| Unified Theory of
Human Cardiovascular Disease Leading the Way to the Abolition
of This Disease as a Cause for Human Mortality (1992)
Rath M, Pauling L. Journal of Orthomolecular Medicine,
7: 5-15.
Summary
Until now therapeutic concepts for human cardiovascular disease
(CVD) were targeting individual pathomechanisms or specific risk
factors. On the basis of genetic, metabolic, evolutionary, and
clinical evidence we present here a unified pathogenetic and therapeutic
approach. Ascorbate deficiency is the precondition and common
denominator of human CVD. Ascorbate deficiency is the result of
the inability of man to synthesize ascorbate endogenously in combination
with insufficient dietary intake.
The invariable morphological consequences of chronic
ascorbate deficiency in the vascular wall are the loosening of
the connective tissue and the loss of the endothelial barrier
function. Thus human CVD is a form of pre-scurvy. The multitude
of pathomechanisms that lead to the clinical manifestation of
CVD are primarily defense mechanisms aiming at the stabilization
of the vascular wall.
After the loss of endogenous ascorbate production
during the evolution of man these defense mechanisms became life-saving.
They counteracted the fatal consequences of scurvy and particularly
of blood loss through the scorbutic vascular wall. These countermeasures
constitute a genetic and a metabolic level. The genetic level
is characterized by the evolutionary advantage of inherited features
that lead to a thickening of the vascular wall, including a multitude
of inherited diseases. The metabolic level is characterized by
the close connection of ascorbate with metabolic regulatory systems
that determine the risk profile for CVD in clinical cardiology
today.
The most frequent mechanism is the deposition of
lipoproteins, particularly lipoprotein(a) [Lp(a)], in the vascular
wall. With sustained ascorbate deficiency, the result of insufficient
ascorbate uptake, these defense mechanisms overshoot and lead
to the development of CVD.
Premature CVD is essentially unknown in all animal
species that produce high amounts of ascorbate endogenously. In
humans, unable to produce endogenous ascorbate, CVD became one
of the most frequent diseases. The genetic mutation that rendered
all human beings today dependent on dietary ascorbate is the universal
underlying cause of CVD.
Optimum dietary ascorbate intake will correct this
common genetic defect and prevent its deleterious consequences.
Clinical confirmation of this theory should largely abolish CVD
as a cause for mortality in this generation and future generations
of mankind.
Full Study
Introduction
We have recently presented ascorbate deficiency as the primary
cause of human CVD. We proposed that the most frequent pathomechanism
leading to the development of atherosclerotic plaques is the deposition
of Lp(a) and fibrinogen/fibrin in the ascorbate-deficient vascular
wall (1, 2). In the course of this work we discovered that virtually
every pathomechanism for human CVD known today can be induced
by ascorbate deficiency. Beside the deposition of Lp(a) this includes
such seemingly unrelated processes as foam cell formation and
decreased reverse-cholesterol transfer, and also peripheral angiopathies
in diabetic or homocystinuric patients. We did not accept this
observation as a coincidence.
Consequently we proposed that ascorbate deficiency
is the precondition as well as a common denominator of human CVD.
This far-reaching conclusion deserves an explanation; it is presented
in this paper. We suggest that the direct connection of ascorbate
deficiency with the development of CVD is the result of extraordinary
pressure during the evolution of man. After the loss of the endogenous
ascorbate production in our ancestors, fatal blood-loss through
the scorbutic vascular wall became a life-threatening condition.
The resulting evolutionary pressure favored genetic and metabolic
mechanisms predisposing to CVD.
The Loss of Endogenous Ascorbate
Production in the Ancestor of Man
With few exceptions all animals synthesize their own ascorbate
by conversion from glucose. In this way they manufacture a daily
amount of ascorbate that varies between about 1 gram and 20 grams,
when compared to the human body weight. About 40 million years
ago the ancestor of man lost the ability for endogenous ascorbate
production. This was the result of a mutation of the gene encoding
for the enzyme L-gulono-g -lactone oxidase (GLO), a key enzyme
in the conversion from glucose to ascorbate. As a result of this
mutation all descendants became dependent on dietary ascorbate
intake.
