Juvenile localized scleroderma: Clinical and epidemiological features in 750 children. An international study

F. Zulian; B. H. Athreya; R. Laxer; A. M. Nelson; S. K. Feitosa de Oliveira; M. G. Punaro; R. Cuttica; G. C. Higgins; L. W A Van Suijlekom-Smit; T. L. Moore; C. Lindsley; J. Garcia-Consuegra; M. O. Esteves Hilário; L. Lepore; C. A. Silva; C. Machado; S. M. Garay; Y. Uziel; G. Martini; I. Foeldvari; A. Peserico; P. Woo; J. Harper

doi:10.1093/rheumatology/kei251

Juvenile localized scleroderma: Clinical and epidemiological features in 750 children. An international study

F. Zulian, B. H. Athreya, R. Laxer, A. M. Nelson, S. K. Feitosa de Oliveira, M. G. Punaro, R. Cuttica, G. C. Higgins, L. W A Van Suijlekom-Smit, T. L. Moore, C. Lindsley, J. Garcia-Consuegra, M. O. Esteves Hilário, L. Lepore, C. A. Silva, C. Machado, S. M. Garay, Y. Uziel, G. Martini, I. FoeldvariA. Peserico, P. Woo, J. Harper

Pediatrics

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364 Scopus citations

Abstract

Objective. Juvenile localized scleroderma (JLS) includes a number of conditions often grouped together. With the long-term goal of developing uniform classification criteria, we studied the epidemiological, clinical and immunological features of children with JLS followed by paediatric rheumatology and dermatology centres. Methods. A large, multicentre, multinational study was conducted by collecting information on the demographics, family history, triggering environmental factors, clinical and laboratory features, and treatment of patients with JLS. Results. Seven hundred and fifty patients with JLS from 70 centres were enrolled into the study. The disease duration at diagnosis was 18 months. Linear scleroderma (LS) was the most frequent subtype (65%), followed by plaque morphea (PM) (26%), generalized morphea (GM) (7%) and deep morphea (DM) (2%). As many as 15% of patients had a mixed subtype. Ninety-one patients (12%) had a positive family history for rheumatic or autoimmune diseases; 100 (13.3%) reported environmental events as possible trigger. ANA was positive in 42.3% of the patients, with a higher prevalence in the LS-DM subtype than in the PM-GM subtype. Scl70 was detected in the sera of 3% of the patients, anticentromere antibody in 2%, anti-double-stranded DNA in 4%, anti-cardiolipin antibody in 13% and rheumatoid factor in 16%. Methotrexate was the drug most frequently used, especially during the last 5 yr. Conclusion. This study represents the largest collection of patients with JLS ever reported. The insidious onset of the disease, the delay in diagnosis, the recognition of mixed subtype and the better definition of the other subtypes should influence our efforts in educating trainees and practitioners and help in developing a comprehensive classification system for this syndrome.

Original language	English (US)
Pages (from-to)	614-620
Number of pages	7
Journal	Rheumatology
Volume	45
Issue number	5
DOIs	https://doi.org/10.1093/rheumatology/kei251
State	Published - May 2006

Keywords

Morphea
Parry-Romberg syndrome
Progressive hemifacial atrophy
Scleroderma
Scleroderma en coup de sabre

ASJC Scopus subject areas

Rheumatology
Pharmacology (medical)

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Zulian, F., Athreya, B. H., Laxer, R., Nelson, A. M., Feitosa de Oliveira, S. K., Punaro, M. G., Cuttica, R., Higgins, G. C., Van Suijlekom-Smit, L. W. A., Moore, T. L., Lindsley, C., Garcia-Consuegra, J., Esteves Hilário, M. O., Lepore, L., Silva, C. A., Machado, C., Garay, S. M., Uziel, Y., Martini, G., ... Harper, J. (2006). Juvenile localized scleroderma: Clinical and epidemiological features in 750 children. An international study. Rheumatology, 45(5), 614-620. https://doi.org/10.1093/rheumatology/kei251

