LncRNA HULC通过增强YAP活性和自噬作用,促进高糖相关性胰腺癌的进展和耐药性。

IF 2.4 4区 生物学 Q4 CELL BIOLOGY
Ankita Sharma, Shibasish Chowdhury, Sudeshna Mukherjee, Rajdeep Chowdhury
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引用次数: 0

摘要

背景信息:高血糖是胰腺癌(PC)发病机制的干扰因素之一。人们对高血糖(HG)影响胰腺癌严重程度的分子机制知之甚少。我们的研究深入探讨了肝癌中高度上调的lncRNA(HULC)及其与是相关蛋白(YAP)的相互作用在HG诱导条件下调控胰腺导管腺癌细胞(PDAC)命运的影响。我们在正常或 HG 条件下培养 PDAC 细胞。随后,我们测定了HG对PDAC细胞活力、迁移潜力和耐药性的影响。我们通过生物信息学分析筛选出了可能在PC和糖尿病中调控失调的lncRNAs,然后进行了湿实验室功能验证:结果:HG导致PDAC细胞增殖和耐药性增强。通过生物信息学分析,HULC被确定为主要的失调lncRNA之一。siRNA 介导的 HULC 消减导致 YAP 转录活性同时下降。重要的是,研究发现 HULC 和 YAP 可共同调节细胞自噬的平衡过程,从而增强 PDAC 细胞的抗药性和增殖潜力。此外,抑制自噬或YAP会导致HULC水平下降,这表明存在一个相互调节的反馈回路:结论:我们观察到 HG 会引发 PDAC 细胞的侵袭性。从机理上讲,lncRNA HULC的上调导致YAP的激活和自噬的不同调节,从而增加了PDAC细胞的增殖:意义:抑制HULC和YAP可能是治疗PDAC的一种新策略。此外,本研究还描绘了 HULC、YAP 和自噬在 PDAC 发病机制中错综复杂的分子相互作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

LncRNA HULC augments high glucose-associated pancreatic cancer progression and drug resistance by enhancing YAP activity and autophagy

LncRNA HULC augments high glucose-associated pancreatic cancer progression and drug resistance by enhancing YAP activity and autophagy

LncRNA HULC augments high glucose-associated pancreatic cancer progression and drug resistance by enhancing YAP activity and autophagy

Background Information: One of the confounding factors in pancreatic cancer (PC) pathogenesis is hyperglycemia. The molecular mechanism by which high glucose (HG) influences PC severity is poorly understood. Our investigation delved into the impact of lncRNA highly upregulated in liver cancer (HULC) and its interaction with yes-associated protein (YAP) in regulating the fate of pancreatic ductal adenocarcinoma cells (PDAC) under HG-induced conditions. PDAC cells were cultured under normal or HG conditions. We thereafter measured the effect of HG on the viability of PDAC cells, their migration potential and drug resistance properties. The lncRNAs putatively dysregulated in PC and diabetes were shortlisted by bioinformatics analysis followed by wet lab validation of function. Results: HG led to enhanced proliferation and drug refractoriness in PDAC cells. HULC was identified as one of the major deregulated lncRNAs following bioinformatics analysis. HULC was found to regulate the expression of the potent transcriptional regulator – YAP through selective histone modifications at the YAP promoter. siRNA-mediated ablation of HULC resulted in a concurrent decrease in YAP transcriptional activity. Importantly, HULC and YAP were found to co-operatively regulate the cellular homeostatic process autophagy, thus inculcating drug resistance and proliferative potential in PDAC cells. Moreover, inhibition of autophagy or YAP led to a decrease in HULC levels, suggesting the existence of an inter-regulatory feedback loop. Conclusions: We observed that HG triggers aggressive properties in PDAC cells. Mechanistically, up-regulation of lncRNA HULC resulted in activation of YAP and differential regulation of autophagy coupled to increased proliferation of PDAC cells. Significance: Inhibition of HULC and YAP may represent a novel therapeutic strategy for PDAC. Furthermore, this study portrays the intricate molecular interplay between HULC, YAP and autophagy in PDAC pathogenesis.

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来源期刊
Biology of the Cell
Biology of the Cell 生物-细胞生物学
CiteScore
5.30
自引率
0.00%
发文量
53
审稿时长
>12 weeks
期刊介绍: The journal publishes original research articles and reviews on all aspects of cellular, molecular and structural biology, developmental biology, cell physiology and evolution. It will publish articles or reviews contributing to the understanding of the elementary biochemical and biophysical principles of live matter organization from the molecular, cellular and tissues scales and organisms. This includes contributions directed towards understanding biochemical and biophysical mechanisms, structure-function relationships with respect to basic cell and tissue functions, development, development/evolution relationship, morphogenesis, stem cell biology, cell biology of disease, plant cell biology, as well as contributions directed toward understanding integrated processes at the organelles, cell and tissue levels. Contributions using approaches such as high resolution imaging, live imaging, quantitative cell biology and integrated biology; as well as those using innovative genetic and epigenetic technologies, ex-vivo tissue engineering, cellular, tissue and integrated functional analysis, and quantitative biology and modeling to demonstrate original biological principles are encouraged.
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