| Current
Vascular Pharmacology
ISSN: 1570-1611
Current Vascular Pharmacology
Volume 3, Number 1, January 2005
Contents
Micronized Purified Flavonoid Fraction (MPFF)*:
A Review of its Pharmacological Effects, Therapeutic Efficacy
and Benefits in the Management of Chronic Venous Insufficiency
Pp.1-9
Konstantinos Katsenis
[Abstract] [Full
text article]
Molecular Pathways of Endothelial Cell Activation
for (Targeted) Pharmacological Intervention of Chronic Inflammatory
Diseases Pp.11-39
Joanna M. Kuldo, Ken Ichi Ogawara, Naomi Werner, Sigridur
A. Asgeirsdottir,Jan A.A.M. Kamps, Robbert J. Kok and Grietje
Molema
[Abstract] [Full
text article]
Evidence for, and Importance of, cGMP-Independent
Mechanisms with NO and NO Donors on Blood Vessels and Platelets
Pp.41-53
Janet C. Wanstall, Kerry L. Homer and Sheila A. Doggrell
[Abstract] [Full
text article]
Transforming Growth Factor-β, Cell Signaling
and Cardiovascular Disorders Pp.55-61
Alex Agrotis, Natalia Kalinina and Alex Bobik
[Abstract] [Full
text article]
Macrophage Activation in Atherosclerosis: Pathogenesis
and Pharmacology of Plaque Rupture Pp.63-68
J.J. Boyle
[Abstract] [Full
text article]
Modulation of Cardiovascular Remodeling with Statins:
Fact or Fiction? Pp.69-79
Rajasekhar Reddy, Georges Chahoud and J.L. Mehta
[Abstract] [Full
text article]
Role of Vascular Nitric Oxide in Experimental
Liver Cirrhosis Pp.81-85
Noemi M. Atucha, F. Javi A. Nadal, David Iyu, Antonia
Alcaraz, Alicia Rodriguez-Barbero, M. Clara Ortiz, Jose Miguel
Lopez-Novoa and Joaquin Garcia-Estan
[Abstract] [Full
text article]
Fenofibrate: Metabolic and Pleiotropic Effects
Pp.87-98
Vasilis Tsimihodimos, George Miltiadous, Stella S. Daskalopoulou,
Dimitri P. Mikhailidis and Moses S. Elisaf
[Abstract] [Full
text article]
Abstracts
[Back to top]
Micronized Purified Flavonoid Fraction (MPFF)*: A
Review of its Pharmacological Effects, Therapeutic Efficacy
and Benefits in the Management of Chronic Venous Insufficiency
Konstantinos Katsenis
[Full
text article]
Initially, the progression of chronic venous insufficiency
is related to venous hypertension. The earliest complaints
or symptoms, as well as vessel wall deterioration, valve restructuring,
and, eventually, varicose veins, result not only from elevation
of pressure, but also from a cascade of biochemical events
related to both the macro- and the microcirculation. Thickening
and remodelling of the venous wall are influenced by two parameters:
abnormal shear stress and hypoxia that activate the endothelium
first at the level of valve cusps and then in large veins.
Hypoxia leads to activation of the endothelium and leukocyte
accumulation.
By inhibiting endothelial activation, micronized purified
flavonoid fraction (MPFF) (Daflon 500 mg), an edemaprotective
agent, can prevent the inflammatory cascade resulting from
the leukocyte-endothelium interaction. This subsequently delays
the appearance of reflux and inhibits the initiation of the
vicious circle ending in enhanced venous pressure. This is
how Daflon 500 mg relieves patients from symptoms and edema
and possibly also prevents the appearance of varicose veins.
Rheological disturbances also play a major role in the appearance
of these disorders. Furthermore, venous hypertension provokes
leakage from the vessels and capillaries exhibiting increased
permeability, leading to increases in hydrostatic load, and
overloading of the lymphatic network, which subsequently results
fluid exudation causing edema. Microcirculatory dysfunction
leads to capillary damage, skin changes and venous leg ulcers.
The clinical efficacy of Daflon 500 mg in venous leg ulcers
has been demonstrated by several randomised controlled studies,
in which the rate of ulcer healing was significantly shortened.
