|
Anti-Infective
Agents in Medicinal Chemistry
ISSN: 1871-5214
Anti-Infective Agents in Medicinal
Chemistry
Volume 6, Number 3, July 2007
Contents
Dendrimers and Dendritic Polymers as Anti-infective
Agents: New Antimicrobial Strategies for Therapeutic Drugs
Pp. 151-174
J. Rojo and R. Delgado
[Abstract]
Antibacterial Peptides – A Bright Future or
a False Hope Pp. 175-184
R. Bucki, I. Levental and P.A. Janmey
[Abstract]
Novel Antiinflammatory and Antiinfective Agents
Pp. 185-200
Patrick Garidel, Jörg Andrä, Jörg Howe,
Thomas Gutsmann and Klaus Brandenburg
[Abstract]
The Echinocandins: Total and Semi-Synthetic Approaches
in Antifungal Drug Discovery Pp. 201-212
Adam R. Renslo
[Abstract]
Pharmacology of Current and Investigational Human
Immunodeficiency virus (HIV) Nucleoside/Nucleotide Reverse
Transcriptase Inhibitors in Adults Pp. 213-221
Laura Waters and Marta Boffito
[Abstract]
Abstracts
[Back to top]
Dendrimers and Dendritic Polymers as Anti-infective
Agents: New Antimicrobial Strategies for Therapeutic Drugs
J. Rojo and R. Delgado
Nearly 3 decades ago, a dendritic structure was stepwise synthesized
for the first time as a new type of molecules with promising
applications. During years a huge effort has been devoted
to implement the synthetic skills concerning the synthesis
of these molecules and especially, new methods for purification
and characterization of these compounds that are in the nanoscale
range. The chemical manipulation of the surface and inner
core of dendrimers were strategically used to allow a tailor-made
control of physical-chemical properties and to discover new
applications in material science and biomedicine. Although
several examples have been reported in the literature describing
applications of functionalized dendrimers and acclaiming a
key role of these molecules, very scarce examples are actually
close to the market.
This review summarizes the state of the art of dendrimers
and dendritic polymers as anti-infective agents, with a special
focus on the strategies to block receptors used by pathogens
for attachment, cell entry and dissemination. These nanometre
size molecules are very attractive compounds as new drugs
easily to be manipulated to improve their activity and scope.
This is already a very active area of research, where we are
involved, with interesting potential as demonstrated by the
Phase I clinical trial of a functionalized dendrimer with
real possibilities to reach the market soon. The success of
this compound should provoke an enormous stimulus to scientists
working in this area as well as in the industrial companies
for investment in this topic.
[Back to top]
Antibacterial Peptides – A Bright Future or
a False Hope
R. Bucki, I. Levental and P.A. Janmey
The increasing number of antibiotic resistant bacterial strains
presents an emerging world health problem that demands continued
effort to develop new antibacterial compounds. Endogenous
antibacterial peptides (ABPs) that are constitutively and/or
inducibly produced in tissues exposed to external surroundings
represent new candidates for development of such compounds.
Most ABPs target bacterial membranes initially by electrostatic
interactions between positively charged amino acids and negatively
charged molecules present on bacterial walls, followed by
compromise of the permeability barrier of bacterial membranes
through the formation of pores, leading to rapid cell death
and efficient bacterial elimination. Other mechanisms, such
as the inhibition of bacterial protein and DNA synthesis or
receptor-mediated stimulation of host defense mechanisms are
also ascribed to these molecules. The activities of ABPs correlate
positively with a gradient of hydrophobicity along the peptide
backbone, net positive charge at neutral pH, and secondary
structure. More than 850 sequences with antibacterial activity
have been described, and this number continues to grow with
the addition of newly discovered, as well as synthetic, peptides.
Many strategies, including increasing net positive charge,
increasing net hydrophobicity, conjugation of peptides with
lipophilic acids, incorporation of carbonate bonds, and synthesis
of their hybrids and truncated sequences that omit hemolytic
regions, have been proposed to increase efficiency of synthetic
ABPs. Additionally peptide-mimicking molecules such as cationic
steroid antibiotics (CSAs) may be useful alternatives to natural
ABPs. Current challenges for practical application of ABPs
are the high cost of synthesis/isolation, inactivation by
blood plasma, confinement by anionic polyelectrolytes, and
possible unknown toxicity.
