2. History
Methods of drug discovery
› Traditional
› Current
Life cycle of drug discovery
› Traditional
› CADD
Introduction to CADD
Objectives of CADD
Priciples involoved in CADD
Softwares for CADD
Advantages over traditional method of drug design
Future trends
Success stories of CADD
References
3. Early 19th century - extraction of compounds from
plants (morphine, cocaine).
Late 19th century - fewer natural products used, more
synthetic substances. Dye and chemical companies
start research labs and discover medical applications.
(Bayer)
1905 - John Langley: Theory of receptive substances
which stated “The concept of specific receptors that
bind drugs or transmitter substances onto the cell,
thereby either initiating biological effects or inhibiting
cellular functions”
4. 1909 - First rational drug design.
› Goal: safer syphilis treatment than Atoxyl.
› Paul Erhlich and Sacachiro Hata wanted to maximize
therapeutic index .
› Synthetic: 600 compounds; evaluated ratio of
minimum curative dose and maximum tolerated dose.
They found Salvarsan (which was replaced by
penicillin in the 1940’s)
1960 - First successful attempt to relate chemical
structure to biological action quantitatively.
As As
OH
NH2
OH
NH2
5. Mid to late 20th century - understand disease states,
biological structures, processes, drug transport,
distribution, metabolism. Medicinal chemists use
this knowledge to modify chemical structure to
influence a drug’s activity, stability, etc.
6. The time from conception to approval of a new
drug is typically 10-15 years.
• The estimated cost to bring to market a successful
drug is now $800 million!
• 20% cost increase per year.
7. Mainly by accident
Can be discovered by
› screening of new drugs
› modification for improvement
› mechanistic based drug design
› combining techniques
10. Where?
Random screening
› Synthetic chemicals
› Natural products
Epibatidine
Pacific yew tree
Taxol
11. Existing drugs
› Previously marketed for same disease
› Used for other diseases
O
NH
S
O
O
NH
tolbutamide
N
O
HS
HO2C
captopril
N
N
S
O
O
N
N
N
HN
O
O
viagra
12. Existing drugs
Natural substrate or product
› Alter structure (cimetidine)
› Product of enzyme catalysis
› Enzyme inhibitor
› Allosteric substrate
SS
EE
ES
PP
EE
EP
PP
EE
E + P
EE
SS
E + S
EE
23. Computer Aided drug design
lies In the hand of computational scientists, who
are able to manipulate molecule on the screen
Rather it is a complex process involving many
scientist from various stream working together.
24. Molecular mechanics or molecular dynamics
Drug design with the help of computers may be used at
any of the following stages of drug discovery:
› hit identification using virtual screening (structure- or
ligand-based design)
› hit-to-lead optimization of affinity and selectivity
(structure-based design, QSAR, etc.)
› lead optimization optimization of other pharmaceutical
properties while maintaining affinity.
25. Strucuture Based
Crystal Strucuture
Analysis
Homolgy Modeling
Computional Analysis of
Protien Lignad Interaction
Modification of Ligand within the
Active Site for Better Design
Lignad Based
QSAR Lead
Identification
In-Silico solubility, BBB
& Toxicity Prediction
Lead Optimization
Preclinical Trail
26. Structure Known Structure Unknown
Active Site Analysis
Ligand Binding Model via
Docking
Ligand Modification
Identify Template & Build
Model
Model Validation &
Optimization
Receptor Based Search in 3D
New Scaffold
database
search
combiLib
Synthesis
27. Ligand activites known Qualitative property information
optimization
Descriptor calculation Generate conformer
Feature
genreation
Pharmacophore
hypothesis
3D database
search
New scaffold
2D database
CombiLib with
new Scaffold
QSAR
Alignment
2D QSAR
CombiLib
Screening
of Library
Synthesis
28. To change from:
› Random screening against disease assays
› Natural products, synthetic chemicals
To:
› Rational drug design and testing
› Speed-up screening process
› Efficient screening (focused, target directed)
› De novo design (target directed)
› Integration of testing into design process
› Fail drugs fast (remove hopeless ones as early as possible)
30. Molecular mechanics refers to the use of classical mechanics
to model the geometry and motions of molecules.
