Current
Pharmaceutical Design
ISSN: 1381-6128
Current Pharmaceutical Design
Volume 13, Number 16, 2007
Contents
Modifying Coronary Risk Factors: C-Reactive Protein, Haemostatic
Factors and Cardiovascular Risk
Executive Editor: Aurelio Leone
Editorial: Pp. 1617-1618
C-Reactive Protein and Asymmetric Dimethylarginine:
Markers or Mediators in Cardiovascular Disorders?
Pp. 1619-1629
C.L. Smith
[Abstract]
C-Reactive Protein: Interaction with the Vascular
Endothelium and Possible Role in Human Atherosclerosis
Pp. 1631-1645
C. Ferri, G. Croce, V. Cofini, G. De Berardinis, D. Grassi,
R. Casale, G. Properzi and G. Desideri
[Abstract]
Fibrinogen: A Predictor of Vascular Disease
Pp. 1647-1659
A.I. Kakafika, E.N. Liberopoulos and D.P. Mikhailidis
[Abstract]
Smoking, Haemostatic Factors, and Cardiovascular Risk
Pp. 1661-1667
A. Leone
[Abstract]
Platelets and Vascular Risk: An Option for Treatment
Pp. 1669-1683
I.A. Jagroop, A.I. Kakafika and D.P. Mikhailidis
[Abstract]
Platelets in Atherothrombosis: New and Evolving Roles
Pp. 1685-1691
A. Weyrich, F. Cipollone, A. Mezzetti and G. Zimmerman
[Abstract]
C-Reactive Protein and Hypertension: Is there A Causal
Relationship? Pp. 1693-1698
A. Virdis, L. Ghiadoni, Y. Plantinga, S. Taddei and A.
Salvetti
[Abstract]
Circulating Endothelial Progenitor Cells Characterization,
Function and Relationship with Cardiovascular Risk Factors
Pp. 1699-1713
A. Balbarini, M.C. Barsotti, R. Di Stefano, A. Leone and
T. Santoni
[Abstract]
COX-2: Friend or Foe? Pp. 1715-1721
A. Iezzi, C. Ferri, A. Mezzetti and F. Cipollone
[Abstract]
Abstracts
[Back to top]
Editorial: Modifying Coronary Risk Factors: C-Reactive
Protein, Haemostatic Factors and Cardiovascular Risk
There has been conflicting debate about the relationship among
those parameters which are generally involved in cardiovascular
events such as C-Reactive Protein, haemostatic factors and
other major cardiovascular risk factors. The debate seems
to be a result for establishing the exact mechanisms of cardiovascular
damage, that is believed to be due to either a direct action
on coagulation/fibrinolysis cascade components either a consequence
of interaction between haemostatic factors, inflammatory factors
and the other cardiovascular risk factors.
Cardiovascular damage expresses itself mainly as thromboembolic
damage because of structural and biochemical components of
coagulation/fibrinolysis cascade involved.
Clot formation and lysis involve a large series of structures
at different levels: vascular level, cellular level, and plasmatic
level. Physiologically, the whole mechanism is directed to
stop haemorrhage and keep vessel lumen patency. Damage at
any of these levels may cause alterations potentially harmful
against cardiovascular system.
After a vasoconstriction following a stimulus of different
types, endothelium is the first structure involved in coagulation/
fibrinolysis cascade.
If the endothelium is intact, physiological stimulation not
only causes vessel vasodilation, but also protects the vessel
wall against the development of atherosclerosis and thrombotic
vascular events. On the contrary, in presence of endothelial
damage and/or dysfunction a series of occurrences produced
by biochemical factors activates platelets (cellular level)
that increase their secretion, adhesiveness, and aggregation
initiating those processes that, in case of pathological response,
may lead to thrombi formation. Plasmatic factors (plasmatic
level) mainly fibrinogen and fibrin, together a reduced activity
of plasminogen activators, impair further the phenomenon.
