|
Current Protein & Peptide
Science
ISSN: 1389-2042
Current Protein and Peptide
Science
Volume 8, Number 4, August 2007
Contents
Structure Based Drug Design
Guest Editor: K.V. Radha Kishan
Editorial Pp. 311
Structure-Based Drug Design: Docking and Scoring
Pp. 312-328
Romano T. Kroemer
[Abstract]
Virtual Screening in Drug Discovery – A Computational
Perspective Pp. 329-351
A. Srinivas Reddy, S. Priyadarshini Pati, P. Praveen Kumar,
H.N. Pradeep and G. Narahari Sastry
[Abstract]
Structure-Based Approaches in the Design of GSK-3
Selective Inhibitors Pp. 352-364
Dhilon S. Patel, Nigus Dessalew, Pansy Iqbal and Prasad
V. Bharatam
[Abstract]
Structure-Based Approaches to Drug Discovery Against
Tuberculosis Pp. 365-375
Simon J. Holton, Manfred S. Weiss, Paul A. Tucker and
Matthias Wilmanns
[Abstract]
Structural Biology, Protein Conformations and Drug
Designing Pp. 376-380
K.V. Radha Kishan
[Abstract]
General Articles
Free Resources to Assist Structure-Based Virtual Ligand
Screening Experiments Pp. 381-411
Bruno O. Villoutreix, Nicolas Renault, David Lagorce,
Olivier Sperandio, Matthieu Montes and Maria A. Miteva
[Abstract]
Recent Advances with TLR2-Targeting Lipopeptide-Based
Vaccines Pp. 412-417
Emily M.Y. Eriksson and David C. Jackson
[Abstract]
Abstracts
[Back to top]
Editorial
Structure based drug design is a phrase heard nowadays
quite frequently among people in the pharmaceutical industry
as well as in academic circles. The techniques used in structure
determination, both X-ray crystallography and NMR methods,
saw rapid advancements causing deposition of huge number of
structures in the Protein Databank (PDB). Numerous validation
methods and deposition of high resolution structures also
made the PDB more reliable for drug designing projects. With
time, the designing of drugs using protein/enzyme structures
is becoming more automated and robust. To cater to the needs
of the drug design process many methods have been developed,
using different algorithms, different strategies and different
scoring functions. Although many reviews have been published
in this area, new methods and protocols have been developed
which deserve constant reviewing. Therefore, it was felt that
a special issue on structure based drug design is required
with a different perspective.
In recent years the drug design is routinely done by screening
a virtual library of drug-like compounds. Since the number
of such compounds has increased in huge numbers, virtual screening
using docking methods are practiced. In this issue the review
by Romano Kroemer addresses the concepts used in receptor-ligand
docking and scoring methods, different approaches and algorithms.
He also outlined major challenges involved in structure based
design and addressed some of these challenges. Narahari Sastry’s
group has outlined the virtual screening process with a computational
perspective. His group described various computational methods
and their relative assessment. In their review Prasad Bharatam’s
group described the efforts made in the design of selective
inhibitors for Glycogen synthase kinase-3, a serine/threonine
kinase and a potential drug target for cancer, diabetes and
Alzheimer’s disease. In their review Matthias Wilmanns
and his colleagues outlined the key efforts by the German
groups involved in the Mycobacterium tuberculosis
structural genomics as a consortium. They highlighted some
important potential drug targets involved in metabolic pathways
from M. tuberculosis proteome. Finally, I have reviewed
the challenges posed by drug targets derived with multiple
conformations towards docking as well as virtual screening.
I would like to emphasize that this special issue was planned
to have a variety of articles addressing different topics
in structure based drug design. Structure based design has
now grown to a wide extent and these are not the only topics
considered in a design project. I believe that I am successful
in bringing out a collection of useful reviews for the drug
design community. I am very much thankful to all the authors
who contributed in this issue and patiently addressed the
shortcomings raised by various reviewers. I also thank all
the anonymous reviewers who were instrumental in bringing
out this issue. I take this opportunity to thank Prof. Ben
Dunn, who encouraged me to take up this editorial responsibility
and helped me at every stage of the editorial process.
