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Structure Activity Relationship

This document discusses structure-activity relationships (SAR) and quantitative structure-activity relationships (QSAR) in medicinal chemistry. SAR examines how minor changes to a drug's structure, such as additions or substitutions of functional groups, affect its biological activity. QSAR uses mathematical models and physicochemical parameters to quantify a drug's potency. Parameters include lipophilicity, electron distribution, and size. Case studies demonstrate how SAR analysis can discover more potent drug candidates through iterative modifications. Lipophilic parameters like partition coefficients and substituent constants are important for developing QSAR models to predict biological effects.

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812 views37 pages

Structure Activity Relationship

This document discusses structure-activity relationships (SAR) and quantitative structure-activity relationships (QSAR) in medicinal chemistry. SAR examines how minor changes to a drug's structure, such as additions or substitutions of functional groups, affect its biological activity. QSAR uses mathematical models and physicochemical parameters to quantify a drug's potency. Parameters include lipophilicity, electron distribution, and size. Case studies demonstrate how SAR analysis can discover more potent drug candidates through iterative modifications. Lipophilic parameters like partition coefficients and substituent constants are important for developing QSAR models to predict biological effects.

Uploaded by

naheed jalil
Copyright
© © All Rights Reserved
We take content rights seriously. If you suspect this is your content, claim it here.
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Medicinal Chemistry/ CHEM

458/658
Chapter 3- SAR and QSAR

Bela Torok
Department of Chemistry
University of Massachusetts Boston
Boston, MA

1
Introduction
• Structure-Activity Relationship (SAR)
- similar structures –similar effects
- more potency or improved side effects

• Quantitative Structure-Activity Relationship (QSAR)


- similar structures –similar effects but uses parameters to
describe the potency
- parameters – anything (related to drug action) that can be
represented by a numerical values

2
Structure-Activity Relationship (SAR)

• Usually go through minor changes on the lead structure


- the and shape of the carbon skeleton
- the nature and degree of substitution
- stereochemistry

3
Structure-Activity Relationship (SAR)

• Changing size and shape

- number of methylene groups in chains and rings

- increasing or decreasing the degree of unsaturation

- introducing or removing a ring system

4
Structure-Activity Relationship (SAR)

• Changing the number of methylene groups

- increases lipophilicity (increased activity)


- decreases water solubility (decreased activity)
- aliphatic compounds – micelle formation – no selective binding

antipsychotic antidepressant

5
Structure-Activity Relationship (SAR)
• Changing the degree of unsaturation

- increasing – rigidity
- E-Z isomers might complicate the picture
- more sensitivity
- increased toxicity

1 : 30 antipsychotic antidepressant

6
Structure-Activity Relationship (SAR)
• Introduction or removal of a ring system
- addition – size increase, shape changes (effect mostly
unpredictable
- increasing size – better fills the hydrophobic pocket

- small ring to substitute C=C double bonds - stability

antidepressant

7
Structure-Activity Relationship (SAR)
• Introduction of an aromatic ring
- increases rigidity, shape changes resistance toward metabolism
might improve

8
Structure-Activity Relationship (SAR)
• Modifying the ring system of drugs of natural origin
- fine tuning of effect and side effects

more potent less potent


(highly addictive)

equally potent
less potent (less addictive)
(less addictive)
9
Structure-Activity Relationship (SAR)
• Introduction of new substituents
methyl groups increases lipophilicity
Compound Structure P Analogue Structure P

benzene 135 toluene 490

acetamide CH3 CONH 2 83 propionamide CH3 CH 2 CONH 2 360

urea NH2 CONH 2 15 N-methylurea CH 3NHCONH 2 44

steric hindrance – might block activity

0
1 3.7 10
Structure-Activity Relationship (SAR)
• Introduction of methyl group
- methyl group on aromatic rings – increased rate of metabolism

- demethylation – easy on heteroatoms, especially on N+, S+

- reduce the rate of metabolism

- reduce unwanted side effects

11
Structure-Activity Relationship (SAR)
• Introduction of halogens

Mostly F and Cl - C-X bond stability - reactivity


O
H3C
O
CF3 is also very popular CF3
O
HO

O F
O
CH3
N
H
location

12
Structure-Activity Relationship (SAR)
• Introduction of hydroxyl groups

Mostly to increase hydrophilic character

Phenolic OH is special

13
Structure-Activity Relationship (SAR)
• Introduction of basic groups

Mostly to increase binding via H-bonding/acid base


interactions

14
Structure-Activity Relationship (SAR)
• Introduction of COOH and SO3H groups

Mostly to increase binding via H-bonding/acid base


interactions – in vivo salt formation
introduction to small leads – usually changes the activity

SO3H – no significant effect except faster excretion

Other S groups are rare - metabolism


15
Structure-Activity Relationship (SAR)

• Changes the existing substituents of a lead


isosteres - bioisosteres

16
Structure-Activity Relationship (SAR)

• Changes the existing substituents of a lead


isosteres - bioisosteres

17
Structure-Activity Relationship (SAR)

• Case Study: SAR investigation to discover potent geminal


bisphosphonates

first generation

second generation

18
Structure-Activity Relationship (SAR)
• Case Study: SAR investigation to discover potent geminal
bisphosphonates

19
Structure-Activity Relationship (SAR)
• Case Study: SAR investigation to discover potent geminal
bisphosphonates

20
Structure-Activity Relationship (SAR)
• Case Study:
SAR investigation
to discover potent geminal
bisphosphonates

21
Structure-Activity Relationship (SAR)

• Case Study: SAR investigation to discover potent geminal


bisphosphonates

22
Quantitative Structure-Activity Relationship
(QSAR)
• QSAR – mathematical relationship (equations)
biological effect vs. physicochemical parameters