An explanation for the ability to speed ulcer healing comes
from the protection Daflon 500 mg exerts on the microcirculation.
[Back to top]
Molecular Pathways of Endothelial Cell Activation for (Targeted)
Pharmacological Intervention of Chronic Inflammatory Diseases
Joanna M. Kuldo, Ken Ichi Ogawara, Naomi Werner,
Sigridur A. Asgeirsdottir,Jan A.A.M. Kamps, Robbert J. Kok
and Grietje Molema
[Full
text article]
In chronic inflammatory conditions, endothelial cells actively
recruit immune cells from the circulation into the underlying
tissue and participate in angiogenesis to support the continuous
demand for oxygen and nutrients. They do so in response to
activation by cytokines and growth factors such as tumour
necrosis factor α
(TNFα),
interleukin-1 (IL-1), vascular endothelial growth factor (VEGF),
and fibroblast growth factors (FGFs). Receptor triggering
initiates intracellular signal transduction leading to activation
of nuclear factor κB
(NFκB),
mitogen activated protein kinase (MAPK) activity, and nitric
oxide and reactive oxygen species production, among others.
As a result, adhesion molecules, cytokines and chemokines,
and a variety of other genes are being expressed that mediate
and control the inflammatory process. In recent years, different
classes of drugs have been developed that interfere with selected
enzymes involved in the intracellular signalling cascades.
In endothelial cell cultures, they exert potent inhibitory
effects on the expression of genes, while several studies
also report on in vivo effectiveness to confine the
inflammatory responses. To prevent undesired toxicity and
to improve drug behaviour and efficacy, drug carrier systems
have been developed that selectively deliver the therapeutics
into the activated endothelial cells. The above subjects are
recapitulated to give an overview on the status of development
of endothelial cell directed therapeutic strategies to pharmacologically
interfere with chronic inflammatory diseases.
[Back to top]
Evidence for, and Importance of, cGMP-Independent Mechanisms
with NO and NO Donors on Blood Vessels and Platelets
Janet C. Wanstall, Kerry L. Homer and Sheila
A. Doggrell
[Full
text article]
In the vasculature it is well established that cGMP is involved
in the relaxant response to nitric oxide (NO) and NO donors.
However, there is an increasing evidence that alternative/additional
pathways that are cGMP-independent may also exist. A key criterion
for a response to NO or a NO donor drug to be classified as
cGMP-independent is lack of (or incomplete) inhibition by
the selective inhibitor of soluble guanylate cyclase, ODQ
(1H-[1,2,4]oxadiazole[4,3- a]quinoxalin-1-one). In
many blood vessels cGMP-independent mechanisms contribute
to the vasorelaxation, and in certain vascular beds cGMP-independent
relaxation may be the predominant mechanism of action of NO
and NO donors. NO donor drugs that generate NO ‘spontaneously’,
like authentic NO (i.e. solutions of NO gas), appear to exhibit
a larger component of cGMP-independent vasorelaxation than
do those drugs that require bioactivation in the tissue. The
long lasting inhibition of responses to vasoconstrictors by
S-nitrosothiols, persisting after removal of these NO donors,
may be a cGMP-independent process, at least in some vessels.
The mechanisms involved in the inhibition of vascular growth
by NO and NO donors are predominantly cGMP-independent, as
are the mechanisms responsible for the effects of NO donors
on apoptosis in vascular smooth muscle and endothelial cells.
The ability of NO and NO donors to inhibit platelet aggregation
has a significant cGMP-independent component. cGMP-independent
pathways are most often, though not exclusively, seen at high
concentrations (μM
- mM) of NO and NO donors. Hence, in relation to the actions
of endogenous NO, these pathways may be particularly important
in settings when the inducible isoform of NO-synthase is expressed.
Furthermore, cGMP-independent pathways are enhanced in animal
models of atherosclerosis and ischaemia. This suggests that
it may be possible to target cGMP-independent mechanisms with
selected NO donors in disease states.
