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首页> 外文期刊>International immunopharmacology >Pharmacological modulation of carcinoembryonic antigen in human cancer cells: studies with staurosporine.
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Pharmacological modulation of carcinoembryonic antigen in human cancer cells: studies with staurosporine.

机译:人体癌细胞中癌胚抗原的药理学调节:星形孢菌素的研究。

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Preliminary studies, performed in our laboratory, showed that staurosporine (ST), a protein-kinase (PK) inhibitor, increases the expression of the carcinoembryonic antigen (CEA) in a human colon cancer cell line. The present study explores the cellular and molecular effects of ST on the CEA expression in breast cancer MCF-7 line and in a number of colon cancer cell lines characterized by the different basal levels of the antigen, including two cloned sublines (i.e. C22.20 and C6.6, expressing low and high CEA levels, respectively). In all cases, increase of the CEA expression was observed at drug concentrations devoid of marked cytostatic effects (e.g. 5 nM) and was accompanied by the enhanced CEA shedding in the supernatant. Moreover, the increase of the CEA levels both occurred in the cell membranes and in the cytosolic compartments and appeared to be the result of the enhanced CEA gene transcription. Similar results have been previously obtained with interferon-gamma. However, ST treatment, different from interferon-gamma, did not up-regulate the level of the HLA class I molecules. A preliminary investigation also showed that other PKC inhibitors did not substantially modulate the CEA expression. Therefore, the biochemical mechanism underlying the effect of ST should not be correlated with that involved in the PKC inhibition. The present study suggests that ST and, presumably, its analogs used in the cancer treatment could enhance the CEA expression on neoplastic cells in patients affected by the CEA-positive malignancies. This appears to be of potential clinical interest for the development of new immunotherapeutic or diagnostic approaches based on the pharmacological modulation of this antigenic marker.
机译:在我们实验室中进行的初步研究表明,星形孢菌素(ST)是一种蛋白激酶(PK)抑制剂,可增加人结肠癌细胞系中癌胚抗原(CEA)的表达。本研究探讨了ST对乳腺癌MCF-7系和以不同基础水平抗原为特征的许多结肠癌细胞系CEA表达的细胞和分子影响,包括两个克隆的亚系(即C22.20)。和C6.6,分别表示低和高的CEA水平)。在所有情况下,在没有明显的细胞抑制作用(例如5nM)的药物浓度下观察到CEA表达的增加,并伴随着上清液中CEA脱落的增强。而且,CEA水平的增加都发生在细胞膜和胞质区室中,并且似乎是CEA基因转录增强的结果。先前已经用干扰素-γ获得了类似的结果。然而,与干扰素-γ不同,ST治疗并未上调HLA I类分子的水平。初步研究还表明,其他PKC抑制剂并未实质性调节CEA表达。因此,ST的潜在生化机制不应与PKC抑制相关。本研究表明,ST及其可能用于癌症治疗的类似物可增强受CEA阳性恶性肿瘤影响的肿瘤细胞中CEA的表达。对于基于这种抗原标记物的药理学调节的新的免疫治疗或诊断方法的开发,这似乎具有潜在的临床意义。

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