| Current
Drug Metabolism
ISSN: 1389-2002
Current Drug Metabolism
Volume 6, Number 1, February 2005
Contents
Clinical Investigations (Endothelial Function and
Thrombosis),Intracellular Metabolism and Cell Culture Studies
with Infectious Agents
Guest Editor: Olaf Stanger
Editorial
[Editorial
In PDF]
Asymmetric Dimethyl-L-Arginine (ADMA): A Possible Link
Between Homocyst(e)ine and Endothelial Dysfunction Pp.3-14
Markus C. Stuhlinger and Olaf Stanger
[Abstract] [Full
text article]
Effects of Betaine Intake on Plasma Homocysteine Concentrations
and Consequences for Health Pp.15-22
M.R. Olthof and P. Verhoef
[Abstract] [Full
text article]
Homocysteine and the Kidney Pp.23-26
Coen van Guldener
[Abstract] [Full
text article]
Mechanisms of Increased Vascular Oxidant Stress in Hyperhomocysteinemia
and Its Impact on Endothelial Function Pp.27-36
N. Weiss
[Abstract] [Full
text article]
Gene-Nutrient Interactions in One-Carbon Metabolism Pp.37-46
Simonetta Friso and Sang-Woon Choi
[Abstract] [Full
text article]
The Usefulness of Holotranscobalamin in Predicting Vitamin
B12 Status in Different Clinical Settings Pp.47-53
Wolfgang Herrmann, Rima Obeid, Heike Schorr and Jurgen
Geisel
[Abstract] [Full
text article]
Abstracts
[Back to top]
Editorial
[Editorial
In PDF]
When Vincent du Vigneaud isolated homocysteine in 1932, it
was his intention to identify the origin of sulfur within
the insulin molecule, discovered by Banting and Best in Toronto
(1921). Cystine and methionine were likely candidates. However,
du Vigneaud was to later recall that all of the work that
led ultimately to the discovery of the transsulfuration and
transmethylation pathways would not have taken place had he
known that methionine was in fact not part of insulin.
Around 1960 all reactions and metabolites participating in
the metabolism of methionine and homocysteine were identified
and known, but clinicians only began to realize the relevance
when homocystine was first identified in the urine of children
with inherited enzyme deficiencies in 1962.
A few cases of extremely rare inborn genetic defects with
the common feature of hyperhomocysteinemia enabled McCully
in 1968/69 to establish the hypothesis that homocysteine might
have a role to play in the etiology of vascular pathologies.
The full metabolism as it is known today was published in
“Science” (1964) and after another decade and
with the development of more sensitive diagnostic technology
and new markers and its introduction for routine use, homocysteine
research began to explode and continues to be a very active
field of research today. In fact it has become almost impossible
to keep up with the number of daily published works.
Beyond its potential role as a major risk factor in atherothrombotic
disease, homocysteine has increasingly been found to participate
directly and indirectly in a large number of basic functions
of cell physiology. Consequently research has expanded to
new fields of interest and these promise to yield new insights
and understanding in molecular pathology with important clinical
implications.
In this special issue of Current Drug Metabolism the reader
will find a number of selected reviews that are very closely
linked to each other - by the amino acid homocysteine. My
intention as guest editor is to cover some of the new fields
of research that homocysteine has led the way to. The authors
are dedicated researchers and much respected investigators
in their own particular and very demanding fields. I am very
grateful to them for their valuable contributions to this
special issue. Their reviews provide current insight into
homocysteine-mediated interactions with DNA-methylation, ADMA,
betaine, cobalamin metabolism, renal function and oxygen radical
formation. As such, they add to our understanding of the etiology
and progression of diseases and serve to encourage further
research.
Olaf Stanger, M.D.
St. John`s Hospital
Private Medical University
Dept. of Cardiac Surgery
Cardiovascular Research
Salzburg, Austria
[Back to top]
Asymmetric Dimethyl-L-Arginine (ADMA): A Possible Link
Between Homocyst(e)ine and Endothelial Dysfunction
Markus C. Stuhlinger and Olaf Stanger
[Full
text article]
Hyperhomocyst(e)inemia is associated with an increased risk
for atherosclerotic disease and venous thromboembolism. The
impact of elevated plasma homocysteine levels seems to be
clinically relevant, since the total cardiovascular risk of
hyperhomocyst(e)inemia is comparable to the risk associated
with hyperlipidemia or smoking.
There is substantial evidence for impairment of endothelial
function in human and animal models of atherosclerosis, occurring
even before development of overt plaques. Interestingly endothelial
dysfunction appears to be a sensitive indicator of the process
of atherosclerotic lesion development and predicts future
vascular events. NO is the most potent endogenous vasodilator
known. It is released by the endothelium, and reduced NO bioavailability
is responsible for impaired endothelium-dependent vasorelaxation
in hyperhomocyst(e)inemia and other metabolic disorders associated
with vascular disease. Substances leading to impaired endothelial
function as a consequence of reduced NO generation are endogenous
NO synthase inhibitors such as ADMA. Indeed there is accumulating
evidence from animal and human studies that ADMA, endothelial
function and homocyst(e)ine might be closely interrelated.