The interference with other cardiovascular risk factors increases
heavily the appearance of cardiovascular events by a complex
series of chemical, biological, and inflammatory mechanisms,
the exact action of which has yet to be clarified. However,
C-Reactive Protein and haemostatic system alterations play
a fundamental part in causing cardiovascular events.
The paper of Carolyn Smith from London [1] underlines the
role of ADMA as a mediator of cardiovascular disorders as
well as its relationship with C-reactive protein.
The complex interaction between C-reactive protein with the
vascular endothelium is widely discussed by Claudio Ferri
and Coworkers [2] from the University of L’Aquila, Italy.
Human atherosclerosis is characterized by a multifactorial
etiology, but endothelial dysfunction has a significant role
in determining the appearance of atherosclerotic alterations.
Among haemostatic factors, three papers [3-5] discuss the
role of fibrinogen as a predictor of vascular disease, the
interference of smoking with coagulation-fibrinolysis cascade,
and the mechanisms by which platelets may be related to cardiovascular
risk as well as those measures able to prevent cardiovascular
damage. Moreover, the new role played by platelets in atherothrombosis
is widely discussed by Weyrich and Coworkers [6].
The relationship between C-reactive protein and hypertension
[7] is discussed by Virdis and Coworkers of Pisa, Italy. Nowdays,
there is no clear evidence of a strong link between those
two factors.
An emerging role to explain many hypotheses of cardiovascular
risk seems to be due to the knowledge of the circulating endothelial
progenitor cells. The paper of Balbarini and Co-workers [8]
clarifies the physiologic characteristics of the circulating
endothelial progenitor cells as well as their relationship
with cardiovascular risk.
Finally, an overview of the relevant biology and pharmacology
of COX 2 in atherosclerosis [9] is assessed in the paper of
Iezzi and Coworkers from Chieti and L’Aquila, Italy.
The articles in this issue provide a current summary to how
understand the mechanisms and interactions of the main cardiovascular
risk factors with C-Reactive Protein and some haemostatic
system components, analysing the newest knowledges yet under
study. Therefore, I believe that the present issue can up
to date researchers, physicians, and also students on the
state of art of a subject that is continuously in growth.
References
[1] Smith C. C-reactive protein and asymmetric dimethylarginine:
markers or mediators in cardiovascular disorders ? Curr Pharm
Des 2007; 13(16): 1619-1629.
[2] Ferri C, Croce G, Cofini V, De Berardinis G, Grassi D,
Casale R, et al. C-reactive protein. Interaction
with the vascular endothelium and possible role in human atherosclerosis.
Curr Pharm Des 2007; 13(16): 1631-1645.
[3] Kakafika AI, Liberopoulos EN, Mikhailidis DP. Fibrinogen
: a predictor of vascular disease. Curr Pharm Des 2007; 13(16):
1647-1659.
[4] Leone A. Smoking, haemostatic factors, and cardiovascular
risk. Curr Pharm Des 2007; 13(16): 1661-1667.
[5] Jagroop JA, Kakafika AI, Mikhailidis DP. Platelets and
cardiovascular risk: an option for treatment. Curr Pharm Des
2007; 13(16): 1669-1683.
[6] Weyrich A, Cipollone F, Mezzetti A, Zimmerman G. Platelets
in atherothrombosis: new and evolvine role. Curr Pharm Des
2007; 13(16): 1685-1691.
[7] Virdis A, Ghiadoni L, Plantinga Y, Taddei S, Salvetti
A. C-reactive protein and hypertension: is there a causal
relationship? Curr Pharm Des 2007; 13(16): 1693-1698.
[8] Balbarini A, Barsotti MC, Di Stefano R, Leone A, Santoni
T. Circulating endothelial progenitor cells . Characterization,
function and relationship with cardiovascular risk factors.
Curr Pharm Des 2007; 13(16): 1699-1713.
[9] Iezzi A, Ferri C , Mezzetti A, Cipollone F. Cox-2: Friend
or foe? Curr Pharm Des 2007; 13(16): 1715-1721.
