Clinical and histologic features of Mycoplasma pneumoniae-related erythema multiforme: a single-center series of 33 cases compared with 100 cases induced by other causes

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Amode, Reyhan | Ingen-Housz-Oro, Saskia | Ortonne, Nicolas | Bounfour, Touda | Pereyre, Sabine | Schlemmer, Frédéric | Bequignon, Emilie | Royer, Gérard | Wolkenstein, Pierre | Chosidow, Olivier

Edité par CCSD ; Elsevier -

International audience. Background: Mycoplasma pneumoniae infection has been documented in erythema multiforme (EM) and Stevens-Johnson syndrome-toxic epidermal necrosis (SJS-TEN). Clinical aspects of M pneumoniaee related EM have been poorly described in the literature. Objective: To highlight differences between M pneumoniae EM and noneM pneumoniae EM. Methods: This single-center, retrospective cohort study included all patients admitted to our dermatology department for EM during 2000-2015. We compared epidemiologic, clinical, and histologic data and follow-up for M pneumoniae EM and noneM pneumoniae EM cases. Results: Thirty-three patients with M pneumoniae EM were compared with 100 patients with noneM pneumoniae EM. Disease onset in winter was more frequent with M pneumoniae EM (P = .003). Acrally distributed lesions (32% vs 88%, P < .0001) and typical targets (45% vs 74%, P = .01) were less common in M pneumoniae EM than noneM pneumoniae EM. Multiple (>= 2) mucousal membrane involvement was more frequent in M pneumoniae EM than noneM pneumoniae EM (97% vs 60%; P < .0001), as were mucosal and respiratory tract sequelae (P < .05). The mean hospital stay was longer with M pneumoniae EM patients: 9.5 days versus 5.1 days (P = .0002). A TEN-like pattern was observed in all 14 (100%) M pneumoniae EM skin biopsies versus 10 of 27 (48%) noneM pneumoniae EM biopsies (P < .001). Limitations: The retrospective design. Conclusion: M pneumoniae EM has a distinctive presentation compared with noneM pneumoniae EM, with more diffuse and atypical targets, more mucositis and respiratory tract sequelae. Histologic data show a TEN-like pattern in all M pneumoniae EM skin samples.

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