Clinicopathologic and immunohistochemical study of early colorectal cancer with liver metastases

被引:0
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作者
Keiichi Okano
Tadakazu Shimoda
Yasuhiro Matsumura
机构
[1] Department of Surgical Oncology,
[2] National Cancer Hospital,undefined
[3] Tokyo,undefined
[4] Japan,undefined
[5] Clinical Laboratory Division,undefined
[6] National Cencer Hospital,undefined
[7] 5-1-1 Tsukiji,undefined
[8] Chuo-ku,undefined
[9] Tokyo 104-0045,undefined
[10] Japan,undefined
[11] Department of Medical Oncology,undefined
[12] National Cancer Center Hospital,undefined
[13] Tokyo,undefined
[14] Japan,undefined
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Key words: early colorectal cancer; liver metastases; p53; CD44; mucin;
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摘要
Seven (3.3%) of 213 patients who underwent surgery for early colorectal cancer (invasion limited to no deeper than the submucosa) at the National Cancer Center Hospital, Tokyo, between 1986 and 1995 had synchronous (2 patients) or metachronous (5 patients) liver metastases. The average period from surgical resection of the primary colorectal cancer to the diagnosis of liver metastases was 25 months (range, 0–52 months). The clinicopathologic and immunohistochemical features of the primary lesions in these patients were compared with these features in the lesions in consecutive patients with early colorectal cancer who had no evidence of liver metastases within at least 5 years after colorectal resection. Venous invasion was more frequent in the primary lesions with liver metastases than in those without liver metastases (57% vs 0%; P = 0.0035). Expression of p53 and CD44v9 was more frequent in the primary lesions with liver metastases (71% and 100%) than in those without metastases (56% and 72%). In contrast, MUC2 expression was more frequent in the primary lesions without liver metastases (72%) than in those with metastases (43%). Venous invasion is considered to be closely related to liver metastasis, and the immunohistochemical expression of p53 and CD44v9 provides useful information for identifying those patients with early colorectal cancer who have a high risk of developing liver metastases.
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页码:334 / 340
页数:6
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