrine, thereby producing few symptoms. This can be more dangerous,
since we are unaware that our glucose reserve is falling until we develop
obvious neurological symptoms, such as difficulty thinking and a sensation
of lightheadedness.
The brain is one of the most glucose dependent organs known, since
it has a limited ability to burn other substrates such as fats. There
is some evidence that several of the neurodegenerative diseases are
related to either excessive insulin release, as with Alzheimer’s disease,
or impaired glucose utilization, as we have seen in the case of Parkinson’s
disease and Huntington’s disease.
It is my firm belief, based on clinical experience and physiological
principles, that many of these diseases occur primarily in the face
of either reactive hypoglycemia or "brain hypoglycemia". In
at least two well conducted studies it was found that pure Alzheimer’s
dementia was rare in those with normal blood sugar profiles, and that
in most cases Alzheimer’s patients had low blood sugars, and high CSF
(cerebrospinal fluid) insulin levels. In my own limited experience with
Parkinson’s and ALS patients I have found a disproportionately high
number suffering from reactive hypoglycemia.
I found it interesting that several ALS patients have observed an association
between their symptoms and gluten. That is, when they adhere to a gluten
free diet they improve clinically. It may be that by avoiding gluten
containing products, such as bread, crackers, cereal, pasta, etc., they
are also avoiding products that are high on the glycemic index, i.e.
that produce reactive hypoglycemia. Also, all of these food items are
high in free iron. Clinically, hypoglycemia will worsen the symptoms
of most neurological disorders. We know that severe hypoglycemia can,
in fact, mimic ALS both clinically and pathologically. It is also known
that many of the symptoms of Alzheimer’s disease resemble hypoglycemia,
as if the brain is hypoglycemic in isolation.
In studies of animals exposed to repeated mild episodes of hypoxia
(lack of brain oxygenation), it was found that such accumulated injuries
can trigger biochemical changes that resemble those seen in Alzheimer’s
patients. One of the effects of hypoxia is a massive release of glutamate
into the space around the neuron. This results in rapid death of these
sensitized cells. As we age, the blood supply to the brain is frequently
impaired, either because of atherosclerosis or repeated syncopal episodes,
leading to short periods of hypoxia. Hypoglycemia produces lesions very
similar to hypoxia and via the same glutamate excitotoxic mechanism.
In fact, recent studies of diabetics suffering from repeated episodes
of hypoglycemia associated with over medication with insulin, demonstrate
brain atrophy and dementia.
Again, it should be realized that excessive glutamate stimulation triggers
a chain of events that in turn triggers the generation of large numbers
of free radical species, both as nitrogen species and oxygen species.
Once this occurs, especially with the accumulation of the hydroxyl ion,
destruction of the lipid components of the membranes occurs, as lipid
peroxidation. In addition, these free radicals damage proteins and DNA
as well. The most immediate DNA damage is to the mitochondrial DNA,
which controls protein expression within that particular cell and its
progeny. It is suspected that at least some of the neurodegenerative
diseases, Parkinson’s disease in particular, are inherited in this way.
But more importantly, it may be that accumulated damage to the mitochondrial
DNA secondary to progressive free radical attack (somatic mitochondrial
injury) is the cause of most of the neurodegenerative diseases that
are not inherited. This would result from an impaired reserve of antioxidant
vitamins/minerals and enzymes, increased cellular stress, chronic infection,
free radical generating metals and toxins, and impaired DNA repair enzymes.
It is estimated that the number of oxidative free radical injuries
to DNA number about 10,000 a day in humans. Normally, these injuries
are repaired by special repair enzymes. It is known that as we age these
repair enzymes decrease or become less efficient. Also, some individuals
are born with deficient repair enzymes from birth as, for example, in
the case of xeroderma pigmentosum. Recent studies of Alzheimer’s patients
also demonstrate a significant deficiency in DNA repair enzymes and
high levels of lipid peroxidation products in the affected parts of
the brain. It is also important to realize that the hippocampus of the
brain, most severely damaged in Alzheimer’s dementia, is one of the
most vulnerable areas of the brain to low glucose supply as well as
low oxygen supply. That also makes it very susceptible to glutamate
toxicity.
