Current Drug Targets - Cardiovascular & Haematological Disorders, Volume 3, Number 2, 2003
Contents
Novel and Emerging Therapies
in Cardiology and Haematology Pp.101-123
John E. Pimanda
, Harry C. Lowe , Philip J. Hogg, Colin N. Chesterman and Levon M. Khachigian
Inhibition of Platelet
Adhesion to Collagen as a New Target for Antithrombotic Drugs Pp.123-140
K. Vanhoorelbeke
, H. Ulrichts, A. Schoolmeester and H. Deckmyn
Erythropoietin:
Cytoprotection in Vascular and Neuronal Cells Pp.141-154
Zhao Zhong Chong , Jing-Qiong Kang and Kenneth Maiese
Observations on the Use of
the Avian Chorioallantoic Membrane (
Mary Richardson and Gurmit Singh
Regulatory Light Chains of
Striated Muscle Myosin. Structure, Function and Malfunction Pp.187-197
Danuta Szczesna
Abstracts
[Back to top] Novel and Emerging Therapies in Cardiology and Haematology
John E. Pimanda
, Harry C. Lowe , Philip J. Hogg, Colin N. Chesterman and Levon M. Khachigian
Reviewing advances in cardiology and haematology together may appear at first sight to require some artificiality to make a satisfying fit. For two reasons, at least, this is not the case. Firstly, convergence in biology has become very clear over the past decade and this could not be better illustrated by the demonstration that the haemangioblast is the common progenitor of both haemapoietic stem cells and vascular endothelium. This opens the way to common (and differential) approaches to the manipulation of these cells, a field at present in its infancy. A second convergence is the common goal of understanding the processes resulting in haemostasis, thrombosis and vascular occlusion and the means for developing effective antithrombotics. This is exemplified by a number of agents either in use or in clinical trial as a result of haematological and cardiological collaboration. This collaboration is recognisable with the development, many years ago, of streptokinase and the use of aspirin in vascular disease and continues to this day with specific antiplatelet inhibitors and oral thrombin inhibitors as they become accepted into clinical use over the next few years. Here we review current advances in pharmacological treatments in cardiology and haematology, grouped primarily by disease process, focusing on novel and emerging therapies likely to be of importance in the future.
[Back to top] Inhibition of Platelet
Adhesion to Collagen as a New Target for Antithrombotic Drugs
K.
Vanhoorelbeke , H. Ulrichts, A. Schoolmeester and H. Deckmyn
Platelet adhesion to a damaged blood vessel is the initial trigger for arterial hemostasis and thrombosis. Platelets adhere to the subendothelium through an interaction with von Willebrand factor (VWF), which forms a bridge between collagen within the damaged vessel wall and the platelet receptor glycoprotein Ib/V/IX (GPIb), an interaction especially important under high shear conditions[1]. This reversible adhesion allows platelets to roll over the damaged area, which is then followed by a firm adhesion mediated by the collagen receptors (a2b1, GPVI,…) in addition[2] resulting in platelet activation. This leads to the conformational activation of the platelet aIIbb3 receptor, fibrinogen binding and finally to platelet aggregation.
Over the past decades, modulation of platelet function has been a strategy for the control of cardiovascular disease. Lately, drugs have been developed that target the fibrinogen receptor aIIbb3 or the ADP receptor and many of these promising compounds have been tested in clinical trials. However the development of products that interfere with the first step of hemostasis, i.e. the platelet adhesion, has lagged behind. In this review we want to discuss (i) the in vivo studies that were performed with compounds that target proteins involved in different adhesion steps i.e. the VWF-GPIb-axis, the collagen-VWF axis and the collagen-collagen receptor axis and (ii) the possible advantages these putative new drugs could have over the current antiplatelet agents.
[Back to top] Erythropoietin:
Cytoprotection in Vascular and Neuronal Cells
Zhao Zhong
Chong , Jing-Qiong Kang and
Kenneth Maiese
One of the principal functions of erythropoietin (EPO) is to stimulate the survival, proliferation, and differentiation of immature erythroid cells. Yet, EPO has recently been shown to modulate cellular signal transduction pathways to perform multiple functions other than erythropoiesis. EPO is cytoprotective through the prevention of programmed cell death in both vascular and neuronal systems by modulating two distinct components of programmed cell death that involve the degradation of genomic DNA and the externalization of cellular membrane phosphatidylserine (PS) residues. Cytoprotection by EPO is initiated by the activation of the EPO receptor (EPOR) and subsequent signal transduction pathways that originate with the Janus-tyrosine kinase 2 (Jak2) protein. Further down-stream cellular pathways include the activation of signal transducers and activators of transcription (STATs), Bcl-xL, phosphoinositide-3-kinase/Akt, mitogen-activated protein kinases, cysteine proteases, protein tyrosine phosphatases, and nuclear factor kB. Further understanding of the cellular pathways that modulate EPO cytoprotection in the nervous system will be crucial for the development of therapeutic strategies against neurodegenerative diseases.
[Back to top] Observations on the Use of
the Avian Chorioallantoic Membrane (
Mary
Richardson and Gurmit Singh
The chorioallantoic membrane (
In this review, the major
methodologies for all aspects of the use of the
The need for a standardized
approach to the use of the
[Back to top] Regulatory
Light Chains of Striated Muscle Myosin. Structure, Function and Malfunction
Danuta Szczesna
Striated (skeletal and cardiac) muscle is activated by the binding of Ca2+ to troponin C and is regulated by the thin filament proteins, tropomyosin and troponin. Unlike in molluscan or smooth muscles, the myosin regulatory light chains (RLC) of striated muscles do not play a major regulatory role and their function is still not well understood. The N-terminal domain of RLC contains a 'Ca2+-Mg2+'-binding site and, analogous to that of smooth muscle myosin, also contains a phosphorylation site. During muscle contraction, the increase in Ca2+ concentration activates the Ca2+/calmodulin-dependent myosin light chain kinase and leads to phosphorylation of the RLC. In agreement with other laboratories we have demonstrated that phosphorylation and Ca2+ binding to the RLC play an important modulatory role in striated muscle contraction. Furthermore, the ventricular isoform of human cardiac RLC has been shown to be one of the sarcomeric proteins associated with familial hypertrophic cardiomyopathy (FHC), an autosomal dominant disease characterized by left ventricular hypertrophy, myofibrillar disarray and sudden cardiac death. Our recent studies have demonstrated that phosphorylation and Ca2+ binding to human ventricular RLC are significantly altered by the FHC mutations and that their detrimental effects depend upon the specific position of the missense mutation, whether located in the proximity of the RLC 'Ca2+-Mg2+'-binding site or the phosphorylation site (Serine 15). We have also shown that there is a functional coupling between Ca2+ and/or Mg2+ binding to the RLC and phosphorylation and that the FHC mutations can affect this relationship. Further in vivo studies are necessary to investigate the mechanisms involved in the pathogenesis of RLC-linked FHC.