Circ_0067997 boosted the growth while repressed the apoptosis of SGC-7901/DDP cells via repressing miR-615-5p/AKT1 pathway.

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2023-01-01 DOI:10.3233/CBM-220145
Yuwen Jiao, Yue Fu, Yu Gong, Guangyao Wang, Shuai Chen, Gengdi Cai, Siyuan Wu, Liming Tang
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Abstract

Background: Gastric cancer (GC) remains a huge challenge to the heathy of human beings, largely due to lacking of effective therapeutic measures. Though an oncogenic role for circular RNAs (circRNAs) circ_0067997 in the progression of GC has been described recently, the molecular modulatory mechanism of it still remains to be further explored. The aim of present study is to examine the molecular network of circ_0067997 in GC.

Methods: qRT-PCR was carried out to determine the mRNA levels of circ_0067997, miR-615-5p and AKT1 in cisplatin (DDP)-insensitive or sensitive GC tumor tissues and cells, while the correlations among the contents of these molecules were determined by statistical analysis. The expression of circ_0067997 was manipulated by short-hairpin RNA and lentiviral-mediated approaches, while that of miR-615-5p was achieved by the application of its inhibitor or mimic. The in vivo action of circ_0067997 on tumor formation was determined by measuring tumor weight/volume/size and analyzing tumor apoptosis through TUNEL staining in mouse xenograft model and, while the in vitro effects of this circRNA and its target miR-615-5p on the cell survival and death were separately evaluated by CCK-8 assay and flow cytometry. Additionally, luciferase reporter assays were executed to determine the sequentially regulatory relationships of circ_0067997, miR-615-5p, and AKT1.

Results: Our data demonstrated that the level of circ_0067997 level was increased in DDP-insensitive GC tissues and cell line, while miR-615-5p presented the opposite results. Moreover, the relationships between circ_0067997 and miR-615-5p levels, circ_0067997 and AKT1 contents presented negative and positive correlations in clinic samples, respectively. Importantly, circ_0067997 was found to repress miR-615-5p expression, consequently leading to increased growth while reduced apoptosis of GC cells in the presence of DDP. Furthermore, the validated sequential regulation was circ_0067997 modulating miR-615-5p adjusting AKT1.

Conclusions: This study demonstrated that circ_0067997 functioned as a sponge of miR-615-5p to target AKT1 expression, thereby enhancing the growth and restricting the apoptosis of DDP-insensitive GC cells. These new findings offered a valuable target for the detection and management of GC.

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Circ_0067997通过抑制miR-615-5p/AKT1通路促进SGC-7901/DDP细胞生长,同时抑制凋亡。
背景:胃癌仍然是人类健康的巨大挑战,主要原因是缺乏有效的治疗措施。尽管环状rna (circRNAs) circ_0067997在GC进展中的致癌作用最近已被描述,但其分子调节机制仍有待进一步探索。本研究的目的是研究circ_0067997在GC中的分子网络。方法:采用qRT-PCR检测circ_0067997、miR-615-5p和AKT1在顺铂(DDP)不敏感或敏感胃癌组织和细胞中的mRNA水平,并通过统计分析确定这些分子含量之间的相关性。circ_0067997的表达是通过短发夹RNA和慢病毒介导的方法来操纵的,而miR-615-5p的表达是通过其抑制剂或模拟物来实现的。在小鼠异种移植瘤模型中,通过测量肿瘤重量/体积/大小和TUNEL染色分析肿瘤凋亡来确定circ_0067997在体内对肿瘤形成的作用,并通过CCK-8法和流式细胞术分别评估该circRNA及其靶点miR-615-5p对细胞存活和死亡的影响。此外,通过荧光素酶报告基因测定来确定circ_0067997、miR-615-5p和AKT1的顺序调控关系。结果:我们的数据显示,circ_0067997水平在ddp不敏感的GC组织和细胞系中升高,而miR-615-5p的结果相反。此外,circ_0067997与miR-615-5p水平、circ_0067997与AKT1含量在临床样本中分别呈负相关和正相关。重要的是,circ_0067997被发现抑制miR-615-5p的表达,从而导致DDP存在下GC细胞的生长增加,同时减少凋亡。此外,经过验证的顺序调控是circ_0067997调节miR-615-5p调节AKT1。结论:本研究表明circ_0067997作为miR-615-5p的海绵靶向AKT1表达,从而促进ddp不敏感GC细胞的生长并限制其凋亡。这些新发现为GC的检测和管理提供了有价值的靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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