Toxic epidermal necrolysis, DRESS, AGEP: Do overlap cases exist?

Adverse cutaneous reactions to drugs are frequent, affec-ting 2% to 3% of all hospitalized patients [1]. Only about 2% of these adverse cutaneous reactions are considered severe [1]. The spectrum of severe cutaneous adverse reactions to drugs (SCARs) include acute generalized exanthematous pustulosis (AGEP), drug reaction with eosinophilia and systemic symptoms (DRESS) and epidermal necrolysis (Stevens-Johnson syndrome-SJS, toxic epidermal necrolysis -TEN). These conditions are defined by clinical features associated more or less with specific biological and histological findings [2, 3].

AGEP is characterized by a pustular eruption arising quickly after administration of the causative drug (usually aminopenicillin, pristinamycin, diltiazem) [4, 5]. DRESS, also known as drug-induced hypersensitivity syndrome, is a severe, systemic drug reaction most commonly associated with aromatic anticonvulsants, allopurinol and sulfonamides [6‐8]. Patients typically present fever, facial oedema, lymphadenopathy and morbilliform eruption, which may progress to erythematous rash and exfoliative dermatitis. Hematologic abnormalities, including eosinophilia and atypical lymphocytosis, are a hallmark of the condition. Visceral organ involvement typically manifests as hepatitis but may include nephritis, interstitial pneumonitis or myocarditis [8]. Epidermal necrolysis is characterized by extensive epidermal loss with mucous membrane erosions and often presents as impaired general condition. These SCARs are defined as SJS, “transitional SJS-TEN” or TEN, depending on the extent of epidermal detachment (< 10%, 10–30%, > 30%, respectively) [9]. The conditions have been strongly associated with anti-infective sulfonamides, allopurinol, carbamazepine, phenobarbital, phenytoin, oxicam, and more recently nevirapine, lamotrigine and amifostine [10, 11].

For each of these SCARs, diagnostic criteria have been established [4, 8]. These scoring systems take into account clinical patterns (presentation, evolution), biological data (for AGEP and DRESS) and histological findings. The diagnostic scales are used to retrospectively score data and with consensus to classify cases as definitive, probable, possible or excluded.

Because the initial presentation of such adverse drug reactions may vary, diagnosis is difficult and suggests the possibility of overlap among SCARs. For instance, cases of AGEP may present facial oedema, atypical targets or blisters [12, 13], and 20% of cases may show mucous involvement [4]. Early descriptions of AGEP pointed to non-rare suspicion of TEN with a confluence of pustules resulting in superficial detachment, and even recently AGEP cases similar to TEN were reported [14]. Elevated neutrophil count may be accompanied by mild eosinophilia in up to one-third of cases in certain series [15]. Internal organ involvement is not common in AGEP, although lymph-node enlargement [15], slightly reduced creatinine clearance or slight elevation of liver enzyme levels may be observed [4].

Concerning DRESS, pustules may be found in up to 20% of cases [16]. Vesicles, blisters, atypical target lesions or mucous membrane involvement have been reported [6], occasionally with mild mucosal erosions [17]. Cases of “overlap” between DRESS and TEN have been reported, which suggests the difficulty in classifying these SCARs under certain circumstances [18].

Finally, in SJS-TEN, internal organ involvement is not rare and can include elevated levels of liver enzymes, eosinophilia, and transitory proteinuria [19‐21].

Therefore, because several conditions are suspected, clinicians may have difficulty diagnosing these SCARs [22]. Cases of overlapping SCARs – fulfilling diagnostic criteria for different SCARs -- may exist. We investigated cases of SCARs in our referral center to determine prevalence of overlapping SCARs, defined as fulfilling the criteria for definite or probable diagnosis of at least two ADRs accor-ding to scoring systems for AGEP, DRESS and SJS-TEN.

Among 383 patient cases with a discharge diagnosis of AGEP, DRESS, SJS-TEN or “drug rash”, only 250 were selected because a skin biopsy specimen was available. Data for 34 cases were excluded because of missing data for clinical presentation or biological results or wrong discharge diagnosis (Table 1). Eventually, 216 cases were analysed: 45 cases with a discharge diagnosis of AGEP, 47 with DRESS, 80 with SJS-TEN and 44 with drug rashes. The flow chart of the selection of cases is in Figure 1.

According to the scoring systems, among these 216 cases, 181 cases had at least one possible diagnosis: 107 had only one diagnosis (with definite or probable disease), 35 had 3 excluded diagnoses, 29 had a possible single diagnosis. The remaining 45 (21%) had several possible, distinct SCARs (possible, probable or definite) (Figure 2). Among the 45 cases, 35 had a single predominant diagnosis (definite or probable), 7 had several possible diagnoses and 3 (2.1% of confirmed 145 confirmed SCARs cases) were “true” overlap, with definite or probable diagnosis of 2 distinct SCARs: one overlap between AGEP and DRESS and 2 overlaps between SJS-TEN and DRESS (Figure 3).

