1. Idiosyncratic Drug Reactions�What are They, Why & How Do We Study Them?
Amy Sharma
Ph.D. Candidate
Uetrecht Lab
Leslie Dan Faculty of Pharmacy, University of Toronto
2. Overview Adverse Drug Reactions (ADRs)
Idiosyncratic Drug Reactions (IDRs)
Characteristics of IDRs
Proposed Mechanism of IDRs
Drugs Known to Induce IDRs
Studying IDRs
Future Directions
3. I. Adverse Drug Reactions
4. The World Health Organization definition:
any noxious, unintended, and undesired effect of a drug, which occurs at doses used in humans for prophylaxis, diagnosis, or therapy
ADRs are common
2,216,000 hospitalized patients/year experienced a serious ADR and 106,000/year died from an ADR
Fatal ADRs rank 4th to 6th in leading causes of death in US (Bond CA et al. Pharmacotherapy 2006) I. Adverse Drug Reactions
5. I. Adverse Drug Reactions
6. I. Adverse Drug Reactions ADRs can be divided into two basic types:
Type A:
Can be predicted from the pharmacology of the drug
Are typically dose-dependent
Type B:
Cannot be predicted on the basis of the known pharmacology of the drug
Also known as idiosyncratic adverse reactions
7. Rare & unpredictable reactions
Incidence: 1/103 - 1/106 patients
25% of all ADRs
Still very prevalent because of the number of drugs involved and the number of people taking these drugs
Do not occur in most patients at any dose
No simple dose-response relationship
Effects not related to pharmacological properties of the drug
Can be very severe
most serious ADRs in drug therapy II. Idiosyncratic Drug Reactions
8. Organs affected:
Most thought to be immune-mediated
Detected during the late stage of development or when drug is released on to market
May lead to withdrawal
Significant financial burden
10. If we can understand how drugs induce IDRs we can:
Scan for drugs that have high risk of causing IDRs early in the drug development process, and avoid later losses to both patients and manufacturers
Devise therapy that prevents IDRs in patients
(administer concomitant therapy)
There is circumstantial evidence that indicates a potential role of reactive metabolites (RMs) in development of IDRs
IV. Mechanisms of IDRs
11. Drug Metabolism:
Process whereby therapeutically active drugs are converted to a more soluble form (metabolites) and are cleared by renal or biliary excretion
Reactive Metabolites (RMs) and Covalent Binding
During metabolism, usually through P450 oxidation, drugs can form RMs (chemically reactive species) that can covalently bind to endogenous proteins or other macromolecules
12. Reactive Metabolites Reactive metabolites are electrophiles or free radicals
Sulfates/sulfonates
Epoxides/arene oxides
Michael Acceptors
Nitroso amines
14. Generation of Halothane Reactive Metabolite and Covalent Binding to Protein IV. Example of Covalent Binding
15. IV. Where Does Metabolism Occur? Metabolizing enzymes are present in the following organs:
Cytochrome P450, Sulphotransferases,
Peroxidases
White blood cells (macrophages and neutrophils) that become activated to kill bacteria, and do so by releasing oxidants such as H2O2 and HOCl.
16. Once formed, reactive metabolites tend to bind to the proteins or macromolecules near the site of their formation. Thus, toxicity most often occurs at sites of RM formation.
Example Clozapine:
Clozapine is oxidized to a RM in both the liver and neutrophils. The main toxic effects of clozapine are liver and neutrophil toxicity (hepatotoxicity and agranulocytosis). IV. Where Does Metabolism Occur?
17. Basic paradigm in Immunology
To discriminate against pathogens, the immune system learns to recognize self from non-self. In this way, autoimmunity is avoided and immune responses are mounted against foreign invaders.
Hapten Hypothesis
Once drug is covalently bound to a host protein it forms a novel antigen known as the hapten-carrier complex. Host immune system then perceives the modified endogenous protein as foreign, and mounts an immune response against it. IV. Step 2: Immune Response
19. IV. IDR Characteristics that Indicate Immune Involvement
20. Penicillin-induced anaphylaxis
Aminopyrine-induced agranulocytosis
Halothane-induced hepatitis V. Clinical Evidence in Support of Hapten Hypothesis
23. V. Aminopyrine-Induced Agranulocytosis
24. V. Drugs Known to Cause IDRs
25. V. Felbamate
26. V. Nevirapine
27. V. D-Penicillamine
28. V. Clozapine
29. V. Carbamazepine
31. VI. Step 1: Metabolism Microsomes
32. VI. Step 1: Metabolism Microsomes
33. VI. Step 1: Metabolism - Neutrophils
34. VI. Step 1: Metabolism - Neutrophils
35. VI. Step 2: RM Formation Complete same experiments as when looking at metabolism but with an additional step
Reactive metabolite may be so reactive that it is not detected on the HPLC chromatogram
Must add GSH or NAC to the reaction mixture to trap the reactive metabolite in a stable form that can be detected by HPLC and later identified by LC/MS and NMR
36. VI. Step 3: Protein Binding in Target �Tissues Require an antibody that recognizes the reactive metabolite (the hapten)
Must prepare antigen by linking the reactive metabolite to an immunogenic carrier protein e.g., KLH
Immunize rabbits with this antigen
Sera obtained from the blood of these rabbits is polyclonal, and contains antibodies against the hapten
37. VI. Step 3 Contd Complete in vivo and in vitro studies
in vitro studies are similar to metabolism studies
in vivo studies involve administering the drug to animals (rats or mice)
38. VI. Step 3 Contd Take tissues from either in vitro or in vivo experiment and perform Western blot analysis to detect covalent binding of reactive metabolites to proteins:
Run the protein sample on an SDS polyacrylamide gel
Transfer separated proteins from gel to nitrocellulose membrane
Blot membrane with an antibody against the HAPTEN
Visualize antibody binding with a detection system; presence of covalent adducts will thus be elucidated
39. VI. Step 4: Hapten Immunogenicity
40. VI. Animal Models in Study of IDRs
41. VI. Nevirapine Animal Model
42. VI. Hopes for the Future
43. Summary
