AI Article Synopsis

  • Progressive ovarian cancer triggers the production of type I and type III procollagens in both the tumor tissue and surrounding peritoneal cavity.
  • Our research involved analyzing these proteins' different forms through gel filtration and immunological tests using fluid samples from patients with both benign and malignant ovarian tumors.
  • Findings show that while procollagen processing is effective in tumor tissue, leading to more free propeptides in benign cases, malignant tumors exhibit incomplete processing in peritoneal ascitic fluid, revealing a significant difference in the structure of type I procollagen between benign and malignant cases.

Article Abstract

Progressive ovarian carcinoma induces the synthesis of type I and type III procollagens both in the tumour tissue and in the peritoneal cavity. We studied the processing of these proteins by determining the different antigen forms related to their propeptide parts by gel filtration and subsequent immunological assays. Samples of ovarian cyst fluid and peritoneal ascitic fluid were obtained from patients with benign and malignant ovarian tumours. In both benign and malignant ovarian cysts, the predominant procollagen antigens were the free propeptides, with few or no larger components, indicating efficient processing of types I and III procollagens in the tumour tissue. In ascitic fluid the processing was more variable. The aminoterminus of type III procollagen was partially unprocessed in all samples studied, whereas that of type I procollagen was nearly always completely processed. There was a clear difference between malignant and benign tumours in the processing of the carboxyterminus of type I procollagen: a significant part of the carboxyterminal propeptide antigen was invariably associated with a collagenous domain in malignant tumours, whereas in benign tumours the free propeptide predominanted. The results indicate that interstitial procollagens are effectively processed in the tumour tissue during the fibroproliferative reaction typical of malignant ovarian tumours, whereas the processing of the procollagens released into peritoneal ascitic fluid is incomplete.

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http://dx.doi.org/10.1016/0009-8981(94)90231-3DOI Listing

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