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A novel tissue engineered three-dimensional in vitro colorectal cancer model.

机译:一种新型组织工程三维体外结直肠癌模型。

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摘要

The interactions of cancer cells within a solid mass with the surrounding reactive stroma are critical for growth and progression. The surrounding vasculature is recruited into the periphery of the growing tumour to supply cancer cells with nutrients and O2. This study focuses on developing a novel three-dimensional (3-D) in vitro biomimetic colorectal cancer model using colorectal cancer cells and connective tissue cells. The 3-D model comprises a dense artificial cancer mass, created by partial plastic compression of collagen type I containing HT29 colorectal cancer cells, nested in a non-dense collagen type I gel populated by fibroblasts and/or endothelial cells. HT29 cells within the dense mass proliferate slower than when cultured in a two-dimensional system. These cells form tumour spheroids which invade the surrounding matrix, away from the hypoxic conditions in the core of the construct, measured using real time O2 probes. This model is also characterized by the release of vascular endothelial growth factor (VEGF) by HT29 cells, mainly at the invading edge of the artificial cancer mass. This characterization is fundamental in establishing a reproducible, complex model that could be used to advance our understanding of cancer pathology and will facilitate therapeutic drug testing.
机译:癌细胞在固体质量内与周围的反应性基质的相互作用对生长和进展至关重要。周围的脉管系统被招募到不断增长的肿瘤周围,以供应患有营养和O2的癌细胞。该研究侧重于使用结肠直肠癌细胞和结缔组织细胞开发一种新型三维(3-D)体外染色结肠直肠癌模型。 3-D模型包括致密的人造癌细胞,通过含有HT29结直肠癌细胞的胶原型I型胶原型I的部分塑料压缩而产生,嵌套在由成纤维细胞和/或内皮细胞填充的非致密胶原型I凝胶中。 HT29细胞在致密质量内的细胞增殖慢于二维系统中培养时的较慢。这些细胞形成肿瘤球状体,其侵入周围基质,远离构建体的核心中的缺氧条件,使用实时o2探针测量。该模型的特征还在于HT29细胞释放血管内皮生长因子(VEGF),主要是人造癌症质量的入侵边缘。该表征是建立可重复的复杂模型的基础,可用于推进我们对癌症病理学的理解,并促进治疗药物检测。

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