Another interesting finding is that when cells are exposed to glutamate
they develop certain inclusions (cellular debris) that not only resembles
the characteristic neurofibrillary tangles of Alzheimer’s dementia,
but are immunologically identical as well. Similarly, when experimental
animals are exposed to the chemical MPTP, they not only develop Parkinson’s
disorder, but the older animals develop the same inclusions (Lewy bodies)
as see in human Parkinson’s.
Eicosanoids and Excitotoxins
It is known that one of the destructive effects triggered by excitotoxins
is the release of arachidonic acid from the cell membrane and the initiation
of the eicosanoid reactions. Remember, glutamate primarily acts by opening
the calcium pore, allowing calcium to pour into the cell’s interior.
Intracellular calcium in high concentrations initiates the enzymatic
release of arachidonic acid from the cell membrane, where it is then
attacked by two enzymes systems, the cyclooxygenase system and the lipooxgenase
system. These in turn produce a series of compounds that can damage
cell membranes, proteins and DNA, primarily by free radical production,
but also directly by the "harmful eicosanoids."
Biochemically, we know that high glycemic carbohydrate diets, known
to stimulate the excess release of insulin, can trigger the production
of "harmful eicosanoids." We should also recognize that simple
sugars are not the only substances that can trigger the release of insulin.
One of the more powerful triggers includes certain amino acids, including
leucine, alanine, and taurine. Glutamine, while not acting as an insulin
trigger itself, markedly potentiates insulin release by leucine. This
is why, except under certain situations, individual "free"
amino acids should be avoided.
It is known that excitotoxins can also stimulate the release of these
"harmful eicosanoids." So that in the situation of a hypoglycemic
individual, they would be subjected to production of harmful eicosanoids
directly by the high insulin levels, as well as by elevated glutamate
levels. Importantly, both of these events significantly increase free
radical production and hence, lipid peroxidation of cellular membranes.
It should be remembered that diets high in arachidonic acid, such as
egg yellows, organs meats, and liver, may be harmful to those subjected
to excessive excitotoxin exposure.
And finally, in one carefully conducted experiment, it was shown that
insulin significantly increases glutamate toxicity in cortical cell
cultures and that this magnifying effect was not due to insulin’s effect
on glucose metabolism. That is, the effect was directly related to insulin
interaction with cell membranes. Interestingly, insulin increased toxic
sensitivity to other excitotoxins as well.
The Special Role of Flavonoids
Flavonoids are diphenylpropanoids found in all plant foods. They are
known to be strong antioxidants and free radical scavengers. There are
three major flavonols - quercetin, Kaempferol, and myricetin, and two
major flavones - luteolin and apigenin. Seventy percent of the flavonoid
intake in the average diet consist of quercetin, the main source of
which is tea (49%), onions (29%), and apples (7%). Fortunately, flavonoids
are heat stable, that is, they are not destroyed during cooking. Other
important flavonoids include catechin, leucoanthocyanidins, anthocyanins,
hesperedin and naringenin.
Most interest in the flavonoids stemmed from their ability to inhibit
tumor initiation and growth. This was especially true of quercetin and
naringenin, but also seen with hesperetin and the isoflavone, genistein.
There appears to be a strong correlation between their anticarcinogenic
potential and their ability to squelch free radicals. But, in the case
of genistein and quercetin, it also has to do with their ability to
inhibit tyrosine kinase and phosphoinositide phosphorylase, both necessary
for mammary cancer and glioblastoma (a highly malignant brain tumor)
growth and development.
As we have seen, there is a close correlation between insulin, excitotoxins,
free radicals and eicosanoid production. Of particular interest, is
the finding that most of the flavonoids, especially quercetin, are potent
and selective inhibitors of delta-5-lipooxygenase enzyme which initiates
the production of eicosanods. Flavones are also potent and selective
inhibitors of the enzyme cyclooxygenase (COX) which is responsible for
the production of thromboxane A2, one of the "harmful eicosanoids".
The COX-2 enzymes is associated only with excitatory type neurons in
the brain and appears to play a major role in neurodegeneration.
