Cheminformatics

Cheminformatics

Noel M. O‟Boyle

July 2012
EMBL-EBI/Wellcome Trust Course: Resources for
Computational Drug Discovery

Cheminformatics
• Hard to define in words:
– David Wild: “The field that studies all aspects of the representation and use
of chemical and related biological information on computers”
– Design, creation, organization, management, retrieval, analysis,
dissemination, visualization and use of chemical information
• Hard to agree on spelling:
– Sometimes chemoinformatics
• More easily thought of as encompassing a range of concepts
and techniques
– Molecular similarity
– Quantitative-structure activity relationships (QSAR)
– Substructure search
– (Automated) Molecular depiction
– Encoding/decoding of molecular structures
– 3D structure generation from a 2D or 0D structure
– Conformer generation
– Algorithms: ring perception, aromaticity, isomers

References
• An introduction to cheminformatics, A. R.
Leach, V. J. Gillet
• Cheminformatics, Johann Gasteiger and
Thomas Engel (Eds)
• Molecular modelling – Principles and
Applications, A. R. Leach

• I571 Chemical Information Technology, David
Wild, University of Indiana
http://i571.wikispaces.com/

Molecular representation

Mike Hann (GSK): “Ceci n'est pas une molecule serves
to remind us that all of the graphics images presented
here are not molecules, not even pictures of molecules,
but pictures of icons which we believe represent some
aspects of the molecule's properties.”
http://mgl.scripps.edu/people/goodsell/mgs_art/hann.html

Computer representations of molecules
• How can a molecular structure be stored on
a computer?
– Common names: aspirin
– IUPAC name: 2-acetoxybenzoic acid
– Formula: C9H8O4
– As an image (PNG, GIF, etc.)
– CAS number: 50-78-2
– File format: ChemDraw file, MOL file, etc.
– SMILES string: O=C(Oc1ccccc1C(=O)O)C
– Binary Fingerprint:
10000100000001100000100100000001
http://en.wikipedia.org/wiki/Aspirin

• How should it be stored?
– …if I want to use it for computation
– ...if I want a unique identifier
– …if I want to retain stereochemical information

Computer representations of molecules
• The structure of a molecule can be represented by
a graph
– Graph = collection of nodes and edges, nodes and
edges have properties (atomic number, bond order)
• Represent the molecular graph somehow
– Connection table (which nodes are connected to which
other nodes)
– Line notation (e.g. SMILES)

Fig 12.2: Molecular modelling – principles and applications, Andrew R Leach, Pearson, 2nd edn.

Chemical file formats

• A large number of file formats have been developed, but there are certain de-facto
standards
• 2D/3D structures:
– MOL file for small-molecule structures
– PDB files for protein structures from crystallography
– MOL2 files for protein structures from modelling software (e.g. after manipulation of the PDB
file)
• Line notations:
– SMILES format, InChI format

A chemical file format: MOL file
Fig 12.3: Molecular modelling – principles and applications, Andrew R Leach, Pearson, 2nd edn.

• This file format can represent 0D, 2D information (a
depiction) as well as 3D

SMILES format
• Simplified Molecular Input Line Entry System
– Weininger, J Chem Inf Comput Sci, 1988, 28, 31
– More recently, a community developed description:
http://opensmiles.org
– Linear format (“line notation”) that describes the connection table
and stereochemistry of a molecule (i.e. 0D)
– Convenient to enter as a query on-line, store in a spreadsheet,
pass by email, etc.
• Examples:
– CC represents CH3CH3 (ethane)
– CC(=O)O represents CH3COOH (acetic acid)
• Basic guidelines:
– Hydrogens are implicit
– Parentheses indicate branches
– Each atom is connected to the preceding atom to its left (excluding
branches in-between)
– Single bonds are implicit, = for double, # for triple
• What does the SMILES string OCC represent?

SMILES format II
• To represent rings, you need to break a ring bond and replace it
by a ring opening symbol and a corresponding ring closure
symbol Br

1 1 C C
C1CCC=CC1
Cl

• To represent double bond stereochemistry you use / and
• Cl/C=C/Br (trans), Cl/C=CBr (cis)
• To represent tetrahedral stereochemistry you use @ or @@
• Br[C@](Cl)(I)F means that looking from the Br, the Cl, I, and
F are arranged anticlockwise
• To represent aromaticity, use lower case
• C1CCCCC1 (cyclohexane)
• c1ccccc1 (benzene)

Canonical SMILES
• In general, many different SMILES strings can be written
for the same molecule
– Not a unique identifier (one-to-many)
– Ethanol: CCO, OCC, C(O)C
• Algorithms for producing “canonical SMILES” have been
developed
– The same unique SMILES string is always created for a
particular molecule
– One-to-one relationship between structure and
representation
– Note however, that different software implement different
canonicalisation algorithms
• Uses:
– Can be used to remove duplicate molecules from a database
• Generate the canonical SMILES for each molecule and ensure that
they are unique
– Check identity (compare two molecules)
• Did this software change the structure? Or get the stereochemistry
confused?

