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Current
Pharmaceutical Design
ISSN: 1381-6128
Current Pharmaceutical Design
Volume 13, Number 36, 2007
Contents
Immune-Mediated Mechanisms in Atheroclerosis: Prevention
and Treatment of Clinical Manifestations
Executive Editor: Emilio Jirillo
Editorial Pp. 3648
Inflammation in Fish As Seen from A Morphological
Point of View with Special Reference to the Vascular Compartment
Pp. 3649-3655
E.O. Koppang, U. Fischer, M. Satoh and E. Jirillo
[Abstract]
Hereditary Haemorrhagic Telangiectasia: A Rare Disease
As A Model for the Study of Human Atherosclerosis
Pp. 3656-3664
G.M. Lenato, P. Suppressa, P. Giordano, G. Guanti, E.
Guastamacchia, V. Triggiani, L. Amati, F. Resta, V. Covelli,
E. Jirillo and C. Sabbà
[Abstract]
Porphyromonas Gingivalis Mediated Periodontal Disease
and Atherosclerosis: Disparate Diseases with Commonalities
in Pathogenesis Through TLRs Pp. 3665-3675
F.C. Gibson III and C.A. Genco
[Abstract]
Leptin and Adipocytokines: Bridging the Gap Between
Immunity and Atherosclerosis Pp. 3676-3680
G. Matarese, C. Mantzoros and A. La Cava
[Abstract]
Advanced Glycation: A Novel Outlook on Atherosclerosis
Pp. 3681-3687
C.L. Price and S.C. Knight
[Abstract]
Non Enzymatic Glycated Proteins in the Blood and Cardiovascular
Disease Pp. 3688-3695
G. Misciagna, G. De Michele and M. Trevisan
[Abstract]
Early Pathogenesis of Atherosclerosis: The Childhood
Obesity Pp. 3696-3700
L. Amati, M. Chiloiro, E. Jirillo and V. Covelli
[Abstract]
Immune-Mediated Mechanisms in Atherosclerosis: Prevention
and Treatment of Clinical Manifestations Pp. 3701-3710
J.J. Goronzy, C.M. Weyand and A. Niessner
[Abstract]
Immunological Properties of Donkey’s Milk: Its
Potential Use in the Prevention of Atherosclerosis
Pp. 3711-3717
A. Tafaro, T. Magrone, F. Jirillo, G. Martemucci, A.G.
D’Alessandro, L. Amati and E. Jirillo
[Abstract]
Red Wine Consumption and Prevention of Atherosclerosis: An
In Vitro Model Using Human Peripheral Blood Mononuclear
Cells Pp. 3718-3725
T. Magrone, A. Tafaro, F. Jirillo, M.A. Panaro, P. Cuzzuol,
A.C. Cuzzuol, V. Pugliese, L. Amati, E. Jirillo and V. Covelli
[Abstract]
Pharmacogenomics: A Tool to Prevent and Cure Coronary
Heart Disease Pp. 3726-3734
G. Candore, C.R. Balistreri, M. Caruso, M.P. Grimaldi,
E. Incalcaterra, F. Listì, S. Vasto and C. Caruso
[Abstract]
Abstracts
[Back to top]
Editorial: Immune-Mediated Mechanisms
in Atheroclerosis: Prevention and Treatment of Clinical Manifestations
Atherosclerosis is a disease of multifactorial origin which
represents a major global cause of morbidity and mortality.
The presence of macrophages, as a major cell-type, in the
atheromatous plaque and the role played by Toll-like receptors
(TLRs) in its pathogenesis clearly support a robust immunological
involvement in this disease.
On these grounds, the present issue of Current Pharmaceutical
Design, entitled: “Immune-Mediated Mechanisms in Atherosclerosis:
Prevention and Treatment of Clinical Manifestations”
will place emphasis on animal and human models of atherosclerosis,
pathogenesis and clinical aspects, potential new drug targets
and pharmacogenomics.
Koppang and associates [1] will present, as an animal model
of atherosclerosis, some immunophatological pictures of coronary
disease in salmon which resemble those observed in humans.
