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Blood, Vol. 93 No. 12 (June 15), 1999:
pp. 4125-4130
By
From the Division of Hematology/Oncology, Ida M. and Cecil H. Green
Cancer Center, Scripps Clinic, La Jolla, CA.
Langerhans-cell histiocytosis (LCH) results from the accumulation of
tissue histiocytes derived from the same progenitor cells as monocytes.
Because cladribine is potently toxic to monocytes, we conducted a phase
II trial of cladribine. Cladribine was administered to 13 LCH patients
at 0.14 mg/kg per day by 2-hour intravenous infusion for 5 consecutive
days, every 4 weeks for a maximum of six courses. Median age was 42 years (range, 19 to 72) and median pretreatment disease duration was 99 months (range, 6 to 252). One patient was untreated, one had received
prior prednisone only, one prior radiation only, six prior radiation
and chemotherapy, and four prior surgery, radiation, and chemotherapy.
Seven patients had cutaneous involvement, six multifocal osseous, six
pulmonary, two each with soft tissue and nodal involvement, and four
had diabetes insipidus. Of 13 patients, 12 were evaluable for response and all for toxicity. After a median of three courses (range, 1 to 6),
seven (58%) patients achieved complete responses (two pathologic and
five clinical) and two (17%) patients achieved partial responses;
overall response rate, 75%. Median response follow-up duration was 33 months (range, 1 to 65). Seven patients experienced grade 3 to 4 neutropenia. Only one patient had a documented infection, dermatomal
herpes zoster. At a median follow-up of 42 months (range, 5 to 76), 12 patients remain alive and one patient has died. Thus, cladribine has
major activity in adult LCH and warrants further investigation in both
pediatric and adult LCH as a single agent and in combination with other drugs.
LANGERHANS-CELL histiocytosis (LCH)
results from the clonal proliferation and accumulation of tissue
histiocytes, clinically manifested as osteolytic lesions, hypothalamic
insufficiency, and seborrheic and vesiculopustular lesions on the
scalp, perineum, rectum, and vulva.1,2 The clinical
presentation and course of individual patients varies from indolent to
aggressive and from spontaneous remission to rapid death. Prognosis is
determined by the number of affected organs and their
dysfunction.3,4 The diagnosis is established by identifying
Langerhans or histiocytosis X cells, associated occasionally with
multinucleated giant cells, in affected lymph nodes, bones, skin
and lungs by microscopy or immunohistochemical staining, such as
positivity for the S-100 protein.5 Birbeck granules seen on
electron microscopy and characterized by the indentation across the
nucleus of mononuclear cells, are pathognomonic.
Treatment of LCH is principally palliative. The therapeutic modalities
most frequently used are corticosteroids, alkylating agents,
antimetabolites, vinca alkaloids, combination chemotherapy, irradiation, and immunotherapy.6-8 2-Chlorodeoxyadenosine
(2-CdA) (cladribine, Leustatin [Ortho Biotech, Raritan, NJ]), a
purine analogue with activity in indolent lymphoproliferative
disorders9,10 and myeloid leukemias11,12 is
potently toxic to monocytes in vitro.13 Cladribine was
approved by the Food and Drug Administration (FDA) in 1993 for the
treatment of hairy cell leukemia, an uncommon chronic B-cell
lymphoproliferative disorder characterized by mononuclear cells
displaying cytoplasmic projections, as single courses of treatment
induce long-lasting complete remissions in the vast majority of
patients treated.9 Because tissue histiocytes and circulating monocytes have common progenitor cell origins, cladribine was a rational therapeutic option. Previously, we reported on three
patients with LCH, all of whom obtained complete and durable remissions
after cladribine administration.14,15 We, therefore, conducted a phase II study evaluating the efficacy and toxicity of
cladribine in larger numbers of patients with LCH.
