A 14-year multicentric follow-up study of atypical pemphigus variants in Italy: the VARIANT_P study

L. Quintarelli; I. Bonanni; E. B. Mariotti; L. Atzori; Clara De Simone; C. Vassallo; Zenzo G. Di; S. Caccavale; E. Cozzani; G. Girolomoni; A. V. Marzano; A. Conti; P. Vezzoli; G. Damiani; Lernia V. Di; R. Balestri; R. Maglie; A. Corra; A. Magnatta; M. Donati; di Calabria V. Ruffo; A. Verdelli; A. Coi; E. Antiga; M. Caproni

doi:10.1093/ced/llaf438

A 14-year multicentric follow-up study of atypical pemphigus variants in Italy: the VARIANT_P study

L. Quintarelli
, I. Bonanni
, E. B. Mariotti
, L. Atzori
, Clara De Simone
, C. Vassallo
, Zenzo G. Di
, S. Caccavale
, E. Cozzani
, G. Girolomoni
, A. V. Marzano
, A. Conti
, P. Vezzoli
, G. Damiani
, Lernia V. Di
, R. Balestri
, R. Maglie
, A. Corra
, A. Magnatta
, M. Donati

di Calabria V. Ruffo, A. Verdelli, A. Coi, E. Antiga, M. Caproni^*

^*Autore corrispondente per questo lavoro

University of Florence
University of Cagliari
IRCCS Fondazione Policlinico San Matteo - Pavia
IRCCS Istituto Dermopatico dell'Immacolata - Roma
University of Campania Luigi Vanvitelli
San Martino Hospital Genoa
University of Verona
Infermi Hospital Rimini
ASST Papa Giovanni XXIII
IRCCS Istituto Ortopedico Galeazzi - Milano
IRCCS Azienda Unità Sanitaria Locale di Reggio Emilia
CNR Institute of Clinical Physiology

Risultato della ricerca: Contributo in rivista › Articolo

Abstract

Background The clinical, epidemiological and immunopathological profiles of atypical forms of pemphigus remain only partially known. Objectives To define the clinical, epidemiological and immunological characteristics, therapies and outcomes in patients with atypical pemphigus variants. Methods This was a 14-year multicentre retrospective observational study (VARIANT_P) on atypical variants of pemphigus across Italy. We collected demographic, immunopathological and clinical data, as well as information on comorbidities and prescribed treatments. Results We enrolled 61 patients [female/male sex ratio 1.77; 13 paraneoplastic pemphigus (PNP), 26 IgA pemphigus (PIgA), 22 pemphigus herpetiformis (PH)]. The median ages at onset and diagnosis were 70.6 (range 43.1–86.8) and 71.1 (range 46.9–86.9) for PNP; 62.2 (range 3.8–81.0) and 63.6 (range 4.0–82.4) for PIgA; and 49.4 (range 5.4–84.4) and 52.3 (range 5.9–85.9) for PH, respectively. The median diagnostic delay was 3.0 (range 0.0–45.6) months for PNP, 9.5 (range 1.0–140.0) months for PIgA and 2.0 (range 0–30.4) months for PH. The mortality rate was 55% (6/11) for PNP, 4% (1/26) for PIgA and 6% (1/17) for PH. Cutaneous involvement was present in all patients with PIgA and PH, and in 83% (10/12) of the patients with PNP. In contrast, oral mucosal involvement was observed in all patients with PNP with data (n= 12), but only in 8% (2/26) of those with PIgA and 21% (4/19) of those with PH. Histology, direct immunofluorescence, indirect immunofluorescence and enzyme-linked immunosorbent assay data demonstrated variable concordance with previously known data. Comorbidities included mainly solid malignancies for people with PNP, whereas cardiovascular and metabolic diseases were the most prevalent for those with PIgA and PH. Treatment mostly relied on systemic steroids and rituximab. Conclusions The VARIANT_P study contributes to data collection relating to atypical pemphigus variants in order to promote the development of specific therapeutical guidelines in the future.

Lingua originale	Inglese
pagine (da-a)	250-262
Numero di pagine	13
Rivista	Clinical and Experimental Dermatology
Volume	51
Numero di pubblicazione	2
DOI	https://doi.org/10.1093/ced/llaf438
Stato di pubblicazione	Pubblicato - 2026

OSS delle Nazioni Unite

Questo processo contribuisce al raggiungimento dei seguenti obiettivi di sviluppo sostenibile

SDG 3 Salute e benessere

All Science Journal Classification (ASJC) codes

Dermatologia

Keywords

pemphigus

Accesso al documento

10.1093/ced/llaf438

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Quintarelli, L., Bonanni, I., Mariotti, E. B., Atzori, L., De Simone, C., Vassallo, C., Di, Z. G., Caccavale, S., Cozzani, E., Girolomoni, G., Marzano, A. V., Conti, A., Vezzoli, P., Damiani, G., Di, L. V., Balestri, R., Maglie, R., Corra, A., Magnatta, A., ... Caproni, M. (2026). A 14-year multicentric follow-up study of atypical pemphigus variants in Italy: the VARIANT_P study. Clinical and Experimental Dermatology, 51(2), 250-262. https://doi.org/10.1093/ced/llaf438

