1. Drug Design Optimizing Target Interactions
Chapter 13 Part 3

2. 1. Drug design - optimizing binding interactions
Aim - To optimize binding interactions with target
Reasons
To increase activity and reduce dose levels
To increase selectivity and reduce side effects
Strategies
Vary alkyl substituents
Vary aryl substituents
Extension
Chain extensions / contractions
Ring expansions / contractions
Ring variation
Isosteres
Simplification
Rigidification

3. 2. Vary alkyl substituents
Rationale:
Alkyl group in lead compound may interact with hydrophobic
region in binding site
Vary length and bulk of group to optimise interaction

4. 2. Vary alkyl substituents
Rationale:
Vary length and bulk of alkyl group to introduce selectivity
Binding region for N
Receptor 1
Receptor 2

5. 2. Vary alkyl substituents
Rationale:
Vary length and bulk of alkyl group to introduce selectivity
Example:
Selectivity of adrenergic agents for b-adrenoceptors over a-adrenoceptors

6. 2. Vary alkyl substituents
Adrenaline
Salbutamol
(Ventolin)
(Anti-asthmatic)
Propranolol
(b-Blocker)

7. a-Adrenoceptor H-Bonding region Ionic bonding Van der Waals

8. a-Adrenoceptor
ADRENALINE

9. a-Adrenoceptor

10. b-Adrenoceptor
ADRENALINE

11. b-Adrenoceptor
SALBUTAMOL

12. b-Adrenoceptor

13. a-Adrenoceptor
SALBUTAMOL

14. a-Adrenoceptor
SALBUTAMOL

15. a-Adrenoceptor
SALBUTAMOL

16. a-Adrenoceptor
SALBUTAMOL

17. a-Adrenoceptor
SALBUTAMOL

18. a-Adrenoceptor
SALBUTAMOL

19. a-Adrenoceptor
SALBUTAMOL

20. a-Adrenoceptor

21. 2. Vary alkyl substituents
Synthetic feasibility of analogues
Feasible to replace alkyl substituents on heteroatoms with other alkyl substituents
Difficult to modify alkyl substituents on the carbon skeleton of a lead compound.

22. 2. Vary alkyl substituents
Methods

23. 2. Vary alkyl substituents
Methods

24. 3. Vary aryl substituents
Vary substituents
Vary substitution pattern
Weak
H-Bond
Binding Region
(H-Bond)
(for Y)
Strong
H-Bond
(increased
activity)

25. 3. Vary aryl substituents
Vary substituents
Vary substitution pattern
Benzopyrans
Anti-arrhythmic activity best when substituent is at 7-position

26. Inductive electron withdrawing effect
3. Vary aryl substituents
Vary substituents
Vary substitution pattern
Para substitution:
Electron withdrawing effect due to resonance + inductive effects leading to a weaker base
Meta substitution:
Inductive electron withdrawing effect
Notes
Binding strength of NH2 as HBD affected by relative position of NO2
Stronger when NO2 is at para position

27. 4. Extension - extra functional groups
Rationale: To explore target binding site for further binding
regions to achieve additional binding interactions
RECEPTOR
RECEPTOR
Extra
functional
group
Unused
binding
region
DRUG
DRUG
Drug
Extension
Binding regions
Binding group

28. 4. Extension - extra functional groups
Example: ACE Inhibitors
Hydrophobic pocket
Vacant
EXTENSION
Hydrophobic pocket
Binding
site
Binding
site

29. 4. Extension - extra functional groups
Example: Nerve gases and medicines
Sarin
(nerve gas)
Ecothiopate
(medicine)
Notes:
Extension - addition of quaternary nitrogen
Extra ionic bonding interaction
Increased selectivity for cholinergic receptor
Mimics quaternary nitrogen of acetylcholine
Acetylcholine

30. 4. Extension - extra functional groups
Example: Second-generation anti-impotence drugs
Viagra
Notes:
Extension - addition of pyridine ring
Extra van der Waals interactions and HBA
Increased target selectivity

31. 4. Extension - extra functional groups
Example: Antagonists from agonists
Propranolol
(b-Blocker)
Adrenaline
Cimetidine (Tagamet)
(Anti-ulcer)
Histamine

32. 5. Chain extension / contraction
Rationale:
Useful if a chain is present connecting two binding groups
Vary length of chain to optimise interactions
Weak
interaction
Strong
interaction A B
Chain
extension A B
RECEPTOR
RECEPTOR
Binding regions
Binding groups
A & B

33. 5. Chain extension / contraction
Example: N-Phenethylmorphine
Binding
group
Optimum chain length = 2

34. Better overlap with hydrophobic interactions
6. Ring expansion / contraction
Rationale:
To improve overlap of binding groups with their binding regions R
Ring
expansion R
Better overlap with hydrophobic interactions
Hydrophobic regions

