Increasing toxicity during neoadjuvant radiochemotherapy as positive prognostic factor for patients with esophageal carcinoma |
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Authors: | S. Hennies R. M. Hermann J. Gaedcke M. Grade C. F. Hess H. A. Wolff |
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Affiliation: | 1. Department of Radiotherapy, University Medicine Goettingen, , G?ttingen, Germany;2. Radiotherapy, ?rztehaus an der Ammerlandklinik, , Westerstede, Germany;3. Department of General Surgery, University Medicine Goettingen, , G?ttingen, Germany |
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Abstract: | The aim of this study was to correlate acute organ toxicity during preoperative radiochemotherapy with overall survival and tumor regression for patients with primarily operable esophageal carcinoma. From 1995 to 2002, 60 patients with primarily operable esophageal carcinoma were treated in a preoperative setting at our department. Thirty‐three percent of the patients had International Union against Cancer (UICC)‐stage II tumors, 62% had UICC‐stage III tumors, and 5% had UICC‐stage IVA tumors. All patients received irradiation (40 Gy at 2 Gy/fraction). Chemotherapy for all patients with adenocarcinoma and, from 2001, also for patients with squamous cell carcinoma consisted of two cycles, 5‐fluorouracil and cisplatinum; between 1995 and 2001, patients with squamous cell carcinoma received three courses of chemotherapy (folinic acid, etoposide, 5‐fluorouracil, and cisplatinum every 3 weeks) before and further cisplatinum and etoposide during radiotherapy. We found a significant correlation between acute organ toxicity and histopathological tumor regression, as well as overall survival. The probability to achieve tumor regression grade 1 after radiochemotherapy was nearly four times higher for patients with worsening of odynophagia than for those without an increase (odds ratio: 3.97). Patients with worsening of odynophagia had a 5‐year overall‐survival rate of 66% compared with 39% in patients without (P = 0.048). Our data indicate that normal tissue and tumor tissue may behave similar with respect to treatment response, as acute organ toxicity showed to be an independent prognostic marker in our patient population. The hypothesis should be further analyzed on biomolecular and clinical level in future clinical trials. |
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Keywords: | acute toxicity esophageal carcinoma overall survival preoperative radiochemotherapy tumor regression |
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