A Comparative Analysis Between Antibiotic- and Nonantibiotic-Associated Delayed Cutaneous Adverse Drug Reactions

A Comparative Analysis Between Antibiotic- and Nonantibiotic-Associated Delayed Cutaneous Adverse Drug Reactions

Background The difference in clinical presentation, causality assessments, and outcomes of patients with delayed antibiotic-associated cutaneous adverse drug reactions (AA-cADR) and nonantibiotic-associated (NA)-cADR is ill defined. Objective We examined the etiology of AA-cADR, with regard to the t...

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Veröffentlicht in:The journal of allergy and clinical immunology in practice (Cambridge, MA) MA), 2016-11, Vol.4 (6), p.1187-1193
Hauptverfasser: Trubiano, Jason A., MBBS, BBiomedSci, FRACP, Aung, Ar Kar, MBBS, Nguyen, Mary, BPharm, Fehily, Sasha R., MBBS, Graudins, Linda, BPharm, Cleland, Heather, MBBS, Padiglione, Alex, MBBS, PhD, Peleg, Anton Y., MBBS, PhD
Format: Artikel
Sprache:eng
Schlagworte:
Adult
Age
Aged
Allergy
Allergy and Immunology
Anti-Bacterial Agents - adverse effects
Antibiotics
Antimicrobial agents
Causality
Comorbidity
Drug Eruptions - etiology
Drug Labeling
Drug reactions
Female
Hospitalization - statistics & numerical data
Humans
Immunoglobulins
Internal Medicine
Male
Middle Aged
Mortality
Patients
Pharmaceutical industry
Side effects
Staphylococcus infections
Steven-Johnson syndrome
Toxic epidermal necrolysis
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Zusammenfassung:Background The difference in clinical presentation, causality assessments, and outcomes of patients with delayed antibiotic-associated cutaneous adverse drug reactions (AA-cADR) and nonantibiotic-associated (NA)-cADR is ill defined. Objective We examined the etiology of AA-cADR, with regard to the type of antibiotic exposure, allergy labeling, and patient outcomes, in comparison with NA-cADR. Methods A retrospective observational inpatient cohort study of cADR was performed from January 2004 to August 2014. Patients were divided into AA-cADR and NA-cADR groups for analysis. cADR was defined as erythema multiforme, fixed drug eruption, acute generalized erythematous pustulosis, drug reaction with eosinophilia and systemic symptoms (DRESS), drug-associated linear IgA disease, Stevens-Johnson syndrome, and toxic epidermal necrolysis. Results Of the 84 patients with cADR, 48% were AA-cADR. Male sex (60% vs 32%, P  = .004), median length of stay (14.5 vs 11 days, P  = .05), median Charlson comorbidity index (3 vs 1, P  = .03), and inpatient mortality (20% vs 5%, P  = .04) were higher in AA-cADR compared with NA-cADR. The median drug latency was lower in AA-cADR (6 vs 20 days, P  = .001). Sulfonamide antibiotics and glycopeptides were implicated in 20% of AA-cADR. DRESS was more frequently reported in AA-cADR. After cADR diagnosis, further antibiotic therapy was administered in 64% of patients, higher in AA-cADR (75%, 30 of 40) compared with NA-cADR (55%, 24 of 44) ( P  = .06). Fluoroquinolones (53% vs 21%, P  = .02), glycopeptides (vancomycin and teicoplanin; 70% vs 38%, P  = .05), and carbapenems (33% vs 13%, P  = .11) were used more commonly in AA-cADR. Conclusions Antibiotics were the cause of cADR requiring hospital admission in 48% of episodes, and were associated with longer length of stay, higher age-adjusted Charlson comorbidity index, shorter drug latency, and mortality. In AA-cADR, glycopeptide and sulfonamide antibiotic exposure predominated.
ISSN:2213-2198
2213-2201
DOI:10.1016/j.jaip.2016.04.026