Zulian, F, Athreya, BH, Laxer, R, Nelson, AM, Feitosa de Oliveira, SK, Punaro, MG, Cuttica, R, Higgins, GC, Van Suijlekom-Smit, LWA, Moore, TL, Lindsley, C, Garcia-Consuegra, J, Esteves Hilário, MO, Lepore, L, Silva, CA, Machado, C, Garay, SM, Uziel, Y, Martini, G, Foeldvari, I, Peserico, A, Woo, P & Harper, J 2006, 'Juvenile localized scleroderma: Clinical and epidemiological features in 750 children. An international study', Rheumatology, vol. 45, no. 5, pp. 614-620. https://doi.org/10.1093/rheumatology/kei251

@article{1158e09835f9403795b2fd8d4d56c2f8,

title = "Juvenile localized scleroderma: Clinical and epidemiological features in 750 children. An international study",

abstract = "Objective. Juvenile localized scleroderma (JLS) includes a number of conditions often grouped together. With the long-term goal of developing uniform classification criteria, we studied the epidemiological, clinical and immunological features of children with JLS followed by paediatric rheumatology and dermatology centres. Methods. A large, multicentre, multinational study was conducted by collecting information on the demographics, family history, triggering environmental factors, clinical and laboratory features, and treatment of patients with JLS. Results. Seven hundred and fifty patients with JLS from 70 centres were enrolled into the study. The disease duration at diagnosis was 18 months. Linear scleroderma (LS) was the most frequent subtype (65%), followed by plaque morphea (PM) (26%), generalized morphea (GM) (7%) and deep morphea (DM) (2%). As many as 15% of patients had a mixed subtype. Ninety-one patients (12%) had a positive family history for rheumatic or autoimmune diseases; 100 (13.3%) reported environmental events as possible trigger. ANA was positive in 42.3% of the patients, with a higher prevalence in the LS-DM subtype than in the PM-GM subtype. Scl70 was detected in the sera of 3% of the patients, anticentromere antibody in 2%, anti-double-stranded DNA in 4%, anti-cardiolipin antibody in 13% and rheumatoid factor in 16%. Methotrexate was the drug most frequently used, especially during the last 5 yr. Conclusion. This study represents the largest collection of patients with JLS ever reported. The insidious onset of the disease, the delay in diagnosis, the recognition of mixed subtype and the better definition of the other subtypes should influence our efforts in educating trainees and practitioners and help in developing a comprehensive classification system for this syndrome.",

keywords = "Morphea, Parry-Romberg syndrome, Progressive hemifacial atrophy, Scleroderma, Scleroderma en coup de sabre",

author = "F. Zulian and Athreya, {B. H.} and R. Laxer and Nelson, {A. M.} and {Feitosa de Oliveira}, {S. K.} and Punaro, {M. G.} and R. Cuttica and Higgins, {G. C.} and {Van Suijlekom-Smit}, {L. W A} and Moore, {T. L.} and C. Lindsley and J. Garcia-Consuegra and {Esteves Hil{\'a}rio}, {M. O.} and L. Lepore and Silva, {C. A.} and C. Machado and Garay, {S. M.} and Y. Uziel and G. Martini and I. Foeldvari and A. Peserico and P. Woo and J. Harper",

year = "2006",

month = may,

doi = "10.1093/rheumatology/kei251",

language = "English (US)",

volume = "45",

pages = "614--620",

journal = "Rheumatology",

issn = "1462-0324",

publisher = "Oxford University Press",

number = "5",

}

TY - JOUR

T1 - Juvenile localized scleroderma

T2 - Clinical and epidemiological features in 750 children. An international study

AU - Zulian, F.

AU - Athreya, B. H.

AU - Laxer, R.

AU - Nelson, A. M.

AU - Feitosa de Oliveira, S. K.

AU - Punaro, M. G.

AU - Cuttica, R.

AU - Higgins, G. C.

