Article

The danger hypothesis applied to idiosyncratic drug reactions.

Department of Pharmaceutical Sciences, University of Toronto, Ontario M5S 3M2, Canada.
Handbook of experimental pharmacology 01/2010; DOI:10.1007/978-3-642-00663-0_18 pp.493-509
Source: PubMed

ABSTRACT The danger hypothesis has had a profound effect on the way immunologists view the immune response. This hypothesis proposes that the major determinant of whether an immune response is mounted against some agent is determined by whether that agent causes some type of cell damage. Assuming that most idiosyncratic drug reactions (IDRs) are immune-mediated, this hypothesis also has the potential to explain many aspects of the mechanism of these adverse drug reactions. For example, most IDRs appear to be caused by chemical metabolites rather than the parent drug, but not all drugs that form reactive metabolites are associated with a significant incidence of IDRs. Therefore, using the danger hypothesis, one feature of a drug candidate that may predict whether it causes an IDR is whether the drug, or more likely its reactive metabolites, cause cell damage. Although the range of molecules that can act as danger signals is unknown, the most attractive candidates are high mobility group box 1 protein (HMGB1), heat shock proteins, and S100 proteins. These molecules act through the same receptors (toll-like receptors) as pathogen-associated molecules that stimulate the immune system. Therefore, other environmental factors such as infections or trauma might determine which patients would be at increased risk for IDRs. Although there are examples where this appears to be the case, in most cases there are no obvious environmental factors that determine IDR risk. In addition, in animal models of immune-mediated reactions, stimulation of toll-like receptors often does not increase the immune response, and depending on the timing, it can actually be protective. Therefore, there may be additional unknown control mechanisms that are involved. A better understanding of these fundamental immune mechanisms has the potential to have a significant impact on many areas of medicine.

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Keywords

adverse drug reactions
 
agent causes
 
animal models
 
cause cell damage
 
cell damage
 
chemical metabolites
 
determine IDR risk
 
environmental factors
 
form reactive metabolites
 
fundamental immune mechanisms
 
idiosyncratic drug reactions
 
immune response
 
immune system
 
immune-mediated reactions
 
obvious environmental factors
 
profound effect
 
reactive metabolites
 
significant incidence
 
toll-like receptors
 
way immunologists view
 

Jinze Li