Cytochrome p450

Question 1

How many CYP genes?

Answer 1

> 200 CYP genes characterised, 12 mammalian families

Question 2

Evolutionary changes in location:

Answer 2

• Prokaryotic- cytoplasmic

- Eukaryotic- membrane bound

Question 3

CYP membrane:

Answer 3

Endoplasmic* reticulum (microsomes):

• Exogenous* (drugs, pollutants)
• Endogenous (fatty acids, prostaglandins)

Mitochondria:
- Steroidogenesis

Question 4

How many CYPs isolated and sequenced in human genome?

Answer 4

> 50 different CYPs

- Classified based on amino acid sequence (primary structure

Question 5

How many families of CYPs?

Answer 5

12
> 40% homology
- Families 1, 2 and 3 important for drug metabolism

Question 6

How many CYP subfamilies?

Answer 6

• > 60% homology
  e. g., Family 2 has 6 subfamilies - 2A, 2B, 2C, 2D, 2E, 2F
• Each has 1- 15 members (different gene products)
• Each CYP enzyme has a different molecular weight

Question 7

CYP nomenclature?

e.g. CYP2D6

Answer 7

• 2 represents the family
• D designates the subfamily
• 6 = individual gene

Usually different genes are for different animal species –
e.g. CYP2D6 (human), CYP2D1 (rat), CYP2D15 (dog)

Question 8

What does the CYP system do?

Answer 8

• Provides metabolic ‘safety
  net’
• Acts on a wide variety of chemical structures
• Common goal to introduce/expose functional groups
• Regulation via multiple mechanisms, both genetic and environmental (prior drug and chemical exposure)
• Large inter-individual variability

Question 9

CYP expression and activity in disease:

Answer 9

• Reported reduced activity of CYP2D6, CYP3A4 in cancer and HIV1

Downregulation of CYPs mediated by pro-inflammatory mediators affecting gene transcription 
interleukin 6 (IL-6), tumor necrosis factor alpha (TNF-α) 

Inconsistent and limited data on the effect of obesity on CYP expression and activity2,3

Effect of coeliac disease, CKD, liver cirrhosis on certain CYPs4

Question 10

Multicomponent system – operates in two steps.

Answer 10

1) Activation of O2 (potentially dangerous)

2) Oxidation of drug

Question 11

Components of CYP system:

Answer 11

1) Haemoproteins
- cytochrome P450
- cytochrome b5

2) Flavoproteins
- FP1 - NADPH-cytochrome P450 reductase (FAD and FMN)
- FP2 - NADH-cytochrome b5 reductase

3) Lipid component - phosholipid membrane (endoplasmic reticulum in the intact cell)

Question 12

Central role and binding properties of CYPs:

Answer 12

• CYP oxidation cycle
• -> Efficient, protects activated O2 species
• Two binding sites
• -> Substrate - active site on protein, site of catalysis
• O2 (or CO) - haeme ligand
• -> CO binding has an absorption spectrum with a maximum at 450nm
• Enzyme kinetics often described by Michaelis-Menten principles
• -> Assumes a single substrate binding site
• -> Rapid equilibrium and formation of Enzyme-Substrate complex

Question 13

CYP cycle – activation of O2 :

Answer 13

1) Start with drug molecule (RH) binded to CYP450
2) Binding of molecule = conformational change from low to high spin status
3) Changed reduction potential of enzyme – more likely to accept electrons
4) The donor of electron = NADPH
5) TO FACILIATE ELECTRON TRANDFER YOU NEED FP1
6) Iron now reduced – enzyme is ready to bind to oxygen
7) The oxygen then binds
8) Ready to accept another electron (two electron transfers) – source = NADPH again
9) Peroxy state = active – will very quickly be protonated which will trigger release of water molecule
10) Cytrop450??
11) Release of oxidated drug molecule (R-OH)
12) Enzyme now goes back to initial form where the water molecule is bound

Question 14

Function of other microsomal components:

Answer 14

• FP2 (second reductase) uses:
• -> NAD not NADP
• -> cytochrome b5 not cytochrome P450
• Cytochrome b5 uses:
  –> FP2 not FP1
  –> can transfer electrons directly to cytochrome P450
  Provides flexibility in electron supply and transfer