The precondition for the mutation of the GLO gene
was a sufficient supply of dietary ascorbate. Our ancestors at
that time lived in tropical regions. Their diet consisted primarily
of fruits and other forms of plant nutrition that provided a daily
dietary ascorbate supply in the range of several hundred milligrams
to several grams per day. When our ancestors left this habitat
to settle in other regions of the world the availability of dietary
ascorbate dropped considerably and they became prone to scurvy.
Fatal Blood Loss Through
the Scorbutic Vascular Wall - An Extraordinary Challenge to the
Evolutionary Survival of Man
Scurvy is a fatal disease. It is characterized by structural
and metabolic impairment of the human body, particularly by the
destabilization of the connective tissue. Ascorbate is essential
for an optimum production and hydroxylation of collagen and elastin,
key constituents of the extracellular matrix. Ascorbate depletion
thus leads to a destabilization of the connective tissue throughout
the body. One of the first clinical signs of scurvy is perivascular
bleeding. The explanation is obvious: Nowhere in the body does
there exist a higher pressure difference than in the circulatory
system, particularly across the vascular wall. The vascular system
is the first site where the underlying destabilization of the
connective tissue induced by ascorbate deficiency is unmasked,
leading to the penetration of blood through the permeable vascular
wall. The most vulnerable sites are the proximal arteries, where
the systolic blood pressure is particularly high. The increasing
permeability of the vascular wall in scurvy leads to petechiae
and ultimately hemorrhagic blood loss.
Scurvy and scorbutic blood loss decimated the ship
crews in earlier centuries within months. It is thus conceivable
that during the evolution of man periods of prolonged ascorbate
deficiency led to a great death toll. The mortality from scurvy
must have been particularly high during the thousands of years
the ice ages lasted and in other extreme conditions, when the
dietary ascorbate supply approximated zero. We therefore propose
that after the loss of endogenous ascorbate production in our
ancestors, scurvy became one of the greatest threats to the evolutionary
survival of man. By hemorrhagic blood loss through the scorbutic
vascular wall our ancestors in many regions may have virtually
been decimated and brought close to extinction.
The morphologic changes in the vascular wall induced
by ascorbate deficiency are well characterized: the loosening
of the connective tissue and the loss of the endothelial barrier
function. The extraordinary pressure by fatal blood loss through
the scorbutic vascular wall favored genetic and metabolic countermeasures
attenuating increased vascular permeability.
Ascorbate Deficiency and
Genetic Countermeasures
The genetic countermeasures are characterized by an evolutionary
advantage of genetic features and include inherited disorders
that are associated with atherosclerosis and CVD. With sufficient
ascorbate supply these disorders stay latent. In ascorbate deficiency,
however, they become unmasked, leading to an increased deposition
of plasma constituents in the vascular wall and other mechanisms
that thicken the vascular wall. This thickening of the vascular
wall is a defense measure compensating for the impaired vascular
wall that had become destabilized by ascorbate deficiency. With
prolonged insufficient ascorbate intake in the diet these defense
mechanisms overshoot and CVD develops.
The most frequent mechanism to counteract the increased
permeability of the ascorbate-deficient vascular wall became the
deposition of lipoproteins and lipids in the vessel wall. Another
group of proteins that generally accumulate at sites of tissue
transformation and repair are adhesive proteins such as fibronectin,
fibrinogen, and particularly apo(a). It is therefore no surprise
that Lp(a), a combination of the adhesive protein apo(a) with
a low density lipoprotein (LDL) particle, became the most frequent
genetic feature counteracting ascorbate deficiency (1). Beside
lipoproteins, certain metabolic disorders, such as diabetes and
homocysteinuria, are also associated with the development of CVD.
Despite differences in the underlying pathomechanism, all these
mechanisms share a common feature: they lead to a thickening of
the vascular wall and thereby can counteract the increased permeability
in ascorbate deficiency.
In addition to these genetic disorders, the evolutionary
pressure from scurvy also favored certain metabolic countermeasures.
