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Salvage Chemotherapy with Cisplatin,Ifosfamide, and Paclitaxel in Aggressive Variant of Metastatic Castration-Resistant Prostate Cancer
Authors:Gunhild von Amsberg,Mirjam Zilles,Wael Mansour,Philipp Gild,Winfried Alsdorf,Moritz Kaune,Lukas Bö  ckelmann,Jessica Hauschild,Christoph Krisp,Tina Rohlfing,Ceren Saygi,Malik Alawi,Alexandra Zielinski,Claudia Langebrake,Su Jung Oh-Hohenhorst,Sven Perner,Derya Tilki,Hartmut Schlü  ter,Markus Graefen,Sergey A. Dyshlovoy,Carsten Bokemeyer
Abstract:Significant progress has been achieved in the treatment of metastatic castration-resistant prostate cancer (mCRPC). However, results in patients with aggressive variant prostate cancer (AVPC) have been disappointing. Here, we report retrospectively collected data from intensively pretreated AVPC patients (n = 17; 88.2% visceral metastases; 82% elevation of neuroendocrine markers) treated with salvage chemotherapy consisting of cisplatin, ifosfamide, and paclitaxel (TIP). At the interim analysis, 60% of patients showed radiographic response or stable disease (PFS = 2.5 months; OS = 6 months). In men who responded to chemotherapy, an OS > 15 months was observed. Preclinical analyses confirmed the high activity of the TIP regimen, especially in docetaxel-resistant prostate cancer cells. This effect was primarily mediated by increased cisplatin sensitivity in the emergence of taxane resistance. Proteomic and functional analyses identified a lower DNA repair capacity and cell cycle machinery deficiency to be causative. In contrast, paclitaxel showed inconsistent effects, partially antagonizing cisplatin and ifosfamide in some AVPC models. Consequently, paclitaxel has been excluded from the TIP combination for future patients. In summary, we report for the first time the promising efficacy of TIP as salvage therapy in AVPC. Our preclinical data indicate a pivotal role for cisplatin in overcoming docetaxel resistance.
Keywords:cisplatin   ifosfamide   paclitaxel   TIP combinational therapy   aggressive variant of prostate cancer   metastatic castration-resistant prostate cancer   DNA damage   DDR alteration
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