[Back to top]
Novel Antiinflammatory and Antiinfective Agents
Patrick Garidel, Jörg Andrä, Jörg Howe,
Thomas Gutsmann and Klaus Brandenburg
Despite the availability of antibiotics, infectious diseases
become an even increasing threatening for human health, in
particular due to resistance development, for example in animal
husbandry. Furthermore, the sepsis shock syndrome, which in
many cases is a result of the fact that antibiotics may kill
bacteria, but do not inactivate bacterial virulence factors
such as endotoxins (lipopolysaccharides), is worldwide of
increasing importance regarding the very high death rate (40
to 50 %). Therefore, the development of suitable antimicrobial
drugs is urgently requested. In recent years, various groups
focus on the use of antimicrobial peptides (AMP) derived from
natural, innate immunity proteins, which in vivo
bind to the virulence factors. Such binding proteins are,
for example, lactoferrin, the Limulus anti-LPS-factor, and
the family of saposin-like proteins (NK-lysins, granulysins),
which all have particular binding domains for example for
bacterial endotoxin. Furthermore, an alternative approach
to combat infections is the use of cyclooxygenase and lipoxygenase
inhibitors.
From the reviewed literature the mechanisms of action of antiinfective
compounds on bacteria, on pathogenicity factors of the bacteria,
and on viruses are summarized. In the last years, considerable
progresses have been made in the fight against infections,
specially also to overcome bacterial resistance.
[Back to top]
The Echinocandins: Total and Semi-Synthetic Approaches
in Antifungal Drug Discovery
Adam R. Renslo
The echinocandins are a new class of antifungal lipopeptides
for the treatment of serious nosocomial mycoses. The three
currently approved drugs, caspofungin, micafungin, and anidulafungin,
were each discovered through the synthetic modification of
echinocandin natural products obtained from fermentation.
This review is intended for the medicinal chemist who is actively
pursuing or has a general interest in the synthetic modification
of natural products as a means to identify drug candidates.
It provides a survey of the synthetic strategies that produced
the approved echinocandin therapeutics and a discussion of
more recent efforts to identify a new generation of echinocandin
drug candidates. Both total synthetic approaches starting
from the constituent amino acids and semi-synthetic approaches
relying on fermentation-produced lipopeptide are addressed.
These various efforts by chemists from industry and academia
have not only illuminated the interesting chemistry of these
natural products, but have provided the means by which improvements
in antifungal potency and spectrum, pharmacokinetic profile,
solubility, stability, and safety can be realized. The ultimate
success of these efforts can be judged by considering the
important role the echinocandins are already playing in the
treatment of serious fungal infection.
[Back to top]
Pharmacology of Current and Investigational Human
Immunodeficiency virus (HIV) Nucleoside/Nucleotide Reverse
Transcriptase Inhibitors in Adults
Laura Waters and Marta Boffito
Since the mid-1980s, the nucleoside reverse transcriptase
inhibitors (NRTIs) have established their position as valuable
antiretroviral (ARV) agents in the treatment of human immunodeficiency
virus (HIV) infection. Today, NRTIs still constitute the “backbone”
of highly active ARV therapy regimens. The combination of
different ARV classes has enabled the goal of successful suppression
of HIV replication to be achieved in most HIV infected patients
and is currently standard of care to prevent the development
of AIDS.
The NRTIs and nucleotide reverse transcriptase inhibitors
(NtRTIs) are prodrugs which require intracellular phosphorylation
before they become active compounds. Apart from zidovudine
they are all water soluble, and generally have a wide volume
of distribution. The NRTIs undergo a three step phosphorylation
process whilst the one currently available NtRTI, tenofovir,
only requires two phosphorylation steps to create a clinically
active diphosphate metabolite. The active phosphorylated derivatives
then compete with the endogenous nucleotides for viral reverse
transcriptase. Several steps in intracellular phosphorylation
are rate limiting and a number of intracellular factors can
affect this metabolism. There are also external influences
which can affect this process. The intracellular factors include:
cell type; timing within the cell cycle; levels of dideoxynucleoside
analogue triphosphates (ddNTPs) created by the phosphorylation
of NRTIs, and endogenous cellular deoxynucleotide triphosphates
(dNTPs) which compete for substrate binding to reverse transcriptase.
Importantly, drug-drug interactions involving NRTIs with other
ARVs as well as with non-HIV classes of drugs are complex
and may lead to the development of toxicity or limit drug
efficacy. This is of particular importance with the numerous
new agents in development.
The review will discuss the main pharmacological characteristics
of the available and investigational NRTI/NtRTIs and a brief
summary of the possible drug interactions which may occur
between different ARV agents. An extensive discussion of drug-drug
interactions between ARVs and other agents is outside the
scope of this review.
|
