EWS-FLI1表达细胞EF与NIH-3T3的蛋白质组学比较及(R/W)9细胞穿透肽的肌动蛋白重塑作用

Q4 Biochemistry, Genetics and Molecular Biology
Séverine Clavier , Françoise Illien , Sandrine Sagan , Gérard Bolbach , Emmanuelle Sachon
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引用次数: 3

摘要

EWS-FLI1在NIH-3T3成纤维细胞中的表达对表型有深远的影响,导致细胞骨架和粘附能力紊乱(EF细胞)。此外,细胞穿透肽(CPP) (R/W)9在EF细胞中具有内在的肌动蛋白重塑活性。为了评估致癌蛋白EWS-FLI1对蛋白表达水平的影响,我们对肿瘤EF和非肿瘤3T3蛋白组进行了定量比较。然后,为了了解EWS-FLI1的致癌转化是否与(R/W)9诱导的表型逆转有关,我们评估了(R/W)9对EF细胞蛋白质组的影响。据我们所知,以前还没有进行过这样的研究。生物学意义迄今为止,全球定量蛋白质组学研究很少发表,以帮助了解EWS-FLI1融合蛋白诱导的癌性转化并导致Ewing肉瘤的发生和传播。我们在本研究中对模型肿瘤细胞系EF和非肿瘤对应细胞系(3T3)进行了比较,使我们能够突出大多数肿瘤类型共同或尤因肉瘤特有的几个特征。特别是,肌动蛋白细胞骨架组织的缺乏很可能是由于许多重要的肌动蛋白结合蛋白的下调。这些结果符合被动/随机传播模式的假设,赋予尤因肉瘤肿瘤细胞高转移潜力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Proteomic comparison of the EWS-FLI1 expressing cells EF with NIH-3T3 and actin remodeling effect of (R/W)9 cell-penetrating peptide

Proteomic comparison of the EWS-FLI1 expressing cells EF with NIH-3T3 and actin remodeling effect of (R/W)9 cell-penetrating peptide

EWS-FLI1 expression in NIH-3T3 fibroblasts has a profound impact on the phenotype, resulting in the cytoskeleton and adhesive capacity disorganization (EF cells). Besides this, (R/W)9, a cell-penetrating peptide (CPP), has an intrinsic actin remodeling activity in EF cells. To evaluate the impact of the oncogenic protein EWS-FLI1 on proteins expression levels, a quantitative comparison of tumoral EF and non-tumoral 3T3 proteomes was performed. Then to see if we could link the EWS-FLI1 oncogenic transformation to the phenotype reversion induced by (R/W)9, (R/W)9 influence on EF cells proteome was assessed. To our knowledge no such ⿿CPPomic⿿ study has been performed before.

Biological significance

Up to now very few global quantitative proteomic studies have been published to help understand the oncogenic transformation induced by EWS-FLI1 fusion protein and leading to Ewing sarcoma development and dissemination. The comparison we did in this study between a model tumoral cell line EF and its non-tumoral counterpart (3T3) allowed us to highlight several features either common to most tumor types or specific to Ewing sarcoma. Particularly, lack of actin cytoskeleton organization could very likely be explained by the down-regulation of many important actin binding proteins. These results are in accordance with the hypothesis of a passive/stochastic mode of dissemination conferring Ewing sarcoma tumoral cell a high metastatic potential.

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来源期刊
EuPA Open Proteomics
EuPA Open Proteomics Biochemistry, Genetics and Molecular Biology-Biochemistry
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