K.V. Radha Kishan
Guest Editor
Current Protein and Peptide Science
GVK Bioscience Pvt. Ltd., S-1, Phase-1
TIE, Balanagar
Hyderabad 500 037
India
[Back to top]
Structure-Based Drug Design: Docking and Scoring
Romano T. Kroemer
This review gives an introduction into ligand – receptor
docking and illustrates the basic underlying concepts. An
overview of different approaches and algorithms is provided.
Although the application of docking and scoring has led to
some remarkable successes, there are still some major challenges
ahead, which are outlined here as well. Approaches to address
some of these challenges and the latest developments in the
area are presented. Some aspects of the assessment of docking
program performance are discussed. A number of successful
applications of structure-based virtual screening are described.
[Back to top]
Virtual Screening in Drug Discovery – A Computational
Perspective
A. Srinivas Reddy, S. Priyadarshini Pati, P. Praveen Kumar,
H.N. Pradeep and G. Narahari Sastry
Virtual screening emerged as an important tool in our quest
to access novel drug like compounds. There are a wide range
of comparable and contrasting methodological protocols available
in screening databases for the lead compounds. The number
of methods and software packages which employ the target and
ligand based virtual screening are increasing at a rapid pace.
However, the general understanding on the applicability and
limitations of these methodologies is not emerging as fast
as the developments of various methods. Therefore, it is extremely
important to compare and contrast various protocols with practical
examples to gauge the strength and applicability of various
methods. The review provides a comprehensive appraisal on
several of the available virtual screening methods to-date.
Recent developments of the docking and similarity based methods
have been discussed besides the descriptor selection and pharmacophore
based searching. The review touches upon the application of
statistical, graph theory based methods machine learning tools
in virtual screening and combinatorial library design. Finally,
several case studies are undertaken where the virtual screening
technology has been applied successfully. A critical analysis
of these case studies provides a good platform to estimate
the applicability of various virtual screening methods in
the new lead identification and optimization.
[Back to top]
Structure-Based Approaches in the Design of GSK-3
Selective Inhibitors
Dhilon S. Patel, Nigus Dessalew, Pansy Iqbal and Prasad
V. Bharatam
Glycogen Synthase Kinase-3 (GSK-3) is a serine/threonine kinase
with varied number of actions in cellular signalling systems
making it an emerging target for diseases such as diabetes
mellitus, cancer, chronic inflammation, bipolar affective
disorders and Alzheimer’s disease. Various efforts have
produced many potent small molecule inhibitors of GSK-3, which
are being tested for modulation of glycogen metabolism, gene
transcription, apoptosis and enhancement of insulin-stimulated
glucose transport. Majority of the reported inhibitors show
their inhibitory effects towards other phy-logenetically related
kinases also, like cyclin dependant kinases (CDKs). Thus it
is important to develop inhibitors that can inhibit GSK-3
selectively. Rational approaches based on the knowledge of
the receptor are best suited to address the selectivity problem.
Several crystal structures of GSK-3β
with different ligands are being reported. These are providing
the necessary clues regarding the interaction in the ligand
binding domain. Several molecular docking efforts are being
taken up to identify the clues for enhancing selectivity towards
GSK-3. In this review we present current efforts and future
opportunities in designing selective GSK-3 inhibitors.
[Back to top]
Structure-Based Approaches to Drug Discovery Against
Tuberculosis
Simon J. Holton, Manfred S. Weiss, Paul A. Tucker and
Matthias Wilmanns
Tuberculosis has become one of the deadliest global emergencies
due to the widespread existence of multiple drug resistance
strains of Mycobacterium tuberculosis and the increase
of immuno-compromised populations in large parts of the world.
Although the complete genome of M. tuberculosis became
available in 1998, opening unprecedented opportunities for
target-specific drug development, the progress since then
has been slow, mainly due to a lack of a sufficiently strong
interest by pharmaceutical and biotechnology industries. One
of the most promising tools for future drug discovery lies
in the elucidation of the molecular structures of potential
drug targets from the M. tuberculosis proteome. During
the last five years, the structures of about 200 unique targets
have already been determined, which comprise about 5% of the
entire M. tuberculosis proteome. As an example, we
present the approach and some of the key achievements of the
X-MTB consortium based in Germany. We summarize and discuss
some recent highlights of potential drug targets of M.
tuberculosis involved in lipid metabolism, protein phosphorylation/dephosphorylation
and amino acid biosynthesis. The achievements of several structural
genomics consortia that focus on targets from the M. tuberculosis
proteome are now providing a solid framework to support coordinated
international approaches for future structure-based drug discovery
programs at the interface between industrial enterprises and
academic research. One of the objectives will be to focus
on target complexes, in addition to single targets that dominate
the present repository of structures from the M. tuberculosis
proteome.