One of the critical steps in the production of eicosanoids is the liberation
of arachidonic acid from the cell membrane by phospholipase A2. Flavonones
such as naringenin (from grapefruits) and hesperetin (citrus fruits)
produce a dose related inhibition of phospholipase A2 (80% inhibition),
thereby inhibiting the release of arachidonic acid. The non-steroidal
anti-inflammatory drugs act similarly to block the production of inflammatory
eicosanoids.
What makes all of this especially interesting is that recently, two
major studies have found that not only can non-steroidal anti- inflammatories
slow the course of Alzheimer’s disease, but they may prevent it as well.
But, these drugs can have significant side effects, such as GI bleeding,
liver and kidney damage. In high doses, the flavonoids have shown a
similar ability to reduce "harmful eicosanoid" production
and should have the same beneficial effect on the neurodegenerative
diseases without the side effects. Also, these compounds are powerful
free radical scavengers and would be expected to reduce excitotoxicity
as well.
But, there is another beneficial effect. There is experimental, as
well as clinical evidence, that the flavonoids can reduce capillary
leakage and strengthen the blood brain barrier. This has been shown
to be true for rutin, hesperedin and some chalcones. Rutin and hesperedin
have also been shown to strengthen capillary walls. In the form of hesperetin
methyl chalcone, the hesperedin molecule is readily soluble in water,
significantly increasing its absorbability. Black currents have the
highest concentration of hesperetin of any fresh fruit, and in a puree
form, is even more potent.
The importance of these compounds again emphasizes the need for high
intakes of fruits and vegetables in the diet, and may explain the low
incidence of many of these disorders in strict vegetarians, since this
would supply a high concentration of flavonoids, carotenoids, vitamins,
minerals, and other antioxidants to the body. Normally, the flavonoids
from fruits and vegetables are only incompletely absorbed, so that relatively
high concentrations would be needed to attain the same therapeutic levels
seen in these experiments. Juice Plus allows us to absorb high, therapeutic
concentrations of these flavonoids by a process called cryodehydration.
This process removes the water and sugar from fruits and vegetable but
retains their flavonoids in a fully functional state. Also the process
allows one to consume large amounts of fruits and vegetables that would
be impossible with the whole plant.
Iron and Health
For decades we, especially women, have been told that we need extra
iron for health -that it builds healthy blood. But, recent evidence
indicates that iron and copper may be doing more harm than good in most
cases. It has been well demonstrated that iron and copper are two of
the most powerful generators of free radicals. This is because they
catalyze the conversion of hydrogen peroxide into the very powerful
and destructive hydroxyl radical. It is this radical that does so much
damage to membrane lipids and DNA bases within the cell. It also plays
a major role in the oxidation of LDL-cholesterol, leading to heart attacks
and strokes.
Males begin to accumulate iron shortly after puberty and by middle
age have 1000mg of stored iron in their bodies. Women, by contrast,
because of menstruation, have only 300 mg of stored iron. But, after
menopause they begin to rapidly accumulate iron so that by middle age
they have about 1500 mg of stored iron. It is also known that the brain
begins to accumulate iron with aging. Elevated iron levels are seen
with all of the neurodegenerative diseases, such as Alzheimer’s dementia,
Parkinson’s disease, and ALS. It is thought that this iron triggers
free radical production within the areas of the brain destroyed by these
diseases. For example, the part of the brain destroyed by Parkinson’s
disease, the substantia nigra, has very high levels of free iron.
Normally, the body goes to great trouble to make sure all iron and
copper in the body is combined to a special protein for transport and
storage. But, with several of these diseases, we see a loss of these
transport and storage proteins. This is where flavonoids come into play.
We know that many of the flavonoids (especially quercitin, rutin, hesperidin,
and naringenin) are strong chelators of iron and copper. In fact, drinking
iced tea with a meal can reduce iron absorption by as much as 87%. But,
flavonoids in the diet will not make you iron deficient.
