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稳定同位素分辨代谢组学显示,与二维细胞培养相比,三维球体对抗癌亚硒酸盐具有代谢抗性。

Stable Isotope-Resolved Metabolomics Shows Metabolic Resistance to Anti-Cancer Selenite in 3D Spheroids versus 2D Cell Cultures.

作者信息

Fan Teresa W-M, El-Amouri Salim S, Macedo Jessica K A, Wang Qing Jun, Song Huan, Cassel Teresa, Lane Andrew N

机构信息

Center for Environmental and Systems Biochemistry, Markey Cancer Center, and Depart of Toxicology and Cancer Biology, University of Kentucky, Lexington, KY 40506, USA.

Department of Ophthalmology and Visual Sciences, University of Kentucky, Lexington, KY 40506, USA.

出版信息

Metabolites. 2018 Jul 10;8(3):40. doi: 10.3390/metabo8030040.

Abstract

Conventional two-dimensional (2D) cell cultures are grown on rigid plastic substrates with unrealistic concentration gradients of O₂, nutrients, and treatment agents. More importantly, 2D cultures lack cell⁻cell and cell⁻extracellular matrix (ECM) interactions, which are critical for regulating cell behavior and functions. There are several three-dimensional (3D) cell culture systems such as Matrigel, hydrogels, micropatterned plates, and hanging drop that overcome these drawbacks but they suffer from technical challenges including long spheroid formation times, difficult handling for high throughput assays, and/or matrix contamination for metabolic studies. Magnetic 3D bioprinting (M3DB) can circumvent these issues by utilizing nanoparticles that enable spheroid formation and growth via magnetizing cells. M3DB spheroids have been shown to emulate tissue and tumor microenvironments while exhibiting higher resistance to toxic agents than their 2D counterparts. It is, however, unclear if and how such 3D systems impact cellular metabolic networks, which may determine altered toxic responses in cells. We employed a Stable Isotope-Resolved Metabolomics (SIRM) approach with C₆-glucose as tracer to map central metabolic networks both in 2D cells and M3DB spheroids formed from lung (A549) and pancreatic (PANC1) adenocarcinoma cells without or with an anti-cancer agent (sodium selenite). We found that the extent of C-label incorporation into metabolites of glycolysis, the Krebs cycle, the pentose phosphate pathway, and purine/pyrimidine nucleotide synthesis was largely comparable between 2D and M3DB culture systems for both cell lines. The exceptions were the reduced capacity for de novo synthesis of pyrimidine and sugar nucleotides in M3DB than 2D cultures of A549 and PANC1 cells as well as the presence of gluconeogenic activity in M3DB spheroids of PANC1 cells but not in the 2D counterpart. More strikingly, selenite induced much less perturbation of these pathways in the spheroids relative to the 2D counterparts in both cell lines, which is consistent with the corresponding lesser effects on morphology and growth. Thus, the increased resistance of cancer cell spheroids to selenite may be linked to the reduced capacity of selenite to perturb these metabolic pathways necessary for growth and survival.

摘要

传统的二维(2D)细胞培养是在刚性塑料基质上进行的,其氧气、营养物质和治疗剂的浓度梯度不符合实际情况。更重要的是,二维培养缺乏细胞间和细胞与细胞外基质(ECM)的相互作用,而这些相互作用对于调节细胞行为和功能至关重要。有几种三维(3D)细胞培养系统,如基质胶、水凝胶、微图案板和悬滴法,克服了这些缺点,但它们也面临技术挑战,包括球体形成时间长、高通量检测操作困难和/或代谢研究中的基质污染。磁性三维生物打印(M3DB)可以通过利用纳米颗粒来规避这些问题,这些纳米颗粒能够通过磁化细胞实现球体的形成和生长。M3DB球体已被证明能够模拟组织和肿瘤微环境,同时比二维对应物表现出更高的对毒性剂的抗性。然而,尚不清楚这种三维系统是否以及如何影响细胞代谢网络,而细胞代谢网络可能决定细胞中改变的毒性反应。我们采用了以C₆-葡萄糖为示踪剂的稳定同位素分辨代谢组学(SIRM)方法,来绘制由肺癌(A549)和胰腺癌(PANC1)腺癌细胞形成的二维细胞和M3DB球体中的中心代谢网络,有无抗癌剂(亚硒酸钠)。我们发现,对于这两种细胞系,在二维和M3DB培养系统之间,C标记掺入糖酵解、三羧酸循环、磷酸戊糖途径以及嘌呤/嘧啶核苷酸合成代谢物中的程度在很大程度上是可比的。例外情况是,与A549和PANC1细胞的二维培养相比,M3DB中嘧啶和糖核苷酸的从头合成能力降低,以及PANC1细胞的M3DB球体中存在糖异生活性,而二维对应物中不存在。更引人注目的是,相对于两种细胞系中的二维对应物,亚硒酸盐在球体中对这些途径的扰动要小得多,这与对形态和生长的相应较小影响一致。因此,癌细胞球体对亚硒酸盐抗性的增加可能与亚硒酸盐干扰生长和存活所需的这些代谢途径的能力降低有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/080f/6161115/43d259da3c9b/metabolites-08-00040-g001.jpg

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