35. Carboxylate ion out of range
6. Ring expansion / contraction
Vary n
to vary
ring size
Example:
Binding regions
Binding site
Binding site
Two interactions
Carboxylate ion out of range
Three interactions
Increased binding

36. 7. Ring variations Rationale:
Replace aromatic/heterocyclic rings with other ring systems
Often done for patent reasons
General structure
for NSAIDS
Core
scaffold

37. 7. Ring variations Rationale: Sometimes results in improved properties
Example:
UK-46245
Improved selectivity
Ring
variation
Structure I
(Antifungal agent)
UK-46245
Improved selectivity
Ring
variation
Structure I
(Antifungal agent)

38. 7. Ring variations Example - Nevirapine (antiviral agent) Additional
binding group

39. Selective for b-adrenoceptors over a-adrenoreceptors
7. Ring variations
Example - Pronethalol (b-blocker)
Selective for b-adrenoceptors
over a-adrenoreceptors

40. 8. Isosteres and bio-isosteres
Rationale for isosteres:
Replace a functional group with a group of same valency (isostere)
e.g. OH replaced by SH, NH2, CH3
O replaced by S, NH, CH2
Leads to more controlled changes in steric / electronic properties
May affect binding and / or stability

41. 8. Isosteres and bio-isosteres
Useful for SAR
Propranolol (b-blocker)
Propranolol (b-blocker)
Notes
Replacing OCH2 with CH=CH, SCH2, CH2CH2 eliminates activity
Replacing OCH2 with NHCH2 retains activity
Implies O involved in binding (HBA)

42. 8. Isosteres and bio-isosteres
Rationale for bio-isosteres:
Replace a functional group with another group which retains the same biological activity
Not necessarily the same valency
Example:
Antipsychotics
Sultopride DU DU
Pyrrole ring =
bio-isostere for
amide group
Improved selectivity for D3 receptor over D2 receptor

43. 9. Simplification Rationale:
Lead compounds from natural sources are often complex and difficult to synthesize
Simplifying the molecule makes the synthesis of analogues easier, quicker and cheaper
Simpler structures may fit the binding site better and increase activity
Simpler structures may be more selective and less toxic if excess functional groups are removed

44. 9. Simplification Methods: Retain pharmacophore
Remove unnecessary functional groups

45. 9. Simplification Methods: Remove excess rings Example:
Excess functional groups
Excess ring

46. 9. Simplification
Methods:
Remove asymmetric center
Asymmetric center

47. 9. Simplification Methods:
Simplify in stages to avoid oversimplification
Pharmacophore
Notes:
Simplification does not mean ‘pruning groups’ off the lead compound
Compounds usually made by total synthesis

48. INT104

49. INT104

50. INT104

51. INT104

52. INT104

53. 9. Simplification Example: Important binding groups retained
Pharmacophore
Important binding groups retained
Unnecessary ester removed
Complex ring system removed

54. 9. Simplification Disadvantages:
Oversimplification may result in decreased activity and selectivity
Simpler molecules have more conformations
More likely to interact with more than one target binding site
May result in increased side effects

55. INT115
Target binding site

56. INT116
Target binding site

57. Rotatable bonds
INT116
Target binding site

58. Rotatable bonds
INT116
Target binding site

59. Rotatable bonds
INT116
Target binding site

60. Rotatable bonds
INT116
Target binding site

61. Rotatable bonds
INT116
Target binding site

62. Rotatable bonds
INT116
Target binding site

63. Rotatable bonds
INT116
Target binding site

64. Rotatable bonds
INT116
Target binding site

65. Rotatable bonds
INT116
Target binding site

66. Rotatable bonds
INT116
Target binding site

67. Rotatable bonds
INT117
Target binding site

68. Rotatable bonds
INT118
Different binding site leading to side effects

69. 9. Simplification
Oversimplification of opioids

70. MORPHINE C C O C C C C
MOR062.WAV N
SIMPLIFICATION

71. LEVORPHANOL C C O C C C C
MOR064.WAV N
SIMPLIFICATION

72. LEVORPHANOL C C O C C C C
MOR064.WAV N
SIMPLIFICATION

73. METAZOCINE C C O C C C C
MOR065.WAV N
SIMPLIFICATION

74. C C O C C C C
MOR065.WAV N
OVERSIMPLIFICATION

75. TYRAMINE C C O C C C C
MOR065.WAV N
OVERSIMPLIFICATION

76. AMPHETAMINE C C O C C C C
MOR065.WAV N
OVERSIMPLIFICATION

77. 10. Rigidification
Note
Endogenous lead compounds are often simple and flexible
Fit several targets due to different active conformations
Results in side effects
Strategy
Rigidify molecule to limit conformations - conformational restraint
Increases activity - more chance of desired active conformation being present
Increases selectivity - less chance of undesired active conformations
Disadvantage
Molecule is more complex and may be more difficult to synthesise

