Juvenile xanthogranuloma: Forms of systemic disease and their clinical implications,☆☆,,★★

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Abstract

OBJECTIVE: Juvenile xanthogranuloma (JXG) with systemic (extracutaneous) involvement is a rare histiocytic disorder in which significant morbidity and occasional deaths may occur. The objective of this study was to characterize the spectrum of anatomic involvement, associated clinical problems, and management considerations in children with systemic JXG. STUDY DESIGN: Two current cases and literature reports of 34 children with various forms of systemic JXG were analyzed with respect to age, clinical presentation, site(s) of involvement, therapy, and outcome. RESULTS: The median age of the 36 patients was 0.3 years (range, birth to 12 years). Symptoms were usually referable to bulky or infiltrative disease. Twenty patients had disease in two or more sites. Cutaneous lesions were present in fewer than half the patients. The most frequent extracutaneous sites of disease were the subcutaneous soft tissue (12); central nervous system (8); liver/spleen (8); lung (6); eye/orbit, oropharynx, and muscle (4 each); with three or fewer instances of disease in each of several other sites. Most patients were treated with excision or had spontaneous regression (some with organ involvement). However, 12 patients received treatment that included radiation or systemic chemotherapy. Survivors, some with long-term disabilities, included young children who had received radiation therapy to the brain, eye, skin, or heart. Two patients died of disease. CONCLUSIONS: Systemic JXG may involve varying numbers and combinations of extracutaneous sites. The extent of disease should be determined in patients with JXG who are suspected to have systemic involvement. In contrast to the cutaneous form, systemic JXG may be associated with significant complications requiring aggressive medical care. When feasible, surgical excision of lesions may be curative. Optimal treatment for symptomatic, unresectable disease is currently undefined but should be selected to minimize toxic effects in these children who are typically younger than 1 year old at presentation. (J PEDIATR 1996;129:227-37)

Section snippets

Patient 1

A white male infant was first noted to have skin lesions at the age of 1 month. A biopsy of a skin lesion at age 5 months was considered suggestive of LCH. At that time, results of the complete blood cell count, serum biochemical profile, and erythrocyte sedimentation rate were normal; chest x-ray films showed increased interstitial markings. Serum cholesterol and triglyceride levels determined from a random specimen during a nonfasting state were 162 mg/dl and 219 mg/dl, respectively

Nosology of juvenile xanthogranuloma

The histiocytoses represent a family of presumably related disorders characterized by the proliferation of mononuclear phagocytes or so-called professional antigen-presenting cells that include Langerhans cells.7 Until recently, incomplete knowledge of the developmental biology of histiocytes has hampered the formulation of an accurate and meaningful classification of histiocytic disorders. With the identification of ultrastructural, antigenic, and functional cellular markers by newer

Acknowledgements

The biopsy specimens of patient 2 were also reviewed by Blaise E. Favara, MD. We thank Ms. Thelma Boroff for expert secretarial assistance.

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    From the Departments of Pediatrics and Pathology, DeVos Children's Hospital, Grand Rapids, Michigan, the Department of Pediatrics, Michigan State University College of Human Medicine, East Lansing, and the Division of Pediatric Hematology/Oncology, Children's Health Care-Minneapolis, Minneapolis, Minnesota, and the Lauren V. Ackerman Laboratory of Surgical Pathology, Washington University Medical Center, St. Louis, Missouri

    ☆☆

    Supported in part by the Peter C. and Pat Cook Health Sciences and Research Education Institute.

    Reprint requests: David R. Freyer, DO, Division of Pediatric Hematology/Oncology, DeVos Children's Hospital, 100 Michigan, N.E., Mailcode 85, Grand Rapids, MI 49503.

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