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体外和体内比较 KRAS 野生型和突变型 NSCLC 细胞的代谢组学特征。

Comparative metabolomics profiling of isogenic KRAS wild type and mutant NSCLC cells in vitro and in vivo.

机构信息

Protein and Gene Biomarkers Unit, Laboratory of Mass Spectrometry, Department of Environmental Health Sciences, IRCCS-Istituto di Ricerche Farmacologiche "Mario Negri", Milan, Italy.

Laboratory of Molecular Pharmacology, Department of Oncology, IRCCS-Istituto di Ricerche Farmacologiche "Mario Negri", Milan, Italy.

出版信息

Sci Rep. 2016 Jun 22;6:28398. doi: 10.1038/srep28398.

Abstract

Oncogenes induce metabolic reprogramming on cancer cells. Recently, G12C KRAS mutation in isogenic NSCLC cell line has been shown to be a key player in promoting metabolic rewiring mainly through the regulation of glutamine metabolism to fuel growth and proliferation. Even though cell lines possessing many of the genetic backgrounds of the primary cancer they derive from could be a valuable pre-clinical model, they do not have the additional complexity present in the whole tumor that impact metabolism. This preliminary study is aimed to explore how cancer cell metabolism in culture might recapitulate the metabolic alterations present in vivo. Our result highlighted that the gross metabolic changes observed in G12C KRAS mutant cells growing in culture were also maintained in the derived xenograft model, suggesting that a simple in vitro cell model can give important insights into the metabolic alterations induced by cancer. This is of relevance for guiding effective targeting of those metabolic traits that underlie tumor progression and anticancer treatment responses.

摘要

癌基因诱导癌细胞的代谢重编程。最近,同基因 NSCLC 细胞系中的 G12C KRAS 突变被证明是促进代谢重排的关键因素,主要通过调节谷氨酰胺代谢为生长和增殖提供燃料。尽管具有许多源自原发性癌症的遗传背景的细胞系可能是一种有价值的临床前模型,但它们没有影响代谢的整个肿瘤中存在的额外复杂性。本初步研究旨在探讨培养中的癌细胞代谢如何再现体内存在的代谢改变。我们的结果强调,在培养中生长的 G12C KRAS 突变细胞中观察到的总体代谢变化在衍生的异种移植模型中也得到维持,这表明简单的体外细胞模型可以深入了解癌症诱导的代谢改变。这对于指导针对肿瘤进展和抗癌治疗反应的基础代谢特征的有效靶向治疗具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5d6a/4916601/2a0a16c67bfb/srep28398-f1.jpg

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