Lenalidomide long-term neurotoxicity
Clinical and neurophysiologic prospective study
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Abstract
Objective: To evaluate long-term lenalidomide neurotoxicity and correlation with cumulative dose and hematologic response.
Methods: Nineteen myeloma patients (7 men, mean age 63.2 years) underwent clinical and neurophysiologic assessment at baseline and at 2 (8 patients, group A) or 5 years (11 patients, group B) after starting lenalidomide therapy for relapsed/refractory multiple myeloma. Neuropathy was scored with Total Neuropathy Score clinical version (TNSc). Lenalidomide cumulative dose was correlated with severity of neuropathy and hematologic response.
Results: At enrollment, 7/19 patients (3 in group A, 4 in group B) had neurophysiologic signs of neuropathy secondary to previous chemotherapy, in 2 of them subclinical. Neurophysiologic evidence of sensory axonal neuropathy occurred in 4/8 patients at 2 years follow-up (group A) and in 3/11 patients at 5 years follow-up (group B). Dorsal sural nerve sensory action potential amplitude was the earliest neurophysiologic abnormality. No relevant (≥4) clinical changes were found in TNSc score. Hematologic overall response was 62% in group A and 100% in group B. No correlation was found between lenalidomide cumulative dose and neuropathy or between neuropathy and hematologic response.
Conclusions: In our study, up to 50% of myeloma patients on long-term lenalidomide therapy developed sensory axonal neuropathy. Reduced dorsal sural nerve sensory action potential amplitude was the first neurophysiologic alteration. Neuropathy was usually subclinical or mild, however. Neurotoxicity was independent of lenalidomide cumulative dose and hematologic response.
GLOSSARY
- CIPN=
- chemotherapy-induced peripheral neuropathy;
- CR=
- complete response;
- PR=
- partial response;
- QLQ-C30=
- Core Quality of Life Questionnaire;
- SD=
- stable disease;
- SNAP=
- sensory nerve action potential;
- TNSc=
- Total Neuropathy Score clinical version;
- VGPR=
- very good partial response
Footnotes
Go to Neurology.org for full disclosures. Funding information and disclosures deemed relevant by the authors, if any, are provided at the end of the article.
- Received January 11, 2016.
- Accepted in final form May 26, 2016.
- © 2016 American Academy of Neurology
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