Ascorbate Deficiency and
Metabolic Countermeasures
The metabolic countermeasures are characterized by the
regulatory role of ascorbate for metabolic systems determining
the clinical risk profile for CVD. The common aim of these metabolic
regulations is to decrease the vascular permeability in ascorbate
deficiency. Low ascorbate concentrations therefore induce vasoconstriction,
hemostasis and affect vascular wall metabolism in favor of atherogenesis.
Towards this end ascorbate interacts with lipoproteins, coagulation
factors, prostaglandins, nitric oxides, and second messenger systems
such as cyclic monophosphates (1, 3-5). It should be noted that
ascorbate can affect these regulatory levels in a multiple way.
In lipoprotein metabolism low density lipoproteins (LDL), Lp(a),
and very low density lipoproteins (VLDL) are inversely correlated
with ascorbate concentrations, whereas ascorbate HDL levels are
positively correlated. Similarly, in prostaglandin metabolism
ascorbate increases prostacyclin and prostaglandin E concentrations
and decreases thromboxane levels. In general, ascorbate deficiency
induces vascular constriction and hemostatis, as well as cellular
and extracellular defense measures in the vascular wall.
In the following sections we will exemplify the
role of ascorbate for frequent and well established pathomechanisms
of human CVD. In general, the inherited disorders described below
are polygenic. Their separate description, however, will allow
the characterization of the role of ascorbate on the different
genetic and metabolic levels.
Apo(a) and Lp(a), the Most
Effective and Most Frequent Countermeasures
After the loss of endogenous ascorbate production, apo(a)
and Lp(a) were greatly favored by evolution. The frequency of
occurrence of elevated Lp(a) plasma levels in species that had
lost the ability to synthesize ascorbate is so great that we formulated
the theory that apo(a) functions as a surrogate for ascorbate
(6). There are several genetically determined isoforms of apo(a).
They differ in the number of kringle repeats and in their molecular
size (7). An inverse relation between the molecular size of apo(a)
and the number of synthesized Lp(a) molecules has been established.
Patients with the high molecular weight apo(a) isoform carry fewer
LDL particles in their Lp(a) fraction. Vice versa, patients with
the genetic pattern of low apo(a) isoform have more LDL particles
in their Lp(a) plasma fraction and thus have increased Lp(a) plasma
levels. In most population studies the genetic pattern of high
apo(a) isoform/low Lp(a) plasma level proved to be the most advantageous
and therefore most frequent pattern.
In ascorbate deficiency Lp(a) is selectively retained
in the vascular wall. Apo(a) counteracts increased permeability
by compensating for collagens, by its binding to fibrin, as a
proteinthiol and antioxidant, and as an inhibitor of plasmin-induced
proteolysis (1). Moreover, as an adhesive protein apo(a) is effective
in tissue-repair processes (8). Chronic ascorbate deficiency leads
to a sustained accumulation of Lp(a) in the vascular wall. This
leads to the development of atherosclerotic plaques and premature
CVD particularly in individuals with genetically determined high
plasma Lp(a) levels. Because of its association with apo(a), Lp(a)
is the most specific repair particle among all lipoproteins. Lp(a)
is predominantly deposited at predisposition sites and it is therefore
found to be significantly correlated with coronary, cervical,
and cerebral atherosclerosis but not with peripheral vascular
disease.
The mechanism by which ascorbate resupplementation
prevents CVD in any condition is by maintaining the integrity
and stability of the vascular wall. In addition, ascorbate exerts
in the individual a multitude of metabolic effects that prevent
the exacerbation of a possible genetic predisposition and the
development of CVD. If the predisposition is a genetic elevation
of Lp(a) plasma levels the specific regulatory role of ascorbate
is the decrease of apo(a) synthesis in the liver and thereby the
decrease of Lp(a) plasma levels. Moreover, ascorbate decreases
the retention of Lp(a) in the vascular wall by lowering fibrinogen
synthesis and by increasing the hydroxylation of lysine residues
in vascular wall constituents, thereby reducing the affinity for
Lp(a) binding (1).