Because the initial presentation of severe adverse drug reactions may vary, diagnosis may be difficult in that several conditions may be suspected. Our retrospective study of cases of SCARs in our referral centre revealed the frequent occurrence (n = 45; 21%) of SCARs cases of several possible diagnoses (possible, probable or certain), which reflects the clinical ambiguity among several SCARs. In such situations, the clinician is confronted with an uncertain diagnosis of several disease entities. For these 45 cases, when several diagnoses were at least possible, the retrospective assignment of a score often led to a single final diagnosis. Indeed, for 35 of the 45 cases, we could establish a single predominant diagnosis (probable or definite), with one (or several) other possible diagnosis(es). Seven of the 10 remaining cases could not be classified because several SCARs were possible. Only 3 “true” overlap SCARs were documented, representing 2.1% of the 145 confirmed cases of SCARs.

Finally, for the patient with a severe cutaneous reaction, determining the offending drug may be more important than a precise diagnosis with the reaction but is not totally acceptable because of different risks and the nature of long-term sequelae. Sequelae have never been reported after AGEP, are infrequent after DRESS and mostly auto-immune [23], and are nearly always present after SJS/TEN [24]. Therefore, follow-up will differ depending on the final diagnosis.

Not all SCARs have a similar weight in the evaluation of the benefit/risk balance by regulatory agencies and pharmaceutical companies. The mortality rate is 10 times lower for AGEP (2%) than SJS/TEN (20–25%) [10]. For a newly released drug, the report of one case as “AGEP” will have a different impact than a report of “TEN”.

The pathophysiology of drug eruption is not completely clear. AGEP, DRESS and SJS-TEN are all categorized as type IV reactions according to the classification by Coombs and Gell. Type IV reactions are mediated by T cells, causing so-called delayed hypersensitivity [25, 26]. Recently, several immunohistochemical and functional studies of drug-reactive T cells in patients with distinct forms of SCARs revealed that distinct T-cell functions led to different clinical phenotypes. These T cells recruit and activate monocytes, eosinophils or neutrophils. Drug-specific T cells also orchestrate inflammatory skin reactions by releasing various cytokines and chemokines. For instance, granulysin is the dominant cytokine inducing the destruction of epidermis in SJS-TEN [27], eotaxine and IL5 in DRESS [28, 29], and IL-8, IL-17 and IL-22 in AGEP [30, 31]. In considering the heterogeneity of T-cell function, Pichler et al. suggested further sub-classifying delayed hypersensitivity reactions into T-cell reactions, which through the release of certain cytokines and chemokines preferentially activate and recruit monocytes (type IVa), eosinophils (type IVb), or neutrophils (type IVD) [32]. Various drug-hypersensitivity diseases can be related to the preferential activation of drug-specific T cells with distinct functions. These complexe immune reactions are not exclusive and may be combined. An overlap of immune reactions is common, even if one type is often dominant, and would explain clinical ambiguities among SCARs [32, 33]. Research, especially into immunological mechanisms and pharmacogenetics, should be based on well-characterized phenotypes and drug causality. In such settings, diagnostic ambiguity could skew the results and must be avoided. A striking example was the finding in Taiwan that among carbamazepine-related SCARs, human leukokyte antigen B*1502 positivity was associated with all SJS or TEN cases but no cases of DRESS or mild eruptions [34]. If investigations had been performed on all carbamazepine-related cutaneous reactions, such clear results would not be missed.

The limitations of this study include its retrospective nature and selection bias. Indeed, patients hospitalized for SCARs may show a more severe or atypical presentation. The study was monocentric, and our department is a referral center for toxic bullous diseases, so recruitment of patients may have been biased because cases are addressed when particularly life-threatening. Cases were selected by exhaustivity of discharge diagnosis charts and their validity. Missing data might have caused the loss of many cases and could contribute to underestimating overlap cases. Interpretation bias was limited because clinical and histological data were scored by use of a predefined scoring algorithm, and the review committee was blinded to patient identity and exposure to risk factors and biological data. The strengths of this retrospective study are its exhaustiveness and use of pre-established diagnostic scales.

Our results suggest that even if ambiguities among SCARs are not rare, confirmation of overlap cases are rare. AGEP, DRESS and SJS-TEN are distinct entities with no evidence of a wide pathological spectrum. Differentiating different SCARs may lead to quicker diagnosis and more effective disease management.

This work was presented in part as an oral communication at Journées Dermatologiques de Paris, France in December 2007 and at the 3^rd Drug Hypersensitivity Meeting, Paris 2008 as a poster presentation.