IRINOTECAN AND CYTARABINE IN ACUTE MYELOID LEUKEMIA
Project Number5R21CA089938-02
Contact PI/Project LeaderBAER, MARIA R
Awardee OrganizationROSWELL PARK CANCER INSTITUTE CORP
Description
Abstract Text
Treatment outcome has improved in acute myeloid leukemia (AML),
AML. To improve treatment outcomes in AML, there is a compelling need to
develop treatments which attack novel cellular targets and which are not
affected by known mechanisms of resistance. Irinotecan (CPT-11) is a
topoisomerase I-interactive drug which, as a single agent, has shown limited
activity against 5-florouracil (5-FU)-refractory colorectal cancer, but, in
combination with 5-FU, is very effective against the disease both in
preclinical models and in clinical trials. The efficacy of this combination is
highly schedule-dependent. We have found that CPT-11 is highly active against
multidrug-resistant human leukemia xenografts in vivo. Moreover, preclinical
data from our laboratory demonstrate that the schedule-dependent synergistic
drug interaction which has been found for CPT-11 and 5-FU also applies to
CPT-11 in combination with Ara-C. Based on these preclinical findings, a Phase
I clinical protocol was designed and initiated combining CPT-11 with Ara-C in
the treatment of refractory AML and chronic myelogenous leukemia in myeloid
blast transformation (CML-MBT). The objective of this application is to develop
CPT-11 and Ara-C combination chemotherapy as a treatment for myeloid leukemias
resistant to current therapies; this approach would then subsequently be
applied to untreated AML with a low likelihood of response to current regimens.
The specific aims presented are: 1. To define the efficacy of CPT-11 and Ara-C
combination chemotherapy in refractory AML and in CML-MBT; 2. To optimize the
schedule of CPT-11 and Ara-C combination chemotherapy based on laboratory
correlates of efficacy; and 3. To identify correlates of sensitivity and
resistance to CPT-11 and Ara-C combination chemotherapy.
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