Drug metabolism

Question 1

Reactions in phase I metabolism

Answer 1

oxidation
reduction
hydrolysis

Adds a functional group to the drug which increases its polarity and provides a site for phase II reactions

N.B. Some oxidations do not involve P450 enzymes, e.g. ethanol metabolised in the cytosol. Hydrolytic reactions occur in the plasma and many tissues

Question 2

Mixed function oxidase system

Answer 2

combination of molecular oxygen, NADPH and NADPH cytochrome P45o reductase.

Required for cytochrome P450 enzymes to function

Question 3

Oxidation of a drug by cytochrome P450

Answer 3

The process of drug oxidation involves both oxidation and reduction.

CYP450 catalyses the transfer of one oxygen atom to the substrate (drug) while the other oxygen atom is reduced to water. Occurs in a P450 cycle of reduction and oxidation

Overall reaction:
DH+O2+NADPH+H > DOH+H2O+NADP

Question 4

Major cytochrome P450 isoforms

Answer 4

CYP3A

CYP2D6

CYP2C

CYP2E1
CYP1A2

Question 5

Isoforms of CYP450 involved in drug metabolism

Answer 5

CYP3A is the major enzyme involved in drug metabolism and is the most abundant in the liver

CYP2D6 is the second enzyme involved in metabolism but is found in significantly lower quantities.

Question 6

Phase II reactions

Answer 6

Involve conjugation of a large chemical group to a functional group on a drug molecule.

The resulting conjugate is almost always pharmacologically inactive and is more hydrophilic and more easily excreted from the body.

Drug molecules that possess a suitable site what was present before, or as a result of phase I reactions are susceptible to phase II metabolism.

Question 7

Examples of chemical groups used for conjugation in the liver

Answer 7

Glucoronyl

Acetyl

Methyl

Glutathione

Conjugation occurs mainly in the liver but other tissues e.g. lung and kidney are involved. Product is inactive

Question 8

Factors affecting drug metabolism

Answer 8

Age

Genetics

Drug interactions and environmental influences e.g. herbal medication

Liver disease

Question 9

How does age affect drug metabolism?

Answer 9

Neonates: Hepatic drug-metabolising enzyme systems are immature. Renal clearance is also inefficient. Lower doses of all drugs are needed

Children: Metabolic clearance can be quicker in children than in adults (CYPs are mature and their relative liver mass and hepatic blood flow are higher. Therefore doses of medicines may be need to be higher, using body surface area and age as a guide.

Elderly: Overall capacity of hepatic drug metabolism is reduced because relative liver mass and hepatic blood flow are lower (phase I reactions particularly affected). Simultaneous use of drugs in the elderly is also common due to co-morbidities. Start drug treatment with smallest effective dose and minimise number of drugs used.

Question 10

How does genetics influence drug metabolism

Answer 10

The population may have differential expression of some CYP450 enzymes, Some patients will metabolise poorly which causes a polymorphic distribution.

e.g. some patients do not metabolise codeine to morphine. There is very little pain relief but patients experience slow, shallow breathing, nausea and vomiting, constipation, conscious depression.

Question 11

Describe drug interactions at the level of Hepatic metabolism.

Answer 11

Normally due to interaction of phase I, CYP450 enzymes than phase II. Risk of interactions increases exponentially with 4 or more medications

Question 12

Name 5 drug classes metabolised by CYP3A

Answer 12

Calcium channel blockers

Benzodiazepines

HIV protease inhibitors

HMG-CoA reductase inhibitors

Cyclosporine

Oral contraceptives

Question 13

Name 3 drugs which inhibit drug metabolism of CYP3A

Answer 13

Anti-fungal drugs (azole drugs)

Cimetidine (H2 histamine receptor antagonist)

Macrolide antibiotics (e.g. Erythromycin)

Interactions that inhibit CYP3A lead to reduced clearance and higher blood levels of the primary drug. Potentially toxic drug levels and adverse effects can result.

Question 14

Drugs which induce CYP3A enzymes

Answer 14

Carbamazepine: anti-convulsant

Rifampicin: anti-TB

Ritonavir: antiviral

St. John’s Wort: herbal

This leads to increased clearance and lower blood levels of the primary drug. Lack of therapeutic efficacy can result.