Aurelio Leone, MD Chief
Former Director Department of Internal Medicine
City Hospitals Massa and Carrara, Italy
Consultant Cardiologist at the Cardio-thoracic Department
University of Pisa, Italy
Fellow of the Royal Society for Promotion of Health, UK
Member of the American Society of Hypertension, American
Society of Geriatric Cardiology, and World Heart Federation
Via Provinciale 27
19030 Castelnuovo Magra SSP
Italy
[Back to top]
C-Reactive Protein and Asymmetric Dimethylarginine:
Markers or Mediators in Cardiovascular Disorders?
C.L. Smith
C-reactive protein (CRP) has received much attention as a
cardiovascular risk factor and has been recommended to be
used in screening to assist in predicting the occurrence of
cardiovascular disorders. There are numerous association studies
documenting changes in circulating CRP concentrations, there
are, however, fewer studies providing evidence that CRP mediates
the progression of cardiovascular pathologies. Elucidating
the potential mechanisms for CRP has been confounded by recent
reports that contaminants of CRP are partially responsible
for observed effects.
In this review the use of CRP as a tool to predict cardiovascular
disorders will be discussed alongside a more recently described
cardio-vascular risk factor asymmetric dimethylarginine (ADMA).
An endogenously occurring nitric oxide synthase inhibitor,
ADMA, is formed by the action of protein arginine methyltransferases
and subsequent proteolysis and it is metabolised in vivo
by the dimethylarginine dimethylaminohydrolases (DDAH). The
evidence available documenting the effects of CRP and ADMA,
the regulatory mechanisms and the genetic influences, will
be discussed in order to determine whether CRP and ADMA are
mediators in the progression of cardiovascular disorders or
merely useful biomarkers.
[Back to top]
C-Reactive Protein: Interaction with the Vascular
Endothelium and Possible Role in Human Atherosclerosis
C. Ferri, G. Croce, V. Cofini, G. De Berardinis, D. Grassi,
R. Casale, G. Properzi and G. Desideri
C-reactive protein (CRP) is the first acute phase protein
that has been described in the literature. It is phylogenetically
ancient and - with serum amyloid P - belongs to proteins named
as “pentraxin”. After being considered a marker
of acute inflammation for several decades and fruitfully used
in clinical practice, CRP has been recently considered as
a potential contributor to inflammatory diseases including
atherosclerosis as well as a marker of cardiovascular risk.
With regard to the first topic, inflammation is now believed
to represent the underlying mechanism leading to the formation
of human atheroma and favouring both the destabilization of
vulnerable plaques and the formation of occlusive thrombi.
In this regard, numerous studies indicated that modest changes
in circulating CRP levels, as detected by highly sensitive
methods, can be extremely useful in predicting cardiovascular
and perhaps cerebrovascular diseases in apparently healthy
individuals as well as in patients affected by atherosclerosis.
Subjects manifesting with identical low density cholesterol
and/or blood pressure levels have different rates of cardiovascular
accidents on the basis of different circulating CRP concentrations.
In addition, women with identical cardiovascular risk profiles
developed more type 2 diabetes in the presence of higher circulating
CRP levels and thereby are expected to display divergent cardiovascular
prognosis. Therefore, even slight changes in circulating CRP
concentrations – assuming that blood is collected appropriately
and CRP is measured with correct methods – could help
clinicians in defining individual cardiovascular risk.
In this review, we have firstly described the current understanding
of the structure of CRP, its function, and interaction with
the vascular endothelial cell. Then, we have discussed how
to measure circulating CRP and the more recent findings on
the suggested role of circulating CRP as a novel cardiovascular
risk factor.
[Back to top]
Fibrinogen: A Predictor of Vascular Disease
A.I. Kakafika, E.N. Liberopoulos and D.P. Mikhailidis
Raised plasma fibrinogen levels are associated with an increased
risk of vascular events. This may be mediated by adverse effects
of fibrinogen on plasma viscosity, coagulation, platelet activity,
inflammation and atherogenesis. However, there is as yet no
drug that specifically lowers plasma fibrinogen levels on
a long-term basis. Thus, we do not have intervention trials
demonstrating that lowering plasma fibrinogen levels will
result in a decreased risk of vascular events. However, such
a trial may never happen unless a specific agent is discovered
or designed.