In about half of the CVD patients the mechanism
of Lp(a) deposition contributes significantly to the development
of atherosclerotic plaques. Other lipoprotein disorders are also
frequently part of the polygenic pattern predisposing the individual
patient to CVD in the individual.
Other Lipoprotein Disorders
Associated with CVD
In a large population study Goldstein identified three
frequent lipid disorders, familial hypercholesterolemia, familial
hypertriglyceridemia, and familial combined hyperlipidemia (9).
Ascorbate deficiency unmasks these underlying genetic defects
and leads to an increased plasma concentration of lipids (e.g.
cholesterol, triglycerides) and lipoproteins (e.g. LDL, VLDL)
as well as to their deposition in the impaired vascular wall.
As with Lp(a), this deposition is a defense measure counteracting
the increased permeability. It should, however, be noted that
the deposition of lipoproteins other than Lp(a) is a less specific
defense mechanism and frequently follows Lp(a) deposition. Again,
these mechanisms function as a defense only for a limited time.
With sustained ascorbate deficiency the continued deposition of
lipids and lipoproteins leads to atherosclerotic plaque development
and CVD. Some mechanisms will be described in more detail:
Hypercholesterolemia, LDL-receptor
defect.
A multitude of genetic defects lead to an increased synthesis
and/or a decreased catabolism of cholesterol or LDL. A well characterized
although rare defect is the LDL-receptor defect. Ascorbate deficiency
unmasks these inherited metabolic defects and leads to an increased
plasma concentration of cholesterol-rich lipoproteins, e.g. LDL,
and their deposition in the vascular wall. Hypercholesterolemia
increases the risk for premature CVD primarily when combined with
elevated plasma levels of Lp(a) or triglycerides.
The mechanisms by which ascorbate resupplementation
prevents the exacerbation of hypercholesterolemia and related
CVD include an increased catabolism of cholesterol. In particular,
ascorbate is known to stimulate 7a-hydroxylase, a key enzyme in
the conversion of cholesterol to bile acids and to increase the
expression of LDL receptors on the cell surface. Moreover, ascorbate
is known to inhibit endogenous cholesterol synthesis as well as
oxidative modification of LDL (1).
Hypertriglyceridemia, Type
III hyperlipidemia.
A variety of genetic disorders lead to the accumulation
of triglycerides in the form of chylomicron remnants, VLDL and
intermediate density lipoproteins (IDL) in plasma. Ascorbate deficiency
unmasks these underlying genetic defects and the continued deposition
of triglyceride-rich lipoproteins in the vascular wall leads to
CVD development. These triglyceride-rich lipoproteins are particularly
subject to oxidative modification, cellular lipoprotein uptake,
and foam cell formation. In hypertriglyceridemia non specific
foam cell formation has been observed in a variety of organs (10).
In the vascular wall foam cell formation, although a less specific
repair mechanism than the extracellular deposition of Lp(a), may
have also conferred stability on the ascorbate-deficient vascular
wall.
Ascorbate resupplementation prevents the exacerbation
of CVD associated with hypertriglyceridemia, Type III hyperlipidemia,
and related disorders by stimulating lipoprotein lipases and thereby
enabling a normal catabolism of triglyceride-rich lipoproteins
(11). Ascorbate prevents the oxidative modification of these lipoproteins,
their uptake by scavenger cells and foam cell formation. Moreover,
we propose here that, analogous to the LDL receptor, ascorbate
also increases the expression of the receptors involved in the
metabolic clearance of triglyceride-rich lipoproteins, such as
the chylomicron remnant receptor.
The degree of build-up of atherosclerotic plaques
in patients with lipoprotein disorders is determined by the rate
of deposition of lipoproteins and by the rate of the removal of
deposited lipids from the vascular wall. It is therefore not surprising
that ascorbate is also closely connected with this reverse pathway.
Hypoalphalipoproteinemia.
A frequent lipoprotein disorder is the genetically determined
decreased synthesis of HDL particles. HDL is part of the 'reverse-cholesterol-transport'
pathway and is critical for the transport of cholesterol and also
other lipids from the body periphery to the liver. In ascorbate
deficiency this genetic defect is unmasked resulting in decreased
HDL levels and a decreased reverse transport of lipids from the
vascular wall to the liver. This mechanism is highly effective
and the genetic disorder hypoalphalipoproteinemia was greatly
favored during evolution.