Lenato and associates [2] will describe some immune abnormalities
found in hereditary haemorrahagic teleangiectasia, an autosomal
dominant disease, and its relationship with atherosclerosis.
Gibson and Genco [3] will demonstrate that Porphyromonas
gingivalis accelerates atherosclerosis in hyperlipidemic
mice and immunization is effective in the prevention of pathogen-induced
atherosclerosis.
Matarese and associates [4] will review the most recent advances
on adipokine research and the link with atherosclerosis as
an effect of low degree chronic inflammation typical of obesity
and metabolic syndrome.
Price and Knight [5] will illustrate the roles played by glycated
proteins in atherosclerosis development through receptor-mediated
release of progression factors, especially in diabetes.
Misciagna and associates [6] will point out that non enzymatic
glycation of protein in the blood is associated with cardiovascular
disease also in non diabetic subjects, and could be used to
define risk factors of cardiovascular disease.
Amati and associates [7] will describe the immune bases of
obesity and its prevention in order to reduce more serious
complications in adulthood, even including atherosclerosis
development.
Niessner and associates [8] will discuss on the main therapeutic
approaches to atherosclerosis, such as (1) immunomodulatory
effects of existing therapies, (2) therapies targeting inflammatory
triggers, and (3) agents inhibiting specific immune mechanisms.
Tafaro and associates [9] will place emphasis on the effects
on colostrum and milk from donkey on human peripheral blood
mononuclear cells (PBMCs) and its use in the prevention of
atherosclerosis.
Magrone and associates [10] will demonstrate that a moderate
assumption of red wine, as in vitro evaluated on human PBMCs,
leads to a robust production of nitric oxide useful in the
prevention of atherosclerosis.
Candore and associates [11] will illustrate the application
of pharmacogenomics in the prevention and cure of coronary
heart disease, mostly, in terms of early identification of
individuals susceptible to disease and discovery of potential
targets for drugs.
References
[1] Koppang EO, Fischer U, Satoh M, Jirillo E. Inflammation
in fish as seen from a morphological point of view with special
reference to the vascular compartment. Curr Pharm Des 2007;
13(36): 3649-3655.
[2] Lenato GM, Soppressa P, Giordano P, Guanti G, Guastamacchia
E, Triggiani V, Amati L, Resta F, Covelli V, Jirillo E, Sabbà
C. Hereditary Haemorrhagic Teleangiectasia: a rare disease
as a model for the study of human atherosclerosis. Curr Pharm
Des 2007; 13(36): 3656-3664.
[3] Gibson III FC, Genco CA. Porphyromonas gingivalis
mediated periodontal disease and atherosclerosis: disparate
diseases with commonalities in pathogenesis through TLRs.
Curr Pharm Des 2007; 13(36): 3665-3675.
[4] Matarese G, Mantzoros C, La Cava A. Leptin and adipocytokines:
bridging the gap between immunity and atherosclerosis. Curr
Pharm Des 2007; 13(36): 3676-3680.
[5] Price CL, Knight SC. Advanced glycation: a novel outlook
on atherosclerosis. Curr Pharm Des 2007; 13(36): 3681-3687.
[6] Misciagna G, De Michele G, Trevisan M. Non enzymatic proteins
in the blood and cardiovascular disease. Curr Pharm Des 2007;
13(36): 3688-3695.
[7] Amati L, Chiloiro M, Covelli V. Early pathogenesis of
atherosclerosis: the childhood obesity. Curr Pharm Des 2007;
13(36): 3696-3700.
[8] Goronzy JJ, Weyand CM, Niessner A. Immune-mediated mechanisms
in atherosclerosis: prevention and treatment of clinical manifestations.
Curr Pharm Des 2007; 13(36): 3701-3710.
[9] Tafaro A, Magrone T, Jirillo F, Martemucci G, D’Alessandro
AG, Amati L, Jirillo E. Immunological properties of donkey’s
milk: its potential use in the prevention of atherosclerosis.
Curr Pharm Des 2007; 13(36): 3711-3717.
[10] Magrone T, Tafaro A, Jirillo F, Panaro MA, Cuzzuol P,
Cuzzuol AC, Pugliese V, Amati L, Jirillo E, Covelli V. Red
wine and prevention of atherosclerosis: an in vitro model
using human peripheral blood mononuclear cells. Curr Pharm
Des 2007; 13(36): 3718-3725.
