Neurotoxic Side Effects in Children with Refractory or Relapsed T-cell Malignancies Treated with Nelarabine Based Therapy

Overview

Journal Br J Haematol

Specialty Hematology

Date 2017 Aug 4

PMID 28771662

Citations 14

Authors

Michaela Kuhlen

Kirsten Bleckmann

Anja Moricke

Martin Schrappe

Simon Vieth

Gabriele Escherich

Annika Bronsema

Annika Vonalt

Manon Queudeville

C Michel Zwaan

Martin Ebinger

Klaus-Michael Debatin

Thomas Klingebiel

Ewa Koscielniak

Claudia Rossig

Birgit Burkhardt

Reinhard Kolb

Cornelia Eckert

Arndt Borkhardt

Arend von Stackelberg

Christiane Chen-Santel

Affiliations

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Abstract

The prognosis in children with refractory or relapsed (r/r) T-cell acute lymphoblastic leukaemia (T-ALL) or lymphoblastic lymphoma (T-LBL) is poor. Nelarabine (Ara-G) has successfully been used as salvage therapy in these children, but has been associated with significant, even fatal, neurotoxicities. We retrospectively analysed 52 patients with r/r T-ALL/T-LBL aged ≤19 years who were treated with Ara-G alone (n = 25) or in combination with cyclophosphamide and etoposide (n = 27). The majority of patients (45/52) received 1-2 cycles of Ara-G. Seventeen patients (32·7%) had refractory disease, 28 (53·8%) were in first relapse and 7 (13·5%) were in second relapse. A response to Ara-G was achieved in 20 patients and 15 (28·8%) were in remission at last follow-up. Twelve patients (23·1%) had neurotoxic adverse effects (neuro-AE) of any grade, of whom 7 (13·5%) developed neurotoxicity ≥ grade III. The most frequent neuro-AEs were peripheral motor neuropathy (19·2%), peripheral sensory neuropathy (11·5%) and seizures (9·6%). Three patients died of central neuro-AE after 1-2 cycles of combination therapy. Patients with neurotoxicity were significantly older (median 15·17 years) than those without (10·34 years, P = 0·017). No differences were observed between mono- and combination therapy concerning outcome and neuro-AE. The incidence of neuro-AE was not associated with concurrent intrathecal therapy or prior central nervous system irradiation.

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