Eligibility Criteria
Baseline and Follow-Up Studies
Response Criteria A complete response was defined as the absence of active disease on physical examination and imaging studies.17 Disease activity was established on clinical grounds.17 Active disease was defined as chronic progression, new symptomatic, histologically verified organ manifestations or local disease recurrence after initially successful therapy. Inactive disease was defined as no lesion/disease, stable asymptomatic, or stable symptomatic, but not progressive disease. Cutaneous lesions did not require repeat biopsy to document histologic resolution. A partial response was defined as a reduction by more than 50% of all measurable and active disease for more than 1 month. Any response less than partial was designated as no response. All clinical assessments were made by the author (A.S.), and all imaging studies were reviewed by the radiologists at Scripps Clinic.Cladribine Therapy Cladribine was administered at 0.1 mg/kg daily for 7 days by continuous intravenous infusion (patients 1 and 2) and 0.14 mg/kg per day over 2 hours intravenously daily for 5 consecutive days (patients 3 to 13), with courses repeated every 4 weeks, toxicity permitting. If, 4 weeks after the completion of the third course of cladribine, the patient did not achieve a partial or complete response, then no further cladribine was administered. The patient was then switched to alternative therapy if deemed appropriate. If, 4 weeks after the completion of the third course of cladribine a partial response had been achieved, cladribine was administered until maximum response or prohibitive toxicity was encountered. If a complete response had been achieved, then the patient received no further cladribine until documented disease recurrence, when this occurred. The total number of courses of cladribine administered did not exceed a maximum of six courses.Toxicity The National Cancer Institute Common Toxicity Criteria were used for the evaluation of toxicity with grade 3 and 4 being considered significant.18 The initiation of cladribine therapy was delayed for an absolute granulocyte count < 1.0 × 109 per liter, or a > 50% reduction in the pretreatment platelet count. Cladribine was then held until the platelet count was more than 75% of the pretreatment value, or if the platelet count was > 100 × 109 per liter, cladribine could be administered regardless.
Patient Characteristics Patient characteristics at the initiation of cladribine are shown in Table 1. Of the 13 patients treated, seven were men and six were women. The median age at initiation of cladribine was 42 years (range, 19 to 72 years) and the median pretreatment duration was 99 months (range, 6 to 252 months). Using the histopathologic diagnostic criteria proposed by the Writing Group of the Histiocyte Society, five patients had a definitive diagnosis, four had a diagnosis and four had a presumptive diagnosis of LCH.16 One patient had received no prior therapy, one patient had received prior prednisone, one patient radiation only, six patients radiation and chemotherapy, and four patients surgery, radiation, and chemotherapy. Using the staging system as designated by Lavin and Osband,19 eight patients had stage I disease, four patients stage II disease, and one patient had stage III disease. The sites of active disease before the initiation of cladribine was skin in seven patients, bone (all multifocal) in six patients, lung in four patients, soft tissue in two patients, and lymph nodes in two patients. Four patients had prior diabetes insipidus, two patients had loss of teeth from gingival involvement, and two patients had marked pulmonary fibrosis. Patients 1 and 2 have been previously reported,14,15 as have been the pretreatment characteristics of patient 12.20
Responses and Response Duration Of the 13 patients treated, 12 were evaluable for response and all for toxicity. Patient 11, inevaluable for response, received only a single course of therapy and was not seen in follow-up. After a median of three courses of cladribine (range, 1 to 6), seven (58%) patients achieved complete responses (two pathologic and five clinical) and two (17%) patients partial responses, for an overall response rate of 75% (95% confidence interval, 43% to 95%). Three (25%) patients had stable disease and were scored as nonresponders. The median response follow-up duration was 33 months (range, 1 to 65+ months); the median follow-up response duration for complete responders was 33+ months (range, 1 to 65+ months), and the response follow-up duration for the partial responders was 36+ and 8+ months.
Toxicities, Late Events, and Survival
This phase II study has demonstrated that single-agent cladribine has major activity in the treatment of adults with LCH, and this was achieved with a favorable toxicity profile. Responses were documented in patients with cutaneous, oral, osseous, soft tissue, lymph node, and pulmonary sites of involvement. The majority of responses were complete, generally durable, and unmaintained. These results confirm and extend the observations made previously in three adults with LCH treated with cladribine.14,15
Submitted December 14, 1998; accepted February 16, 1999.
Supported in part by Ortho Biotech, Raritan, NJ (manufacturer of cladribine) and the Histiocytosis Association of America, Pitman, NJ.
The publication costs of this article were defrayed in part by page charge payment. This article must therefore be hereby marked "advertisement" in accordance with 18 U.S.C. section 1734 solely to indicate this fact.
Address reprint requests to Alan Saven, MD, Head, Division of Hematology/Oncology, MS217, Scripps Clinic, 10666 North Torrey Pines Rd, La Jolla, CA 92037; e-mail: asaven{at}scrippsclinic.com.
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| Copyright © 1999 by American Society of Hematology Online ISSN: 1528-0020 | |||||||||
TOP
ABSTRACT
INTRODUCTION
a clonal proliferative disease.
N Engl J Med
331:154, 1994