Drug metabolism

Question 1

What is drug metabolism and what is its main purpose?

Answer 1

The biotransformation of pharmaceutical substances in the body so that they can be eliminated more easily. This happens in the liver.

Question 2

What are xenobiotics?

Answer 2

Foreign substance to the body e.g. drugs, plant metabolites, food additives etc.
1. Water soluble are easily excreted in urine.
2. Lipophilic: some are not easily excreted and are deposited in adipose tissue or have to be metabolised to water soluble products.

Question 3

Discuss the 2 phases of liver detoxification.

Answer 3

Phase 1: compound is oxidised, reduced, hydrolysed then excreted.
Phase 2: compound is conjugated to hydrophilic molecule then excreted.

*some compounds go through both phases

Question 4

What is liver activation?

Answer 4

Compound goes through phase 1 but instead of detoxification & excretion, we have an inactive drug that is transformed into an active metabolite/ toxin.

Question 5

What type of oxidation reaction happens in phase 1 reaction?

Answer 5

Monooxygenase (enzymes) reactions that require cytochrome p450.

Question 6

What is cytochrome p450?

Answer 6

They’re electron carriers that have a porphyrin structure (haem group with fe3+).

Question 7

Discuss the Cytochrome P450 nomenclature.

Answer 7

• Name derived from their absorption spectrum.
  It has a max frequency of 450 nanometres in complex with carbon monoxide.
• It has 18 families, 43 subfamilies and 57 genes.

Question 8

What is cytochrome p450’s primary role?

Answer 8

• Hormone synthesis & breakdown
• Metabolism & detoxification of compounds after ingestion
• Drug biotransformation & drug metabolism

Question 9

Discuss the control of cytochrome p450?

Answer 9

1. Inhibition:
   - p450 2B6 - orphenadrine, thiotepa, ticlopidine
   - p450 2e1- Disulfiram, ritonavir.
2. Induction:
   - p450 2B6 - Phenobarbitone, phenytoin, primidone, Rifampin
   - p450 2E1- ethanol, isoniazid.
3. Genetic variation (from person to person)
   - Genetic variants exist with a frequency of at least 1%
   - Lack of functional activity = Specific drug toxicity or Inactivity of pro-drug

Question 10

Discuss drug interactions with CYP P450: activation.

Answer 10

• Some drugs activate P-450 e.g. Phenobarbitone (sedative) induces CYP2C9.
  -For patients on warfarin, may lead to low levels of warfarin. – Increased risk of clotting.
• Warfarin is metabolised by multiple cytochromes including CYP2C9 and CYP3A

Question 11

Discuss drug interactions with CYP P450: inhibition.

Answer 11

• Some drugs inhibit P-450, leads to increased levels of other drugs.
• E.g. patients on warfarin taking the anti-fungal ketoconazole have increased warfarin levels as ketoconazole inhibits CYP3A4. Increased risk of bleeding.

Question 12

What is CYP3A4?

Answer 12

• CYP3A4 is the major isoform in human liver, it oxidatively metabolises > 50% of drugs.

Question 13

What is the fruit that interacts greatly with drugs?

Answer 13

-Grapefruit juice naturally contains CYP3A4 inhibitors (furanocoumarins).
-More than 85 drugs that may interact with the fruit 45 with have serious side-effects (death, AKI).
- Simvastatin combined with a 200 ml glass of grapefruit juice once a day for three days, produces a 330 per cent rise in the systemic concentration of the drug.

Question 14

Recall the types of reaction involved in phase I drug metabolism.

Answer 14

1. Introduction of functional groups; -OH, -NH2, -COOH
2. Prepare substance for conjugation (Phase II metabolism)
3. Reactions: Reduction, Hydrolysis, Oxidation
4. Oxidation: most common phase I reaction type.

Question 15

Phase I Reactions – Reduction.

Answer 15

• Chloramphenicol is a broad-spectrum antibiotic which is reduced by nitro-reductase.

*Reduction implies the addition of two hydrogens to the molecule nitro is the chemistry name given to the –NO2 functional group.

Question 16

Phase I Reactions – Hydrolysis.

Answer 16

• Aspirin at pH 7 is hydrolysed by esterases to salicylate and acetate.

*Hydrolysis implies the addition of water (H2O) to the molecule resulting in the breaking of the molecule into two parts.

Question 17

Phase I Reactions: Oxidation.

Answer 17

• Many oxidation reactions are catalysed by the mixed function oxidase (MFO) system – (Cytochrome P450, NADPH & molecular O2).
• Reaction: RH + O2 + 2H+ + 2e- = ROH + H2O (where R is the drug)
• Oxidation can occur by: Hydroxylation, Dehydrogenation, Oxidative dealkylation.

Question 18

Phase I Reactions: Hydroxylation.

Answer 18

• Addition of “OH” group.
• E.g. RH + O2 + NADPH + H+ = ROH + H2O + NADP+
• Take place mainly on the endoplasmic reticulum of liver cells.
• Lipophilic → hydrophilic compounds → more readily excreted.

Question 19

Example of hydroxylation reaction: lidocaine.

Answer 19

Metabolism involves addition of an - OH group as a first step via P450, NADPH, O2.

