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Transcript 
Lecture 11
Web: pollev.com/ucibio
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Lecture 11 objectives
Understand irreversible enzyme inhibition
Understand how enzyme kinetics relates to drug discovery
Understand the differences between basic and applied research
Apply enzyme kinetic principles to understand metabolic
pathway regulation
Enzyme kinetics
Thermodynamics determine spontaneity and
rate
Enzymes change rate by lowering Ea
Enzymes fold into precise 3D shapes
MM equation approximates enzyme kinetics
Enzymes can be regulated
“Irreversible” regulation
Covalent modification of enzymes
Eg: Phosphorylation
Kinase
Active
Inactive
E1
E1-PO4
Phosphatas
e
Irreversible inhibitors
Bind enzyme very tightly
Very often at active site
Very often covalently binds active
site
“Suicide” inhibitors
Making new drugs
Identify targets
Find candidate drugs
Effective concentration VS toxic
concentration
Phases of clinical trials
Societal implications of discovery pipeline
http://clinuity.com/blog/2009/11/chart-of-the-day-drug-approval-pipeline/
Societal implications of discovery pipeline
Identify targets
Find candidate drugs
Effective concentration VS toxic
concentration
Phases of clinical trials
Failure rates
Time from discovery  Market?
Money, money, money
What does basic research do for me?
Identify targets
Identify candidates
Drives technological innovations
Different approaches to curing disease
Less worried about short term economic
return
Regulating pathways
A
E1
B
E2
C
E3
D
E4
Convert A E ONLY when needed
Intermediates have no role
Therefore
first COMMITTED step
Regulate PATHWAY not necessarily reactions
FEEDBACK INHIBITION
E
Complex pathways
A
E1
B
E2
C
E4
E3
D
Can have many different regulation
points
Feedback + FEEDFORWARD
E
How to study a pathway?
A
E1
B
E2
C
E3
D
E4
E
Studying pathways
Submit assignment to “Studying pathways”
Midnight tonight
Carbs - Isomers
Carbohydrates = HUGE
Diversity
“Isomers”
- Constitutional/Structural
- Stereo
- Enantiomers
- Diastereomers
- Epimers
- Anomers
Isomers
Select best isomer description for the
two molecules below:
A. Epimers
B. Anomers
C. Enantiomers
D. Diastereomers
E. None/Other
Carbohydrate diversity increased by cyclization!
Carbohydrate diversity increased by cyclization!
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