Drug Biotransformation Flashcards
What is Biotransformation?
The metabolic alteration of the chemical structure of a drug.
aka: Drug metabolism
Happens through enzymes (usually)
What does biotransformation do?
Make a lipophilic compound hydrophilic (preparing it for excretion).
Inactivate drug/toxin.
Activate drug/toxin
Consequences of metabolism (4)?
- Transformation: does NOT deactivate.
- Deactivation: inactive
- Makes toxic: reactive
- Activate an inactive drug: active drug
Why is biotransformation important?
- Lipophilic compounds will not be eliminated unless made hydrophilic.
- Inactivation of a drug terminates it’s effect.
- Activating the drug makes it effective.
Prodrugs:
must be activated by metabolism to be effective. (AZT, sulindac)
Metabolism can make some drugs toxic
Benzo(a)pyrene and aflatoxin
Acetaminophen
Acetaminophen toxicity
Higher doses (than recommended) is metabolized to a toxic form in the liver (4 or more g’s in a day).
Reactive form of acetaminophen causes:
hepatic necrosis
One active form to another:
Diazepam (t 1/2 of 43 hours) to desmethyldiazepam (half-life of 100 hrs)
Terfenadine (toxic, no longer used) becomes fexofenadine (allegra, used).
Drug metabolism in liver:
main site of general purpose transformation (most metabolism done here).
Portal circulation: intestines to liver, first pass effect due to this.
GI tract metabolism:
- **Enteral administration
1. The lumen wall: catecholamines
2. Digestive enzymes: proteins
3. Acidity in stomach: penicillin breakdown. (non-specific chemical degradation not generally equal to metabolism).
4. Microorganisms in large intestine.
Lung metabolism:
Inhalants and some IV drugs (anesthesia)
Acts as metabolizer and filter.
Local metabolism:
Esterases: metabolism of sympathetic drugs.
Some are metabolized by local enzymes and made toxic (MPTP)
Ester group
Type of molecular bond that is easily broken.
Have short half-lives.
Some drugs advantages this (heroin becomes morphine).
drug biotransformation makes lipophilic drugs hydrophilic so they can be excreted to urine.
Two phases of metabolism:
- Conversion: opens or adds a hydrophilic or polar site to the drug.
- Conjugation: adds a hydrophilic molecule to the side of the drug.
Phase I: Conversion
Adds a functional group to the molecule: OH, NH2, SH= makes it more polar, prepping for phase II.
- *May make it hydrophilic enough for immediate renal elimination w/out phase II.
- **Take place in smooth microsomes, ER of liver: cytochrome P-450 (or mixed function oxidases, MFO)
Cyt-P450
Adds OH to drug, it’s to chemical metabolism what the immune system is to microbial infections (deactivates and excrete a wide variety of compounds).
Isozymes of P450
P450 cytochrome is a collection of oxidative enzymes.
Phase I reaction via P450:
- Alliphatic/aromatic hydroxylation: adds OH to C
- N-oxidation: adds OH to N
- S-oxidation
- Dealkylation: adding OH to molecule has it split off H2CO
- Desulfuration: replace S with an O
P450 isosozymes inhibition: responsible for most drug interactions.
Two drugs compete for one isozyme, the one with the higher concentration will block the other from being metabolized.
Called drug inhibition
Example of P450 isozyme inhibition:
Erythromycin prevents breakdown of theophylline, allowing Theo to achieve toxic levels.
2 most common P450 isozymes
CYP2D6 and CYP3A4
Bully drugs
Some drugs are powerful P450 inhibitors and can interfere with many reactions.
Cimetidine, spironolactone, ketoconazole, ritonavir do this
Phase II: conjugation
- Transferases add a hydrophilic moietiy to functional group supplied by phase I.
- Compounds added: glucuronide (selectively secreted in bile).
- Or: acetyl group, glutathione, glycine, sulfate, methyl
Phase II and acetaminophen toxicity
This is the phase overwhelmed by too much acetaminophen.
Molecule metabolized by P450 to a reactive form.
Enzymatic induction
Repeat exposure to drugs and xenobiotics causes an increase in enzyme amount and activity: speeds up metabolism of subsequently administered drugs
Example of enzymatic induction
Phenobarbital decreases half-life of ethosuximide from 54 to 29 hours
Inducers:
There are not many
About half are antiepileptics (phenob, carbamazepine).
Some environmental compounds (cig smoke, hydrocarbons).
Some herbs (St. John’s Wort)