Question 15

Determinants of CYP metabolism:

Answer 15

1. Topography of the active site – specificity
2. Degree of steric hindrance restricting access of the iron-oxygen complex to the possible site of metabolism
3. Ease of electron or hydrogen abstraction from the C (or N or S) atom

Mechanism the same for all CYPs

Question 16

Specificity of CYPs:

Answer 16

• CYP enzymes considered for metabolic DDI screening in drug development:
  
  • -> CYP1A2, -2B6, -2C8, -2C9, -2C19, - 2D6 and CYP3A
  • -> Focus will be on three major CYPs:
• CYP2D6, CYP2C9 and CYP3A4
• Each CYP enzyme has its own degree of specificity
  
  • > Some CYPs have narrow specificity (CYP2C9)
  • > Some have broad and overlapping (CYP3A4)
• Chemical structure and phys-chem properties of drug affect the preference for a particular CYP

Question 17

Guidelines for drug substrate preference:

Answer 17

• CYP2D6: Arylalkylamines (basic) with site of oxidation 5-7Å from protonated nitrogen
• CYP2C9: Neutral or acidic molecules with site of oxidation 5-8Å from H-bond donor heteroatom.
• Molecules tend to be amphipathic with a region of lipophilicity at the site of hydroxylation and an area of hydrophilicity around the H-bond forming region
• CYP3A4: Lipophilic and ‘bulky’, neutral or basic molecules with site of oxidation often basic nitrogen (N-dealkylation) or allylic positions

Question 18

What is CYP2D6:

Answer 18

Arylalkylamines (basic) with site of oxidation 5-7 Å from protonated nitrogen

Ecstasy

Fluoxetine

Question 19

What is CYP2C9?

Answer 19

Neutral or acidic molecules with site of oxidation 5-8 Å from H-bond donor heteroatom.

Question 20

What is CYP3A4?

Answer 20

Lipophilic and ‘bulky’, neutral or basic molecules with site of
oxidation often basic nitrogen (N-dealkylation) or allylic positions
(a-carbons)

Question 21

Importance of knowing which CYPs metabolise particular drug:

Answer 21

• Genetic polymorphisms – existence of poor metabolisers (CYP2D6)
• Polymorphism contributes to inter-individual variability in drug pharmacokinetics (also efficacy and safety)
• –> Tacrolimus – CYP3A5
• -> Mycophenolic acid – UGT1A9
• -> 6-mercaptopurine - TPMT
• Drug-drug interaction potential
• -> 2 or more drugs metabolised by the same CYP may compete for metabolism

Question 22

Multimodal distribution of CYP2D6 in population:

Answer 22

• Poor Metaboliser (PM) – lack CYP2D6 gene
• Extensive Metabolizer (EM)
• Ultra-rapid metabolizer (UM)

Question 23

Does ethnicity affect metabolism:

Answer 23

• For example - 7% of Caucasian population are PMs

- New drugs should not be exclusively metabolised by CYP2D6!

Question 24

Therapeutic consequences of CYP2D6 polymorphisms:

PM

Answer 24

• Higher plasma concentrations of CYP2D6 substrates compared to EMs – higher risk of side effects (e.g. fluvoxamine)

Question 25

Therapeutic consequences of CYP2D6 polymorphisms:
Extensive Metabolizer (EM)

Answer 25

normal activity

Question 26

Therapeutic consequences of CYP2D6 polymorphisms:

Ultra-rapid Metabolizer (UM) – gene duplication

Answer 26

• Low plasma concentrations of CYP2D6 substrates compared to EMs – likely risk of therapeutic failure

Question 27

Predicting and avoiding drug-drug interactions:

Answer 27

• Important to know the contribution of CYPs to metabolism of a new drug
• What is the major CYP contributing? Multiple enzymes involved?
• Is the drug an inhibitor of CYPs/transporters?
  (Routine screening - FDA requirement)
• Co-administration of the enzyme inhibitor leads to increased plasma concentrations of the ‘victim’ drug
• Findings have labelling implications!