Phosphotidyl serine and Excitotoxity
Recent clinical studies indicate that phophotidyl serine can significantly
improve the mental functioning of a significant number of Alzheimer’s
patients, especially during the early stages of the disease. We know
that the brain normally contains a large concentration of phosphotidyl
serine. Interestingly, this compound has a chemical structure similar
to L-glutamate, the main excitatory neurotransmitter in the brain. Binding
studies show that phosphotidyl serine competes with L-glutamate for
the NMDA type glutamate receptor. What this means is that phosphotidyl
serine is a very effective protectant against glutamate toxicity. Unfortunately,
it is also very expensive.
The Many Functions of Ascorbic Acid
The brain contains one of the highest concentrations of ascorbic acid
in the body. Most are aware of its function in connective tissue synthesis
and as a free radical scavenger. But, ascorbic acid has other functions
that make it rather unique. Ascorbic acid in solution is a powerful
reducing agent where it undergoes rapid oxidation to form dehydroascorbic
acid. Oxidation of this compound is accelerated by high ph, temperature
and some transitional metals, such as iron and copper. The oxidized
form of ascorbic acid can promote lipid peroxidation and protein damage.
This is why it is vital that you take antioxidants together, since several,
such as vitamin E (as D- alpha-tocopherol) and alpha-lipoic acid, act
to regenerate the reduced form of the vitamin.
In man, we know that certain areas of the brain have very high concentrations
of ascorbic acid, such as the nucleus accumbens and hippocampus. The
lowest levels are seen in the substantia nigra. These levels seem to
fluctuate with the electrical activity of the brain. Amphetamine acts
to increase ascorbic acid concentration in the corpus striatum (basal
ganglion area) and decrease it in the hippocampus, the memory imprint
area of the brain. Ascorbic acid is known to play a vital role in dopamine
production as well.
One of the more interesting links has been between the secretion of
the glutamate neurotransmitter by the brain and the release of ascorbic
acid into the extracellular space. This release of ascorbate can also
be induced by systemic administration of glutamate or aspartate, as
would be seen in diets high in these excitotoxins. The other neurotransmitters
do not have a similar effect on ascorbic acid release. This effect appears
to be an exchange mechanism. That is, the ascorbic acid and glutamate
exchange places. Theoretically, high concentration of ascorbic acid
in the diet could inhibit glutamate release, lessening the risk of excitotoxic
damage. Of equal importance is the free radical neutralizing effect
of ascorbic acid.
There is now substantial evidence that ascorbic acid modulates the
electrophysiological as well as behavioral functioning of the brain.
It also attenuates the behavioral response of rats exposed to amphetamine,
which is known to act through an excitatory mechanism. In part, this
is due to the observed binding of ascorbic acid to the glutamate receptor.
This could mean that ascorbic acid holds great potential in treating
disease related to excitotoxic damage. Thus far, there are no studies
relating ascorbate metabolism in neurodegenerative diseases. There is
at least one report of ascorbic acid deficiency in guineas pigs producing
histopathological changes similar to ALS.
It is known that as we age there is a decline in brain levels of ascorbic
acid. When accompanied by a similar decrease in glutathione peroxidase,
we see an accumulation of H202 and hence, elevated levels of free radicals
and lipid peroxidation. In one study it was found that with age not
only does the extracellular concentration of ascorbic acid decrease
but the capacity of the brain ascorbic acid system to respond to oxidative
stress is impaired as well.
In terms of its antioxidant activity, vitamin C and E interact in such
a way as to restore each others active antioxidant state. Vitamin C
scavenges oxygen radicals in the aqueous phase and vitamin E in the
lipid, chain breaking, phase. The addition of vitamin C suppresses the
oxidative consumption of vitamin E almost totally, probably because
in the living organism the vitamin C in the aqueous phase is adjacent
to the lipid membrane layer containing the vitamin E.
When combined, the vitamin C was consumed faster during oxidative stress
than the vitamin E. Once the vitamin C was totally consumed, the vitamin
E began to be depleted at an accelerated rate. N-acetyl-L- cysteine
and glutathione can reduce vitamin E consumption as well, but less effectively
than vitamin C. The real danger is when vitamin C is combined with iron.