[11] Candore G, Balistreri CR, Caruso M, Grimaldi MP, Incalcaterra
E, Listì F, Vasto S, Caruso C. Pharmacogenomics: a
tool to prevent and cure coronary heart disease. Curr Pharm
Des 2007; 13(36): 3726-3734.
Emilio Jirillo
University of Bari and IRCCS “ De Bellis”
Castellana Grotte, Bari
Italy
[Back to top]
Inflammation in Fish As Seen from A Morphological Point of
View with Special Reference to the Vascular Compartment
E.O. Koppang, U. Fischer, M. Satoh and E. Jirillo
Modern bony fishes or teleosts are increasingly being
used as model organisms for human diseases. Ambitious mapping
pro-grammes have revealed parts of or entire genomes of several
species. This information suggests that there are several
similarities between the mammalian and teleost immune systems,
but also important differences. These differences are especially
evident in the anatomical and functional constructions. However,
compared to mammals, morphological studies of the immune system
and in particular the inflammatory responses in fish are scarce,
much due to a general lack of good cell markers. This review
seeks to give an overview of the current knowledge of the
teleost immune system related to inflammation and morphological
research. The emphasis is placed on coronary changes which
may be observed in salmonids over the size of 10 cm. Here,
the immunopathological picture has some resemblance to that
observed in similar changes in humans.
[Back to top]
Hereditary Haemorrhagic Telangiectasia: A Rare Disease As
A Model for the Study of Human Atherosclerosis
G.M. Lenato, P. Suppressa, P. Giordano, G. Guanti, E.
Guastamacchia, V. Triggiani, L. Amati, F. Resta, V. Covelli,
E. Jirillo and C. Sabbà
Hereditary Haemorrhagic Telangiectasia (HHT) or Rendu-Osler-Weber
syndrome is an autosomal dominant disease character-ized by
local angiodysplasia affecting different organism districts.
From a clinical viewpoint, HHT patients suffer from epistaxis,
mucocutaneous telangiectases and arteriovenous malformations
in various organs. Mutations in two known genes (ENG and ALK1)
account for the majority of HHT patients. Additional loci
are predicted, but the underlying genes are still to be identified.
Moreover, SMAD4 mutations have been reported to cause JP-HHT
combined syndrome.
Both endoglin and ALK-1 bind to various growth factors in
the context of the Transforming Growth Factors (TGF)-β
superfamily and their expression is restricted to vascular
endothelial cells and very few other cell types, such as activated
monocytes. Endoglin and ALK1 mutations are thought to affect
endothelial cell metabolism, angiogenesis and vascular remodelling,
even if the precise mechanism leading to the HHT lesions is
still obscure. Endoglin is also overexpressed in smooth muscle
cells of atherosclerotic plaques, suggesting a role for this
protein in atherogenesis and plaque progression, as well as
in other cardiovascular diseases. Recently, we demonstrated
that HHT adult patients display several deficits of both innate
and adaptive immune system. Here, we investigated the function
of immune cells in HHT pediatric patients. Our results clearly
show that HHT children have a normal functionally immune system,
and suggest that HHT patients become immunocompromised host
during their lifetime, likely due to a precocious immunosenescence.
Moreover, the relationship between immune responsiveness in
HHT and atherosclerosis are discussed.
[Back to top]
Porphyromonas Gingivalis Mediated Periodontal Disease and
Atherosclerosis: Disparate Diseases with Commonalities in
Pathogenesis Through TLRs
F.C. Gibson III and C.A. Genco
Toll-like receptors (TLRs) are a group of pathogen-associated
molecular pattern receptors, which play an important role
in in-nate immune signaling in response to microbial infection.
It has been demonstrated that TLRs are differentially up regulated
in response to microbial infection and chronic inflammatory
diseases such as atherosclerosis. Furthermore hyperlipidemic
mice deficient in TLR2, TLR4, and MyD88 signaling exhibit
diminished inflammatory responses and decreased atherosclerosis.
