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Chemotherapy for Resectable and Advanced Pancreatic Cancer

Chemotherapy for Resectable and Advanced Pancreatic Cancer


Although a relatively uncommon disease, pancreatic adenocarcinoma has had a major impact on public health (much greater than incidence rates would suggest) because of associated high morbidity and mortality rates.[1] Drs. Berlin and Rothenberg have written a comprehensive synopsis of the state of conventional cytotoxic chemotherapy and radiation therapy for surgically resected and advanced pancreatic cancer. They provide the historical precedents for the treatment algorithms that have traditionally governed clinical management of the disease. We will highlight several points from their article, including (1) combination chemotherapy in advanced disease, (2) treatment controversies surrounding locally advanced disease, and (3) limitations of available data with regard to adjuvant therapy.

The Hope of Future Strategies

Berlin and Rothenberg discuss emerging strategies such as the use of gemcitabine (Gemzar)-based combinations and protracted-dose infusion gemcitabine. The latter is an example of a rationally designed tactic aimed at increasing the therapeutic index of gemcitabine by promoting higher levels of intracellular triphosphate, the active metabolite of gemcitabine. It remains to be seen whether this approach will prove to be superior to single-agent gemcitabine and whether metered-dose infusion gemcitabine can be combined with other active agents, the limiting factor being hematologic toxicity.

The gemcitabine-based combinations of perhaps most interest include those with irinotecan (CPT-11, Camptosar),[2] docetaxel (Taxotere),[3] cisplatin (Platinol), and fluorouracil (5-FU).[4,5] Although, to date, multiple phase II trials have demonstrated improved response rates and median survivals compared to historical controls, no combination has proven to be superior to single-agent gemcitabine in a randomized comparison. Several ongoing trials in North America and Europe have been designed to help clarify the relative efficacy of these combinations. It is possible that among selected patient groups (including those with good performance status), combination therapy will prove to be superior to single-agent gemcitabine. In addition, as pointed out by the authors, the ultimate goal of improved therapies for metastatic disease is to move them forward into the adjuvant setting, where modest responses may lead to meaningful gains in survival.

With regard to locally advanced, unresectable, nonmetastatic disease, the authors discuss the issue of how best to treat this patient population. In short, we currently do not know what the optimal strategy should be. Clinical trials in inoperable pancreatic cancer have increasingly incorporated both locally advanced patients and patients with overt metastatic disease in the same study, while stratifying for disease stage. The omission of irradiation in locally advanced patients is controversial, but the true effect of radiation therapy, in the absence of a significant pain syndrome, is currently unknown.

For patients with borderline resectable/unresectable disease, the combination of chemotherapy and radiation remains experimental, ie, an effort to facilitate surgical resection. The number of patients whose disease is truly unresectable but becomes resectable by virtue of chemoradiation is considered to be anecdotal, the interpretation depending on how resectability is defined.

A Potent Radiosensitizer


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