Transcription of International Consensus (ICON) - EAACI.org
1 International Consensus (ICON) on Drug AllergyAllergy 2014; 69: 420 437 Pascal Demoly, N. Franklin Adkinson, Knut Brockow, Mariana Castells, Anca M. Chiriac, Paul A. Greenberger, David A. Khan, David M. Lang, Hae-Sim Park, Werner Pichler, Mario Sanchez-Borges, Tetsuo Shiohara, Bernard Yu-Hor summary was drafted by Dr Rik Schrijvers and Dr Anca M. Chiriac under the supervision of Professor Pascal to Dr Rik Schrijvers and Dr Anca Mirela Chiriac, 2 EAACI JMAs and FS recipients, for their precious help for this extensive of contents4 PREFACE4 DEFINITIONS 5 CLASSIFICATIONS6 PATHOPHYSIOLOGY7 CLINICAL PRESENTATIONS8 NATURAL HISTORY8 DIAGNOSIS10 CLINICAL HISTORY11 SKIN TESTS 12 DRUG PROVOCATION TESTS13 BIOLOGICAL TESTS14 MANAGEMENT15 LIST OF ABBREVIATIONS4 PREFACEDrug hypersensitivity reactions (DHRs)
2 Comprise all drug reactions resembling allergy . DHRs constitute 15% of all adverse drug reactions affecting more than 7% of the general population. DHRs can be allergic or non-allergic with immunologically-mediated DHRs being named drug allergies. They are typically unpredictable, necessitate treatment changes and can potentially be life-threatening. A definitive diagnosis enabling the institution of adequate treatment options and proper preventive measures typically requires a complete drug allergy work up.
3 Several guidelines and Consensus statements on general or specific drug class-induced DHRs are available to support medical decisions on drug allergy ; however, a standardized systematic approach for the diagnosis and management of DHRs is still a major challenge. The International Collaboration in Asthma, allergy and Immunology (iCAALL), formed in 2012 by EAACI, AAAAI, ACAAI, and WAO, addresses this unmet need in this International Consensus (ICON) on Drug allergy document.
4 The purpose of this document is to: Highlight the key messages that are common to many existing guidelines. Critically review and comment on differences, thus providing a concise Drug hypersensitivity reactions (DHRs) are adverse effects of drugs that clinically resemble allergic reactions. Drug allergies are DHRs for which a definite immunologic mechanism is demonstrated. For general communication, when a drug reaction is suspected, DHR is the preferred generally accepted classification of DHRs is usefull for management, comparison of studies and validation of diagnostic : DHRs are classified as immediate or non-immediate/delayed depending on their onset during treatment (Figure 1).
5 Immediate DHRs occur within 1-6 hours after the last drug administration (typically within the first hour following the first administration of a new course of treatment). Typical symptoms include urticaria, angioedema, conjunctivitis, rhinitis, bronchospasm, gastro-intestinal symptoms (nausea, vomiting, diarrhea, abdominal pain), anaphylaxis or anaphylactic shock. Immediate DHRs are possibly induced by an IgE-mediated mechanism. The term anaphylactoid reactions, considered previously in case of non-IgE- dependent DHRs mimicking anaphylaxis, is abandoned in certain guidelines and the term non-allergic DHRs is DHRs occur at any time as from 1 hour after the initial drug administration.
6 Common symptoms include maculopapular exanthems and delayed urticaria. Often, a delayed T-cell-dependent type of allergic mechanism is administration route, drug metabolites, or presence of co-factors or co-prescribed drugs altering DHRs onset or progression must be taken into account when considering this 1 - Chronology of DHRs. Setting the cut-off at 1 hour (between immediate and non-immediate reactions), may not sufficiently reflect the extension of the pathophysiologically determined immediate-type reactions up to 6 hours (Late) and the delayed-type clinical manifestations occasionally starting as early as 8 to 12 hours (Accelerated).
7 However, this approach facilitates the comparison of studies and should help to enhance and validate diagnostic (immediate)Lateimmediate (< 1h) non-immediate (> 1h)HoursDays0 4 8 12 16 20 24 2 4 Exanthemas(delayed)Accelerated6 Mechanistically: DHRs can be defined as allergic (Table) and non-allergic:PATHOPHYSIOLOGYDrug allergies are adverse reactions whereby antibodies and/or activated T-cells are directed against the drugs or against one of its metabolites.
8 Immediate allergic DHRs develop as a result of IgE production by antigen-specific B-lymphocytes after sensitization. Following subsequent drug exposure, the antigen (presumably a hapten-protein complex) cross-links the IgE bound to mast cells and basophils, stimulating the release of pre-formed mediators ( , histamine, tryptase, some cytokines like TNF ) and the production of new mediators ( , leukotrienes, prostaglandins, kinins, other cytokines). Non-immediate allergic DHRs are mostly mediated through the actions of T-lymphocytes.
9 TypeType of immune responsePathophysiologyClinical symptomsTypical chronology of the reactionIIgEMast cell and basophil degranulationAnaphylactic shock, Angio-oedema, Urticaria, BronchospasmWithin 1 to 6 hours after the last intake of the drugIIIgG and complementIgG and complement-dependent cytotoxicityCytopenia5-15 days after the start of the eliciting drugIIIIgM or IgG and complement or FcRDeposition of immune complexesSerum sickness, Urticaria, Vasculitis7-8 days for serum sickness/urticaria7-21 days after the start of the eliciting drug for vasculitisIVaTh1 (IFN )Monocytic inflammationEczema1-21 days after the start of the eliciting drugIVbTh2 (IL-4 and IL-5)Eosinophilic inflammationMaculo-papular exanthema, DRESS1 to several days after the start of the eliciting drug for MPE2-6 weeks after the start of the eliciting drug for DRESSIVcCytotoxic T-cells (perforin, granzyme B, FasL)
10 Keratinocyte death mediated by CD4 or CD8 Maculo-papular exanthema, SJS / TEN, pustular exanthema1-2 days after the start of the eliciting drug for fixed drug eruption4-28 days after the start of the eliciting drug for SJS / TENIVdT-cells(IL-8/CXCL8)Neutrophilic inflammationAcute generalized exanthematous pustulosisTypically 1-2 days after the start of the eliciting drug (but could be longer)DRESS, Drug reaction with Eosinophilia and Systemic Symptoms; SJS, Stevens-Johnson Syndrome; TEN, Toxic Epidermal Necrolysis; MPE, maculo-papular to the hapten hypothesis, in order to stimulate a reaction, a drug should act as a hapten and bind irreversibly to proteins, generating antigens.