Several drugs that are used in vascular disease prevention
(e.g. lipid lowering agents and antihypertensives) may influence
plasma fibrinogen levels. Whether such an additional effect
accounts for variations in the benefit resulting from the
use of different drugs within the same class remains to be
established.
The debate continues as to whether fibrinogen is just a marker
of vascular risk or whether lowering its circulating levels
will result in a significant decrease in clinically relevant
endpoints. Whatever the case, the measurement of plasma fibrinogen
levels is likely to provide a more comprehensive estimation
of risk.
[Back to top]
Smoking, Haemostatic Factors, and Cardiovascular Risk
A. Leone
There is a strong relationship between cigarette smoking and
haemostatic parameters to increase the risk of cardiovascular
events.
Smoking influences negatively coagulation-fibrinolysis cascade
at any level, although it acts primarily on those pathways
that are most important for an effective clot formation: endothelium,
platelets, and fibrinogen.
Endothelial dysfunction is a main consequence of smoke compounds
with significant changes in initiating physiologic coagulation
proc-ess; platelet adhesiveness and aggregation increases
as a result of smoking; finally, fibrinogen/fibrin framework
strengthens clot thick-ness. Therefore, the whole coagulation
cascade activates the thrombi formation pathway under smoking
action. The risk of thrombotic cardiovascular events increases
its frequency with more severe atherosclerotic alterations
if compared to similar events in nonsmokers.
Changes in haemostatic factors produced by smoking appear
to be related to female sex, especially for those women who
use oral contra-ceptives. Thrombosis of coronary and cerebral
arteries are found with a major incidence in young women who
are users.
In conclusion, cigarette smoking modifies haemostatic parameters
via thrombosis with consequently more rate of cardiovascular
events.
[Back to top]
Platelets and Vascular Risk: An Option for Treatment
I.A. Jagroop, A.I. Kakafika and D.P. Mikhailidis
Epidemiological studies have linked platelet hyperactivity
with an increased risk of vascular events. Even more convincing
is the evidence from appropriately designed clinical trials
showing that antiplatelet agents decrease the risk of vascular
events (e.g. myocardial infarction, MI and stroke). These
findings are compatible with the known thrombotic action of
platelets.
A considerable limitation in platelet research is the absence
of a reliable, universally accepted marker of platelet activity.
Therefore, it is difficult to reliably identify the ‘high
risk patient’ and/or evaluate the efficacy of any administered
treatment other than by calculating event rates over a period
of time.
This review will focus on the preventive aspects of antiplatelet
intervention while also briefly considering the assessment
of platelet hyperactivity and the mechanisms involved in platelet-induced
thrombosis.
[Back to top]
Platelets in Atherothrombosis: New and Evolving Roles
A. Weyrich, F. Cipollone, A. Mezzetti and G. Zimmerman
The functional interplay of platelets with leukocytes and
endothelial cells is critical both in physiological conditions,
such as host defense, wound repair and tissue healing, and
in pathological conditions, such as thrombotic and inflammatory
diseases. The understanding of the specific molecular links
underlying these cellular interactions and the functional
changes that they induce could suggest new targets for pharmacological
intervention. In this review, we summarize some of the newly-recognized
aspects of interaction between platelets and monocytes, neutrophils
and endothelial cells, that are relevant to all of the phases
of atherosclerosis progression, since the early steps of atherogenesis
to plaque rupture and thrombosis, the main causes of acute
coronary syndromes.
[Back to top]
C-Reactive Protein and Hypertension: Is there A Causal
Relationship?