SMILES format III
• There a couple of nice features of the SMILES format that
can come in handy when manipulating structures

• Concatentating SMILES strings creates a bond between
fragments
– CC and CO gives CCCO
– Can be used for combinatorial chemistry, e.g. generating all
possible products from a 4-component Ugi reaction
– Can be used to prepare polymers by concatenating
monomers
– Open Babel can be used to prepare suitable SMILES strings

• In file format conversion, the atom order in a SMILES
string is usually preserved in the output format
– Sometimes you need a particular atom to be atom#1 in the
file format (e.g. for covalent docking in GOLD)
• Write the corresponding SMILES and convert to a 3D format

InChI
• International Chemical Identifier
– Line notation developed by NIST and IUPAC
– Goal: An index for uniquely identifying a molecule

Aspirin
InChI=1/C9H8O4/c1-6(10)13-8-5-3-2-4-7(8)9(11)12/h2-5H,1H3,(H,11,12)/f/h11H

• Features
– Derived from the structure (unlike CAS number)
– One-to-one relationship between InChI and structure (“canonical”)
– Layers (of specificity)
• Can distinguish between stereoisomers, isotopes, or can leave out those layers
– Different tautomeric forms give rise to the same InChI (unlike SMILES)
• Notes
– Not human readable or writeable
– All implementations use the same (open source) code which is provided
by the InChI Trust
• “The Trust's goal is to enable the interlinking and combining of chemical, biological
and related information, using unique machine-readable chemical structure
representations to facilitate and expedite new scientific discoveries.”
• For more info, see http://www.inchi-trust.org under Downloads

A unique identifier makes it easy to link databases

DrugBank
ChEBI

US Generic Legislation
• Comprehensive Drug Abuse and Control Act, 1970
• Controlled Substances Act, 1970
• Federal Analog Act, 1986

• The term “controlled substance analog” means a substance
– The chemical structure of which is substantially similar to the chemical structure of a
controlled substance in schedule I or II

Slide courtesy Dr. J.J. Keating, School of Pharmacy, University College Cork

Molecular similarity
• Similarity principle:
– Structurally similar molecules tend to have similar properties
• Properties: biological activity, solubility, color and so on

• If we can measure similarity somehow…
– Can construct a distance matrix
• Distance = inverse of similarity
• Such matrices can be used to cluster compounds, to create a 2D
depiction showing the spread of molecular structures in a dataset,
to select a diverse subset
– Can use to find molecules in a database similar to a
particular query
– Can use to see whether a particular property is correlated
with molecular similarity

• ...But how to measure similarity?
– One way is using molecular fingerprints

Molecular fingerprints
• A molecular fingerprint is an encoding of the molecular structure
onto a (long) binary string
– 100100010000001011000000000001...

• Path-based fingerprints (e.g. Daylight fingerprint)
– Break the molecule up into all possible fragments of length 1, 2,
3...7
– Create a string representing each fragment
– Hash each string onto a number between 1 and 1024 (for example)
• Wikipedia: “A hash function is any well-defined procedure or mathematical
function that converts a large, possibly variable-sized amount of data into a
small datum, usually a single integer that may serve as an index to an array”
– Set the corresponding bit of the fingerprint to 1 (all others will be 0)

• Key-based fingerprints (e.g. MACCS keys)
– A (long) list of pre-generated questions about a chemical structure
• “Are there fewer than 3 oxygens?”
• “Is there an S-S bond?”
• “Is there a ring of size 4?”
– Each answer, true or false, corresponds to a 1 or 0 in the binary
fingerprint

Similarity of molecular fingerprints
• Molecules with the same bits set will be more similar than
molecules with different bits set

• To quantify this, we can use the Tanimoto coefficient
– Tanimoto Similarity = Intersection/Union
– Bounded by 0 and 1 (no similarity to perfect similarity)
– A value of greater than 0.7 or 0.8 indicates structural similarity

• How similar are aspirin (A) and salicylic acid (B)?

• Using a path-based fingerprint, 64 bits are set for A, 38 for B
• Intersection is 38 (Note: B is a substructure of A)
• Union is 64
• Similarity = 0.59

Similarity of atom environments
• Fingerprints can also be used to measure similarity
of atom environments
• Circular fingerprints (HOSE codes)
– Bremser, W., HOSE – a novel substructure code. Anal.
Chim. Acta 1978, 103, 355.
– Describe atom environment in terms of atom types at
various bond distances from a particular atom
• Can be used for proton NMR prediction
– Hydrogens attached to similar atoms tend to have
similar NMR shifts
– Given a database of molecules with assigned NMR Image: T. Davies, W. Robien, J. Seymour.
spectra, try to find Hs in the same environment up to as Spectroscopy Europe, 2006, 18, 22
many levels as possible and use their NMR shifts to (http://www.modgraph.co.uk/Downloads/T
predict the shift for your proton D_18_1.pdf)
• The same database can be used for structure
identification
– Given a proton NMR spectrum, what chemical structures
are consistent with the NMR