Accumulating evidence has implicated specific infectious agents
including the periodontal disease pathogen Porphyromonas
gingivalis in the progression of atherosclerosis. Evidence
in humans suggesting that periodontal infection predisposes
to atherosclerosis is derived from studies demonstrating that
the periodontal pathogen P. gingivalis resides in
the wall of atherosclerotic vessels and seroepidemiological
studies demonstrating an association between pathogen-specific
IgG antibodies and atherosclerosis. We have established that
the inflammatory signaling pathways that P. gingivalis
utilizes is dependent on the cell type and this specificity
clearly influences innate immune signaling in the context
of local and distant chronic inflammation induced by this
pathogen. We have demonstrated that P. gingivalis
requires TLR2 to induce oral in-flammatory bone lose in mice.
Furthermore, we have demonstrated that P. gingivalis
infection accelerates atherosclerosis in hyperlipidemic mice
with an associated increase in expression of TLR2 and TLR4
in atherosclerotic lesions. Our recent work with P. gingivalis
has demonstrated the effectiveness of specific intervention
strategies (immunization) in the prevention of pathogen-accelerated
atherosclerosis. Improved understanding of the mechanisms
driving infection, and chronic inflammation during atherosclerosis
may ultimately provide new targets for therapy.
[Back to top]
Leptin and Adipocytokines: Bridging the Gap Between Immunity
and Atherosclerosis
G. Matarese, C. Mantzoros and A. La Cava
The role of the adipose tissue in immunity has recently
emerged, and there is now ample evidence that this role is
elucidated by a number of cytokine-like hormones produced
by adipocytes – called adipokines. The most relevant
adipokines are leptin, adiponectin and visfatin, and all have
marked effects on metabolic and immune function. The discovery
of adipokines has led to the development of a novel concept
that the pathogenesis of atherosclerosis can be associated
with low-degree inflammation associated with slow (auto)immune
attack of the endothelial wall of arteries. This model considers
therefore adipokines as the bridge between atherosclerosis,
inflammation and immunity. We review here the most recent
advances on adipokine research, with a particular emphasis
on the model that considers atherosclerotic lesions as effects
of the (auto)immune-mediated damage of the endothelium that
is sustained by low-degree chronic inflammation typical of
obesity and metabolic syndrome.
[Back to top]
Advanced Glycation: A Novel Outlook on Atherosclerosis
C.L. Price and S.C. Knight
Atherosclerosis is a major global cause of morbidity
and mortality, and diabetes patients are at increased risk
of coronary heart disease development. Advanced glycation
of proteins occurs in the body due to raised concentrations
of reducing sugars and reactive oxygen species, and is a causal
factor behind complications of diabetes. Glycated proteins,
through alteration of protein structure and function, and
from ligation with their receptors, lead to widespread vascular
damage. The α-oxoaldehyde,
methylglyoxal (MG) is the most reactive glycation precursor,
and is increased in the blood of diabetes patients. There
is debate about the triggering events leading to atherosclerosis,
but the inflammatory action of glycated proteins, including
those with MG adducts, through their receptor, RAGE, is a
major candidate for initiating plaque formation. In addition
glycation may cause cross-links on proteins of the extracellular
matrix, stiffening arteries and ‘trapping’ other
macromolecules. MG is also likely to form adducts on many
other proteins, enzymes, lipids, DNA or RNA, changing their
structure, and may disrupt enzyme activity, hormone regulation
and immune function. In the latter context, MG disrupts function
of the potent antigen presenting cells, dendritic cells. This
effect may be a double edged sword: Poor control of infections
may contribute to persistent inflammation, whilst inhibition
of immune activation by dendritic cells may inhibit plaque
progression. This review aims to present these ideas as a
novel slant on the role of the glycation process in atherosclerosis.
