(a) Vitamin E influences responses of cells in the artery wall and inhibits
lipoprotein oxidation in ways which would be anti-atherogenic if occurring
in the organism.
(b) Long-term vitamin E deficiency in animals causes atherosclerotic-like
vessel lesions which can be limited, if not reversed, by vitamin E administration.
(c) Dietary vitamin E supplementation suppresses atherosclerosis in at least
some animal models of atherosclerotic vessel disease.
(d) Vitamin E supplementation may help normalize a pro-atherogenic blood
lipid profile.
(e) Epidemiologists have inversely correlated blood vitamin E levels in
humans with mortality from coronary heart disease.
Although this evidence as a whole strongly suggests that vitamin E has therapeutic
potential against atherosclerosis, definitive proof of such a role in man
is lacking at present. The details can be found in a recent review [2].
Passwater: How does vitamin E affect the function of the endothelial
lining of arteries in ways that might help prevent atherosclerosis?
Janero: Data on this question come mainly from work on isolated
endothelial cells in culture. Vitamin E is a critical antioxidant protector
of endothelial-cell membranes against the consequences of oxidative stress,
particularly lipid peroxidation. More limited data suggest that vitamin
E can promote endothelial repair and even suppress harmful oxidant production
within the endothelium itself which could lead to, for instance, oxidation
of lipoproteins.
Passwater: Would you describe the monocyte-macrophage and
explain how vitamin E affects the functioning of this cell as a potential
antiatherosclerotic agent?
Janero: The monocyte is a type of white blood cell produced
in the bone marrow. Monocytes circulate in the blood for a limited time
(about 40 hours in humans), whereupon they may enter connective tissue throughout
the body, increase in size and metabolic activity, and be recognized operationally
as macrophages. Through production and release of various chemical mediators,
macrophages can recruit more monocytes into connective tissue from the circulation.
Macrophages actively take-up and kill disease-causing microorganisms, making
them critical to the inflammatory response. Active macrophages in the connective
tissue of the artery wall have an impressive capacity for oxidizing biomolecules
and lipoproteins.
The relationship between vitamin E and the macrophage is complex. The vitamin
E in macrophage membranes helps the cell itself withstand oxidative stress.
Vitamin E could prevent lipoprotein oxidation (and, thus, uptake of oxidized
lipoproteins by the macrophage to form foam cells) by limiting macrophage
oxidant production. It is particularly interesting, and more than a little
ironic, that oxidized lipoproteins themselves stimulate monocyte differentiation
to macrophages.
Passwater: You have mentioned oxidized lipoproteins several times
now. Do you feel that lipoprotein oxidation is an important target for vitamin
E as an antiatherosclerotic agent?
Janero: Inhibition of lipoprotein oxidation is increasingly being
recognized as one of the most conceptually attractive and therapeutically
important means by which atherosclerosis might be prevented and possibly
even reversed.
Passwater: Let's discuss oxidized lipoproteins in detail later. You
haven't mentioned ischemia-reperfusion injury to the heart. Isn't this what
brought your work to the attention of classical heart-disease researchers
in the first place?
Janero: My own work in the cardiovascular area began with lipoprotein
synthesis and metabolism. Over the ten years since, my laboratory has conducted
research in several areas, some well outside the cardiovascular system,
largely due to my good fortune of having talented, dedicated colleagues
and collaborators. Discussions with Drs. Adrianne Bendich and Lawrence Machlin
stimulated me to study vitamin E in the heart muscle cell [3].
A constant research focus throughout this time has been cardiac ischemia,
a well-recognized clinical complication of coronary-artery atherosclerosis
because of diminished blood supply to heart muscle. The reduction in nutritive
blood flow does not allow the heart-muscle cell to maintain normal function
and metabolism. Several means (especially "clot busters" such
as streptokinase and tPA) are now being used in the clinic to reperfuse
the ischemic heart. Although reperfusion is essential to prevent death of
ischemic heart muscle, reperfusion itself appears capable of extending ischemic
cardiac damage by killing heart muscle cells which would have been expected
to remain viable.
Our research on ischemia-reperfusion injury has focused on several potential
mechanisms and mediators, including membrane lipids, derangements in energy
metabolism, and oxidative stress [4]. We try to understand what factors
act as determinants of heart muscle injury and how one might intervene to
prevent post-ischemic reperfusion damage. Our overall goal in this area
of our research is to help the cardiologist restore maximal pump function
to the post-ischemic heart. For this discussion, it's especially noteworthy
that vitamin E may have direct beneficial effects against cardiac ischemia
[5].
Passwater: Earlier, you mentioned oxidized lipoprotein as
a major target for the protective effect of vitamin E against atherosclerosis.
What are lipoproteins?
