Cardiovascular
& Hematological Agents in Medicinal Chemistry
ISSN: 1871-5257
Cardiovascular & Hematological
Agents in Medicinal Chemistry
Volume 6, Number 1, January 2008
Contents
New Emerging Prospects in the Pharmacotherap
of Hypertension Pp. 1-19
A. Balsamo, V. Calderone and S. Rapposelli
[Abstract]
Antioxidant Therapy for Prevention of Inflammation,
bIschemic Reperfusion Injuries and Allograft Rejection Pp.
20-43
A. Ma, S. Qi and H. Chen
[Abstract]
A Murine Model of Vasculitis Induced by Fungal Polysaccharide
Pp. 44-52
N. Ohno
[Abstract]
Cardiac Stem Cell-Based Myocardial Regeneration: Towards
a Translational Approach Pp. 53-59
D. Torella, C. Indolfi, D.F. Goldspink and G.M. Ellison
[Abstract]
Stem Cells and Cardiovascular Repair: A Role for Natural
and Synthetic Molecules Harboring Differentiating and Paracrine
Logics Pp. 60-68
C. Ventura, C. Cavallini, F. Bianchi and S. Cantoni
[Abstract]
The Role of COX-2 in Heart Pathology Pp.
69-79
J.M. Streicher and Y. Wang
[Abstract]
Abstracts
[Back to top]
New Emerging Prospects in the Pharmacotherapy
of Hypertension
A. Balsamo, V. Calderone and S. Rapposelli
One of the main approaches to the treatment of cardiovascular
diseases is to block pathways and enzymes within the Renin-Angiotensin
System (RAS) involved in the modulation of Angiotensin II.
Besides this complex system, many other alternative strategies
may represent interesting targets for new and more effective
cardiovascular therapies.
Many different approaches have led medicinal chemists to develop
new molecules with the aim of improving current anti-hypertensive
therapies. The development of these new compounds is based
on different strategies which include the synthesis of new
hybrid compounds in which two or more pharmacophore groups
are combined together to give a new entity with better pharmacodynamic
properties and fewer side effects, and the development of
new molecules with targets such as renin, angiotensin (1-7)
and urotensin-II.
The aim of this review is to present various approaches used
to improve antihypertensive therapy, developing both original
molecules with new mechanisms of action (such as renin inhibitors,
or Mas-agonists) and new hybrid cardiovascular drugs targeting
multiple factors involved in hypertensive disease (NO-ACE
inhibitors, NO-sartans, AT1/ETA antagonists).
[Back to top]
Antioxidant Therapy for Prevention of Inflammation Ischemic
Reperfusion Injuries and Allograft Rejection
A. Ma, S. Qi and H. Chen
Oxidative stress results from an imbalance, an excess
of oxidants, depletion of antioxidants or failure to repair
oxidative damage induced by reactive oxygen species. A vast
amount of evidence implicates oxygen-derived free radicals
and high-energy oxidants as mediators in many pathological
conditions of inflammation, shock, and organ responses to
ischemia/reperfusion, which arise during a number of clinical
surgical interventions, including transplant graft rejection
and coronary bypass surgery, and in such diseases as, diabetes,
atherosclerosis, hypertension, organ ischemia/reperfusion,
cardiovascular inflammation, cardiac/brain infarction, cancer,
pulmonary emphysema and autoimmune diseases. To eliminate
or attenuate oxidative stress, antioxidant therapies have
been developed and may be of great help to these patients.
This review describes recent developments in the field of
oxidative stress research and antioxidant function, summarizes
new pharmacological strategies that are ongoing in antioxidant
therapy with small molecules, free radical-scavenging enzymes,
superoxide dismutases, catalase mimetics, flavonoids, vitamins
and poly polymerase inhibitors, and presents experimental
and clinical evidence of the role of antioxidants in diseases.
[Back to top]
A Murine Model of Vasculitis Induced by Fungal Polysaccharide
N. Ohno
CAWS is a mannoprotein-beta-glucan complex obtained from
the culture supernatant of the fungal pathogen Candida
albicans. CAWS exhibits various biological activities,
and induces prominent vasculitis of the aortic valve and the
coronary arteries in mouse. A significant difference was noted
in the susceptibility to and the degree of vasculitis induction
among mouse lines. The difference in cytokine production among
mouse lines may be strongly related to that difference, namely,
IL-6, IFN-γ
and TNF-α
presumably act as positive factors, and IL-10, as a negative
regulator. On the other hand, as a structural component of
the inducing substance, the presence or absence of β-1,2-mannose
residues was suggested to be closely related to the activity.
An understanding of the molecular mechanisms underlying this
model could lead to the conquest of many modern diseases.