A. Virdis, L. Ghiadoni, Y. Plantinga, S. Taddei and A.
Salvetti
There is a large body of evidence indicating that inflammation
plays a crucial role in all steps characterizing the atherosclerotic
process. C-Reactive Protein is a circulating marker of inflammation
which recently emerged as a powerful independent determinant
of cardiovascular events. Hypertension is closely linked to
inflammation. Experimental data and results from cross-sectional
studies in humans indicate a relationship between CRP levels
and blood pressure. In particular, CRP seems to be related
with markers of arterial stiff-ness, thus suggesting a specific
interaction between CRP and systolic blood pressure. However,
such observational studies cannot provide any direct evidence
for a cause-effect relation. Prospective studies are likely
candidates to better define the putative causal relationship
on this association. Available results from longitudinal studies
are scanty, and do not allow to draw definitive conclusions.
Moreover, prospective, placebo-controlled intervention trials
documenting that reduction of CRP levels by pharmacological
treatment might lead to a reduced risk to develop hypertension
are not yet available. Without such crucial information, at
the present time the causal connection between inflammation
and blood pressure, although regarded as an intriguing possibility,
remains undiscovered.
[Back to top]
Circulating Endothelial Progenitor Cells Characterization,
Function and Relationship with Cardiovascular Risk Factors
A. Balbarini, M.C. Barsotti, R. Di Stefano, A. Leone and
T. Santoni
Since the first description of putative progenitor endothelial
cells mobilized from bone marrow by stimuli like ischemia
and cytokines, several studies in animals have confirmed their
role in neovascularization of ischemic organs. In ischemic
myocardium endothelial progenitor cells can prevent cardiomyocyte
apoptosis, reduce remodeling and improve cardiac function.
These observations led to the hypothesis of endothelial progenitor
cells as possible cell-based therapy in patients by autologous
transplantation in ischemic tissue or by improving peripheral
circulating numbers with mobilization by cytokines.
Early trials, including a randomized one, suggest that the
intracoronary autologous bone marrow cell transfer after myocardial
infarction exerts at least short term functional benefits.
Since endothelial damage and dysfunction play a critical role
in atherosclerosis disease, research interest was addressed
to evaluate the role of progenitor endothelial cells in vascular
endothelial layer maintenance. Opposing to local resident
endothelial cells poor proliferate rate, progenitor endothelial
cells regenerative capacity, homing and integration into blood
vessels have been interpreted as a protective role of these
cells in vascular homeostasis.
Indeed, the number and function of endothelial progenitor
cells relate with the progression of atherosclerosis; the
accumulation of cardiovascular risk factors or an increased
overall risk are inversely associated with endothelial progenitor
cells number and function.
Finally, recent studies have shown a role of progenitor cells
numbers to predict cardiovascular events, raising endothelial
progenitor cells to the podium of novel prognostic biomarker.
[Back to top]
COX-2: Friend or Foe?
A. Iezzi, C. Ferri, A. Mezzetti and F. Cipollone
It wasn't until 1990, when the existence of two different
cyclooxygenases was hypothesized, based on the evidence that
steroids inhibited the increase in COX activity induced by
bacterial lipopolysaccharides in macrophages, without any
effects on the basal production of prostaglandins or leukotrienes.
The first isoform, COX-1 is responsible for the production
of "housekeeping" prostaglandins critical to the
maintenance of normal renal function, gastric mucosal integrity,
platelet aggregation, and the autocrine response to circulating
hormones. COX-2 on the other hand is an inducible enzyme,
upregulated 20-fold in macrophages, monocytes, synoviocytes,
chondrocytes, fibroblasts, osteoblasts and endothelial cells
by various inflammatory stimuli and cytochines. Classical
findings shown that the therapeutics effects of NSAIDs are
largely dependent on COX-2 inhibition, whereas some undesirable
side effects are bound to COX-1 blockade, such as gastrointestinal
bleeding and renal failure. Therefore, agents that selectively
inhibit COX-2 over COX-1 are desirable for the treatment of
inflammation. However, since September 2004 reports of increased
risk of thrombotic cardiovascular events had accumulated for
coxibs, the COX-2 inhibitors. Our goal is to provide an overview
of the relevant biology and pharmacology of this enzyme in
atherosclerosis.
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