Cell-cycle analysis detecting endogenous nuclear antigens: comparison with BrdU-in vivo labeling and an application to lung tumors.

Y Hayashi, M Fukayama, M Koike, S Kaseda, T Ikeda, T Yokoyama
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引用次数: 28

Abstract

The versatility of non-radioactive cell-cycle analysis in detecting endogenous nuclear antigens of the proliferating cells was evaluated. Optimal conditions for immunostaining varied in fixation and pretreatment procedures among antigens, bromodeoxyuridine (BrdU), Ki-67 epitope, DNA polymerase alpha and PCNA. A significant correlation between BrdU labeling index (LI) was observed in each positive ratio (PR, positive/total neoplastic cells) for nuclear antigens in tumor-sections which had been labeled in vivo with BrdU. The best correlation was observed in Ki-67 PR (y = 1.26x + 2.5; y = Ki-67 PR; x = BrdU LI; r = 0.97). To determine its prognostic value, Ki-67 analysis was applied to the surgically resected lung tumors. Ki-67 PR were different according to the histologic types of the tumors: 47.8 +/- 3.4% in small cell carcinoma; 29.5 +/- 3.5% in squamous cell carcinoma; 28.3 +/- 4.7% in large cell carcinoma; 15.2 +/- 1.8% in adenocarcinoma and 0.1 +/- 0.1% in mature carcinoid tumor. When the mean value was used to divide each type to a higher or lower proliferative activity (15% Ki-67 PR for adenocarcinoma and 30% for squamous cell carcinoma), the group with the lower Ki-67 PR showed a significantly more favorable prognosis than that of a higher ratio. Ki-67 PR was not correlated with other pathologic factors such as size, lymph node metastasis or pleural involvement. Non-radioactive cell-cycle analysis was feasible and useful for detecting endogenous nuclear antigens even in the lung tumors, particularly when the analysis was coupled with histologic typing.

细胞周期分析检测内源性核抗原:与brdu体内标记的比较及其在肺肿瘤中的应用。
评价了非放射性细胞周期分析在检测增殖细胞内源性核抗原方面的通用性。不同抗原、溴脱氧尿苷(BrdU)、Ki-67表位、DNA聚合酶α和PCNA的固定和预处理条件不同,免疫染色的最佳条件也不同。在体内用BrdU标记的肿瘤切片中,各核抗原的阳性比率(PR,阳性/肿瘤细胞总数)与BrdU标记指数(LI)呈显著相关。Ki-67 PR相关性最好(y = 1.26x + 2.5;y = Ki-67 PR;x = BrdU LI;R = 0.97)。为了确定其预后价值,Ki-67分析应用于手术切除的肺肿瘤。Ki-67 PR根据肿瘤的组织学类型不同而不同:小细胞癌为47.8 +/- 3.4%;29.5 +/- 3.5%的鳞状细胞癌;大细胞癌28.3 +/- 4.7%;腺癌15.2 +/- 1.8%,成熟类癌0.1 +/- 0.1%。当使用平均值将每种类型划分为较高或较低的增殖活性(腺癌为15% Ki-67 PR,鳞状细胞癌为30%)时,Ki-67 PR较低组的预后明显优于较高比例组。Ki-67 PR与其他病理因素如大小、淋巴结转移或胸膜受累无关。非放射性细胞周期分析对于检测内源性核抗原是可行和有用的,即使在肺肿瘤中,特别是当分析与组织学分型相结合时。
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