This model is also expected to be useful for the development
of new therapeutic drugs for vasculitis and cardiovascular
diseases.
[Back to top]
Cardiac Stem Cell-Based Myocardial Regeneration:
Towards a Translational Approach
D. Torella, C. Indolfi, D.F. Goldspink and G.M. Ellison
The adult mammalian heart, including humans, harbors
bone fide cardiac stem cells (CSCs) distributed throughout
the atria and ventricles. Their discovery almost four years
ago initiated a brand new field of cardiac regenerative biology
that has profoundly changed the outlook of developmental and
adult cardiac biology/physiology and the potential for treating
cardiac failure. Indeed, despite its initial hesitance, the
research community has now accepted that the heart has an
endogenous myocardial regenerative potential owed to CSCs,
which challenges the previous accepted notion of the adult
heart as a post-mitotic organ. Also, burgeoning evidence is
converging to the possibility that CSCs are actually the founder
of the heart in the embryonic life. CSCs are involved in cardiac
cellular homeostasis during aging and adaptation to physiological
and pathological stress. When transplanted into damaged hearts,
CSCs have the capacity to generate significant new myocardial
tissue and ameliorate ventricular function. However, more
relevant for translational research and its application for
future regeneration protocols, this reservoir of CSCs can
also be activated by local injections of several growth factors
or through the administration of systemic drugs, such as statins,
to obtain beneficial results similar to those of CSC transplantation.
The present review highlights current knowledge on the biology
of CSCs and the prospects of CSC activation in situ,
without the need for cell expansion in vitro and
consequent transplantation.
[Back to top]
Stem Cells and Cardiovascular Repair: A Role for Natural
and Synthetic Molecules Harboring Differentiating and Paracrine
Logics
C. Ventura, C. Cavallini, F. Bianchi and S. Cantoni
Stem cells hold considerable promise for cardiovascular
rescue in patients with heart failure due to myocardial infarction
or hereditary cardiomyopathies. However, cardiogenesis, one
of the earliest and most complex morphogenetic events in the
embryo, is only partially exploited at molecular level. The
yield of myocardial cells spontaneously derived from human
embryonic or adult stem cells is extremely low (usually less
than 0.1%). Moreover, it is now evident that secretion of
specific growth factors from transplanted stem cells may activate
angiogenic, antiapoptotic and antifibrotic paracrine patterning
within the recipient heart, playing a major role in tissue
repair. Within this context, targeting stem cell fate at the
level of gene expression represents a potentially powerful
therapeutic approach to afford a high-throughput of cardiovascular
lineage commitment and paracrine secretion of “trophic
factors”. Cell-based phenotypic- and pathway-specific
screens of natural and synthetic compounds have provided a
number of molecules achieving selective control of stem cell
growth and differentiation. Novel hyaluronan mixed esters
of butyric and retinoic acids have been recently synthesized,
emerging as new tools for manipulation of cardio/vasculogenic
gene expression through the modulation of targeted signaling
pathways and chromatin-remodeling enzymes. These molecules
have coaxed both murine embryonic and human mesenchymal stem
cells towards cardiovascular decision and paracrine secretion
of bioactive factors, remarkably enhancing the rescuing potential
of human stem cells in in vivo animal models of myocardial
infarction. These molecules may ultimately provide new insights
in stem cell biology and pave the way to novel approaches
in tissue engineering and cardiovascular repair.
[Back to top]
The Role of COX-2 in Heart Pathology
J.M. Streicher and Y. Wang
Cyclooxygenase-2 (COX-2) is a key enzyme in the production
of prostaglandins, and an important anti-inflammation drug
target. Recent focus has been placed on the role of COX-2
in heart function and pathology, due to the finding that specific
COX-2 inhibitors significantly increased the risk of heart
disease in chronic users. However, the exact role of COX-2
in cardiac physiology and disease remains controversial due
to the conflicting data reported. Roughly equal numbers of
reports have shown either a detrimental role or a protective
role for COX-2 in heart in experimental models. Here we attempt
to provide a background on the more general roles of COX-2
in pathophysiology, as well as molecular mechanisms employed
to control COX-2 expression. This background provides a basis
for better understanding the functional role of COX-2 in human
heart pathologies, based on the results of COX-2 pharmacological
inhibitor studies in humans as well as COX-2 expression in
human heart disease. Furthermore, we will explore the experimental
evidence implicating different intracellular molecular signaling
cascades that regulate COX-2 expression in cardiomyocytes.
All of this data permits a more mechanistic understanding
of the published studies using pharmacological inhibitors
of COX-2 in experimental models of heart pathology. Lastly,
we will examine the use of genetic manipulation of COX-2 in
mice as one of the future avenues in an attempt to resolve
the role of COX-2 in cardiac physiology and pathology.
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