We concluded that measurements of gemcitabine metabolites in the

We concluded that measurements of gemcitabine metabolites in the specimens taken after 4 weeks of radiation therapy

would not provide accurate information on drug accumulation in tumor cells. Therefore, no additional biopsies were performed. In this study, the MTD of gemcitabine delivered twice weekly during the final two weeks of a hyperfractionated RT course was 20 mg/m2, representing 25% of the MTD of gemcitabine administered twice weekly in a larger number of cycles without radiotherapy [15] and [16]. This percentage seems higher than previously reported by our group for once-weekly gemcitabine concurrent with radiotherapy, where the MTD was less than 5% of the MTD of gemcitabine monotherapy [10]. However, this is not likely to represent a clinically meaningful improvement in the therapeutic ratio, as the tolerable gemcitabine doses are still too low. Stem Cell Compound Library supplier In our previous study, we observed undetectable or only trace levels of intracellular tumor phosphorylated gemcitabine following the administration of 10 mg/m2 (before radiotherapy), and low intracellular levels of the active drug

following the administration of 50 mg/m2[10]. In the present study, these measurements could not be repeated because at the time of gemcitabine administration, approximately 4 weeks after the onset of radiotherapy, there was only a small amount of tumor cells in the biopsy specimens. Nevertheless, our previous findings suggest BIBW2992 cost that the concentrations of the active drug in tumors would be very low after the administration of 20 mg/m2. Although twice-weekly administration likely results in an accumulation of the drug in tumor cells over time, Forskolin mw its impact would be restricted with only 5 doses administered over the last 2 weeks of radiotherapy. The clinical results of this study mirror the limited improvement in the therapeutic ratio. The locoregional tumor-control rate of 32% in the current

study is close to that observed in other studies of chemo/radiotherapy for nonresectable head and neck cancer [23] and [24] but lower than the rate of 60% observed in our previous phase I study of once weekly gemcitabine, which included patients with similarly advanced local/regional disease [8]. In that study, the cohorts receiving 50-300 mg/m2 gemcitabine demonstrated measurable tumor cell levels of phosphorylated gemcitabine [8]. It is noteworthy that in both our weekly and bi-weekly concurrent gemcitabine studies, the severe toxicities consisted primarily of mucositis and late dysphagia. This pattern was also reported by others utilizing once-weekly administration of low-dose gemcitabine concurrent with radiotherapy [10] and [11].

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