78. 10. Rigidification
RECEPTOR 2
RECEPTOR 1

79. 10. Rigidification Methods - Introduce rings
Bonds within ring systems are locked and cannot rotate freely
Test rigid structures to see which ones have retained active conformation

80. 10. Rigidification Methods - Introduce rings
Bonds within ring systems are locked and cannot rotate freely
Test rigid structures to see which ones have retained active conformation

81. 10. Rigidification Methods - Introduce rings
Bonds within ring systems are locked and cannot rotate freely
Test rigid structures to see which ones have retained active conformation
Rigidification
Rotatable
bonds

82. Rotatable
bond
INT119

83. Rotatable
bond
Ring
formation
INT120

84. Ring
formation
INT120

85. 10. Rigidification
Methods - Introduce rigid functional groups

86. 10. Rigidification Analogues Examples Inhibits platelet aggregation
Important binding groups
Inhibits
platelet
aggregation
Analogues
Rigid
Rigid

87. 10. Rigidification Examples - Combretastatin (anticancer agent)
Rotatable
bond
Less active
More active

88. 10. Rigidification Methods - Steric Blockers Introduce steric block
Flexible side chain
Introduce
steric block
Orthogonal rings
preferred
Coplanarity allowed

89. 10. Rigidification Methods - Steric Blockers Serotonin antagonist
Introduce
methyl group
Steric
clash
Increase in activity
Active conformation retained

90. 10. Rigidification D3 Antagonist Methods – Steric Blockers
Steric clash
D3 Antagonist
Inactive - active conformation disallowed

91. N CH HN O 3 10. Rigidification
Identification of an active conformation by rigidification N CH 3 HN O

92. N N CH N HN O 3 10. Rigidification
Identification of an active conformation by rigidification N N CH 3 N HN O

93. N N CH N HN O 3 10. Rigidification
Identification of an active conformation by rigidification N N CH 3 N HN O

94. N N CH N HN O 3 10. Rigidification
Identification of an active conformation by rigidification N N CH 3 N HN O

95. N N CH N HN O 3 10. Rigidification
Identification of an active conformation by rigidification N N CH 3 N HN O

96. N N CH N HN O 3 10. Rigidification
Identification of an active conformation by rigidification N N CH 3 N HN O

97. N N CH N HN O 3 10. Rigidification
Identification of an active conformation by rigidification N N CH 3 N HN O

98. 10. Rigidification Planar conformation
Identification of an active conformation by rigidification
Planar conformation

99. 10. Rigidification Orthogonal conformation
Identification of an active conformation by rigidification
Orthogonal conformation

100. 10. Rigidification
Identification of an active conformation by rigidification
CYCLISATION

101. 10. Rigidification
Identification of an active conformation by rigidification
CYCLISATION

102. 10. Rigidification Locked into planar conformation
Identification of an active conformation by rigidification
CYCLISATION
Locked into planar conformation

103. 10. Rigidification
Identification of an active conformation by rigidification
STERIC HINDRANCE

104. 10. Rigidification
Identification of an active conformation by rigidification
STERIC HINDRANCE

105. 10. Rigidification
Identification of an active conformation by rigidification
STERIC HINDRANCE

106. 10. Rigidification
Identification of an active conformation by rigidification
STERIC HINDRANCE

107. 10. Rigidification Locked into orthogonal conformation
Identification of an active conformation by rigidification
STERIC HINDRANCE
Locked into orthogonal conformation

108. 11. Structure-based drug design
Strategy
Carry out drug design based on the interactions between the lead compound and the target binding site
Procedure
Crystallize target protein with bound ligand
Acquire structure by X-ray crystallography
Download to computer for molecular modelling studies
Identify the binding site
Identify the binding interactions between ligand and target
Identify vacant regions for extra binding interactions
Remove the ligand from the binding site in silico
‘Fit’ analogues into the binding site in silico to test binding capability
Identify the most promising analogues
Synthesise and test for activity
Crystallise a promising analogue with the target protein and repeat the process

111. INT024

112. INT024

113. INT024

114. INT024

115. INT024

116. INT024

117. INT024

118. INT024

119. INT024

120. INT024

121. INT024

122. 12. De Novo Drug Design
The design of novel agents based on a knowledge of the target binding site
Procedure
Crystallise target protein with bound ligand
Acquire structure by X-ray crystallography
Download to computer for molecular modelling studies
Identify the binding site
Remove the ligand in silico
Identify potential binding regions in the binding site
Design a lead compound to interact with the binding site
Synthesise the lead compound and test it for activity
Crystallise the lead compound with the target protein and identify the actual binding interactions
Optimise by structure-based drug design