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癌基因转染成纤维细胞多细胞球体中的代谢成像。

Metabolic imaging in multicellular spheroids of oncogene-transfected fibroblasts.

作者信息

Walenta S, Doetsch J, Mueller-Klieser W, Kunz-Schughart L A

机构信息

Institute of Physiology and Pathophysiology, University of Mainz, Mainz, Germany.

出版信息

J Histochem Cytochem. 2000 Apr;48(4):509-22. doi: 10.1177/002215540004800409.

Abstract

Four rat embryo fibroblast (REF) cell lines with defined oncogenic transformation were used to study the relationship between tumorigenic conversion, metabolism, and development of cell death in a 3D spheroid system. Rat1 (spontaneously immortalized) and M1 (myc-transfected) fibroblasts represent early nontumorigenic transformation stages, whereas Rat1-T1 (T24Ha-ras-transfected Rat1) and MR1 (myc/T24Ha-ras-co-transfected REF) cells express a highly tumorigenic phenotype. Localized ATP, glucose, and lactate concentrations in spheroid median sections were determined by imaging bioluminescence. ATP concentrations were low in the nonproliferating Rat1 aggregates despite sufficient oxygen and glucose availability and lack of lactate accumulation. In MR1 spheroids, a 50% decrease in central ATP preceded the development of central necrosis at a spheroid diameter of around 800 micrometer. In contrast, the histomorphological emergence of cell death at a diameter of around 500 micrometer in Rat1-T1 spheroids coincided with an initial steep drop in ATP. Concomitantly, reduction in central glucose and increase in lactate before cell death were recorded in MR1 but not in Rat1-T1 spheroids. As shown earlier, myc transfection confers a considerable resistance to hypoxia of MR1 cells in the center of spheroids, which is reflected by their capability to maintain cell integrity and ATP content in a hypoxic environment. The data obtained suggest that small alterations in the genotype of tumor cell lines, such as differences in the immortalization process, lead to substantial differences in morphological structure, metabolism, occurrence of cell death, and tolerance to hypoxia in spheroid culture.

摘要

使用四种具有明确致癌转化的大鼠胚胎成纤维细胞(REF)系,在三维球体系统中研究致瘤转化、代谢与细胞死亡发展之间的关系。大鼠1(自发永生化)和M1(myc转染)成纤维细胞代表早期非致瘤转化阶段,而大鼠1-T1(T24Ha-ras转染的大鼠1)和MR1(myc/T24Ha-ras共转染的REF)细胞表现出高度致瘤表型。通过成像生物发光测定球体中间切片中的局部ATP、葡萄糖和乳酸浓度。尽管有充足的氧气和葡萄糖供应且无乳酸积累,但在非增殖性大鼠1聚集体中ATP浓度较低。在MR1球体中,中心ATP降低50%先于球体直径约800微米时中心坏死的发生。相比之下,大鼠1-T1球体中直径约500微米时细胞死亡的组织形态学出现与ATP的初始急剧下降同时发生。同时,在MR1球体中记录到细胞死亡前中心葡萄糖减少和乳酸增加,而在大鼠1-T1球体中未记录到。如前所示,myc转染赋予MR1细胞在球体中心对缺氧的相当大抗性,这反映在它们在缺氧环境中维持细胞完整性和ATP含量的能力上。所获得的数据表明,肿瘤细胞系基因型的微小改变,如永生化过程中的差异,会导致球体培养中形态结构、代谢、细胞死亡发生和对缺氧耐受性的显著差异。

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