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329 Tosedostat Plus Low Dose Cytarabine Induces a High Rate of Responses That Can be Predicted By Genetic Profiling in Elderly AML

Acute Myeloid Leukemia: Novel Therapy, excluding Transplantation
Program: Oral and Poster Abstracts
Type: Oral
Session: 616. Acute Myeloid Leukemia: Novel Therapy, excluding Transplantation: New Drugs
Sunday, December 6, 2015: 5:30 PM
W109, Level 1 (Orange County Convention Center)

Giuseppe Visani, M.D.1*, Federica Loscocco, PhD1*, Fabio Fuligni2*, Eliana Zuffa, M.D.3*, Alberto Sensi, M.D.4*, Alfonso Zaccaria, M.D.3*, Gerardo Musuraca, M.D.5*, Barbara Giannini4*, Alessandro Lucchesi5*, Francesca Fabbri5*, Anna Maria Mianulli6*, Patrizia Tosi, MD6*, Michela Tonelli4*, Anna Candoni, MD7*, Renato Fanin8, Giovanni Sparaventi1*, Marco Gobbi, MD9*, Marino Clavio10*, Marco Rocchi11*, Pier Paolo Piccaluga, MD, PhD12 and Alessandro Isidori, MD, PhD1

1Hematology and Stem Cell Transplant Center, AORMN Hospital, Pesaro, Italy
2The Hospital for Sick Children, Paediatric Laboratory Medicine (PLM), Toronto, ON, Canada
3Hematology, Ravenna Hospital, Ravenna, Italy
4Genetica Medica, Centro Servizi Laboratorio Unico AVR, Pievesistina di Cesena, Italy
5Onco-hematology, IRST, Meldola, Italy
6Hematology, Infermi Hospital, Rimini, Italy
7Hematology, Santa Maria della Misericordia University Hospital, Udine, Italy
8Division of Hematology and BMT, Department of Experimental and Clinical Medical Sciences, Azienda Ospedaliero-Universitaria di Udine, Udine, Italy
9Chair of Hematology, Department of Internal Medicine (DiMI), IRCCS AOU San Martino-IST, University of Genoa, Genoa, Italy
10Hematology, S. Martino University Hospital, Genova, Italy
11Institute of Biomathematics, Urbino University, Urbino, Italy
12Department of Experimental, Diagnostic, and Specialty Medicine, Bologna University, Bologna, Italy

Background: Older (age ≥60 years) patients with acute myeloid leukemia (AML) have poor outcomes and intensive induction chemotherapy is frequently unsuitable. Thus, new safe and effective therapies are urgently needed. Tosedostat, a new, orally bioavailable inhibitor of members of the M1 and M17 classes of aminopeptidases, was proven to be effective in both de novo and relapsed AML. We hypothesize that the addition of tosedostat to cytarabine may improve the response rate and remission duration over what is expected with chemotherapy or tosedostat alone.

Methods: This was a phase II, prospective, multicenter study, designed according to Fleming’s method. Fixing the lowest acceptable rate as 10% and the successful rate as 25%, with a significance level alpha=0.05 and a power 1-beta =0.80, the sample size was estimated in 33 patients. Thirty-three patients (median age 75 years) received Tosedostat 120 milligrams orally once daily until disease progression, coupled with intermittent low-dose cytarabine given subcutaneously at 20 milligrams twice/day for 10 days. Courses of cytarabine were repeated every 4 weeks in the absence of disease progression or unacceptable toxicity, up to 8 cycles. Global gene expression profiling (GEP, Affymetrix Human Gene 2.0 Array) was performed on purified AML blasts of 29 patients from peripheral blood or bone marrow at diagnosis before treatment initiation. Unsupervised clustering was generated using a hierarchical algorithm based on the average-linkage method. Principal component analysis (PCA) and supervised gene expression analysis was performed by using GeneSpring GX 12.0 (Agilent, USA).

Results: The characteristic of enrolled patients are listed in table 1 Induction-period mortality was 12%, with 4 deaths occurring in aplasia. According to intent-to-treat, the CR rate was 48.5% (16/33 patients); 2 additional patients obtained a partial response, for an overall response rate of 54.6%. In addition, 4/33 patients remained in stable disease for a median time of 9 months (range: 4-14). Seven patients did not respond and died with progressive disease after having received a median of 2 cycles of cytarabine and 45 days of tosedostat. In responding patients, the median time to best response was 74 days (range 22-145). Responding patients (CR+PR) had a longer median overall survival than non-responders (P=0.018). Six out of 18 (33%) responding patients are still in CR after a median follow-up of 425.5 days (range 208-758);  5 additional patients are alive with stable disease. Twenty-two patients died [while in aplasia (4), in CR (1), due to resistant disease (9) or due to progressive disease (8) after a median CR duration of 192 days (87-535)]. 29 patients had GEP analysis, and a molecular signature associated with the clinical response (CR vs. no CR) was identified. By supervised analysis, 212 genes differentially expressed based on the clinical response (complete remission (CR) vs no CR) were identified (Mann-Whitney, p<0.05; fold change >2). The 212 genes differentially expressed were significantly associated with six relevant biological functions and pathways: β-catenin (βcat); TNFα signaling pathway via NFκB; ERB2; STK33/SKM (serine/threonine kinase 33 expression using the SKM cell line); inflammatory response; and epithelial-mesenchymal transition pathways. 

Conclusions: The tosedostat and low-dose cytarabine combo produced a CR rate superior to what expected (45.4% versus 25%), and thus met the primary endpoint of study. Further, potential biomarkers were identified by GEP. Specifically, the achievement of CR could be efficiently predicted by the gene expression patterns with an overall accuracy exceeding 90%. A validation analysis is currently being conducted on additional 14 patients in order to confirm the ability of GEP to identify potential responders to TST. The study was registered at European Union Drug Regulating Authorities Clinical Trials (EudraCT) n.2012-000334-19.

Acknowledgements: CTI is gratefully acknowledged for providing Tosedostat for the patients. The study was supported in part by AIL Pesaro Onlus.

Table 1.

Characteristic

N = 33

Median age, years (range)

75 (62-85)

Median WBC count, × 109/L (range)

3.05 (0.26–24.53)

Blasts,   %  (range)

60   (20-96)

Cytogenetic risk group*, n

Not evaluable

3 (9%)

Intermediate Karyotype

17 (52%)

Unfavourable Karyotype

13 (39%)

AML, n

De novo

16 (48%)

Secondary, n

17 (52%)

Disclosures: Fanin: Novartis Farma: Speakers Bureau .

*signifies non-member of ASH