Role of DNA ploidy patterns in esophageal squamous cell carcinoma: An ultraviolet microspectrophotometric study

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Abstract

Background. Controversy still exists about the influence of DNA content on the prognosis for patients with esophageal squamous cell carcinoma. Methods. DNA ploidy was determined by microspectrophotometric (MSPM) analysis of paraffin embedded malignant tissue from 78 patients with squamous cell carcinoma of the esophagus. The DNA distribution pattern was classified as diploid, low grade aneuploid (LGA), and high grade aneuploid (HGA) pattern. The relationships among DNA distribution patterns, pathologic features, clinical findings, and prognoses were investigated. Twenty‐seven of 78 patients were also selected for analyses of the DNA ploidy pattern of lymph node metastases. Results. Of 78 cancers, 20 (26%) were diploid, 15 (19%) LGA, and 43 (55%) HGA. The advanced carcinomas had the higher distribution of HGA pattern (55%), whereas the diploid pattern was more frequent in early stage (70%) or superficial (65%) esophageal cancer. In patients with the HGA pattern, there was a significantly higher frequency of lymph mode metastases (79%) and marked lymphatic (74.4%) and vascular (69.8%) invasion compared with those exhibiting the LGA (33.3%) or diploid (25%) pattern. Five‐year survival rates for patients with diploid carcinoma (57%) was significantly better that for those with the HGA pattern (14%). The distribution of nuclear DNA content was much narrower in the metastatic lymph node than in the corresponding primary cases. Conclusions. The HGA of DNA pattern based on spectrophotometry closely correlated with the factors generally indicative of the aggressive behavior of malignat tumors. Therefore, the role of the DNA ploidy pattern as a prognostic factor was emphasized Cancer 1994; 74:578‐85. Copyright © 1994 American Cancer Society

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Minu, A. R., Endo, M., & Sunagawa, M. (1994). Role of DNA ploidy patterns in esophageal squamous cell carcinoma: An ultraviolet microspectrophotometric study. Cancer, 74(2), 578–585. https://doi.org/10.1002/1097-0142(19940715)74:2<578::AID-CNCR2820740208>3.0.CO;2-2

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