Janero: Lipoproteins represent nature's elegant engineering
solution to the following problem: How can a rather large amount of lipid
(fat) be continuously transported through the body in blood, which is water-based
and in which fats are not readily soluble? Lipoproteins are microscopic
complexes of various types of lipid (triglyceride, cholesterol, phospholipid)
and protein ("apoprotein") which, as particles, are blood-soluble.
Structurally, the more polar lipid (i.e., phospholipid) as well as large
portions of water-soluble apoproteins form a "shell" which surrounds
a "core" of nonpolar lipid (triglyceride, cholesterol ester) having
negligible water solubility.
Lipoproteins are classified according to their density, which reflects their
lipid composition and lipid-to-protein ratio. In turn, the specific lipid
and protein contents of the six major types of lipoprotein particle reflect
their different functions and their metabolism. For example, triglyceride-rich
very low density-lipoprotein (VLDL) transports triglyceride from the liver
to peripheral tissues which use triglyceride as fuel, whereas low-density
lipoprotein (LDL) is the major carrier of blood cholesterol. Normal lipoprotein
metabolism interconverts lipoprotein particles of varying densities.
Passwater: What holds lipoproteins together to give them a
particle-like character?
Janero: Several factors define and stabilize the organization
of lipoprotein lipids and proteins. One factor is lipoprotein synthesis
itself, which is highly organized within cells (especially liver cells)
much like an automobile assembly line [6]. Other factors have to do with
the physical chemistry of lipid-protein interactions in water: apoproteins
and lipids tend to undergo self-association reactions which result in a
more stable, low-energy aggregate. The three-dimensional structure of apoproteins
also exerts some control over lipoprotein stability.
Recent molecular analyses of apoproteins indicate that they possess lipid-binding
regions which also help keep the lipoprotein particle intact.
Passwater: How does LDL become oxidized? Is it a simple oxidation
reaction?
Janero: "Oxidation" is a very general term encompassing
a variety of degenerative changes to LDL molecular constituents, mainly
as a consequence of the peroxidation of LDL lipid and the decomposition
of the resultant fatty peroxides. [7] Lipid peroxidation, the introduction
of molecular oxygen into a polyunsaturated fatty acid to form a fatty hydroperoxide,
is chemically complex and not well understood. [8] As with oxidative damage
in any living system, LDL oxidation can occur only when oxidant stress on
the LDL particle exceeds the ability of endogenous LDL antioxidants to detoxify
the stress. LDL can be oxidized by any of the three major cell types in
the artery wall (endothelial cells, smooth-muscle cells, and monocyte-macrophages).
Biochemical studies on LDL isolated from humans clearly show that oxidants
(free radicals/hydrogen peroxide), in the presence of transition metals
(e.g., iron, copper), can initiate the peroxidation of polyunsaturated fatty
acids in LDL phospholipid, cholesterol ester, and triglyceride molecules.
Endogenous LDL antioxidants (e.g., vitamin E, various carotenoids) are consumed
during LDL oxidation. Key intermediates generated during lipid peroxidation
are lipid free-radicals. Lipid radicals can react with other polyunsaturated
fatty acids in LDL particles to set up a "chain reaction" and
rapidly generate oxidatively-modified LDL. The decomposition products of
fatty peroxides damage LDL apoproteins, disrupting the organization of the
LDL particle itself. The end result of LDL oxidation is an LDL particle
with striking physical and chemical abnormalities.
Passwater: Why is oxidized LDL more likely than native, unmodified
LDL to form foam cells?
Janero: Decades ago, pathologists recognized that macrophages
in the arterial wall helped form the lipid-rich atherosclerotic lesion called
the "fatty streak." Studies in the 1970's produced the surprising
result that macrophages do not take up native LDL rapidly enough to become
lipid-loaded, even when exposed to much higher concentrations of LDL particles
than in the body. The Nobel laureates Drs. Brown and Goldstein at the University
of Texas Medical Center, Dallas, provided the following explanation in a
now classic series of experiments which exemplify the power of modern cell
biology: the macrophage has on its surface LDL receptors which not only
bring native LDL into the macrophage, but simultaneously reduce its uptake
as the cholesterol level within the macrophage increases. [9]
Oxidized-LDL is recognized not by this receptor for native LDL, but by so-called
"scavenger" receptors also on the macrophage surface. A critical
distinction between these LDL receptor types is that scavenger receptors
for modified LDL are not sensitive to cholesterol levels within the macrophage.
Thus, the scavenger receptor brings cholesterol-rich, oxidized-LDL into
already cholesterol-loaded macrophages, whereas the receptor for native
LDL would not. With continued uptake of oxidized-LDL, the macrophages become
filled with lipid and trapped within the artery wall. Their now frothy appearance
in the light microscope has given them the name "foam cells."
Accumulations of dead foam cells constitute the earliest overt sign of atherosclerosis,
the fatty streak.