[Back to top]
Non Enzymatic Glycated Proteins in the Blood and Cardiovascular
Disease
G. Misciagna, G. De Michele and M. Trevisan
The study of the role of glycemia in the causation of
cardiovascular disease has been limited by several factors,
above all by its measurement over time. Non enzymatic glycated
proteins in the blood, the product of the non enzymatic reaction
of a reducing sugar with the reactive amino acid of a target
protein, are an integrated measure of blood glucose over days
to weeks. They have been used in the management of clinical
diabetes mellitus, but are still infrequently used in epidemiological
studies in non diabetic subjects. There are few epidemiological
studies that show that glycated hemoglobin, fructosamine,
an index of total non enzymatic glycated proteins in the blood,
and glycated apolipoprotein B and other non enzymatic glycated
proteins in the blood in non diabetic subjects are associated
with cardiovascular diseases. In this paper we review: 1)
the overall mechanisms of non enzymatic glycation of proteins;
2) the measurement of glycated hemoglobin, fructosamine, and
glycated apolipoprotein B and their relationship with blood
glucose levels in non diabetic subjects; 3) the association
of glycated hemoglobin, fructosamine and glycated apolipoprotein
B with cardiovascular disease. We conclude that non enzymatic
glycation of protein in the blood is associated with cardiovascular
disease also in non diabetic subjects, and could be used to
define dietary risk factors of cardiovascular disease.
[Back to top]
Early Pathogenesis of Atherosclerosis: The Childhood Obesity
L. Amati, M. Chiloiro, E. Jirillo and V. Covelli
Obesity represents a chronic inflammatory status and
adipocytes release either cytokines or an array of adipokines
such as leptin, endowed with immunomodulating and systemic
activities. The involvement of cytokines in obesity as well
as of the adipokine leptin is supported by the notion that
weight reduction normalizes mediators of inflammation.
In this framework, we will demonstrate that in obese children,
subjected for a period of six months to a hypocaloric diet,
reduction of major biochemical and anthropometric parameters
correlates with a normalization of immune status. Infact,
absolute numbers of CD4+ cells and CD4/CD8 ratio increase,
while leptin values fluctuate within normal ranges, being
this adipokine involved in the modulation of either innate
or adaptive immune responses.
In the discussion, the immune abnormalities detected in obesity
will be pointed out and emphasis will be placed on the increased
frequency of infectious episodes occurring in obese adolescent
and adults. Finally, the infectious etiology of obesity will
be illustrated in the sense that adipocytes interacting with
infectious agents may cause obesity.
Taken together, the bulk of available data indicate that childhood
obesity should be prevented or reduced to avoid more serious
complications in adulthood.
[Back to top]
Immune-Mediated Mechanisms in Atherosclerosis: Prevention
and Treatment of Clinical Manifestations
J.J. Goronzy, C.M. Weyand and A. Niessner
Accumulation of inflammatory cells identifies atherosclerotic
plaque at risk for rupture. Typically, activated immune cells
oc-cupy the rupture-prone areas of the atherosclerotic lesion.
These cells are an appealing therapeutic target for novel
strategies of plaque stabilization. Biologic consequences
of plaque inflammation ultimately depend not only on the cellular
players populating the lesion but also on triggers of immune
activation originating from within the plaque or arriving
from the circulation, and immune effector mechanisms that
mediate cellular damage and plaque destabilization. Recent
studies have provided insights into particular immune mechanisms
in the atherosclerotic plaque that contribute to plaque vulnerability.
This knowledge provides the basis for potential immunomodulatory
therapies in cardiovascular disease. These therapeutic approaches
can be classified as (1) immunomodulatory effects of existing
therapies, (2) therapies targeting inflammatory triggers,
and (3) agents inhibiting specific immune mechanisms.
[Back to top]
Immunological Properties of Donkey’s Milk: Its Potential
Use in the Prevention of Atherosclerosis
A. Tafaro, T. Magrone, F. Jirillo, G. Martemucci, A.G.
D’Alessandro, L. Amati and E. Jirillo
Donkey’s milk is the best substitute of human milk
for its content in lactose, proteins, minerals, and ω-3
fatty acids. Here, we have evaluated the effects of colostrum
and milk from donkeys (Martina Franca breed) on the function
of human peripheral blood mononuclear cells (PBMCs) at different
intervals from lactation. Colostrum induced more IgA responses,
while milk induced predominantly more IgG responses. Both
milk and colostrum induced expression of CD25 and CD69 on
PBMCs. The ability to induce release of interleukins (IL)
(IL-12, IL-1β
and IL-10) and tumor necrosis factor-α
was confined only to milk, while colostrum was devoid of this
capacity. Finally, both colostrum and milk induced nitric
oxide (NO) release from PBMCs but milk exhibited a greater
capacity than colostrum in NO generation.