[Back to top]
Transforming Growth Factor-β, Cell Signaling and Cardiovascular
Disorders
Alex Agrotis, Natalia Kalinina and Alex Bobik
[Full
text article]
Transforming growth factor-beta (TGF-β)
is a multifunctional growth factor with a wide range of potential
effects on growth, differentiation, extracellular matrix accumulation
and the immune system. It has been implicated in many cardiovascular
disorders. TGF-β’s
actions are mediated via a complex between its type
I and type II receptors resulting in the phosphorylation of
receptor-specific Smads followed by their passage to the nucleus
where they influence many transcriptional responses. TGF-β
has important roles in the development of the neointima and
constrictive remodeling associated with angioplasty. In atherosclerosis
its actions are yet to be fully elucidated but its ability
to control the immune system has profound effects on lesion
development, particularly by influencing the types of lesions
that develop. TGF-β
can also induce arteriogenesis and markedly influences angiogenic
processes, possessing both pro- and anti-angiogenic effects.
It is also a major contributor to the development of various
cardiovascular fibrotic disorders including those in the vasculature,
heart and kidney. Targeting TGF-β
prevents neointima formation and the constrictive remodeling
associated with angioplasty and also prevents the development
of many fibrotic disorders. This review summarizes TGF-β
signaling pathways, the mechanisms by which TGF-β
contributes to many of these cardiovascular diseases and examines
the therapeutic potential of targeting TGF-β
actions in preventing these disorders.
[Back to top]
Macrophage Activation in Atherosclerosis: Pathogenesis
and Pharmacology of Plaque Rupture
J.J. Boyle
[Full
text article]
Atherosclerosis is still an important disease. It accounts
for 39% of deaths in the U.K. and 12 million U.S citizens
have atherosclerosis-associated disease. Atherosclerosis may
exert clinical effects by slow narrowing, producing stable
angina or dramatic rupture, producing acute coronary syndromes
such as unstable angina or myocardial infarction and death.
Macrophages are abundant in ruptured atherosclerotic plaques.
Macrophages are innate immune effectors, i.e. they
are activated without antigenic specificity. This may make
them liable to indiscriminate tissue damage, since they are
less selective than lymphocytes. Macrophages are recruited
and activated by many signals and have an impressive armamentarium
of molecules to promote tissue damage. Macrophage recruitment
by abnormal endothelium over developing atherosclerotic plaques,
is aided by endothelial expression of adhesion molecules (ICAM-1,
VCAM, ELAM). Use of knockout mice has implicated the chemoattractant
cytokine (chemokine) MCP-1 in attracting macrophage recruitment
in atherosclerosis. Macrophage-activation stimuli associated
with atherosclerotic risk factors include oxidized low density
lipoprotein (oxLDL, ‘bad cholesterol’), advanced
glycosylation end products (AGEs) of diabetes, angiotensin
II and endothelin. Substantial work has clarified macrophage
activation by OxLDL via macrophage scavenger receptors (MSRs),
especially MSRA and CD36. Activated macrophages express effector
molecules that kill cells and degrade extracellular matrix.
These include Fas-L and nitric oxide (NO). Macrophage NO is
derived from the high output inducible nitric oxide synthase
(iNOS) pathway and upregulates vascular smooth muscle (VSMC)
cell surface Fas, priming them for apoptosis. Activated macrophages
express surface Fas-L, similar to cytotoxic T-lymphocytes
and natural killer cells. Since VSMCs promote plaque stability,
VSMC apoptosis may promote plaque rupture. Macrophages express
multiple metalloproteinases (e.g. stromelysin) and
serine proteases (e.g. urokinase) that degrade the
extracellular matrix, weakening the plaque and making it rupture
prone. Macrophages secrete numerous other effectors including
reactive oxygen species, eicosanoids, tumour necrosis factor
alpha and interleukin-1. Macrophage-derived transforming growth
factor beta promotes fibrosis. Existing cardiovascular treatments
including angiotensin II receptor antagonists and angiotensin
converting enzyme inhibitors, aspirin, cholesterol reduction
agents especially statins may inhibit macrophages. The interaction
of NO-donors with macrophages and apoptosis is complex and
bifunctional. Traditional anti-inflammatory agents such as
glucocorticoids and cyclophosphamide have very serious side
effects and are probably inappropriate. Novel anti-inflammatory
agents e.g. new immunosuppressives and anti-TNF therapy may
have an improved cost-benefit ratio.
