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Transcript
Advanced Medicinal
Chemistry
Lecture 1:
Target Classes
Dr Jeff Stonehouse
AstraZeneca R&D Charnwood
The Drug Discovery Process
Target
Identification
3 months to
2 years!
HTS
3-4 months
Active-to-Hit
(AtH)
3 months
Hit-to-Lead
(HtL)
6-9 months
New Lead
Optimisation
Projects (LO)
2 years
Candidate
Drug (CD)
Taxonomy of Biological Mechanisms
Receptors -
In vivo
Effectors
agonists
antagonists
partial agonists
inverse agonists
Enzymes -
inhibitors
Ion Channels openers
blockers
Protein-Protein inhibitors
Blockbuster Drugs
Lipitor
HMG CoA inhibitor
HO
Plavix
Anti-platelet
O
OH
Cl
COOMe
OH
F
N
H
N
Enzyme
Cholesterol
Pfizer
$12.0 billion
Norvasc
Calcium channel blocker
Nexium
Proton pump inhibitor
Cl
O
O
O
N
O
O
S
N
N
Anti-ulcer
AstraZeneca
$4.8billion
Receptor
S
Thrombosis
BMS/Sanofi-Aventis
$5.0billion
O
O
N
Enzyme
N
H
O
O
Hyper-tension
Pfizer
$4.8billion
NH2
Ion-channel
Biological Mechanisms
2005 Top 50 drugs by Worldwide sales
Enzyme
Inhibitor
38%
Receptor
Antagonist
24%
Misc
8%
Receptor
Agonist
12%
Biological
10%
Ion Channel
Modulator
8%
Enzyme function
TS
NH2
O
Free Energy
NH
+
H2N
OH
O
NH2
NH
O2
iNOS
H2N
OH
O
E
S
+ NO
Free Energy
HN
TS
S
P
P
Progress of Reaction
E + S
Progress of Reaction
ES
#
E + P
Active Site is tailored to bind the transition state for S
P
Usually, the substrate & inhibitors bind at the active site
Allosteric (non-competitive) binding occurs remotely to the active site
Enzyme Inhibition - Four mechanistic categories
1. Competitive inhibition. Inhibitor competes reversibly with substrate for the
active site.
2. Uncompetitive inhibition. Inhibitor binds only to the ES complex, leading
to EIS intermediates. This is very rare.
3. Non-competitive inhibition. Inhibitor binds non-covalently to sites
other than the active site (Allosteric inhibition). Kinetics are complex and
partially inhibited enzymes can still turn over substrate.
Enzyme Inhibition - Four mechanistic categories
4. Irreversible inhibition. Inhibitor binds covalently, usually to the active
site machinery. Also known as Suicide inhibitors. Examples include
MAO inhibitors and b-lactamase inhibitors:
NH2
p-OH-Ph
NH2
H
N
O
Amoxycillin
b
S
N
OH
turnover
O
p-OH-Ph
O
HO
H
N
S
O HN
CO2H
O
Clavulanic
acid
N
O
CO2H
OH
CO2H
b
Scys
OH
irreversible
inhibition
b
O
O
Proteases
(proteinases, peptidases)
Hydrolytically cleave peptidic amide bonds
Endopeptidases
Exopeptidases
cleavage site may be anywhere in the substrate
terminal residue (carboxypeptidase, aminopeptidase)
Four Mechanistic Classes
Nucleophile
pH preference
Endo/Exo
Serine
Ser-CH2OH
~7
endo
Cysteine (thiol)
Cys-CH2SH
~7
endo
Aspartic
H 2O
3-6
endo
Zinc (metallo)
H 2O
~7
endo/exo
Protease Specificity
Determined by the binding of substrate amino acid
side-chains near the cleavage site
Specificity-Pocket nomenclature
(Schechter & Berger, Biochem Biophys Res Com, 1967, 27, 157-162)
substrate
N-terminus
N
H
S3
S1
S2’
P3
P1
P2'
O
H
N
N
H
O
P2
S2
..
E-XH
non-prime side
H
N
O
N
H
O
H
N
Substrate
C-terminus
O
P1'
P3'
S1’
S3’
prime side
Serine Proteases
Thrombin, Tryptase , b-Lactamase, Elastase, Chymotrypsin, HCV-NS3
Asp102
Catalytic triad
O
O
boosts serine nucleophilicity
H
Inhibitors create or mimic
stable tetrahedral
intermediates
N
His57
N
N
enzyme
H
O
O
Ser195
P1
substrate
O
H
N
N
H
b-lactams
O
NHCOR
CF3
trifluoromethyl
ketones
P1'
O
P1 is the primary
specificity site
O
N
O
S
X
O
saccharins
Biological Mechanisms
2005 Top 50 drugs by Worldwide sales
Receptor
Antagonist
24%
Enzyme
Inhibitor
38%
Misc
8%
Receptor
Agonist
12%
Biological
10%
Ion Channel
Modulator
8%
Receptors
Receptors are membrane-bound proteins that bind endogenous
ligands (usually extracellular) to induce a phsiological effect
(usually intracellular)
A receptor is often the first step in a long intracellular signalling
cascade leading to physiological effects
G-Protein Coupled, Seven-Transmembrane Spanning Receptors
comprise the majority of known examples
extracellular
7TM GPCR
intracellular
a-adrenoceptor
extracellular loops
ligand recognition & binding
N-terminus
I
membrane
intracellular loops
signalling
G-protein coupling
C-terminus
Binding to Receptors
R
R*
ground-state
receptor
Excited-state
receptor
no signal
signal
Agonist
a ligand that binds to, and provokes a signal from a
receptor via conformational changes in the excited state
Antagonist
a ligand that binds to a receptor and induces no signal.
Blocks agonist binding. Little conformational change
overall
ligands can be proteins, peptides or small molecules
Binding to Receptors
Agonists & Antagonists bind competitively - beware misunderstandings
from binding data without further functional analysis
Endogenous agonists often bind weakly (enthalpy driven)
Successful antagonists often bind tightly (entropy driven)
Agonist
Partial
Agonist
Antagonist
Inverse
Partial
Agonist
Inverse
Agonist
Biological Mechanisms
2005 Top 50 drugs by Worldwide sales
Receptor
Antagonist
24%
Enzyme
Inhibitor
38%
Misc
8%
Receptor
Agonist
12%
Biological
10%
Ion Channel
Modulator
8%
Ion Channels
All of life exists within an electric potential
window of less than one volt
The membrane potential of most cells is 60-70mV
Ion channels regulate passive ion flow through
membranes in an electric or concentration gradient
Channels are ion selective and comprise groups of
glycoprotein subunits in homo- or heteropolymer
arrays. Almost no channels have an open rest state
Channels are involved in cardiac, neuronal, psychiatric and (?) R&I disorders
Which ions?
hERG (iKr) channel:
Na+
K+
Ca++
-
( Cl )
blockade causes prolongation of cardiac Q-T interval
“Long QT syndrome” can lead to sudden death
Ion Channels
Channel families are complex, but all channels are either
Voltage-gated
or
Ligand-gated
Ligands can be other ions, small molecules or toxins & venoms such as
tetrodotoxin, pumiliotoxin, margatoxin & charybdotoxin
Blockbuster antihypertensive drugs have emerged from calciumchannel antagonist programmes
– Nifedipine, Nimodipine, Isradipine, Amlodipine (NorVasc™)