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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Versican overexpression in human breast cancer lesions: known and new isoforms for stromal tumor targeting.
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Versican overexpression in human breast cancer lesions: known and new isoforms for stromal tumor targeting.

机译:人乳癌病变中的Versican过表达:用于基质肿瘤靶向的已知和新亚型。

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Proteoglycans play a key role in cancer development and progression by participating in the constitution of a specific fertile tumor microenvironment. As they are largely overexpressed in the malignant stroma, proteoglycans provide a reservoir of potential new targets for anticancer therapies, because they can serve to convey toxic payloads in the close proximity of cancer cells and subsequently destroy them. In this context, versican, a proteoglycan largely overexpressed in several solid cancers, bears the potential to be such an ideal target. As 4 main versican isoforms have been characterized, we sought to determine which isoform could represent the best target in human breast cancer. We used a series of 10 primary breast cancer lesions that were characterized as overexpressing the versican protein, when compared with matched normal breast tissues, using shotgun mass spectrometry and immunohistochemistry experiments. Quantitative polymerase chain reaction and western-blotting experiments were used to evaluate versican isoform expression in breast cancerormal tissue pairs for which ARN quality was excellent. All known isoforms were significantly overexpressed in the malignant lesions, both at the mRNA and at the protein levels. In the course of this study, we also identified and cloned a new alternatively spliced versican isoform, referred to as V4, which was also found to be upregulated in human breast cancer. This study provides for the first time a comprehensive mRNA and protein analysis of versican isoforms expression in human breast tissues, and offers insights into which therapeutic strategy would be best suited to target versican in human breast cancer lesions.
机译:蛋白聚糖通过参与特定的可育肿瘤微环境的构成在癌症的发展和进展中起关键作用。由于蛋白聚糖在恶性基质中过度表达,因此蛋白聚糖为抗癌治疗提供了潜在的新靶标,因为它们可以在癌细胞附近传递毒性有效载荷并随后将其破坏。在这种情况下,versican(一种在多种实体癌中过度表达的蛋白聚糖)具有成为此类理想靶标的潜力。由于已鉴定出4种主要的versican同工型,我们试图确定哪种同工型可以代表人类乳腺癌的最佳靶标。我们使用shot弹枪质谱和免疫组织化学实验,与匹配的正常乳腺组织相比,使用了一系列10个原发性乳癌病变,这些病变的特征是过表达versican蛋白。定量聚合酶链反应和蛋白质印迹实验用于评估ARN质量优异的乳腺癌/正常组织对中versican亚型的表达。无论是在mRNA还是在蛋白质水平,所有已知的同工型在恶性病变中均明显过表达。在这项研究的过程中,我们还鉴定并克隆了一种新的可变剪接的Verscan异构体,称为V4,在人乳腺癌中也被上调。这项研究首次为人类乳腺组织中的versican同工型表达提供了全面的mRNA和蛋白质分析,并为哪些治疗策略最适合于人类乳腺癌病变中的versican提供了见识。

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