Recent experiments have shown that such combinations can produce widespread
destruction within the striate areas of the brain. This is because the
free iron oxidizes the ascorbate to produce the powerful free radical
hydroxyascorbate. Alpha-lipoic acid acts powerfully to keep the ascorbate
and tocopherol in the reduced state (antioxidant state). As we age,
we produce less of the transferrin transport protein that normally binds
free iron. As a result, older individuals have higher levels of free
iron within their tissues, including brain.
Conclusion
In this discussion, I tried to highlight some of the more pertinent
of the recent findings related to excitotoxicity in general and neurodegenerative
diseases specifically. In no way is this an all inclusive discussion
of this topic. There are many areas I had to omit because of space,
such as alpha-lipoic acid, an antioxidant that holds great promise in
combatting many of these diseases. Also, I did not go into detail concerning
the metabolic stimulants, the relationship between exercise and degenerative
nervous system diseases, the protective effect of methycobalamin, and
the various disorders related to excitotoxins.
I also purposely omitted discussions of magnesium to keep this paper
short. It is my experience, that magnesium is one of the most important
neuroprotectants known. I would encourage those who suffer from one
of the excitotoxin related disorders to avoid, as much as possible,
food borne excitotoxin additives and to utilize the substances discussed
above. The fields of excitotoxin research, in combination with research
on free radicals and eicosanoids, are growing very rapidly and new information
arises daily. Great promise exist in the field of flavonoid research
as regards many of these neurodegenerative diseases as well as in our
efforts to prevent neurodegeneration itself.
A recent study has demonstrated that aspartame feeding to animals results
in an accumulation of formaldehyde within the cells, with evidence of
significant damage to cellular proteins and DNA. In fact, the formaldehyde
accumulated with prolonged use of aspartame. With this damning evidence,
one would have to be suicidal to continue the use of aspartame sweetened
foods, drinks and medicines. The use of foods containing excitotoxin
additives is especially harmful to the unborn and small children. By
age 4 the brain is only 80% formed. By age 8, 90% and by age 16 it is
fully formed, but still undergoing changes and rewiring (plasticity).
We know that the excitotoxins have a devastating effect on formation
of the brain (wiring of the brain) and that such exposure can cause
the brain to be "miswired." This may explain the significant,
almost explosive increase in ADD and ADHD. Glutamate feeding to pregnant
animals produces a syndrome almost identical to ADD. It has also been
shown that a single feeding of MSG after birth can increase free radicals
in the offspring’s brain that last until adolescence. Experimentally,
we known that infants are 4X more sensitive to the toxicity of excitotoxins
than are adults. And, of all the species studied, cats, dogs, primates,
chickens, guinea pigs, and rats, humans are by far the most sensitive
to glutamate toxicity. In fact, they are 5x more sensitive than rats
and 20x more sensitive than non-human primates.
I have been impressed with the dramatic improvement in children with
ADD and ADHD following abstention from excitotoxin use. It requires
care monitoring of these children. Each time they are exposed to these
substances, they literally go bonkers. It is ludicrous, with all we
know about the destructive effects of excitotoxins, to allow our children
and ourselves to continue on this destructive path.
 Dr.
Blaylock is a board certified neurosurgeon engaged in a private neurosurgical
practice for the past 21 years. During this time he has had a strong
interest in nutritional treatment of neurological disorders and in the
biochemical basis of diseases of the nervous system. ADD and ADHD have
been a part of his interest because of the relationship to the excitotoxic
process. In 1994 he wrote a book on this subject, Excitotoxins, The
Taste That Kills, and revised and updated it in 1998. He has written
and illustrated three chapters in medical textbooks and a patient care
booklet on multiple sclerosis. In addition he has published several
papers in peer reviewed journals on a variety of subjects from the pathology
and treatment of pituitary tumors to immunothearpy of brain tumors.
He has appeared on the 700 Club approximately 7 times, Life Style Magazine
once, and 30 plus syndicated radio programs discussing the book. While
he does not treat ADD in his practice, he has given advice to a number
of mothers and have found that a significant number improve and some
quite dramatically.
Excitotoxins, The Taste That Kills by Russell L Blaylock, M.D.
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