[Back to top]
Modulation of Cardiovascular Remodeling with Statins: Fact
or Fiction?
Rajasekhar Reddy, Georges Chahoud and J.L. Mehta
[Full
text article]
The concept of cardiac remodeling implies a complex mixture
of myocardial ischemia, and increased wall stress that results
in molecular, cellular and interstitial changes in the heart.
Clinically, cardiac remodeling is manifested as a change in
size, shape and function of the heart. Morphologically the
key feature of remodeling is myocyte hypertrophy, myocyte
loss from necrosis or apoptosis, as well as interstitial cell
growth especially fibroblast proliferation leading to myocardial
fibrosis. Cardiac remodeling is influenced by hemodynamic
load, neurohumoral activation, and other factors that can
further affect the remodeling process. Despite advances in
the management of heart failure, morbidity and mortality still
present major health care issues in these patients. Statins
(HMG Coenzyme A reductase inhibitors) play a key role in the
management of ischemic heart disease. Recent studies indicate
that statins may modulate cardiac remodeling by affecting
signals that cause fibroblast growth, and myocyte hypertrophy
and loss. In this paper we review the mechanisms of cardiac
remodeling and the mechanisms of potential beneficial effects
of statins on cardiac remodeling.
[Back to top]
Role of Vascular Nitric Oxide in Experimental Liver Cirrhosis
Noemi M. Atucha, F. Javi A. Nadal, David Iyu,
Antonia Alcaraz, Alicia Rodriguez-Barbero, M. Clara Ortiz,
Jose Miguel Lopez-Novoa and Joaquin Garcia-Estan
[Full
text article]
One of the most important features of liver cirrhosis is
the splanchnic and systemic arterial vasodilation, related
to an increase in vascular capacity and an active vasodilation.
This arterial vasodilation seems to be the consequence of
the excessive generation of vasodilating substances, which
also contributes to a lower than normal pressor response to
circulating nervous or humoral substances. The following review
analyzes the mechanisms responsible for the vascular hyporesponse
to vasoconstrictors observed in the experimental models of
liver cirrhosis. It has become increasingly clear that, among
the great variety of substances studied, nitric oxide (NO)
seems to be one of the main contributors to this vascular
alteration, since elimination of the endothelium or inhibition
of its synthesis corrects it. The mechanism by which NO interferes
with the contractile apparatus in smooth muscle cells seems
to be related to a direct effect on calcium entry from the
extracellular space and release from the internal stores.
[Back to top]
Fenofibrate: Metabolic and Pleiotropic Effects
Vasilis Tsimihodimos, George Miltiadous, Stella
S. Daskalopoulou, Dimitri P. Mikhailidis and Moses S. Elisaf
[Full
text article]
Disturbances of lipoprotein metabolism represent one of the
most important risk factors for vascular events. However,
dyslipidaemic patients often have a number of additional abnormalities
(such as endothelial dysfunction, hypertension, low-grade
inflammation, haemostatic abnormalities and hyperuricaemia)
that may accelerate the atherosclerotic process. Thus, the
ideal lipid-modifying drug, along with exerting beneficial
effects on lipoprotein metabolism, should also improve these
coexisting disturbances.
Fibric acid derivatives (fibrates) are a class of lipid-modifying
drugs mainly used in patients with elevated triglyceride levels.
These drugs mainly exert their actions via the activation
of specific nuclear receptors called peroxisome proliferator-activated
receptors α
(PPARα).
In this review, we summarize the current evidence suggesting
that fenofibrate, one of the most widely used fibric acid
derivatives, along with its well established actions on lipids
also exerts several other antiatherogenic actions. Based on
recently published studies, fenofibrate is a useful option
for patients with primary combined dyslipidaemias or secondary
dyslipidaemias, such as those associated with diabetes mellitus,
metabolic syndrome or HIV infection. Additionally, in cases
of refractory dyslipidaemia, the combination of fenofibrate
with statins is a therapeutic option.
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