• NMRShiftDB (http://nmrshiftdb.org)
– Freely available Open database of NMR spectra – add your own spectra (with assigned
peaks) – predict assignments
– Tutorial: http://nmrshiftdb.sourceforge.net/nmrshiftdbebitraining.pdf

Substructure search using SMARTS
• SMARTS – an extension of SMILES for substructure searching
– Can be used to find molecules with a particular substructure
– Can be used to filter out molecules with a particular substructure

• Simple example
– Ether: [OD2]([#6])[#6]
• Any oxygen with exactly two bonds each to a carbon
• Can get (a lot) more complicated
– Carbonic Acid or Carbonic Acid-Ester:
[CX3](=[OX1])([OX2])[OX2H,OX1H0-1]
• Hits acid and conjugate base. Won't hit carbonic acid diester

SMARTSviewer
http://smartsview.zbh.uni-hamburg.de/
K. Schomburg, H.-C. Ehrlich, K.
Stierand, M.Rarey. “From Structure Diagrams
to Visual Chemical Patterns” J. Chem. Inf.
Model., 2010, 50, 1529.

[CX3](=[OX1])([OX2])[OX2H,OX1H0-1]

Substructure search using SMARTS
• SMARTS – an extension of SMILES for substructure searching
– Can be used to find molecules with a particular substructure
– Can be used to filter out molecules with a particular substructure

• Simple example
– Ether: [OD2]([#6])[#6]
• Any oxygen with exactly two bonds each to a carbon
• Can get (a lot) more complicated
– Carbonic Acid or Carbonic Acid-Ester:
[CX3](=[OX1])([OX2])[OX2H,OX1H0-1]
• Hits acid and conjugate base. Won't hit carbonic acid diester

• Examples of use
– Filtering structures
– Identify substructures that are associated with toxicological
problems
– Develop or use a group contribution descriptor such as TPSA

FAF-Drugs2: Free ADME/tox filtering tool to assist drug discovery
and chemical biology projects, Lagorce et al, BMC Bioinf, 2008, 9, 396.

Calculation of Topological Polar Surface Area

• TPSA
• Ertl, Rohde, Selzer, J. Med.
Chem., 2000, 43, 3714.
• A fragment-based method
for calculating the polar
surface area

Quantitative Structure-Activity Relationships (QSAR)

• Also QSPR (Structure-Property)
– Exactly the same idea but with some physical property
• Create a mathematical model that links a molecule‟s structure to a
particular property or biological activity
– Could be used to perceive the link between structure and function/property
– Could be used to propose changes to a structure to increase activity
– Could be used to predict the activity/property for an unknown molecule

• Problem: Activity = 2.4 * Does not compute!

• Need to replace the actual structure by some values that are a
proxy for the structure - “Molecular descriptors”
• Numerical values that represent in some way some physico-chemical
properties of the molecule
• We saw one already, the Total Polar Surface Area
• Others: molecular weight, number of hydrogen bond donors, LogP
(octanol/water partition coefficient)
• It is usual to calculate 100 or more of these

Building and testing a predictive QSAR model

• Need dataset with known values for the property of
interest
– Divide into 2/3 training set and 1/3 test set
• Choose a regression model
– Linear regression, artificial neural network, support vector
machine, random forest, etc.
• Train the model to predict the property values for the
training set based on their descriptors
• Apply the model to the test set
– Find the RMSEP and R2
• Root-mean squared error of prediction and correlation coefficient

• Practical Notes:
– Descriptors can be calculated with the CDK or RDKit
– Models can be built using R (r-project.org)
– For a combination of the two, see rcdk

Lipinski‟s Rule of Fives
Chris Lipinski
Note: Rule of thumb

Rule of Fives
Oral bioavailability

• Lipinski took a dataset of drug candidates that made it to Phase II
• He examined the distribution of particular descriptor values related to
ADME
• An orally active drug should not fail more than one of the following
„rules‟:
– Molecular weight <= 500
– Number of H-bond donors <= 5
– Number of H-bond acceptors <= 10
– LogP <= 5
• These rules are often applied as an pre-screening filter
Image: http://collaborativedrug.com/blog/blog/2009/10/07/cdd-community-meeting/

Open Source cheminformatics software resources

• GUI:
– Open Babel
– LICSS – Excel-CDK interface

• Command-line interface:
– Open Babel (“babel”)
– MayaChemTools

• Programming toolkits:
– Open Babel (C++, Perl, Python, .NET, Java), RDKit (C++, Python),
Chemistry Development Kit [CDK] (Java, Jython, ...), PerlMol (Perl),
MayaChemTools (Perl)
– Cinfony (by me!) presents a simplified interface to some of these

• Specialized toolkits:
– OSRA: image to structure
– OPSIN: name to structure
– OSCAR: Identify chemical terms in text

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