- lipophilicity
- electron distribution
- shape
- size
- partition coefficients
- Hammett or Tafts constants

Biological activity = F {parameters (s)}

23
Quantitative Structure-Activity Relationship
(QSAR)
• Regression Analysis

24
Quantitative Structure-Activity Relationship
(QSAR)
• Lipophilic parameters
Partition coefficient

log (1/C) = k1 log P +k2

(1) Toxicity of alcohols to red spiders:


log (1/C) = 0.69 log P + 0.16 r = 0.979, n = 14, s = 0.087

(2) The binding of misc. neutral molecules to bovine serum:


log (1/C) = 0.75 log P +2.30 r = 0.96, n = 42, s = 0.159

(3) The binding of misc. neutral molecules to haemoglobin:


log (1/C) = 0.71 log P +1.51 r = 0.95, n = 17, s = 0.16

(4) Inhibition of phenols on the conversion of P-450 to P-420 cytochromes:


log (1/C) = 0.57 log P +036 r = 0.979, n = 13, s = 0.132

25
Quantitative Structure-Activity Relationship
(QSAR)
• Lipophilic parameters
Partition coefficient – often parabolic

log (1/C) = -k1 (log P)2 + k2log P + k3

26
Quantitative Structure-Activity Relationship
(QSAR)
• Lipophilic parameters
hypnosis (mice) with barbiturates

log (1/C) = - 0.44 (log P)2 + 1.58 log P + 1.93 (r=0.969)

Hansch – logP ~ 2 hypnotic (CNS drug)

27
Quantitative Structure-Activity Relationship
(QSAR)
• Lipophilic parameters

lipophilic substituent constants (π) (or hydrophobic)


contribution of substituents to P

π = logPX – logPH

π = logP(C6H5Cl) – logP(C6H6) = 2.84 – 2.13 = 0.71

π = π (substituent 1) + π (substituent 2) …..+ π (substituent n)

28
Quantitative Structure-Activity Relationship
(QSAR)
• Lipophilic parameters

lipophilic substituent constants (π)

Substituent X Aliphatic systems R-X X O2 N X HO X

-H 0.00 0.00 0.00 0.00


- CH 3 0.50 0.56 0.52 0.49
-F - 0.17 0.14 0.31
- Cl 0.39 0.71 0.54 0.93
- OH - 1.16 - 0.67 0.11 - 0.87
- NH 2 - 1.23 - 0.46 - 1.63
- NO 2 - 0.28 - 0.39 0.50
- OCH3 0.47 - 0.02 0.18 - 0.12

log (1/C) vs π high r and low s – important contributor


29
Quantitative Structure-Activity Relationship
(QSAR)
• Lipophilic parameters
distribution coefficients (D)

ionization
[ HAorganic ]
D=
[ H+aqueous ] + [ A-aqueous ]

for acids log (P/D-1) = pH -pK a

for bases log (P/D-1) = pK a - pH

30
Quantitative Structure-Activity Relationship
(QSAR)
• Electronic parameters

The Hammett constant (σ)

σx = log K x
K
σ x = log K x - log K

σ x = pK - pK x 31
Quantitative Structure-Activity Relationship
(QSAR)
• Electronic parameters

The Hammett constant (σ)

log (1/C) = 2.282 σ - 0.348

32
Quantitative Structure-Activity Relationship
(QSAR)
• Steric parameters

The Taft steric parameter (Es)

k (XCH2COOCH3)
Es = log = k (XCH2COOCH3) - k (CH3COOCH3)
k (CH3COOCH3)

log BR = 0.440Es - 2.204 (n=30; s=0.37; r= 0.886)

33
Quantitative Structure-Activity Relationship
(QSAR)
• Steric parameters

Molar refractivity (MR)

(n2 - 1) M
MR =
(n2 +2) ρ

additive – functional groups

34
Quantitative Structure-Activity Relationship
(QSAR)
• Hansch analysis

drug activity vs. measurable chemical properties


multiparameter approach

two stages: - transport to the site of action


- binding to the target site

log 1/C = k 1 (partition parameter)+k 2(electronic parameter)+k 3 (steric parameter)+k 4

log 1/C = k 1 P - k 2P2 +k 3σ +k 4 Es+ k 5


Quantitative Structure-Activity Relationship
(QSAR)
• Hansch analysis

Accuracy :

- Greater number of analogs – n=5x (x= number of parameters)


- biological data
- the choice of parameters

Use:
- Asses the factors controlling the activity
- predict optimum activity (ideal parameter values)

Sources of parameters
- CRC, CAS, Merck Index, etc.
Quantitative Structure-Activity Relationship
(QSAR)
• Craig plots

Use with Hansch analysis:

log 1/C = 2.67π – 2.56σ + 3.92

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