Taken together, these immunological activities exerted by
both colostrum and milk from donkeys may be useful in the
treatment of human immune-related diseases. In particular,
NO induction by donkey’s milk may be very useful in
the prevention of atherosclerosis, being a strong vasodilator
and an effective antimicrobial agent since pathogens and/or
their products may play a proatherogenic role.
[Back to top]
Red Wine Consumption and Prevention of Atherosclerosis: An
In Vitro Model Using Human Peripheral Blood Mononuclear
Cells
T. Magrone, A. Tafaro, F. Jirillo, M.A. Panaro, P. Cuzzuol,
A.C. Cuzzuol, V. Pugliese, L. Amati, E. Jirillo and V. Covelli
Evidence has been provided that red wine possesses antiatherogenic
activities in virtue of its content in polyphenols (flavono-ids
and non-flavonoids substances).
Here, some red wines (Negroamaro, Primitivo and Lambrusco)
were tested for their ability to trigger nitric oxide (NO)
production from human healthy peripheral blood mononuclear
cells (PBMC). Negroamaro was the strongest inducer of NO from
PBMC and deprivation of polyphenols did not influence its
NO generation capacity. This fact supports the involvement
of polyphenols in the NO production even in the absence of
alcohol, which also per se does not exert any significant
activity. These results are also corroborated by the evidence
that PBMC inducible-nitric oxide synthase expression occured
by the effect of samples containing polyphenols but this expression
was very weak when polyphenols were removed from the whole
Negroamaro.
In synthesis, flavonoids and resveratrol, major constitutents
of red wine, once absorbed at intestinal level, enter circulation
and trigger monocytes for NO production. To the best of our
knowledge, this is the first demonstration of a direct effect
of red wine on monocytes for NO release to occur. On the other
hand, also the macrophage contingent from gut-associated lymphoid
tissue can contribute to NO generation, besides the aliquot
produced by endothelial cells, as previously demonstrated
by various authors. Taken together, these results support
the concept that moderate intake of red wine can prevent atherosclerosis
via production of NO, a potent vasodilator of terminal
vessels.
[Back to top]
Pharmacogenomics: A Tool to Prevent and Cure Coronary Heart
Disease
G. Candore, C.R. Balistreri, M. Caruso, M.P. Grimaldi,
E. Incalcaterra, F. Listì, S. Vasto and C. Caruso
Inflammation and genetics play an important role in the
pathogenesis of coronary heart disease (CHD). This is supported
by epidemiological studies which have thoroughly investigated
the association between CHD and gene polymorphisms of the
inflammatory molecules. Moreover, efforts to find elective
therapy have not been rewarding and, despite the increasing
appreciation of the role of genetics in CHD and myocardial
infarction (MI) pathogenesis, pharmacogenomic approaches to
uncover drug target have not been extensively explored. A
critical search of published literature has suggested few
inflammatory genes directly involved in the risk to develop
CHD and MI. The selected genes are, the pro- and anti-inflammatory
cytokines, Toll-like receptor 4 (TLR4), CD14, CCR5, cyclooxygenases
(COXs) and lipoxygenases (LOXs). The associations between
candidate gene polymorphisms and CHD/MI are difficult and
complex as a consequence of pleiotropy, variations with age,
selection due to the lethality of the disease, and interactions
with other genes and environmental factors. However, current
data indicate that screening for interleukin (IL)-6, IL-10,
TLR4, CCR5, COX and LOX polymorphisms are likely to be a useful
tool for CHD and MI risk assessment. What we believe is that
dissecting out the influence of genetics polymorphism within
the complex pathophysiology of CHD and MI will help to provide
a more complete risk assessment and complement known classical
cardiological risk factors. The detection of a risk profile
will potentially allow both the early identification of individuals
susceptible to disease and the possible discovery of potential
targets for drug of lifestyle modification.
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