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CD44 alternative splicing in gastric cancer cells is regulated by culture dimensionality and matrix stiffness

机译:胃癌细胞中CD44的选择性剪接受培养物尺寸和基质硬度的调节

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摘要

Two-dimensional (2D) cultures often fail to mimic key architectural and physical features of the tumor microenvironment. Advances in biomaterial engineering allow the design of three-dimensional (3D) cultures within hydrogels that mimic important tumor-like features, unraveling cancer cell behaviors that would not have been observed in traditional 2D plastic surfaces. This study determined how 3D cultures impact CD44 alternative splicing in gastric cancer (GC) cells. In 3D cultures, GC cells lost expression of the standard CD44 isoform (CD44s), while gaining CD44 variant 6 (CD44v6) expression. This splicing switch was reversible, accelerated by nutrient shortage and delayed at lower initial cell densities, suggesting an environmental stress-induced response. It was further shown to be dependent on the hydrogel matrix mechanical properties and accompanied by the upregulation of genes involved in epithelial-mesenchymal transition (EMT), metabolism and angiogenesis. The 3D cultures reported here revealed the same CD44 alternative splicing pattern previously observed in human premalignant and malignant gastric lesions. These findings indicate that fundamental features of 3D cultures such as soluble factors diffusion and mechanical cues influence CD44 expression in GC cells. Moreover, this study provides a new model system to study CD44 dysfunction, whose role in cancer has been in the spotlight for decades. (C) 2016 Elsevier Ltd. All rights reserved.
机译:二维(2D)培养通常无法模仿肿瘤微环境的关键结构和物理特征。生物材料工程学的进步允许在水凝胶中设计模仿重要肿瘤样特征的三维(3D)培养物,从而揭开传统2D塑料表面无法观察到的癌细胞行为。这项研究确定了3D培养物如何影响胃癌(GC)细胞中的CD44选择性剪接。在3D培养物中,GC细胞失去了标准CD44同种型(CD44s)的表达,而获得了CD44变体6(CD44v6)的表达。这种剪接开关是可逆的,由于营养缺乏而加速,并在较低的初始细胞密度下延迟,提示环境胁迫诱导的应答。进一步表明,它依赖于水凝胶基质的机械性能,并伴随着上皮-间质转化(EMT),代谢和血管生成的基因上调。此处报道的3D培养物揭示了以前在人类恶变前和恶性胃部病变中观察到的相同CD44替代剪接模式。这些发现表明3D培养物的基本特征,例如可溶性因子扩散和机械提示会影响GC细胞中CD44的表达。此外,这项研究提供了一个新的模型系统来研究CD44功能障碍,其在癌症中的作用已受到关注数十年。 (C)2016 Elsevier Ltd.保留所有权利。

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