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Current
Medicinal Chemistry
ISSN: 0929-8673
Current Medicinal Chemistry
Volume 13, Number 5, 2006
Contents
Prodrugs of Anthracyclines in Cancer Chemotherapy
Pp. 477-523
F. Kratz, A. Warnecke, B. Schmid, D.-E. Chung and M. Gitzel
[Abstract]
Copper in Medicine: Homeostasis, Chelation Therapy and Antitumor
Drug Design Pp. 525-537
Tuo Wang and Zijian Guo
[Abstract]
Heterocyclic Nucleosides: Chemical Synthesis and Biological
Properties Pp. 539-545
Pedro Merino
[Abstract]
Thiol Proteases: Inhibitors and Potential Therapeutic
Targets Pp. 547-581
Regis Leung-Toung, Yanqing Zhao, Wanren Li, Tim F. Tam, Khashayar
Karimian and Michael Spino
[Abstract]
AMP-Activated Protein Kinase and Type 2 Diabetes
Pp. 583-589
Nicolas Musi
[Abstract]
An Inflammatory Pathomechanism for Parkinson's Disease?
Pp. 591-602
Christophe Wersinger and Anita Sidhu
[Abstract]
Abstracts
[Back to top]
Prodrugs of Anthracyclines in Cancer
Chemotherapy
F. Kratz, A. Warnecke, B. Schmid, D.-E. Chung and M. Gitzel
Designing and developing truly tumor-specific prodrugs remains
a challenge in the field of cancer chemotherapy. Active targeting
strategies, on the one hand, aim at exploiting membrane-associated
receptors or antigens for drug delivery; on the other hand,
the enhanced vascular permeability and retention of macromolecules
in tumor tissue substantiates the concept of passive targeting.
Consequently, research efforts have concentrated on conjugating
anticancer agents with a wide spectrum of carriers including
antibodies, peptides, serum proteins, and synthetic polymers.
Conversely, low-molecular weight prodrugs of anticancer agents
have been developed that do not bear an active or passive
targeting moiety, but are activated by tumor-associated enzymes
at the tumor site.
Anthracyclines probably represent the class of anticancer
agents that has been most widely used for the development
of prodrugs. This overview gives an update of the various
low- and high-molecular weight prodrugs of anthracyclines,
e.g. with antibodies, peptides, carbohydrates, serum proteins
or synthetic polymers, that have been developed over the past
20 years and that exemplify the salient features of a respective
drug delivery system. A detailed description will be dedicated
to anthracycline prodrugs that have reached an advanced stage
of preclinical testing or that have entered clinical trials.
[Back to top]
Copper in Medicine: Homeostasis, Chelation Therapy
and Antitumor Drug Design
Tuo Wang and Zijian Guo
As one of the most important essential transition metals,
copper is involved in a variety of biological processes such
as embryo development, connective tissue formation, temperature
control and nerve cell function. It is also related to severe
diseases such as Wilson’s and Menkes diseases and some
neurological disorders. Novel components of copper homeostasis
include copper-transporting P-type ATPases, Menkes and Wilson
proteins, and copper chaperones in humans have been identified
and characterized at the molecular level. These findings have
paved the way towards better understanding of the role of
copper deficiency or copper toxicity in physiological and
pathological conditions. Therefore, organic compounds that
can interfere with copper homeostasis may find therapeutic
application in copper-dependent diseases. The antitumor activity
of copper complexes was reported several decades ago, and
many new complexes have demonstrated great antitumor potential.
Copper complexes may have relatively lower side effects than
platinum-based drugs, and are suggested to be able to overcome
inherited or acquired resistance of cisplatin. In this overview,
the most recent advances in copper homeostasis, copper-related
chelation therapy and design of copper-based antitumor complexes
will be summarized.
[Back to top]
Heterocyclic Nucleosides: Chemical Synthesis
and Biological Properties
Pedro Merino
This update covers the literature for 2002 and 2003 dealing
with the main topic of the previous review entitled Heterocyclic
nucleosides. Chemical synthesis and biological properties
and published in Curr. Med. Chem.-AIA, 2002, 1, 389.