@article{a6c9214fcc224ca9aa0040af500ae62d,

title = "A 14-year multicentric follow-up study of atypical pemphigus variants in Italy: the VARIANT\_P study",

abstract = "Background The clinical, epidemiological and immunopathological profiles of atypical forms of pemphigus remain only partially known. Objectives To define the clinical, epidemiological and immunological characteristics, therapies and outcomes in patients with atypical pemphigus variants. Methods This was a 14-year multicentre retrospective observational study (VARIANT\_P) on atypical variants of pemphigus across Italy. We collected demographic, immunopathological and clinical data, as well as information on comorbidities and prescribed treatments. Results We enrolled 61 patients [female/male sex ratio 1.77; 13 paraneoplastic pemphigus (PNP), 26 IgA pemphigus (PIgA), 22 pemphigus herpetiformis (PH)]. The median ages at onset and diagnosis were 70.6 (range 43.1–86.8) and 71.1 (range 46.9–86.9) for PNP; 62.2 (range 3.8–81.0) and 63.6 (range 4.0–82.4) for PIgA; and 49.4 (range 5.4–84.4) and 52.3 (range 5.9–85.9) for PH, respectively. The median diagnostic delay was 3.0 (range 0.0–45.6) months for PNP, 9.5 (range 1.0–140.0) months for PIgA and 2.0 (range 0–30.4) months for PH. The mortality rate was 55\% (6/11) for PNP, 4\% (1/26) for PIgA and 6\% (1/17) for PH. Cutaneous involvement was present in all patients with PIgA and PH, and in 83\% (10/12) of the patients with PNP. In contrast, oral mucosal involvement was observed in all patients with PNP with data (n= 12), but only in 8\% (2/26) of those with PIgA and 21\% (4/19) of those with PH. Histology, direct immunofluorescence, indirect immunofluorescence and enzyme-linked immunosorbent assay data demonstrated variable concordance with previously known data. Comorbidities included mainly solid malignancies for people with PNP, whereas cardiovascular and metabolic diseases were the most prevalent for those with PIgA and PH. Treatment mostly relied on systemic steroids and rituximab. Conclusions The VARIANT\_P study contributes to data collection relating to atypical pemphigus variants in order to promote the development of specific therapeutical guidelines in the future.",

keywords = "pemphigus, pemphigus",

author = "L. Quintarelli and I. Bonanni and Mariotti, \{E. B.\} and L. Atzori and \{De Simone\}, Clara and C. Vassallo and Di, \{Zenzo G.\} and S. Caccavale and E. Cozzani and G. Girolomoni and Marzano, \{A. V.\} and A. Conti and P. Vezzoli and G. Damiani and Di, \{Lernia V.\} and R. Balestri and R. Maglie and A. Corra and A. Magnatta and M. Donati and Ruffo, \{di Calabria V.\} and A. Verdelli and A. Coi and E. Antiga and M. Caproni",

year = "2026",

doi = "10.1093/ced/llaf438",

language = "English",

volume = "51",

pages = "250--262",

journal = "Clinical and Experimental Dermatology",

issn = "0307-6938",

publisher = "Oxford University Press",

number = "2",

}

Quintarelli, L, Bonanni, I, Mariotti, EB, Atzori, L, De Simone, C, Vassallo, C, Di, ZG, Caccavale, S, Cozzani, E, Girolomoni, G, Marzano, AV, Conti, A, Vezzoli, P, Damiani, G, Di, LV, Balestri, R, Maglie, R, Corra, A, Magnatta, A, Donati, M, Ruffo, DCV, Verdelli, A, Coi, A, Antiga, E & Caproni, M 2026, 'A 14-year multicentric follow-up study of atypical pemphigus variants in Italy: the VARIANT_P study', Clinical and Experimental Dermatology, vol. 51, n. 2, pagg. 250-262. https://doi.org/10.1093/ced/llaf438

TY - JOUR

T1 - A 14-year multicentric follow-up study of atypical pemphigus variants in Italy: the VARIANT_P study

AU - Quintarelli, L.

AU - Bonanni, I.

AU - Mariotti, E. B.

AU - Atzori, L.

AU - De Simone, Clara

AU - Vassallo, C.

AU - Di, Zenzo G.

AU - Caccavale, S.

AU - Cozzani, E.

AU - Girolomoni, G.

AU - Marzano, A. V.

AU - Conti, A.

AU - Vezzoli, P.

AU - Damiani, G.

AU - Di, Lernia V.

AU - Balestri, R.

AU - Maglie, R.

