Is there a role for platinum chemotherapy in the treatment of patients with hormone‐refractory prostate cancer?

Oh, William K.; Tay, Miah Hiang; Huang, Jiaoti

doi:10.1002/cncr.22439

Cited by 62 publications

(40 citation statements)

References 93 publications

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“…Until recently, HRPC has been widely considered resistant to chemotherapy, including cisplatin and carboplatin (46), although these studies were limited by traditional measures of radiographic response for treatment assessment (47). Two recent landmark trials, however, showed that docetaxel-based chemotherapy afforded statistically significant improvements in overall survival, prostate-specific antigen (PSA) response, pain relief, and quality of life, setting a new standard of care for HRPC patients (48,49).…”

Section: Clinical Trialsmentioning

confidence: 99%

Current Status and Future Prospects for Satraplatin, an Oral Platinum Analogue

Choy

Park

Yao

2008

Clinical Cancer Research

201

156

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Platinum drugs are major chemotherapeutic agents that are used alone or in combination with other systemic agents and/or radiation therapy in the management of many human malignancies. All three platinum drugs approved by the Food and Drug Administration, cisplatin, carboplatin, and oxaliplatin, are administrated intravenously. Satraplatin is the first orally administered platinum drug under active clinical investigation. Satraplatin and its major metabolite, JM118, have shown antineoplastic activity in in vitro, in vivo, and in clinical settings. Use of satraplatin as an alternative platinum cytotoxic agent is particularly attractive because of the convenience of administration, milder toxicity profile, lack of cross-resistance with cisplatin, theoretical advantage as a radiosensitizer, and activity in cancers historically nonresponsive to platinum drugs. The most mature clinical data for satraplatin come from the recently completed phase III trial that investigated the efficacy of satraplatin and prednisone on hormone-refractory prostate cancer patients who had failed a course of other chemotherapy agents. Preliminary reports show that the combination is statistically superior to placebo and prednisone in multiple end points, including progressionfree survival, prostate-specific antigen response, objective tumor response, pain response, and duration of pain response. The difference in overall survival, however, did not reach statistical significance.

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Section: Clinical Trialsmentioning

confidence: 99%

Current Status and Future Prospects for Satraplatin, an Oral Platinum Analogue

Choy

Park

Yao

2008

Clinical Cancer Research

201

156

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“…Use of capecitabine instead of infusional 5-fluorouracil (ECX) has been at least as effective as ECF in esophagogastric cancer. 15 Oh and colleagues 16 reviewed the use of platinum-based chemotherapy in CRPC and identified objective response rates ranging from 45% to 65% with combinations of estramustine, carboplatin, and either paclitaxel or docetaxel in 6 phase II trials. In a subsequent report studying docetaxel plus carboplatin, the objective response rate was 25% in chemonaive patients who also received with estramustine, and 8% in patients progressing despite docetaxel.…”

Section: Discussionmentioning

confidence: 99%

ECF chemotherapy for liver metastases due to castration-resistant prostate cancer

Gupta¹,

Potvin²,

Ernst³

et al. 2014

CUAJ

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Introduction: Most men with metastatic castration-resistant prostate cancer (CRPC) have biochemical response to docetaxel, but the objective response rate is low. Liver metastases are uncommon with CRPC and associated with shorter survival. More active treatment might benefit these patients. Epirubicin, cisplatin and flurouracil (ECF) is a standard regimen for gastric cancer and response in CRPC liver metastases has been reported. We reviewed our experience with ECF in CRPC with the primary objective of determining its anti-tumour activity in patients with liver metastatic CRPC. Methods: Men with CRPC treated with ECF were identified from electronic databases and data were extracted from medical records. Men with tumours showing neuroendocrine features were excluded. Results: In total, we identified 14 CRPC patients treated with ECF were identified, of which 8 had liver metastases. The median age was 56 (range: 42-76) and all had multiple poor prognostic features. A median of 6 cycles of ECF were administered (range: 1-10) and toxicities were similar to previous reports. Of the 8 patients with liver metastases, 5 had partial remission. Conclusions: ECF was highly active in this small selected group of younger men with liver metastases from CRPC and multiple poor prognostic features. Despite important limitations, this is the third report of high objective response rates with ECF in CRPC. Objective response rates are low with current monotherapies. A higher probability of ORR is preferred for critical organ disease, therefore the anti-tumour activity should encourage testing of ECF in comparison to the most active current therapies.

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“…A phase III trial of satraplatin, an oral platinum that inhibits replication through the formation of DNA adducts, has demonstrated activity as a second line chemotherapy for patients with androgen-independent disease (77). The increased understanding of the relationship between DNA and chromatin structural proteins has led to the development of histone deacetylase inhibitors such as suberoylanilide hydroxamic acid (vorinostat), which interferes with chromatin unfolding and subsequent gene activation (78).…”

Section: Figurementioning

confidence: 99%

The evolving biology and treatment of prostate cancer

Taichman¹,

Loberg²,

Mehra³

et al. 2007

J. Clin. Invest.

119

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Since the effectiveness of androgen deprivation for treatment of advanced prostate cancer was first demonstrated, prevention strategies and medical therapies for prostate cancer have been based on understanding the biologic underpinnings of the disease. Prostate cancer treatment is one of the best examples of a systematic therapeutic approach to target not only the cancer cells themselves, but the microenvironment in which they are proliferating. As the population ages and prostate cancer prevalence increases, challenges remain in the diagnosis of clinically relevant prostate cancer as well as the management of the metastatic and androgen-independent metastatic disease states.

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Is there a role for platinum chemotherapy in the treatment of patients with hormone‐refractory prostate cancer?

Cited by 62 publications

References 93 publications

Current Status and Future Prospects for Satraplatin, an Oral Platinum Analogue

Current Status and Future Prospects for Satraplatin, an Oral Platinum Analogue

ECF chemotherapy for liver metastases due to castration-resistant prostate cancer

The evolving biology and treatment of prostate cancer

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