Abstract

BackgroundSurgery of malignant tumors has long been suspected to be the reason for enhancement of growth of metastases with fatal outcome. This often prevented surgeons from touching the tumor if not absolutely necessary. We have shown in lung cancer patients that surgery, itself, leads to mobilization of tumor cells into peripheral blood. Some of the mobilized cells finding an appropriate niche might grow to form early metastases. Monitoring of tumor cell release during and the fate of such cells after surgery for breast cancer may help to reveal how metastases develop after surgery.MethodWe used the MAINTRAC® analysis, a new tool for online observation of circulating epithelial cells, to monitor the number of epithelial cells before, 30 min, 60 min, three and seven days after surgery and during subsequent variable follow up in breast cancer patients.ResultsCirculating epithelial cells were already present before surgery in all patients. During the first 30–60 min after surgery values did not change immediately. They started increasing during the following 3 to 4 days up to thousand fold in 85% of treated patients in spite of complete resection of the tumor with tumor free margins in all patients. There was a subsequent re-decrease, with cell numbers remaining above pre-surgery values in 58% of cases until onset of chemotherapy. In a few cases, where no further therapy or only hormone treatment was given due to low risk stage, cell numbers were monitored for up to three years. They remained elevated with no or a slow decrease over time. This was in contrast to the observation in a patient where surgery was performed for benign condition. She was monitored before surgery with no cells detectable. Epithelial cells increased up to more than 50 000 after surgery but followed by a complete reduction to below the threshold of detection.ConclusionFrequently before but regularly during surgery of breast cancer, epithelial cells are mobilized into circulation. Part of these cells, most probably normal or apoptotic cells, are cleared from the circulation as also shown to occur in benign conditions. After resection even if complete and of small tumors, cells can remain in the circulation over long times. Such cells may remain "dormant" but might settle and grow into metastases, if they find appropriate conditions, even after years.

Highlights

  • Surgery of malignant tumors has long been suspected to be the reason for enhancement of growth of metastases with fatal outcome

  • Circulating epithelial cells were already present before surgery in all patients

  • Frequently before but regularly during surgery of breast cancer, epithelial cells are mobilized into circulation

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Summary

Introduction

Surgery of malignant tumors has long been suspected to be the reason for enhancement of growth of metastases with fatal outcome. It is assumed that this phenomenon may be due to release of preexistent tumor cells or of micrometastatic single cells and avascular foci present in the patients before diagnosis from dormancy The detection of such "dormant" cells in bone marrow seems to have impact on prognosis and relapse free survival [7]. We have analyzed how surgery effects the level of circulating epithelial cells in different patients using our approach for real-time monitoring of changes in the number of circulating tumor cells [9,10] These analyses may contribute to our understanding of how surgery influences the course of disease in breast cancer

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