Nancy Alnassar, Jacek Hajto, Robin M H Rumney, Suraj Verma, Malgorzata Borczyk, Chandrika Saha, Janos Kanczler, Arthur M Butt, Annalisa Occhipinti, Joanna Pomeroy, Claudio Angione, Michal Korostynski, Dariusz C Górecki
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引用次数: 0
摘要
Dp71 是最普遍的肌营养不良蛋白同工酶,它的表达变化与不同肿瘤患者的存活率有关。耐人寻味的是,在某些恶性肿瘤中,Dp71起着抑制肿瘤的作用,而在另一些恶性肿瘤中则表现出致癌特性。这种多样性可以通过两种 Dp71 剪接变体的表达来解释,这两种变体编码的蛋白具有不同的 C-端,每种蛋白都有特定的特性。这些变体的表达阻碍了对其独特作用的探索。利用 CRISPR/Cas9,我们在不表达标准 C 端变体的肉瘤细胞系中消减了具有替代 C 端的 Dp71f 变体,并对基因敲除细胞进行了分子(RNAseq)和功能鉴定。Dp71f消减诱导了重大的转录组改变,尤其影响了参与钙信号和ECM-受体相互作用通路的基因的表达。基因组范围的代谢分析发现,通过膜囊反应(GLCter)的葡萄糖转运显著下调,糖酵解/糖元生成途径下调。在功能上,这些分子变化与钙反应、细胞粘附、增殖、血清饥饿存活和化疗抗性的增强相对应。尽管基质金属蛋白酶释放增加,但基因敲除细胞显示出 GLUT1 蛋白表达减少、无附着存活以及在体外和体内的迁移和侵袭没有改变。我们的研究结果强调了淀粉样蛋白转录本替代剪接的重要性,并突出了Dp71f变体的作用。这种调控机制的缺失促进了肉瘤细胞的存活和耐药性。因此,Dp71f 是未来探索特定 DMD 转录本在生理学和各种恶性肿瘤中复杂功能的研究目标。
Ablation of the dystrophin Dp71f alternative C-terminal variant increases sarcoma tumour cell aggressiveness.
Alterations in Dp71 expression, the most ubiquitous dystrophin isoform, have been associated with patient survival across tumours. Intriguingly, in certain malignancies, Dp71 acts as a tumour suppressor, while manifesting oncogenic properties in others. This diversity could be explained by the expression of two Dp71 splice variants encoding proteins with distinct C-termini, each with specific properties. Expression of these variants has impeded the exploration of their unique roles. Using CRISPR/Cas9, we ablated the Dp71f variant with the alternative C-terminus in a sarcoma cell line not expressing the canonical C-terminal variant, and conducted molecular (RNAseq) and functional characterisation of the knockout cells. Dp71f ablation induced major transcriptomic alterations, particularly affecting the expression of genes involved in calcium signalling and ECM-receptor interaction pathways. The genome-scale metabolic analysis identified significant downregulation of glucose transport via membrane vesicle reaction (GLCter) and downregulated glycolysis/gluconeogenesis pathway. Functionally, these molecular changes corresponded with, increased calcium responses, cell adhesion, proliferation, survival under serum starvation and chemotherapeutic resistance. Knockout cells showed reduced GLUT1 protein expression, survival without attachment and their migration and invasion in vitro and in vivo were unaltered, despite increased matrix metalloproteinases release. Our findings emphasise the importance of alternative splicing of dystrophin transcripts and underscore the role of the Dp71f variant, which appears to govern distinct cellular processes frequently dysregulated in tumour cells. The loss of this regulatory mechanism promotes sarcoma cell survival and treatment resistance. Thus, Dp71f is a target for future investigations exploring the intricate functions of specific DMD transcripts in physiology and across malignancies.
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