AU - Van Suijlekom-Smit, L. W A

AU - Moore, T. L.

AU - Lindsley, C.

AU - Garcia-Consuegra, J.

AU - Esteves Hilário, M. O.

AU - Lepore, L.

AU - Silva, C. A.

AU - Machado, C.

AU - Garay, S. M.

AU - Uziel, Y.

AU - Martini, G.

AU - Foeldvari, I.

AU - Peserico, A.

AU - Woo, P.

AU - Harper, J.

PY - 2006/5

Y1 - 2006/5

N2 - Objective. Juvenile localized scleroderma (JLS) includes a number of conditions often grouped together. With the long-term goal of developing uniform classification criteria, we studied the epidemiological, clinical and immunological features of children with JLS followed by paediatric rheumatology and dermatology centres. Methods. A large, multicentre, multinational study was conducted by collecting information on the demographics, family history, triggering environmental factors, clinical and laboratory features, and treatment of patients with JLS. Results. Seven hundred and fifty patients with JLS from 70 centres were enrolled into the study. The disease duration at diagnosis was 18 months. Linear scleroderma (LS) was the most frequent subtype (65%), followed by plaque morphea (PM) (26%), generalized morphea (GM) (7%) and deep morphea (DM) (2%). As many as 15% of patients had a mixed subtype. Ninety-one patients (12%) had a positive family history for rheumatic or autoimmune diseases; 100 (13.3%) reported environmental events as possible trigger. ANA was positive in 42.3% of the patients, with a higher prevalence in the LS-DM subtype than in the PM-GM subtype. Scl70 was detected in the sera of 3% of the patients, anticentromere antibody in 2%, anti-double-stranded DNA in 4%, anti-cardiolipin antibody in 13% and rheumatoid factor in 16%. Methotrexate was the drug most frequently used, especially during the last 5 yr. Conclusion. This study represents the largest collection of patients with JLS ever reported. The insidious onset of the disease, the delay in diagnosis, the recognition of mixed subtype and the better definition of the other subtypes should influence our efforts in educating trainees and practitioners and help in developing a comprehensive classification system for this syndrome.

AB - Objective. Juvenile localized scleroderma (JLS) includes a number of conditions often grouped together. With the long-term goal of developing uniform classification criteria, we studied the epidemiological, clinical and immunological features of children with JLS followed by paediatric rheumatology and dermatology centres. Methods. A large, multicentre, multinational study was conducted by collecting information on the demographics, family history, triggering environmental factors, clinical and laboratory features, and treatment of patients with JLS. Results. Seven hundred and fifty patients with JLS from 70 centres were enrolled into the study. The disease duration at diagnosis was 18 months. Linear scleroderma (LS) was the most frequent subtype (65%), followed by plaque morphea (PM) (26%), generalized morphea (GM) (7%) and deep morphea (DM) (2%). As many as 15% of patients had a mixed subtype. Ninety-one patients (12%) had a positive family history for rheumatic or autoimmune diseases; 100 (13.3%) reported environmental events as possible trigger. ANA was positive in 42.3% of the patients, with a higher prevalence in the LS-DM subtype than in the PM-GM subtype. Scl70 was detected in the sera of 3% of the patients, anticentromere antibody in 2%, anti-double-stranded DNA in 4%, anti-cardiolipin antibody in 13% and rheumatoid factor in 16%. Methotrexate was the drug most frequently used, especially during the last 5 yr. Conclusion. This study represents the largest collection of patients with JLS ever reported. The insidious onset of the disease, the delay in diagnosis, the recognition of mixed subtype and the better definition of the other subtypes should influence our efforts in educating trainees and practitioners and help in developing a comprehensive classification system for this syndrome.

KW - Morphea

KW - Parry-Romberg syndrome

KW - Progressive hemifacial atrophy

KW - Scleroderma

KW - Scleroderma en coup de sabre

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Juvenile localized scleroderma: Clinical and epidemiological features in 750 children. An international study

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Keywords

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