Contents
Mode of Action of Plant Defensins Suggests
Therapeutic Potential Pp.
1-8
Bart P.H.J. Thomma, Bruno
P.A. Cammue and Karin Thevissen
b-Lactamases: A Survey of Protein Diversity Pp. 9-23
Marion S. Helfand
and Robert A. Bonomo
Therapy of Chronic Hepatitis C: A Critical Review Pp. 25-32
G. Saracco, A.
Olivero, A. Ciancio, S. Carenzi and M. Rizzetto
Strategy of Computer-Aided Drug Design Pp. 33-40
A.V. Veselovsky and
A.S. Ivanov
Antivirals at the Mirror: The Lack of
Stereospecificity of Some Viral and Human Enzymes Offers Novel Opportunities in
Antiviral Drug Development
Pp. 41-53
Federico Focher,
Silvio Spadari and Giovanni Maga
A Review of Macrolide Treatment of
Atherosclerosis and Abdominal Aortic Aneurysms Pp. 55-63
Jes S. Lindholt,
Jette Støvring, Paul Lehm Andersen, Eskild W. Henneberg and Lars Østergaard
New Approaches for Anti-Infective Drug
Discovery: Antibiotics, Vaccines and Beyond Pp. 65-76
Q. Cheng, S.
Wang and A.A. Salyers
Chitin Synthesis as a Target for Antifungal
Drugs Pp. 77-91
J. Ruiz-Herrera and G. San-Blas
[Back to top] Mode of Action of Plant Defensins Suggests
Therapeutic Potential
Bart P.H.J. Thomma, Bruno P.A. Cammue and
Karin Thevissen
Higher vertebrates can rely both
on an innate as well as an adaptive immune system for defense against invading
pathogens. In contrast, plants can only employ an innate immune system that
largely depends on the production of antimicrobial compounds such as plant
defensins and other pathogenesis-related proteins. Plant defensins are
ubiquitous, cationic, cysteine-rich plant peptides and have a folding pattern
that shares high similarity to defense peptides of mammals and insects,
suggesting an ancient and conserved origin. A large number of plant defensins
appear to display antifungal activity. Some of these defensins have been found
to interact with fungal-specific components in the plasmamembrane, resulting in
membrane permeabilization. This makes them an attractive source of potential
therapeutics to treat fungal infections.
[Back to top] b-Lactamases: A Survey of Protein Diversity
Marion S. Helfand and Robert A. Bonomo
Bacterial resistance to b-lactam antibiotics and â-lactamase inhibitors is an ever increasing problem that threatens the clinical utility of drugs that form the cornerstone of the antibiotic armamentarium. Especially among Gram-negative pathogens, elaboration of structurally and mechanistically novel b-lactamase enzymes is the most important means by which resistance occurs. An appreciation of the tremendous diversity of these drug-modifying enzymes will assist in understanding why so few generally effective inhibitory agents exist for these unique drug targets. This review will give a general background on the reaction mechanisms and classification schemes of the more than 340 b-lactamase enzymes described to date. A discussion will follow highlighting the emerging Class A SHV and TEM-derived extended-spectrum (ESBLs), and inhibitor-resistant enzymes, non-TEM, non- SHV Class A ESBLs, and carbapenemases, Class B metallo- b -lactamases and some of their novel inhibitors, plasmid and chromosomally encoded Class C enzymes, and finally, the OXA-type oxacillinases, ESBLs, and carbapenemases of Class D. The clinical importance of multiple resistance mechanisms in conjunction with the production of b -lactamase enzymes is emphasized.
[Back to top] Therapy of Chronic Hepatitis C: A Critical
Review
G. Saracco, A. Olivero, A. Ciancio, S.
Carenzi and M. Rizzetto
Combination therapy (Interferon plus ribavirin) is the current therapeutic gold standard for naïve Hepatitis C Virus (HCV)-positive patients and with the recent advent of pegylated (PEG) IFN the rate of the sustained virological response (HCV-RNA clearance 6 months after the end of treatment) is about 54%-56% with a therapeutical gain mainly among patients with unfavourable HCV genotype (1a, 1b); in this subset of patients, a 42%-46% sustained response rate is achieved compared with 33%-36% found among genotype 1 patients treated with the standard therapy.
Patients who respond to IFN monotherapy but relapse during the follow-up should be re-treated with combination therapy given for at least 6 months at the minimum dose of 3 MU thrice weekly plus ribavirin 1000 mg/daily. Recent data suggest that prolonging the time of treatment (12 months) may induce a significantly higher rate of sustained response among patients with genotype 1.
The efficacy of the combination of IFN and ribavirin in retreating patients with chronic hepatitis C not responding to IFN monotherapy is controversial as it ranges between 0% and 40%. Recent data show an overall rate of sustained response of 23% when an aggressive approach is adopted but increasing the dosage and the time of treatment induces a significant therapeutic benefit only in patients with genotype 1.
In conclusion, a therapeutic
progress for chronic hepatitis C has been achieved during the last 10 years
(56% vs 20% of sustained response rate obtained with IFN monotherapy) but several
unresolved issues are yet to be addressed.
[Back to top] Strategy of Computer-Aided Drug Design
A.V. Veselovsky and A.S. Ivanov
Modern strategies of
computer-aided drug design (CADD) are reviewed. The task of CADD in the
pipeline of drug discovery is accelerating of finding the new lead compounds
and their structure optimization for the following pharmacological tests. The
main directions in CADD are based on the availability of the experimentally
determined three-dimensional structure of the target macromolecule. If spatial
structure is known the methods of structure-based drug design are used. In the
opposite case the indirect methods of CADD based on the structures of known
ligands (ligand-based drug design) are used. The interrelationship between the
main directions of CADD is reviewed. The main CADD approaches of molecule de
novo design and database mining are described. They include methods of
molecular docking, de novo design, design of pharmacophore and quantity structure-activity
relationship models. New ways and perspectives of CADD are discussed.