As in the first review, the papers in this survey are grouped
by the type of the heterocyclic system that acts as a spacer
between the hydroxymethyl group and the base moiety.
[Back to top]
Thiol Proteases: Inhibitors and Potential Therapeutic
Targets
Regis Leung-Toung, Yanqing Zhao, Wanren Li, Tim F. Tam, Khashayar
Karimian and Michael Spino
A better understanding of the biological roles and the pathological
consequences of thiol-dependent enzymes has emerged in recent
years, and hence considerable progress has been made in identifying
and delineating cysteine proteases that can be considered
promising drug targets from those involved in housekeeping
functions. Cysteine proteases have been implicated in a wide
variety of disease processes ranging from cardiovascular,
inflammatory, viral and immunological disorders to cancer.
The first milestone in drug development of cysteine protease
inhibitors has probably been reached, as IDN-6556 (a broad
spectrum caspase inhibitor) has recently received Orphan Drug
label by the U.S. Food and Drug Administration for use in
the treatment of the patients undergoing liver transplantation
and other solid organ transplantation. IDN-6556, which blocks
apoptosis, is in Phase II human clinical trial in patients
undergoing liver transplantation. In addition, more than ten
cysteine protease inhibitors are presently at various phases
of clinical development/trials for diverse diseases.
This review emphasises on the new development from the literature
reports since the year 2000 in the exploration of potential
cysteine proteases as prospective drug targets, and the investigation
of promising inhibitors that can potentially be developed
for the treatment of human diseases. Transglutaminases, another
class of thiol-dependent enzymes, are not discussed here.
[Back to top]
AMP-Activated Protein Kinase and Type 2 Diabetes
Nicolas Musi
AMP-activated protein kinase (AMPK) is an enzyme that works
as a fuel gauge, being activated in situations of high-energy
phosphate depletion. Upon activation, AMPK functions to restore
cellular ATP by modifying diverse metabolic pathways. AMPK
is activated robustly by skeletal muscle contraction and myocardial
ischemia, and may be involved in the stimulation of glucose
transport and fatty acid oxidation produced by these stimuli.
In liver, activation of AMPK results in enhanced fatty acid
oxidation and in decreased production of glucose, cholesterol,
and triglycerides. Recent studies have shown that AMPK is
the cellular mediator for many of the metabolic effects of
drugs such as metformin and thiazolidinediones, as well as
the insulin sensitizing adipocytokines leptin and adiponectin.
These data, along with evidence from studies showing that
chemical activation of AMPK in vivo with 5-aminoimidazole-4-carboxamide
ribonucleoside (AICAR) improves blood glucose concentrations
and lipid profiles, make this enzyme an attractive pharmacological
target for the treatment of type 2 diabetes and other metabolic
disorders.
[Back to top]
An Inflammatory Pathomechanism for Parkinson's Disease?
Christophe Wersinger and Anita Sidhu
Parkinson’s disease (PD) is a slowly progressive neurodegenerative
disorder characterized by the loss of dopaminergic neurons
in the Substantia Nigra pars compacta (SNpc), striatal
dopamine deficiency and appearance of Lewy bodies. Inflammatory
and immune, or even autoimmune, stigmata, have been described
in post-mortem brains of PD patients. Although disputed in
humans, a reactive astrocytosis and a lymphocytic infiltration
in the SNpc have been observed in animal models of
PD, which need further examination. This review summarizes
the current knowledge on brain inflammation in humans with
PD, and how inflammation and/or (auto)immune reactions within
the SNpc could be linked to other pathophysiological
mechanisms that have been hypothesized for the etiology of
PD, such as oxidative stress, exposure to neurotoxins, and
post-infectious or post-traumatic injuries. In particular,
we discuss how microglial cells could be activated during
the course of PD, and present a new hypothesis that PD-linked
protein (α-synuclein,
in particular) aggregates could be implicated in their activation,
to induce a chronic and sustained inflammation involved in
the progression, at least, of the disease. The current status
of anti-inflammatory agents, either already tried in PD clinical
trials or putatively usefull as adjuvant therapies for PD,
is also discussed.
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