Molecular mechanics methods are based on the following
principles:
1) Nuclei and electrons are lumped into atom-like
particles.
2) Atom-like particles are spherical (radii obtained from
measurements or theory) and have a net charge (obtained
from theory).
3) Interactions are based on springs and classical
potentials.
4) Interactions must be preassigned to specific sets of
atoms.
5) Interactions determine the spatial distribution of atom-
like particles and their energies.
31. The object of molecular mechanics is to predict the energy
associated with a given conformation of a molecule.
A simple molecular mechanics energy equation is given by:
Energy = Stretching Energy + Bending Energy
+Torsion Energy + Non-Bonded
Interaction Energy
32. The stretching energy equation is based on Hooke's law.
This equation estimates the energy associated with
vibration about the equilibrium bond length
In plot we notice that the model tends to break down as a
bond is stretched towards the point of dissociation
33. The bending energy equation is also based on Hooke's
law.
This equation estimates the energy associated with
vibration about the equilibrium bond angle
The larger the value , the more energy is required to
deform an angle (or bond) from its equilibrium value
34. The torsional energy represents the amount of energy
that must be added to or subtracted from the Stretching
Energy + Bending Energy + Non-Bonded Interaction
Energy terms to make the total energy agree with
experiment
A-controls the amplitude of
the curve,
n-controls its periodicity,
Ф- shifts the entire curve
along the rotation angle
axis (tau).
35. The non-bonded energy represents the pair-wise sum
of the energies of all possible interacting non-bonded
atoms i and j:
36. Quantum theory uses well known physical
constants ,such as velocity of light, values for the
masses & charges of nuclear particles to
calcaulate molecular properties
The equation from which molecular properties can
be derived from schrodinger equation
HΨ=EΨ
37. HΨ=EΨ
Full wave function Electron wave function
• E-energy of the system relative to all atomic particles
are separated to infinite distances
• H-is the Hamiltonian operator which includes both
kinetic and potential energy
38. Ab initio method
limited to ten no’s of atoms and & best
performed using super computers.
semiempirical
limited to hundreds of atoms can be
applied to organics ,organometalics and
small oligomers.
39. Nuclei and electrons are distinguished from
each other.
Electron-electron (usually averaged) and
electron-nuclear interactions are explicit.
Interactions are governed by nuclear and
electron charges (i.e. potential energy) and
electron motions.
Interactions determine the spatial distribution
of nuclei and electrons and their energies.
40. To place a ligand (small molecule) into the binding site
of a receptor in the manners appropriate for optimal
interactions with a receptor.
To evaluate the ligand-receptor interactions in a way
that may discriminate the experimentally observed
mode from others and estimate the binding affinity.
ligand
receptor
complex
docking scoring
… etc
X-ray structure
& ∆G
41. To Reduce cost
Core of the target-based structure-based drug design
(SBDD) for lead generation and optimization.
42. Representation of receptor
binding site and ligand
pre- and/or
during docking:
Sampling of configuration space
of the ligand-receptor complex
during docking:
Evaluation of ligand-receptor
interactions
during docking
and scoring:
43. • Protien – Ligand Studies
• Flexible Ligand, Rigid Receptor
• Search much Larger Space
• Search the conformational Space using
Molecular Dynamic
• Protien- Protien Docking
• Both Molecule Usually Considered Rigid
• 6 Degree of freedom
• 1st
aplly stearic Constrains to limits search
Space & then examine Energetic of Possible
Binding Conformation.
44. Determine the lowest free energy structures for
the receptor-ligand complex
Search database and rank hits for lead
generation
Calculate the differential binding of a ligand to
two different macromolecular receptors
Study the geometry of a particular complex
Propose modification of a lead molecules to
optimize potency or other properties
de novo design for lead generation
Library design
45. HIV protease inhibitor amprenavir (Agenerase)
from Vertex & GSK (Kim et al. 1995)
HIV: nelfinavir (Viracept) by Pfizer (& Agouron)
(Greer et al. 1994)
Influenza neuraminidase inhibitor zanamivir
(Relenza) by GSK (Schindler 2000).
46.
