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首页> 外文期刊>Japanese journal of clinical oncology. >Clinical significance of MUC1 and MUC2 mucin and p53 protein expression in colorectal carcinoma.
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Clinical significance of MUC1 and MUC2 mucin and p53 protein expression in colorectal carcinoma.

机译:大肠癌中MUC1和MUC2粘蛋白及p53蛋白表达的临床意义。

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BACKGROUND: Up-regulation of MUC1, down-regulation of MUC2 and p53 overexpression are seen in colorectal carcinomas. However, there have been few reports about the associations between MUC1, MUC2 and p53 expression and metastatic potential. The aim of this study was to investigate MUC1, MUC2 and p53 expression in colorectal carcinoma with special reference to regional and distant metastasis. METHODS: Eighty-six colorectal carcinomas were collected from patients undergoing tumor resection. Sections were used for MUC1, MUC2 and p53 immunostaining. Cancers were regarded as MUC1 or MUC2 positive when the positive cells were beyond 30% of cancer cells. Cancers with diffuse or nested patterns were regarded as having p53 overexpression. RESULTS: Of 86 cancers, 37 (43%) were MUC1 positive, 28 (33%) were MUC2 positive and 59 (69%) showed p53 overexpression. A difference was observed only in the frequency of MUC1 positivity with respect to depth of tumor invasion. Neither depth of tumor invasion nor histological differentiation had a positive correlation with MUC1, MUC2 and p53 overexpression. The frequency of MUC1 positive cells in Dukes' C and D tumors was significantly higher than that in Dukes' A and B tumors. The frequency of MUC1 positivity in tumors with hepatic involvement was significantly higher than that in tumors without hepatic involvement (100 vs 39%; p < 0.01). There was no difference in the frequency of MUC2 or p53 positivity in Dukes' stage or hepatic metastasis. MUC1 immunoreactivity of the surface was identical with that of the whole tumor in 81% (70/86) of carcinomas, MUC 2 in 87% and p53 in 100%. CONCLUSIONS: The results suggest that up-regulation of MUC1 is involved in the progression from the non-metastatic to the metastatic stage and that p53 abnormality is not directly involved in it. The data also imply that immunostaining of preoperative biopsy samples is useful for evaluating the immunoreactivity of the whole tumor.
机译:背景:在结肠直肠癌中,MUC1的表达上调,MUC2的表达下调和p53的过度表达。但是,关于MUC1,MUC2和p53表达与转移潜力之间的关联的报道很少。这项研究的目的是调查大肠癌中MUC1,MUC2和p53的表达,特别是针对区域和远处转移。方法:从接受肿瘤切除的患者中收集了86例大肠癌。将切片用于MUC1,MUC2和p53免疫染色。当阳性细胞超过癌细胞的30​​%时,癌症被视为MUC1或MUC2阳性。具有弥漫性或巢状模式的癌症被认为具有p53过表达。结果:在86例癌症中,MUC1阳性37例(43%),MUC2阳性28例(33%),p53过表达59例(69%)。仅观察到MUC1阳性的频率相对于肿瘤浸润深度的差异。肿瘤的浸润深度和组织学分化均与MUC1,MUC2和p53过表达均无正相关。杜克氏C和D肿瘤中MUC1阳性细胞的频率明显高于杜克氏A和B肿瘤中的MUC1阳性细胞的频率。肝受累肿瘤中MUC1阳性的频率显着高于无肝受累肿瘤中的MUC1阳性频率(100 vs 39%; p <0.01)。在Dukes's期或肝转移中,MUC2或p53阳性的频率没有差异。表面的MUC1免疫反应性与整个肿瘤的81%(70/86)相同,MUC 2的87%和p53的100%。结论:结果提示MUC1的上调参与了从非转移阶段到转移阶段的过程,而p53异常并不直接参与其中。数据还暗示术前活检样本的免疫染色可用于评估整个肿瘤的免疫反应性。

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