Passwater: Although lipoproteins circulate in the blood, it
seems that LDL oxidation would have to occur within the artery wall, below
the endothelial lining, where macrophages reside. How can this be?
Janero: Circulating LDL particles interact with endothelial
cells lining the arteries and, as they move into and out of the subendothelial
space, with macrophages and smooth muscle cells of the middle layer of the
artery wall. All three of these cell types have the capacity to oxidize
LDL. It is likely, although not yet proven, that most of the LDL oxidation
which supports atherosclerosis takes place in LDL-rich "microenvironments"
in the middle layer of the artery wall. Both macrophages and smooth muscle
cells in this layer can internalize oxidized-LDL to form foam cells. Oxidized-LDL
in the artery wall may recruit monocytes into the developing atherosclerotic
lesion, greatly increasing the possibility of foam cell formation.
Passwater: Is there evidence that LDL oxidation represents
a pivotal process in atherosclerosis?
Janero: Most of the evidence indicating that oxidized-LDL
is a critical source of lipid for foam cell formation comes from studies
in animal models of coronary artery disease. In such models, oxidative LDL
modification has been documented, and antioxidant therapy can inhibit the
development of early atherosclerotic lesions. Oxidized-LDL and lipid peroxides
are present in human atherosclerotic lesions and even in the circulation
of coronary heart-disease patients. Administration of a cholesterol-lowering
antioxidant drug, probucol, to hypercholesterolemic patients reduces the
oxidizability of their
LDL. So there are several lines of evidence associating oxidative
LDL modification with early atherosclerosis. [10]
Passwater: How could vitamin E help prevent LDL oxidation
and fatty streak development?
Janero: Vitamin E is the principal, if not sole, chain-breaking
antioxidant in the circulation. As a lipoprotein constituent, it reacts
with lipid free-radicals to neutralize them and suppress LDL lipid-peroxidation.
Indeed, only when endogenous LDL-vitamin E is virtually depleted can peroxidation
of LDL lipid occur at maximal rates. Vitamin E may also modify the physical
properties of the LDL particle, making it more resistant to free-radical
attack, and spare other antioxidants in the LDL particle. At least in principle,
the vitamin E of endothelial calls, smooth muscle cells, and macrophages
could inhibit their ability to oxidize LDL. Equivocal data exist suggesting
that vitamin E can alter LDL lipid composition in a way which would decrease
its content of oxidizable lipid.
Passwater: What blood level of vitamin E would offer optimal
LDL protection?
Janero: This question remains to be answered. The mere presence
of vitamin E in the LDL particle is not enough to suppress LDL oxidation,
suggesting that the ratio of vitamin E to peroxidizable polyunsaturated
fatty acid in the particle must be above some threshold for vitamin E to
be a decisive factor in reducing LDL-oxidation. It is likely that risk-factor
variation within the human population may prohibit definition of a general
"optimal" blood vitamin E level for LDL antioxidant protection.
Passwater: What might increase the need for antioxidant protection
of LDL?
Janero: Any condition which would predispose LDL to oxidative
stress or increase its susceptibility to lipid peroxidation would argue
for fortifying the antioxidant content of LDL. For instance, vitamin E supplementation
inhibits oxidative LDL modification induced by a major risk factor for atherosclerosis,
cigarette smoking, which imposes a major oxidant burden upon the smoker.
Diets which increase the polyunsaturated fatty acid content of LDL would
also potentiate the LDL antioxidant requirement, as might administration
of drugs whose metabolism leads to free-radical production. In contrast,
it is interesting to note that some commonly-prescribed cardiovascular drugs,
such as calcium antagonists, posses antioxidant properties themselves which
may help explain their efficacy in some models of atherosclerosis. [11]
Passwater: Clearly, we don't have all the answers regarding
vitamin E's impact on atherosclerosis. How do you envision research in the
area through the 1990's?
Janero: I am very optimistic about future research on vitamin
E (and other nutrients) and cardiovascular disease. The idea that diseases
such as spontaneous atherosclerosis which develop over a long period of
time are more easily prevented than cured gives particular urgency to defining
the therapeutic potential of dietary vitamin E supplementation. Mechanistic
investigations on nutrients and atherosclerosis, aside from their value
to preventive medicine, should also help improve our understanding of how
atherosclerotic vessel disease develops. Research regarding vitamin E's
ability to protect the ischemic heart should not be forgotten either in
our age of reperfusion injury and increasing awareness of the "silent
ischemic" heart-disease population [12].
Passwater: What supplements do you take?
Janero: Aside from my research, I try to maintain some status
as a "radical fighter" by taking a general antioxidant mixture
including vitamin E, beta-carotene, cysteine, glutathione, and selenium.
(Total vitamin E, 400 IU daily.) I also take a multivitamin-mineral supplement.
REFERENCES