47. visualization:
Program name Web site
Rasmol www.openrasmol.org
MolVis http://molvis.sdsc.edu/visres
PyMol http://pymol.sourceforge.net
DeepView http://us.expasy.org/spdbv/
JMol http://jmol.sourceforge.net
gOpenMol www.csc.fi/gopenmol/
AstexViewer www.astex-therapeutics.com
48. Docking:
Program name Web site
ArgusDock www.Arguslab.com
DOCK https://dock.compbio.uscsf
.edu
FRED www.eyesopen.com
eHITS www.symbiosys.ca/
Autodock www.scripps.edu
FTDock www.bmm.icnet.uk/dockin
g/ftdock.html
49. QSAR Descriptor:
Program name Web site
SoMFA http://bellatrix.pcl.ox.ac.uk/
GRID www.moldiscovery.com/
E-Dragon1.0 http://146.107.217.178/lab/edragon
ALOGPS2.1 http://146.107.217.178/lab/alogps/
Marvin beans www.chemaxon.com/
50. software libraries:
Program name Web site
Chemical development kit http://almost.cubic.uni-
koeln.de/cdk/
Molecular modeling toolkit http://starship.python.net/crew/hise
n/MMTK/
PerlMol www.perlmol.org
JOELib www.ra.informatik.uni-
tuebingen.de/software/joelib/
OpenBabel http://openbabel.sourceforge.net
51. Time
cost
Accuracy
information about the disease
screening is reduced
Database screening
less manpower is required
55. • Aldose reductase inhibitors
• database searching
• Y. Iwata et al., J. Med. Chem. 44, 1718-1728,
2001
Non nucleoside inhibiitor of HIV-1 reverse Transcriptase
› structure and ligand based design
› William L. Jorgensen et al., bioorganic and midicinal
chemistry letters, 16, 663-667, 2006
56. DDT , “Keynote review: Structural biology and drug
discovery” Miles Congreve,Christopher W.Murray and Tom
L.Blundell, Volume 10, Number 13 • July 2005
Current Opinion on Pharmacology“Computer-aided drug-
discovery techniquesthataccountfor receptor flexibility”
Jacob DDurrant and JAndrewMcCammon, 10, 1-5, 2010.
Bioorganic and Medicinal chemistry “Drug Guru: A
computer software program for drug design using medicinal
chemistry rules” , Kent D. Stewart, Melisa Shirodaa and
Craig A. James, 14, 7011–7022, 2010.
57. Chemico-Biological Interactions, “Computer-aided drug
discovery and development (CADDD): Insilico-
chemico-biological approach”, I.M. Kapetanovic, 171,
165–176. (2008) .
Drug Discovery Today “Shape Signatures: speeding up
computer-aided drug discovery”, Peter J. Meek et al. ,
Volume 11, Numbers 19/20 October 2006.
DDT, “Optimizing the use of open-source software
applications in drug discovery”, Werner J.Geldenhuys et
al., Volume 11, Number 3/4 • February 2006.
Bioorganic & Medicinal Chemistry Letters “Computer-
aided design of non-nucleoside inhibitors of HIV-1
reverse transcriptase” , 16, 663–667, 2006.
58. Drug Discovery Today: Technologies, “ New
technologies in computer-aided drug design: Toward
target identification and new chemical entity discovery”,
Yun Tang, Weiliang Zhu, Kaixian Chen, Hualiang Jiang,
Vol. 3, No. 3 2006.
Journal of Molecular Graphics and Modelling,
“Combining structure-based drug design and
pharmacophores”, Renate Griffith, 23, 439–446, 2005.
Chemistry & Biology, “The Process of Structure-Based
Drug Design”, Vol. 10, 787–797, September, 2003.
EMBO-Course: “Methods for Protein Simulation &
Drug Design.” Shanghai, China, September 13-24,
2004.
59. The Organic Chemistry of the drug design & drug
action by Richard B. Silverman
Principles of Medicinal Chemistry by William O.Foye.
Burger’s Medicinal Chemistry & Drug Discovery, Sixth
edition
Wilson & Gisvold’s Textbook of Organic Medicinal &
Pharmaceutical Chemistry, Eleventh edition.
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