Specifically elevations of ADMA associated with impaired endothelium-dependent
relaxation were found in chronic hyperhomocyst(e)inemia, as
well as after acute elevation of plasma homocyst(e)ine following
oral methionine intake. The postulated mechanisms for ADMA
accumulation are increased methylation of arginine residues
within proteins, as well as reduced metabolism of ADMA by
the enzyme DDAH, but they still need to be confirmed to be
operative in vivo.
Hyperhomocyst(e)inemia, as well as subsequent endothelial
dysfunction can be successfully treated by application of
folate and B vitamins. Since ADMA seems to play a central
role in homocyst(e)ine-induced endothelial dysfunction, another
way of preventing vascular disease in patients with elevated
homocyst(e)ine concentrations could be supplementation with
L-arginine to reverse the detrimental effects of ADMA.
[Back to top]
Effects of Betaine Intake on Plasma Homocysteine Concentrations
and Consequences for Health
M.R. Olthof and P. Verhoef
[Full text article]
High plasma concentrations of homocysteine may increase risk
of cardiovascular disease. Folic acid lowers plasma homocysteine
by 25% maximally, because 5-methyltetrahydrofolate is a methyl
donor in the remethylation of homocysteine to methionine.
Betaine (trimethylglycine) is also a methyl donor in homocysteine
remethylation, but effects on homocysteine have been less
thoroughly investigated. Betaine in high doses (6 g/d and
higher) is used as homocysteine-lowering therapy for people
with hyperhomocysteinemia due to inborn errors in the homocysteine
metabolism. Betaine intake from foods is estimated at 0.5-2
g/d. Betaine can also be synthesized endogenously from its
precursor choline. Studies in healthy volunteers with plasma
homocysteine concentrations in the normal range show that
betaine supplementation lowers plasma fasting homocysteine
dose-dependently to up to 20% for a dose of 6 g/d of betaine.
Moreover, betaine acutely reduces the increase in homocysteine
after methionine loading by up to 50%, whereas folic acid
has no effect. Betaine doses in the range of dietary intake
also lower homocysteine. This implies that betaine can be
an important food component that attenuates homocysteine rises
after meals. If homocysteine plays a causal role in the development
of cardiovascular disease, a diet rich in betaine or choline
might benefit cardiovascular health through its homocysteine-lowering
effects. However betaine and choline may adversely affect
serum lipid concentrations, which can of course increase risk
of cardiovascular disease. However, whether the potential
beneficial health effects of betaine and choline outweigh
the possible adverse effects on serum lipids is as yet unclear.
[Back to top]
Homocysteine and the Kidney
Coen van Guldener
[Full text
article]
Plasma homocysteine concentration exhibits a strong relationship
with (indices of) renal function. Hyperhomocysteinemia has
been implicated in the high vascular event rate in patients
with chronic renal failure. The precise pathophysiological
explanation for the occurrence of hyperhomocysteinemia in
renal failure is not yet elucidated. A defective intrinsic
renal metabolism of homocysteine seems unlikely. There are
several indications that whole body homocysteine metabolism
is altered in renal insufficiency. Stable isotope studies
in dialysis patients have shown a decreased homocysteine clearance
by transsulfuration and decreased homocysteine remethylation
and methionine transmethylation. Several, but not all, prospective
studies have linked hyperhomocysteinemia to adverse cardiovascular
outcomes in renal failure patients. Treatment of hyperhomocysteinemia
in renal insufficiency is based on folic acidcontaining regimens,
but so far, none of the regimens has been shown to successfully
normalize plasma homocysteine concentration. Intervention
studies have not yet demonstrated beneficial vascular effects
of homocysteine-lowering treatment in dialysis patients.
[Back to top]
Mechanisms of Increased Vascular Oxidant Stress in Hyperhomocysteinemia
and Its Impact on Endothelial Function
N. Weiss
[Full text
article]
Elevated plasma levels of homocysteine are associated with
an increased generation of reactive oxygen species in aortas
of hyperhomocysteinemic animals and in endothelial cells.
This may contribute to endothelial dysfunction observed in
hyperhomocysteinemia, and promote atherosclerotic vascular
disease. Homocysteine seems to promote the formation of reactive
oxygen species primarily by a biochemical mechanism involving
endothelial nitric oxide synthase, as increased endothelial
lipid peroxidation and oxidation of the redox-sensitve dye
2’,7’-dichlorofluoresceine could only be observed
after incubation of endothelial cells with L-, but not with
D-homocysteine, and could be prevented by inhibition of endothelial
nitric oxide synthase. An increased oxidation rate of aminothiols
in plasma, as observed in patients with hyperhomocysteinemia,
further contributes to increased generation of reactive oxygen
species. These effects are amplified by a homocysteine-specific
inhibition of cellular antioxidant enzymes, like superoxide
dismutase and the cellular isoform of gluthatione peroxidase.
