Results from a randomized trial of salvage chemotherapy followed by lestaurtinib for patients with FLT3 mutant AML in first relapse

Mark J. Levis(Johns Hopkins University), Farhad Ravandi(The University of Texas MD Anderson Cancer Center), Eunice S. Wang(Roswell Park Comprehensive Cancer Center), Maria R. Baer(University of Maryland, Baltimore), Alexander E. Perl(University of Pennsylvania), Steven Coutré(Stanford University), Harry P. Erba(University of Michigan), Robert K. Stuart(Medical University of South Carolina), Michele Baccarani(Istituto Oncologico Romagnolo), Larry D. Cripe(Indiana University Health), Martin S. Tallman(Northwestern University), Giovanna Meloni(Sapienza University of Rome), Lucy A. Godley(University of Chicago Medical Center), Amelia Langston(Emory University), Sergio Amadori(University of Rome Tor Vergata), Ian D. Lewis(South Australia Pathology), Arnon Nagler(Sheba Medical Center), Richard M. Stone(Dana-Farber Cancer Institute), Karen Yee(Princess Margaret Hospital), Anjali S. Advani(Cleveland Clinic), Dan Douer(University of Southern California), W Wiktor-Jędrzejczak(Medical University of Warsaw), Gunnar Juliusson(Lund University), Mark R. Litzow(Mayo Clinic in Arizona), Stephen H. Petersdorf(Seattle Cancer Care Alliance), Miguel Á. Sanz(Hospital Universitari i Politècnic La Fe), Hagop M. Kantarjian(The University of Texas MD Anderson Cancer Center), Takashi Sato(Johns Hopkins University), Lothar Tremmel, Debra M. Bensen-Kennedy, Donald Small(Johns Hopkins University), B. Douglas Smith(Johns Hopkins University)
Blood
January 27, 2011
10.1182/blood-2010-08-301796
Cited by 399Open Access
Full Text

Abstract

In a randomized trial of therapy for FMS-like tyrosine kinase-3 (FLT3) mutant acute myeloid leukemia in first relapse, 224 patients received chemotherapy alone or followed by 80 mg of the FLT3 inhibitor lestaurtinib twice daily. Endpoints included complete remission or complete remission with incomplete platelet recovery (CR/CRp), overall survival, safety, and tolerability. Correlative studies included pharmacokinetics and analysis of in vivo FLT3 inhibition. There were 29 patients with CR/CRp in the lestaurtinib arm and 23 in the control arm (26% vs 21%; P = .35), and no difference in overall survival between the 2 arms. There was evidence of toxicity in the lestaurtinib-treated patients, particularly those with plasma levels in excess of 20 μM. In the lestaurtinib arm, FLT3 inhibition was highly correlated with remission rate, but target inhibition on day 15 was achieved in only 58% of patients receiving lestaurtinib. Given that such a small proportion of patients on this trial achieved sustained FLT3 inhibition in vivo, any conclusions regarding the efficacy of combining FLT3 inhibition with chemotherapy are limited. Overall, lestaurtinib treatment after chemotherapy did not increase response rates or prolong survival of patients with FLT3 mutant acute myeloid leukemia in first relapse. This study is registered at www.clinicaltrials.gov as #NCT00079482.

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