[Back to
top]
Antivirals at the Mirror: The Lack of Stereospecificity of Some Viral and Human
Enzymes Offers Novel Opportunities in
Antiviral Drug Development
Federico Focher, Silvio Spadari and Giovanni
Maga
The enantioselectivity of enzymes, namely the property of enzymes to recognise and metabolise only one of the two enantiomers of chiral molecules, is related to the chiral structure of the enzymes, reflecting the three-dimensional folding of the polypeptide backbone and the orientation of the amino acid side chains in the folded molecule. Because of the chirality of the amino acids (L), the chemistry of life should be highly sensitive to different enantiomers of chiral substrates. However, in a world consisting only of D-nucleosides and L-amino acids, an enzyme which lacks enantio-selectivity does not reduce its fitness, since there is no chance of molecular misunder-standing when no other choice is available. Thus, although enantioselectivity is theoretically essential for life we do not expect to be always present among the biochemical properties of enzymes. If this is the case for key enzymes involved in virus infection or cancer, how to exploit such lack of enantioselectivity for a novel approach to antiviral or anticancer chemotherapy?
The present review will discuss
the possible lack of enantioselectivity of enzymes and its relevance for the
developing of novel drugs with the inverted optical configuration.
[Back to top] A Review of Macrolide Treatment of
Atherosclerosis and Abdominal Aortic Aneurysms
Jes S. Lindholt, Jette Støvring, Paul Lehm
Andersen, Eskild W. Henneberg and Lars Østergaard
Seroepidemiological studies have shown an association between Chlamydia pneumoniae and atherosclerosis, the risk of acute myocardial infarction and abdominal aortic aneurysms (AAA).
Several studies have detected C.
pneumoniae in atherosclerotic lesions from coronary and carotid arteries, in
AAA, and in sclerotic aortic valves. However, culturing of C. pneumoniae is
difficult and has seldomly succeeded from atherosclerotic lesions. Thus, the
pathogenicity is unknown, and the significance of detecting the organism is
unresolved. Nevertheless, in a large observational study comparing the risk of
cardiovascular events among recipients of macrolide versus pencillins,
macrolide treatment reduced the risk of such events after relevant adjustment.
Furthermore, in two out of three minor randomized clinical trials were patients
with ischaemic heart disease were randomized into antibiotic treated and
placebo groups, a significant reduction in serious end-points were noticed in
patients receiving macrolide. Similarly, two other minor randomized trials
showed that macrolide treatment inhibited growth of small AAA. Macrolide
therapy thus seems potential to improve the outcome of severe ischaemic heart
disease, and growth of AAA. If true, it not known whether this is transient because
of macrolide's non-specific anti-inflammatory effect or latent infection, or
permanent because of eradicating C. pneumoniae organisms. In order to clarify
this, large and long term randomized trials are needed, as well as diagnostic
methods that can differentiate between individuals who are or are not infected
with C. pneumoniae. The latter are needed in order to clarify the impact of the
presence of C. pneumoniae and to avoid overconsumption of antimicrobials, which
can result in serious ecological problems.
[Back to
top]
New Approaches for Anti-Infective Drug Discovery: Antibiotics, Vaccines and
Beyond
Q. Cheng, S. Wang and A.A. Salyers
Infectious disease is the leading
cause of death worldwide, and billions of dollars are invested every year in
developing anti-infective drugs. In the meantime, resistant bacteria are on the
steady rise and render many once effective drugs useless. The tremendous
funding and the urgent need to treat the resistant bacterial infections lead to
the rapid progress on development of new drugs and potential new drug targets.
New discoveries are being made that increase our understanding of microbial
pathogenesis. Technological advancement is also being made to accelerate the
drug discovery process. This review will mainly focus on discussing novel
strategies on the development of antibiotics and vaccines for treating
bacterial infections. Details of how some of the emerging technologies such as
genomics and bioinformatics are accelerating the drug discovery process will be
highlighted. Newly emerging concepts in controlling bacterial infections such
as the use of probiotics and enzybiotics will also be briefly described.
[Back to
top] Chitin
Synthesis as a Target for Antifungal Drugs
J. Ruiz-Herrera and G. San-Blas
Human mycoses have become a threat to health world-wide. Unfortunately there are only a limited number of antimycotic drugs in use. Promising targets for drugs specific against fungi are those affecting chitin synthesis. Chitin is absent in vertebrates, and is essential for fungal wall integrity. A thorough knowledge of the mechanism of chitin synthesis is required to design specific inhibitors. We review here our current understanding of the process, and the most promising drugs that inhibit it. Chitin is made by chitin synthases requiring specific microvesicles, the chitosomes, for intracellular transport. Fungi contain several chitin synthases, some of which may be essential at a certain stage. This phenomenon is important to take into account for drug design.
The most widely studied chitin
synthase inhibitors are polyoxins and nikkomycins that probably bind to the
catalytic site of chitin synthases. These are not equally susceptible to the
drugs. In Saccharomyces cerevisiae the order of sensitivity is:
Chs3p>Chs1p>Chs2p. Main problems for their succesful use in vivo are: low
permeability, and different susceptibility of fungal species, and variable
responses in animal models. Chemical modifications have been proposed to make
more potent derivatives. Other synthetic or natural compounds are also
promising as possible inhibitors, but their properties are less well known.
Rational drug design has proceeded only on the basis of existing inhibitors,
because the structure of the active site of chitin synthase is unknown.
Undoubtedly, determination of this, and the biosynthetic mechanism will reveal
unexpected drug targets in the future.