All mechanisms together result in increased levels of superoxide
anion and peroxyl radicals in the vasculature that react with
nitric oxide to form peroxnitrites. This abolishes nitric
oxide’s bioactivity and contributes to endothelial dysfunction.
In addition, increased vascular oxidant stress in hyperhomocysteinemia
has been shown to activate proinflammatory signaling pathways
in endothelial cells, like the transcription factor NF-κB.
This leads to increased endothelial expression of chemokines
and adhesion molecules that promote the recruitment, adhesion
and transmigration of circulating leukocytes to the vessel
wall. All these mechamisms may contribute to the increased
risk for cardiovascular diseases associated with hyperhomocysteinemia.
[Back to top]
Gene-Nutrient Interactions in One-Carbon Metabolism
Simonetta Friso and Sang-Woon Choi
[Full text
article]
Advances in molecular biology greatly contributed, in the
past decades, to a deeper understanding of the role of gene
function in disease development. Environmental as well as
nutritional factors are now well acknowledged to interact
with the individual genetic background for the development
of several diseases, including cancer, cardiovascular disease,
and neurodegenerative diseases. The precise mechanisms of
such gene-nutrient interactions, however, are not fully elucidated
yet. Many micronutrients and vitamins are crucial in regulating
mechanisms of DNA metabolism. Indeed, folate has been most
extensively investigated for its unique function as mediator
for the transfer of one-carbon moieties for nucleotide synthesis/repair
and biological methylation. Cell culture, animal, and human
studies, clearly demonstrated that folate deficiency induces
disruption of DNA synthesis/repair pathways as well as DNA
methylation anomalies. Remarkably, a gene-nutrient interaction
between folate status and a polymorphism in methylenetetrahydrofolate
reductase gene has been reported to modulate genomic DNA methylation.
This observation suggests that the interaction between a nutritional
status and a mutant genotype may modulate gene expression
through DNA methylation, especially when such polymorphism
affects a key enzyme in one-carbon metabolism and limits the
methyl supply. DNA methylation, both genome-wide and gene-specific,
is of particular interest for the study of aging, cancer,
and other pathologic conditions, because it affects gene expression
without permanent alterations in the DNA sequence such as
mutations or allele deletions. Understanding the patterns
of DNA methylation through the interaction with nutrients
is a critical issue, not only to provide pathophysiological
explanations of a disease state, but also to identify individuals
at-risk to conduct targeted diet-based interventions.
[Back to top]
The Usefulness of Holotranscobalamin in Predicting Vitamin
B12 Status in Different Clinical Settings
Wolfgang Herrmann, Rima Obeid, Heike Schorr and Jurgen
Geisel
[Full text
article]
Serum concentrations of homocysteine (Hcy) and methylmalonic
acid (MMA) become increased in B12-deficient subjects and
are therefore, considered specific markers of B12 deficiency.
Serum level of holotranscobalamin (holoTC) becomes decreased
before the development of the metabolic dysfunction. We investigated
the usefulness of holoTC in diagnosing B12 deficiency in some
clinical settings. We measured serum concentrations of holoTC,
MMA, Hcy and total B12 in omnivores, vegetarians, elderly
people and haemodialysis patients. Our results indicated that
the incidence of holoTC <35 pmol/L was highest in the vegans
(76%). Low holoTC and elevated MMA were detected in 64% of
the vegans and 43% of the lacto- and lacto-ovovegetarians.
An elevated MMA and a low holoTC were found in subjects with
total serum B12 as high as 300 pmol/L. The distribution of
holoTC in elderly people was similar to that in younger adults
(median holoTC 55 pmol/L in both groups). A low holoTC and
an elevated MMA were found in 16% of the elderly group. An
elevated MMA and a normal holoTC were found in 20% of the
elderly group who had a relatively high median serum concentration
of creatinine (106.1 µmol/L). Serum concentrations of
holoTC in dialysis patients were considerably higher than
all other groups (median 100 pmol/L). This was also associated
with severely increased serum levels of MMA (median 987 nmol/L).
From these results it can be concluded that serum concentration
of holoTC is a much better predictor of B12 status than total
B12. This was particularly evident in case of dietary B12
deficiency. Serum concentrations of holoTC as well as MMA
can be affected by renal dysfunction. Elevated MMA and normal
holoTC in patients with renal insufficiency may not exclude
vitamin B12 deficiency. HoloTC seems not to be a promising
marker in predicting B12 status in renal patients.
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