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Pattern and course of single-system disease in Langerhans cell histiocytosis data from the DAL-HX 83- and 90-study

✍ Scribed by Titgemeyer, Carola ;Grois, Nicole ;Minkov, Milen ;Flucher-Wolfram, Burgi ;Gatterer-Menz, Irmgard ;Gadner, Helmut


Publisher
John Wiley and Sons
Year
2001
Tongue
English
Weight
165 KB
Volume
37
Category
Article
ISSN
0098-1532

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✦ Synopsis


Abstract

Background

Single‐system (SS) disease is the most common presentation in Langerhans cell histiocytosis (LCH) with a heterogenous clinical picture and course. Mostly bone and rarely skin or lymph nodes are involved.

Procedure

One hundred and seventy patients with SS‐LCH were registered in the DAL‐HX 83/90 studies. They were diagnosed according to uniform diagnostic criteria and followed by a standardised schedule.

Results

Single bone lesions were most common (68%), followed by multiple bone lesions (19%), isolated skin disease (11%), and isolated lymph node involvement (4 patients). In the detection of bone lesions radiographic skeletal survey proved to be superior to bone scan (97% vs. 82%). Treatment comprised surgery, irradiation and local instillation of steroids, and standardised chemotherapy for multifocal bone disease. After initial therapy 81% of the patients remained disease free. Reactivations restricted to the skeleton occurred in 18% of both unifocal and multifocal bone disease. Two skin patients had a chronic course. Fatality occured only in one infant with skin disease who progressed to multi‐system disease. Twenty‐five percent of all patients developed permanent consequences, which were already present at diagnosis in about half of these patients and comprised mainly orthopedic problems related to lesional sites. Diabetes insipidus occurred in 3% and anterior pituitary dysfunction in 2% of the patients.

Conclusions

The course in SS%LCH was benign. In bone disease reactivations remained restricted to the skeleton and did not influence survival. However, reactivations had an impact on morbidity, as permanent consequences were mostly related to the site of disease activity. Med Pediatr Oncol 2001;37:108–114. © 2001 Wiley‐Liss, Inc.