BACKGROUND: To assess the activity of docetaxel in combination with hormonal therapy in preclinical models of prostate cancer. MATERIALS AND METHODS: Since prostate cancer has a predilection for the bone, we assessed the antitumor activity of docetaxel in in vivo models of both bone metastasis and localized prostate cancer, using MDA PCa 2b and PC3 cells in SCID mice. RESULTS: Dramatic antitumor efficacy was observed regardless of whether the tumor cells were implanted in the prostate or in the bone. Antitumor activity was also evident in both osteolytic and osteoblastic lesions. Reasoning that docetaxel efficacy might be enhanced if it were to be used earlier in the course of the disease, we studied the sequence of docetaxel and androgen ablation (part of standard treatment for early-stage prostate cancer) in the MDA PCa 2b xenograft model. The activity was similar whether docetaxel and androgen ablation were used alone, simultaneously, or in sequence, indicating a lack of synergism or antagonism. Finally, we studied the combination of docetaxel and estramustine on androgen-sensitive and androgen-independent cell lines in vitro and in vivo. Estramustine did not increase the activity of docetaxel in these models. CONCLUSION: These results provide a strong preclinical rationale for the clinical development of docetaxel for the treatment of both locally advanced and disseminated prostate cancer.
BACKGROUND: To assess the activity of docetaxel in combination with hormonal therapy in preclinical models of prostate cancer. MATERIALS AND METHODS: Since prostate cancer has a predilection for the bone, we assessed the antitumor activity of docetaxel in in vivo models of both bone metastasis and localized prostate cancer, using MDA PCa 2b and PC3 cells in SCIDmice. RESULTS: Dramatic antitumor efficacy was observed regardless of whether the tumor cells were implanted in the prostate or in the bone. Antitumor activity was also evident in both osteolytic and osteoblastic lesions. Reasoning that docetaxel efficacy might be enhanced if it were to be used earlier in the course of the disease, we studied the sequence of docetaxel and androgen ablation (part of standard treatment for early-stage prostate cancer) in the MDA PCa 2b xenograft model. The activity was similar whether docetaxel and androgen ablation were used alone, simultaneously, or in sequence, indicating a lack of synergism or antagonism. Finally, we studied the combination of docetaxel and estramustine on androgen-sensitive and androgen-independent cell lines in vitro and in vivo. Estramustine did not increase the activity of docetaxel in these models. CONCLUSION: These results provide a strong preclinical rationale for the clinical development of docetaxel for the treatment of both locally advanced and disseminated prostate cancer.
Authors: Zeyu Xiao; Etgar Levy-Nissenbaum; Frank Alexis; Andrej Lupták; Benjamin A Teply; Juliana M Chan; Jinjun Shi; Elise Digga; Judy Cheng; Robert Langer; Omid C Farokhzad Journal: ACS Nano Date: 2012-01-03 Impact factor: 15.881
Authors: Piwen Wang; Susanne M Henning; Clara E Magyar; Yahya Elshimali; David Heber; Jaydutt V Vadgama Journal: J Exp Clin Cancer Res Date: 2016-05-06
Authors: Laia Civit; Ioanna Theodorou; Franziska Frey; Holger Weber; Andreas Lingnau; Carsten Gröber; Michael Blank; Chloé Dambrune; James Stunden; Marc Beyer; Joachim Schultze; Eicke Latz; Frédéric Ducongé; Michael H G Kubbutat; Günter Mayer Journal: Sci Rep Date: 2019-03-21 Impact factor: 4.379