Journal of Clinical Oncology, Vol 10, 406-413, Copyright © 1992 by American Society of Clinical Oncology
Gemcitabine in leukemia: a phase I clinical, plasma, and cellular pharmacology study
R Grunewald, H Kantarjian, M Du, K Faucher, P Tarassoff and W Plunkett
Department of Medical Oncology and Hematology, University of Texas MD Anderson Cancer Center, Houston 77030.
PURPOSE: Phase I clinical and in vitro studies of gemcitabine (2',2'-
difluorodeoxycytidine; dFdC) have demonstrated that the accumulation rate
of dFdC 5'-triphosphate (dFdCTP) in mononuclear and leukemia cells is
saturated when plasma or extracellular dFdC levels exceed 15 to 20 mumol/L.
Thus, we designed a phase I study to maximize the accumulation of dFdCTP by
leukemia cells by administering dFdC at 10 mg/m2/min, a dose rate
calculated to produce steady-state plasma dFdC levels that exceed 15 to 20
mumol/L. PATIENTS AND METHODS: The treatment intensity was increased in
patients (n = 22) with relapsed or refractory acute leukemia or chronic
myelogenous leukemia (CML) in blast crisis by prolonging the infusion
duration but maintaining the same rate. Doses of dFdC between 1,200 mg/m2
and 6,400 mg/m2 were administered weekly for 3 weeks. RESULTS: The
maximum-tolerated dose was 4,800 mg/m2 infused over 480 minutes. The mean
steady-state dFdC level in plasma of all infusions was 26.5 +/- 9 mumol/L
(n = 19). The accumulation rates of dFdCTP in circulating leukemia cells
varied greatly among patients but remained linear in eight patients infused
for 120 to 240 minutes, and up to or beyond 360 minutes in five of eight
additional patients. Elimination of dFdCTP was significantly related to its
cellular concentration: blasts with greater than 450 mumol/L dFdCTP
exhibited biphasic elimination, whereas blasts with lower dFdCTP
concentrations exhibited linear kinetics. Biphasic elimination was
associated with higher dFdCTP areas under the concentration-times-time
curve (AUCs) and greater inhibition of DNA synthesis. CONCLUSION: Studies
of the cellular pharmacology and pharmacodynamics of dFdC may be useful in
optimizing protocol designs for leukemia.
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