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支架 3D 培养中 HepG2 的代谢改变:蛋白质组学方法。

Metabolic alteration of HepG2 in scaffold-based 3-D culture: proteomic approach.

机构信息

Applied Biological Sciences Program, Chulabhorn Graduate Institute, Bangkok, Thailand.

出版信息

Proteomics. 2010 Nov;10(21):3896-904. doi: 10.1002/pmic.201000137.

Abstract

3-D cell culture models are important in cancer biology since they provide improved understanding of tumor microenvironment. We have established a 3-D culture model using HepG2 in natural collagen-based scaffold to mimic the development of small avascular tumor in vivo. Morphological characterization showed that HepG2 colonies grew within the interior of the scaffold and showed enhanced extracellular matrix deposition. High levels of cell proliferation in the outermost regions of the scaffold created a hypoxic microenvironment in the 3-D culture system, as indicated by hypoxia-inducible factor-1α stabilization, detectable by Western blotting and immunohistochemistry. Proteomic studies showed decreased expression of several mitochondrial proteins and increased expression of proteins in anaerobic glycolysis under 3-D culture compared to monolayer culture. Creatine kinase was also upregulated in 3-D culture, indicating its possible role as an important energy buffer system under hypoxic microenvironment. Increased levels of proteins in nucleotide metabolism may relate to cellular energy. Thus, our results suggest that HepG2 cells under 3-D culture adapt their energy metabolism in response to hypoxic conditions. Metabolic alterations in the 3-D culture model may relate to physiological changes relevant to development of small avascular tumor in vivo and their study may improve future therapeutic strategies.

摘要

3-D 细胞培养模型在癌症生物学中非常重要,因为它们可以更好地了解肿瘤微环境。我们使用 HepG2 在天然胶原基支架中建立了 3-D 培养模型,以模拟体内小型无血管肿瘤的发展。形态学特征表明,HepG2 集落生长在支架内部,并表现出增强的细胞外基质沉积。支架最外层的高细胞增殖水平在 3-D 培养系统中产生了缺氧微环境,这一点可通过 Western blot 和免疫组化检测到缺氧诱导因子-1α 的稳定来指示。蛋白质组学研究表明,与单层培养相比,3-D 培养中几种线粒体蛋白的表达降低,而无氧糖酵解蛋白的表达增加。在 3-D 培养中,肌酸激酶也上调,表明其在缺氧微环境下可能作为重要的能量缓冲系统发挥作用。核苷酸代谢中蛋白质水平的增加可能与细胞能量有关。因此,我们的结果表明,HepG2 细胞在 3-D 培养下适应缺氧条件下的能量代谢。3-D 培养模型中的代谢改变可能与体内小型无血管肿瘤发展相关的生理变化有关,对其研究可能改善未来的治疗策略。

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