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Anticancer chemosensitivity profile of freshly separated human pancreatic cancer cells assessed by DNA synthesis inhibition assay
Author(s) -
Masai Yoshikazu,
Nio Yoshinori,
Tsubono Michihiko,
Tseng ChenChiu,
Kawabata Kazuya,
Hayashi Hitoshi,
Ishigami Shunichi,
Imamura Masayuki
Publication year - 1994
Publication title -
journal of surgical oncology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.201
H-Index - 111
eISSN - 1096-9098
pISSN - 0022-4790
DOI - 10.1002/jso.2930570206
Subject(s) - medicine , etoposide , pancreatic cancer , cisplatin , epirubicin , chemosensitivity assay , gemcitabine , cancer research , metastasis , cancer , lymph node , pathology , mitomycin c , lymph , oncology , chemotherapy , breast cancer , surgery
The chemosensitivity of 49 freshly separated human pancreatic cancers to seven kinds of anticancer agents were assessed by a DNA synthesis ( 3 H‐thymidine incorporation) inhibition assay. DNA synthesis is higher in involved lymph nodes (n=7), malignant effusion (n=15), liver metastasis (n=7), primary cancer (n=15), and skin metastasis (n=5). Chemosensitivity assay demonstrates that etoposide, 4‐epirubicin, carboquone, and 5‐fluorouracil are more effective than cisplatin, mitomycin‐C, and Adriamycin. In general, metastatic lesions of pancreatic cancer tend to show higher chemosensitivity than primary lesions. Pathological analysis demonstrates that small primary pancreatic cancers tend to be more responsive than large primary cancers, and primary pancreatic cancers with no regional lymph node involvement also tend to be more responsive than those with nodal involvement. No significant differences are seen in terms of tumor spread, vascular involvement, sex of patient, and histological type. When chemosensitivity assay is not available, the results of the present study may be beneficial to choose the regimens. © 1994 Wiley‐Liss, Inc.