Question 15

Why is it important to ask about herbal medications in a drug history?

Answer 15

St John’s Wort available over the counter - induces the activity of CYP3A and inhibits other CYP450 enzymes.

Inducing CYP3A increases metabolism, and therefore reduces plasma concentration of drugs such as warfarin, anti-epileptics and oral contraceptives.

Question 16

Where in the liver are drugs metabolised?

Answer 16

Hepatocytes

Drugs and toxins in the GIT enters the liver via the portal vein. The majority of drugs metabolised by hepatocytes re-enter the blood via the central vein and pass to the kidneys to be excreted. Drugs with high Mw and hydophobicity re excreted in bile

Question 17

Aim of drug metabolism

Answer 17

To make the drug less active and less lipid soluble sot aht it can be easily excreted from the body.

Phase I reactions add functional groups to the drugs

Phase II reactions add large molecules to functional groups of the drugs so they can be excreted.

Question 18

Where are CYP450 enzymes found?

Answer 18

SER of hepatocytes

Hundreds of isoforms exist which have different specificities of reactions they catalyse. Some are constitutive, other are present when synthesized in response to an appropriate stimulus.

Question 19

Describe the mechanism of paracetamol-induced liver injury following an overdose

Answer 19

Paracetamol can be lethal at 2-3 times the theraputic dose due to accumulation of its metabolite NAPBQI.

Paracetamol is normally metabolised by the phase Ii pathway by conjugation to glucaronic acid or sulphate. NAPBQI is a product of phase I metabolism (5%) and is normally inactivatd by glutathione.

When high doses of paracetamol are ingested, these pathways become saturated and more NAPBQI is produced. When glutathione is depleted, the toxic metabolite reacts with the cell leading to necrosis in the liver and kidneys within 48-72hrs.

Question 20

Initial treatment for paracetamol overdose

Answer 20

Acetylcysteins and methionine. Increase the synthesis of glutathione in the liver.

Question 21

Patient’s most at risk of paracetamol-induced liver damage

Answer 21

Patients taking P450 inducing drugs e.g. St Johns Wort, alcohol

Patients with gluathione depletion eg. eating disorders

Question 22

Side effects of codeine

Answer 22

Slow, shallow breathing

Nausea and vomiting

Constipation

Conscious depression/mood alteration

Question 23

Effects of liver disease on drug action

Answer 23

Liver disease impairs liver function which causes increased bioavailability of drugs and decreased protein binding.

Question 24

How does cirrhosis affect drug action

Answer 24

In cirrhosis chronic inflammation causes scarring and fibrosis of the the liver tissue. Hepatocytes regenerate but the structure of the lobules is lost and nodules are formed.

Nodule formation impairs blood flow and causes portal hypertension, and may result in porto-systemic shunting so drugs are directed away from the liver as a result.

Dead and damaged hepatocytes also decrease the drug-metabolising capacity of the liver.

Question 25

How does liver disease influence response to treatment?

Answer 25

Increased bioavailabiltiy: Orally administered drugs are normally absorbed in the small intestine and metabolised by 1st pass metabolism so less active drug is available in the body. In liver disease 1st pass metabolism is reduced (due to damaged hepatocytes and shunting) and therefore more active drug is available

Decreased protein binding: liver disease causes loss of plasma proteins, clotting factors and binding proteins synthesised by the liver. Therefore more unbound drug is available for distribution and binding to receptors in tissues.

Question 26

Give 2 examples of drugs whose bioavailability is increased in cirrhosis

Answer 26

nicardipine (calcium channel antagonist)

paracetamol

propranolol (b-adrenoceptor antagonist)

verapamil (calcium channel antagonist)

Question 27

What is the effect of liver disease on prodrugs?

Answer 27

Some drugs are activated by phase 1 metabolism. Therefore in liver damage activation of pro-drugs may be slowed or reduced e.g. ACEi.

Question 28

Describe the functional zones in the liver lobule

Answer 28

Zone 1: periportal hepatocytes, receive the most oxygen, and specialise in oxidative metabolism.

Zone 2: intermediate zone

Zone 3: pericentral hepatocytes, least oxygenated, specialise in drug metabolism.