[Back to top]
Structural Biology, Protein Conformations and Drug
Designing
K.V. Radha Kishan
Structure based drug designing is now a popular technique
used for increasing the speed of drug designing process. This
was made possible by the availability of many protein structures
which helped in developing tools to understand the structure
function relationships, automated docking and virtual screening.
Knowledge of structure based functional properties of a drug
target is very essential for a successful in silico
designing of drugs. However, some problems associated with
the structure determination process and lack of knowledge
of conformational freedom associated with available protein
structures are the hurdles involved in structure based drug
designing. Docking and virtual screening processes depend
on the active site structure of the receptor molecule and
subtle differences in the conformations of these molecules
due to flexibility pose a serious threat to the drug designing
process. In this review problems associated with the conformations
of proteins and homology models was reviewed.
[Back to top]
Free Resources to Assist Structure-Based Virtual Ligand
Screening Experiments
Bruno O. Villoutreix, Nicolas Renault, David Lagorce,
Olivier Sperandio, Matthieu Montes and Maria A. Miteva
In today's research environment, a wealth of experimental/theoretical
structural data is available and the number of therapeutically
relevant macromolecular structures is growing rapidly. This,
coupled with the huge number of small non-peptide potential
drug candidates easily available (over 7 million compounds),
highlight the need of using computer-aided techniques for
the efficient identification and optimization of novel hit
compounds. Virtual (or in silico) ligand screening based on
the three-dimensional structure of macromolecular targets
(SB-VLS) is firmly established as an important approach to
identify chemical entities that have a high likelihood of
binding to a target molecule to elicit desired bio-logical
responses. A myriad of free applications and services facilitating
the drug discovery process have been posted on the Web. In
this review, we cite over 350 URLs that are useful for SB-VLS
projects and essentially free for academic groups. We attempt
to provide links for in silico ADME/tox prediction tools,
compound collections, some ligand-based methods, characterization/simulation
of 3D targets and homology modeling tools, druggable pocket
predictions, active site comparisons, analysis of macromolecular
interfaces, protein docking tools to help identify binding
pockets and protein-ligand docking/scoring methods. As such,
we aim at providing both, methods pertaining to the field
of Structural Bioin-formatics (defined here as tools to study
macromolecules) and methods pertaining to the field of Chemoinformatics
(defined here as tools to make better decisions faster in
the arena of drug/lead identification and optimization). We
also report several recent success stories using these free
computer methods. This review should help readers finding
free computer tools useful for their projects. Overall, we
are confident that these tools will facilitate rapid and cost-effective
identification of new hit compounds. The URLs presented in
this review will be updated regularly at www.vls3d.com in
the coming months, “Links” section.
[Back to top]
Recent Advances with TLR2-Targeting Lipopeptide-Based
Vaccines
Emily M.Y. Eriksson and David C. Jackson
The next generation of vaccines are being rationally designed
according to rules that govern the way in which antigen is
recognised by and stimulates the immune system. Amongst the
first cells that encounter potentially dangerous agents such
as viruses and bacteria are cells of the innate immune
system, such as dendritic cells, that are widely distributed
throughout the body including the skin. These cells patrol
most tissues and have on their surface an array of receptors
that have evolved to recognise many of the surface features
of pathogens including the lipids and carbohydrates of structural
lipoproteins, glycolipids and glycoproteins. Once encountered,
recognised and engaged by a particular receptor on the dendritic
cell, pathogenic material may then be transported inside the
cell and processed for presentation to cells of the adaptive
immune system. The result of this concert of events is a specific
cellular or antibody response to particular epitopes of the
invading pathogen. If then ways can be found to specifically
target dendritic cells, through their specific receptors,
then the efficacy and potency of vaccines could well be greatly
improved. This review covers some of the approaches that we
and others are pursuing in order to achieve this result.
|