Question 20

What is Cytochrome P450’s Mechanism of action?

Answer 20

1. Incorporates one atom of molecular oxygen into substrate creating an -OH group
2. The other O is reduced to water
3. NADPH provides reducing equivalents.
4. Hydroxylation may activate/inactivate a drug or make a drug more soluble
5. Or act as a site for conjugation (Phase II) e.g. glucuronidation

Question 21

Describe the complete metabolism of ethanol.

Answer 21

This is a Phase I reactions via dehydrogenation = Elimination of hydrogen (H2).

Question 22

Why is a deficiency in aldehyde dehydrogenase important in ethanol metabolism?

Answer 22

• Leads to Acetaldehyde accumulation
• Symptoms: vasodilation, facial flushing & tachycardia.

Question 23

Explain the mechanism of action of disulfiram (treatment for alcohol abuse).

Answer 23

• Helps to maintain abstinence
• Highly lipid soluble (accumulates in adipose tissue) & has 80% bioavailability after an oral dose.
• MOA: Irreversibly inhibits the oxidation of acetaldehyde by competing with cofactor NAD.
• Causes a 5-10 fold ^ in acetaldehyde concentration which produces unpleasant side effects.

Question 24

Phase I Reaction: oxidative dealkylation.

Answer 24

Removal of alkyl group from an organic compound. E.g. metabolism of Codeine.
1. Oxidative dealkylation: alkyl group of codeine is oxidised to an aldehyde.
2. 10% of codeine converted to morphine
3.The analgesic effect of codeine due to its conversion to morphine.

Question 25

How does a deficiency in CYP2D6 affect codeine metabolism?

Answer 25

• Codeine is a prodrug that requires activation.
• It is metabolised to morphine by P450 2D6
• CYP2D6 has different polymorphisms present in the population. Deficiency = poor/ no activation.

Question 26

Describe the types of conjugation reactions involved in phase II drug metabolism.

Answer 26

• More common following preliminary modification and makes compound more polar = easily excreted in urine or bile.
• Main conjugation reactions are:
  1. Glucuronic acid conjugation (glucuronidation)
  2. Sulfate conjugation
  3. Glycine conjugation
  4. Glutamine conjugation
  5. Glutathione conjugation

Question 27

Discuss Phase II Reaction: Glucuronidation.

Answer 27

• Most common form of conjugation.
• Common for drugs with OH, COOH & NH2 groups
• Glucuronic acid is transferred to the drug from uridine diphosphate glucuronic acid (a reactive intermediate)

Question 28

Discuss Phase II Reaction: Sulfation.

Answer 28

• Common for phenols
• Sulfate is transferred to the drug from the reactive intermediate (PAPS), in the presence of sulfotransferase.
• Glucuronide formation & sulfation often compete for the same substrate e.g. paracetamol.

Question 29

Discuss Phase II Reaction: Glycine and glutamine conjugation.

Answer 29

• Glycine conjugation is common for drugs with –COOH groups.
• Glutamine can also be conjugated to drugs with COOH groups.

Question 30

Discuss Phase II Reaction: Glutathione metabolism.

Answer 30

• Detoxification products containing Sulphur atom derived from Glutathione
• Glutathione tripeptide - Glu, Gly, Cys (Glu & Gly released).
• Final step – acetylation and End product – Mercapturates

Question 31

What are foreign compounds?

Answer 31

Foreign compounds include: aromatic nitro- & halogenated compounds & Phase l oxidation products of polycyclic hydrocarbons, aliphatic halides & epoxides.

Question 32

Describe the metabolism of aspirin.

Answer 32

• Aspirin is readily hydrolysed to salicylic acid, both enzymatically and non-enzymatically. Salicylic acid undergoes conjugation reactions generating the major metabolites salicyluric acid.

Question 33

Describe the metabolism of paracetamol.

Answer 33

• 5% excreted unchanged. 90% conjugated with glucuronide & sulphate before excretion.
• 5% oxidised via Cytochrome P450 (CYP2E1, CYP1A2 subfamilies) to N-acetyl-p-benzoquinoneimine (NAPQI) & combined with glutathione
• Metabolised to cysteine & mercapturate compounds before excretion.

Question 34

Explain why some drugs e.g. paracetamol are toxic at high doses.

Answer 34

• Hepatotoxicity – due to 5% that is oxidised
• Time to become depleted of glutathione – 3-4 days (dependent on nutritional status)
• Few overt symptoms during early stage – in suspected overdose, treat before symptoms appear
• Liver injury following single dose of 15g (30 standard tablets).

Question 35

Treatment of paracetamol overdose.

Answer 35

• Treatment within 12 hr highly effective, some benefit up to 48 hr
• Administration of n-acetylcysteine (NAC) which acts as a glutathione substitute.

Question 36

Define prodrugs.

Answer 36

• A pharmacologically inactive chemical entity that when metabolised or chemically transformed by the mammalian system is converted into a pharmacologically active substance.

Question 37

In what situations are prodrugs used?

Answer 37

• To alter/ improve absorption
• To alter biodistribution
• To alter metabolism
• To alter elimination.
• To improve patient acceptability (decrease pain on injection).