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细胞凋亡和bcl-2蛋白的表达是影响原发性肺类癌肿瘤细胞更新的相反因素。

Apoptosis and expression of bcl-2 protein are inverse factors influencing tumour cell turnover in primary carcinoid tumours of the lung.

作者信息

Zirbes T K, Lorenzen J, Baldus S E, Moenig S P, Wolters U, Ottlik A, Thiele J, Hölscher A H, Dienes H P

机构信息

Department of Pathology, University of Cologne, Germany.

出版信息

Histopathology. 1998 Aug;33(2):123-8. doi: 10.1046/j.1365-2559.1998.00466.x.

Abstract

AIMS

This study evaluates potential regulating factors in primary pulmonary carcinoid tumours, 16 typical and four atypical samples, with special emphasis on apoptosis and the bcl-2 gene family. Furthermore, p53-related oncogenes were analysed in a search for associated biological parameters.

METHODS AND RESULTS

The in-situ end-labelling technique (ISEL) was used to determine apoptotic cells, in addition to immunohistochemical methods, which were used to investigate the expression of the Ki67 antigen (avidinbiotin complex (ABC) method) and bcl-2, bcl-x, p53, p21/waf1, p27 and mdm-2 proteins (catalysed reporter deposition (CARD) technique). The incidence of apoptotic tumour cells was significantly enhanced in typical carcinoids. The bcl-2 protein was expressed to a higher degree in atypical carcinoids, which displayed a higher proliferative capacity as well. In contrast, bcl-x was observed predominantly in so-called typical carcinoids. The tumour cell turnover index was the most distinguishing parameter between both entities. All carcinoid tumours failed to show a staining for p53, p21/waf. p27 and mdm-2 proteins.

CONCLUSIONS

The different biological behaviour of the carcinoid tumours under study seems to be influenced by the bcl-2 gene family preventing programmed cell death. We speculate that this results in a more aggressive course in atypical carcinoid tumours.

摘要

目的

本研究评估原发性肺类癌肿瘤(16例典型和4例非典型样本)中的潜在调节因子,特别强调细胞凋亡和bcl - 2基因家族。此外,分析p53相关癌基因以寻找相关生物学参数。

方法与结果

除免疫组织化学方法外,采用原位末端标记技术(ISEL)确定凋亡细胞,免疫组织化学方法用于研究Ki67抗原的表达(抗生物素蛋白 - 生物素复合物(ABC)法)以及bcl - 2、bcl - x、p53、p21/waf1、p27和mdm - 2蛋白的表达(催化报告沉积(CARD)技术)。典型类癌中凋亡肿瘤细胞的发生率显著增加。bcl - 2蛋白在非典型类癌中表达程度更高,其增殖能力也更高。相比之下,bcl - x主要在所谓的典型类癌中观察到。肿瘤细胞更新指数是这两种实体之间最具区分性的参数。所有类癌肿瘤均未显示p53、p21/waf、p27和mdm - 2蛋白染色。

结论

所研究的类癌肿瘤的不同生物学行为似乎受到bcl - 2基因家族阻止程序性细胞死亡的影响。我们推测这导致非典型类癌肿瘤病程更具侵袭性。

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