With ascorbate resupplementation HDL production
increases (12), leading to an increased uptake of lipids deposited
in the vascular wall and to a decrease of the atherosclerotic
lesion. A look back in evolution underlines the importance of
this mechanism. During the winter seasons, with low ascorbate
intake, our ancestors became dependent on protecting their vascular
wall by the deposition of lipoproteins and other constituents.
During spring and summer seasons the ascorbate content in the
diet increased significantly and mechanisms were favored that
decreased the vascular deposits under the protection of increased
ascorbate concentration in the vascular tissue. It is not unreasonable
for us to propose that ascorbate can reduce fatty deposits in
the vascular wall within a relatively short time. In an earlier
clinical study it was shown that 500 mg of dietary ascorbate per
day can lead to a reduction of atherosclerotic deposits within
2 to 6 months (13).
This concept, of course, also explains why heart
attack and stroke occur today with a much higher frequency in
winter than during spring and summer, the seasons with increased
ascorbate intake.
Other Inherited Metabolic
Disorders Associated with CVD
Beside lipoprotein disorders many other inherited metabolic
diseases are associated with CVD. Generally these disorders lead
to an increased concentration of plasma constituents that directly
or indirectly damage the integrity of the vascular wall. Consequently
these diseases lead to peripheral angiopathies as observed in
diabetes, homocysteinuria, sickle-cell anemia (the first molecular
disease described (14)), and many other genetic disorders. Similar
to lipoproteins the deposition of various plasma constituents
as well as proliferative thickening provided a certain stability
for the ascorbate-deficient vascular wall. We illustrate this
principle for diabetic and homocystinuric angiopathy.
Diabetic angiopathy.
The pathomechanism in this case involves the structural
similarity between glucose and ascorbate and the competition of
these two molecules for specific cell surface receptors (15,16).
Elevated glucose levels prevent many cellular systems in the human
body, including endothelial cells, from optimum ascorbate uptake.
Ascorbate deficiency unmasks the underlying genetic disease, aggravates
the imbalance between glucose and ascorbate, decreases vascular
ascorbate concentration, and thereby triggers diabetic angiopathy.
Ascorbate resupplementation prevents diabetic angiopathy
by optimizing the ascorbate concentration in the vascular wall
and also by lowering insulin requirement (17).
Homocystinuric angiopathy.
Homocystinuria is characterized by the accumulation of
homocyst(e)ine and a variety of its metabolic derivatives in the
plasma, the tissue and the urine as the result of decreased homocysteine
catabolism (18). Elevated plasma concentrations of homocyst(e)ine
and its derivatives damage the endothelial cells throughout the
arterial and venous system. Thus homocystinuria is characterized
by peripheral vascular disease and thromboembolism. These clinical
manifestations have been estimated to occur in 30 per cent of
the patients before the age of 20 and in 60 per cent of the patients
before the age of 40 (19).
Ascorbate resupplementation prevents homocystinuric
angiopathy and other clinical complications of this disease by
increasing the rate of homocysteine catabolism (20).
Thus, ascorbate deficiency unmasks a variety of
individual genetic predispositions that lead to CVD in different
ways. These genetic disorders were conserved during evolution
largely because of their association with mechanisms that lead
to the thickening of the vascular wall. Moreover, since ascorbate
deficiency is the underlying cause of these diseases, ascorbate
resupplementation is the universal therapy.
The Determining Principles
of This Theory
The determining principles of this comprehensive theory
are schematically summarized in Figures 1 to 3.
Figure 1.
Figure 2.
Figure 3.
1. Cardiovascular disease is the direct consequence of the inability
for endogenous ascorbate production in man in combination with
low dietary ascorbate intake
2. Ascorbate deficiency leads to increased permeability
of the vascular wall by the loss of the endothelial barrier function
and the loosening of the vascular connective tissue.
