The morbidity and lethality of AL amyloidosis is caused by the deposition of lg light chains as fibrillar amyloid protein in vital organs, disrupting their function, and not by the generally low burden of clonal plasma cells that produce the paraproteins. Survival of patients with AL amyloidosis is no more than 1 to 2 years from the time of diagnosis with current management approaches. Clearly, more effective therapies are needed for this rapidly lethal disease. Five patients were treated with dose-intensive melphalan and blood stem cell support and followed for a period of 1 year. Patients were diagnosed with AL amyloidosis by tissue biopsy and categorized by performance status and organ involvement. Their plasma cell dyscrasias were evaluated with immunofixation electrophoresis of serum and urine specimens, quantitative serum lgs, and immunohistochemical staining of bone marrow biopsy specimens. After treatment with dose-intensive intravenous melphalan followed by infusion of autologous growth-factor-mobilized blood stem cells, clinical evaluations and plasma cell studies were repeated at 3 and 12 months. Three men and 2 women aged 38 to 53 years were treated. Median performance status (SWOG) was 2 (1 to 3), and clinical presentations included nephrotic syndrome (n = 1), symptomatic cardiomyopathy (n = 1), gastrointestinal involvement with polyneuropathy (n = 2), and hepatomegaly (n = 1). With a median follow-up of 13 months (12 to 17 months), all five patients are well and have shown stable or improved performance status and clinical remission of organ-related dysfunction, including a 50% reduction in daily proteinuria with no change in creatinine, reversal of symptoms of cardiomyopathy and reductions of posterior wall and septal thickening, reversal of polyneuropathy and gastric atony, and resolution of hepatomegaly by computed tomographic scan. In 3 of the 5 patients (60%) at 12 months after treatment, plasma cell dyscrasias could not be detected. Dose-intensive chemotherapy with intravenous melphalan and growth-factor-mobilized blood stem cell support is feasible therapy for patients with AL amyloidosis, even when there is clinical evidence of cardiac involvement. At least some patients with AL amyloidosis achieve complete remission of their plasma cell dyscrasia, improvement in performance status, and clinical remission of organ-specific disease after this form of treatment.
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October 1, 1996
Dose-intensive melphalan with blood stem cell support for the treatment of AL amyloidosis: one-year follow-up in five patients
RL Comenzo,
RL Comenzo
Department of Pathology and Laboratory Medicine, Boston City Hospital, MA, USA.
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E Vosburgh,
E Vosburgh
Department of Pathology and Laboratory Medicine, Boston City Hospital, MA, USA.
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RW Simms,
RW Simms
Department of Pathology and Laboratory Medicine, Boston City Hospital, MA, USA.
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P Bergethon,
P Bergethon
Department of Pathology and Laboratory Medicine, Boston City Hospital, MA, USA.
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D Sarnacki,
D Sarnacki
Department of Pathology and Laboratory Medicine, Boston City Hospital, MA, USA.
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K Finn,
K Finn
Department of Pathology and Laboratory Medicine, Boston City Hospital, MA, USA.
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S Dubrey,
S Dubrey
Department of Pathology and Laboratory Medicine, Boston City Hospital, MA, USA.
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DV Faller,
DV Faller
Department of Pathology and Laboratory Medicine, Boston City Hospital, MA, USA.
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DG Wright,
DG Wright
Department of Pathology and Laboratory Medicine, Boston City Hospital, MA, USA.
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RH Falk,
RH Falk
Department of Pathology and Laboratory Medicine, Boston City Hospital, MA, USA.
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M Skinner
M Skinner
Department of Pathology and Laboratory Medicine, Boston City Hospital, MA, USA.
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Blood (1996) 88 (7): 2801–2806.
Citation
RL Comenzo, E Vosburgh, RW Simms, P Bergethon, D Sarnacki, K Finn, S Dubrey, DV Faller, DG Wright, RH Falk, M Skinner; Dose-intensive melphalan with blood stem cell support for the treatment of AL amyloidosis: one-year follow-up in five patients. Blood 1996; 88 (7): 2801–2806. doi: https://doi.org/10.1182/blood.V88.7.2801.bloodjournal8872801
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October 1 1996
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