AU - Corra, A.

AU - Magnatta, A.

AU - Donati, M.

AU - Ruffo, di Calabria V.

AU - Verdelli, A.

AU - Coi, A.

AU - Antiga, E.

AU - Caproni, M.

PY - 2026

Y1 - 2026

N2 - Background The clinical, epidemiological and immunopathological profiles of atypical forms of pemphigus remain only partially known. Objectives To define the clinical, epidemiological and immunological characteristics, therapies and outcomes in patients with atypical pemphigus variants. Methods This was a 14-year multicentre retrospective observational study (VARIANT_P) on atypical variants of pemphigus across Italy. We collected demographic, immunopathological and clinical data, as well as information on comorbidities and prescribed treatments. Results We enrolled 61 patients [female/male sex ratio 1.77; 13 paraneoplastic pemphigus (PNP), 26 IgA pemphigus (PIgA), 22 pemphigus herpetiformis (PH)]. The median ages at onset and diagnosis were 70.6 (range 43.1–86.8) and 71.1 (range 46.9–86.9) for PNP; 62.2 (range 3.8–81.0) and 63.6 (range 4.0–82.4) for PIgA; and 49.4 (range 5.4–84.4) and 52.3 (range 5.9–85.9) for PH, respectively. The median diagnostic delay was 3.0 (range 0.0–45.6) months for PNP, 9.5 (range 1.0–140.0) months for PIgA and 2.0 (range 0–30.4) months for PH. The mortality rate was 55% (6/11) for PNP, 4% (1/26) for PIgA and 6% (1/17) for PH. Cutaneous involvement was present in all patients with PIgA and PH, and in 83% (10/12) of the patients with PNP. In contrast, oral mucosal involvement was observed in all patients with PNP with data (n= 12), but only in 8% (2/26) of those with PIgA and 21% (4/19) of those with PH. Histology, direct immunofluorescence, indirect immunofluorescence and enzyme-linked immunosorbent assay data demonstrated variable concordance with previously known data. Comorbidities included mainly solid malignancies for people with PNP, whereas cardiovascular and metabolic diseases were the most prevalent for those with PIgA and PH. Treatment mostly relied on systemic steroids and rituximab. Conclusions The VARIANT_P study contributes to data collection relating to atypical pemphigus variants in order to promote the development of specific therapeutical guidelines in the future.

AB - Background The clinical, epidemiological and immunopathological profiles of atypical forms of pemphigus remain only partially known. Objectives To define the clinical, epidemiological and immunological characteristics, therapies and outcomes in patients with atypical pemphigus variants. Methods This was a 14-year multicentre retrospective observational study (VARIANT_P) on atypical variants of pemphigus across Italy. We collected demographic, immunopathological and clinical data, as well as information on comorbidities and prescribed treatments. Results We enrolled 61 patients [female/male sex ratio 1.77; 13 paraneoplastic pemphigus (PNP), 26 IgA pemphigus (PIgA), 22 pemphigus herpetiformis (PH)]. The median ages at onset and diagnosis were 70.6 (range 43.1–86.8) and 71.1 (range 46.9–86.9) for PNP; 62.2 (range 3.8–81.0) and 63.6 (range 4.0–82.4) for PIgA; and 49.4 (range 5.4–84.4) and 52.3 (range 5.9–85.9) for PH, respectively. The median diagnostic delay was 3.0 (range 0.0–45.6) months for PNP, 9.5 (range 1.0–140.0) months for PIgA and 2.0 (range 0–30.4) months for PH. The mortality rate was 55% (6/11) for PNP, 4% (1/26) for PIgA and 6% (1/17) for PH. Cutaneous involvement was present in all patients with PIgA and PH, and in 83% (10/12) of the patients with PNP. In contrast, oral mucosal involvement was observed in all patients with PNP with data (n= 12), but only in 8% (2/26) of those with PIgA and 21% (4/19) of those with PH. Histology, direct immunofluorescence, indirect immunofluorescence and enzyme-linked immunosorbent assay data demonstrated variable concordance with previously known data. Comorbidities included mainly solid malignancies for people with PNP, whereas cardiovascular and metabolic diseases were the most prevalent for those with PIgA and PH. Treatment mostly relied on systemic steroids and rituximab. Conclusions The VARIANT_P study contributes to data collection relating to atypical pemphigus variants in order to promote the development of specific therapeutical guidelines in the future.

KW - pemphigus

UR - https://publicatt.unicatt.it/handle/10807/336914

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U2 - 10.1093/ced/llaf438

DO - 10.1093/ced/llaf438

M3 - Article

SN - 0307-6938

VL - 51

SP - 250

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JO - Clinical and Experimental Dermatology

JF - Clinical and Experimental Dermatology

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ER -

A 14-year multicentric follow-up study of atypical pemphigus variants in Italy: the VARIANT_P study

Abstract

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Keywords

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