3. After the loss of endogenous ascorbate production
scurvy and fatal blood loss through the scorbutic vascular wall
rendered our ancestors in danger of extinction. Under this evolutionary
pressure over millions of years genetic and metabolic countermeasures
were favored that counteract the increased permeability of the
vascular wall.
4. The level is characterized by the fact that
inherited disorders associated with CVD became the most frequent
among all genetic predispositions. Among those predispositions
lipid and lipoprotein disorders occur particularly often.
5. The metabolic level is characterized by the
direct relation between ascorbate and virtually all risk factors
of clinical cardiology today. Ascorbate deficiency leads to vasoconstriction
and hemostasis and affects the vascular wall metabolism in favor
of atherogenesis. The genetic level can be further characterized.
The more effective and specific a certain genetic feature counteracted
the increasing vascular permeability in scurvy, the more advantageous
it became during evolution and, generally, the more frequently
this genetic feature occurs today.
7. The deposition of Lp(a) is the most effective,
most specific, and therefore most frequent of these mechanisms.
Lp(a) is preferentially deposited at predisposition sites. In
chronic ascorbate deficiency the accumulation of Lp(a) leads to
the localized development of atherosclerotic plaques and to myocardial
infarction and stroke.
8. Another frequent inherited lipoprotein disorder
is hypoalphalipoproteinemia. The frequency of this disorder again
reflects its usefulness during evolution. The metabolic upregulation
of HDL synthesis by ascorbate became an important mechanism to
reverse and decrease existing lipid deposits in the vascular wall.
9. The vascular defense mechanisms associated with
most genetic disorders is unspecific. These mechanisms can aggravate
the development of atherosclerotic plaques at predisposition sites.
Other color=#66923c>unspecific mechanisms lead to peripheral
forms of atherosclerosis by causing a thickening of the vascular
wall throughout the cardiovascular system. This peripheral form
of vascular disease is characteristic for angiopathies associated
with Type III hyperlipidemia, diabetes, and many other inherited
metabolic diseases.
10. Of particular advantage during evolution and
therefore particularly frequent today are those genetic features
that protect the ascorbate-deficient vascular wall until the end
of the reproduction age. By favoring these disorders nature decided
for the lesser of two evils: the death from CVD after the reproduction
age rather than death from scurvy at a much earlier age. This
also explains the rapid increase of the CVD mortality today from
the 4th decade onwards.
11. After the loss of endogenous ascorbate production
the genetic mutation rate in our ancestors increased significantly
(21). This was an additional precondition favouring not only the
advantage of apo(a) and Lp(a) but also of many other genetic countermeasures
associated with CVD.
Genetic predispositions are characterized by the
rate of ascorbate depletion in a multitude of metabolic reactionsspecific
for the genetic disorder (22). The overall rate of ascorbate depletion
in an individual is largely determined by polygenic pattern of
disorders. The earlier the ascorbate reserves in the body are
depleted without being resupplemented, the earlier CVD develops.
13. The genetic predispositions with the highest
probability for early clinical manifestation require the highest
amount of ascorbate resupplementation in the diet to prevent CVD
development. The amount of ascorbate for patients at high risk
should be comparable to the amount of ascorbate our ancestors
synthesized in their body before they lost this ability: between
10,000 and 20,000 milligrams per day.
14. Optimum ascorbate resupplementation prevents
the development of CVD independent of the individual predisposition
or pathomechanism. Ascorbate reduces existing atherosclerotic
deposits and thereby decreases the risk for myocardial infarction
and stroke. Moreover, ascorbate can prevent blindness and organ
failure in diabetic patients, thromboembolism in homocystinuric
patients and many other manifestations of CVD.
Conclusion
In this paper we present a unified theory of human CVD. This disease
is the direct consequence of the inability of man to synthesize
ascorbate in combination with insufficient intake of ascorbate
in the modern diet. Since ascorbate deficiency is the common cause
of human CVD, ascorbate resupplementation is the universal treatment
for this disease. The available epidemiological and clinical evidence
is reasonably convincing. Further clinical confirmation of this
theory should lead to the abolition of CVD as a cause of human
mortality for the present generation and future generations of
mankind.
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