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Varied expression and localization of multiple galectins in different cancer cell lines.

机译:多种半乳糖凝集素在不同癌细胞系中的不同表达和定位。

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摘要

Galectins play a key role in oncogenic processes. Although several galectins are known, their relative expression at the mRNA and protein levels, the subcellular localization, and their relationship to the oncogenic manifestation remains unclear. Herein we report a comprehensive characterization of the expression of major galectins in human breast cancer (drug-sensitive MCF-7 and drug-resistant MCF-7/Adr(R)), colon cancer (HCT-116 and HT-29), and glioma (T98G) cell lines, as these cells are common model systems for studying oncogenic processes. The expected approximately 14.5 kDa galectin-1, predominantly cytosolic, was detected in the cancer and normal cell lines. Notably, two different molecular forms of galectin-1 with molecular masses of approximately 13.5 and 15 kDa were detected in T98G cells, the latter being in the extracellular medium, perhaps a result of post-translational processing. Immunocytochemistry indicated that the extracellular galectin-1 bound to the cell surface was punctated in appearance, suggesting that it was bound to specific receptors. Immunohistological studies indicated that metastasizing carcinomas express high levels of galectin-1. On the other hand, galectin-3 was readily detectable in all cancer cell lines but undetectable in normal cell lines, indicating that galectin-3 is a cancer-specific biomarker protein. Galectin-3 was a cytosolic protein but was not detected in the extracellular medium, indicating that cancer cells do not secrete this galectin. Finally, despite the RT-PCR analysis suggesting the presence of two transcripts of galectin-8 in all cancer cell lines, the corresponding approximately 36 kDa protein was only detectable in the nuclear and cytosolic fractions upon cell fractionation. Notably, a different molecular form of galectin-8 of approximately 18 kDa was immunoprecipitated from the extracellular media, suggesting that the secreted galectin-8 undergoes post-translational processing. These results highlight the expression of galectins in different molecular forms in cancers, warranting caution in interpreting the results of functional studies of individual galectins, particularly because these proteins function redundantly in cancer pathways.
机译:半乳凝素在致癌过程中起关键作用。尽管已知几种半乳凝素,但它们在mRNA和蛋白质水平的相对表达,亚细胞定位及其与致癌表现的关系仍不清楚。本文中,我们报告了主要半乳凝素在人类乳腺癌(药物敏感性MCF-7和耐药性MCF-7 / Adr(R)),结肠癌(HCT-116和HT-29)中的表达的全面表征。胶质瘤(T98G)细胞系,因为这些细胞是研究致癌过程的常见模型系统。在癌症和正常细胞系中检测到预期的大约14.5 kDa galectin-1,主要为胞质。值得注意的是,在T98G细胞中检测到了两种不同分子形式的galectin-1,其分子质量分别约为13.5和15 kDa,后者位于细胞外培养基中,可能是翻译后加工的结果。免疫细胞化学表明,与细胞表面结合的细胞外半乳糖凝集素-1在外观上是点状的,表明它与特定的受体结合。免疫组织学研究表明,转移性癌表达高水平的半乳凝素-1。另一方面,galectin-3在所有癌细胞系中都容易检测到,而在正常细胞系中则未检测到,这表明galectin-3是癌症特异性的生物标记蛋白。 Galectin-3是一种胞质蛋白,但在细胞外培养基中未检测到,表明癌细胞不分泌这种Galectin。最后,尽管RT-PCR分析表明在所有癌细胞系中均存在galectin-8的两个转录本,但仅在细胞分级分离后才在核和胞质级分中检测到相应的约36 kDa蛋白。值得注意的是,大约18 kDa的另一种分子形式的galectin-8从细胞外介质中被免疫沉淀出来,这表明分泌的galectin-8经历了翻译后加工。这些结果突出了半乳糖凝集素在癌症中以不同分子形式的表达,在解释单个半乳糖凝集素功能研究的结果时要特别谨慎,特别是因为这些蛋白质在癌症途径中起着多余的作用。

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