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miR-146a 的 SNP 通过 miR-146a 信号通路影响膀胱癌干细胞的功能,从而参与膀胱癌的复发。

A SNP of miR-146a is involved in bladder cancer relapse by affecting the function of bladder cancer stem cells via the miR-146a signallings.

机构信息

Department of Urology, The First Affiliated Hospital of Zhengzhou University, Zhengzhou, China.

出版信息

J Cell Mol Med. 2020 Aug;24(15):8545-8556. doi: 10.1111/jcmm.15480. Epub 2020 Jun 28.

Abstract

MiR-146a-5p in urine samples was recently reported to be possibly used as a prognostic marker for bladder cancer (BC). Interestingly, YAP1 and COX2 were both demonstrated to function as stem cell regulators in BC. Therefore, in this study, we aimed to establish the molecular mechanism underlying the role of miR-146a, YAP1 and COX2 in BC relapse. We also studied the possibility of using the C > G genotype of miR-146a rs2910164 SNP as an indicator of BC relapse. A total of 170 BC patients were assigned into different groups based on their genotypes of rs2910164 SNP. Kaplan-Meier survival curves were plotted to compare the recurrence-free rate among these groups. Real-time PCR, Western Blot, bioinformatic analysis, luciferase assay and IHC assay were conducted to study the role of rs2910164 SNP in the progression of BC. Accordingly, GC/CC-genotyped patients presented a higher risk of recurrence when compared with GG-genotyped patients, while the expression of BC regulators was influenced by the presence of rs2910164. COX2 mRNA and YAP1 mRNA were, respectively, validated as direct target genes of miR-146a, and the expression of YAP1 and COX2 mRNA/protein was both suppressed by miR-146a precursors. The expression of ALDH1A1 mRNA/protein was inhibited upon the down-regulation of YAP1, while the expression of let7 and SOX2 mRNA/protein was inhibited upon the down-regulation of COX2. In conclusion, two signalling pathways, miR-146a/YAP1/ALDH1A1 and miR-146a/COX2/PGE2/let7/SOX2, were modulated by miR-146a. As an SNP regulating the expression of miR-146a, the rs2910164 G > C SNP could be utilized as a biomarker for BC relapse.

摘要

miR-146a-5p 在尿液样本中最近被报道可能用作膀胱癌 (BC) 的预后标志物。有趣的是,YAP1 和 COX2 都被证明在 BC 中作为干细胞调节因子发挥作用。因此,在本研究中,我们旨在确定 miR-146a、YAP1 和 COX2 在 BC 复发中的作用的分子机制。我们还研究了使用 miR-146a rs2910164 SNP 的 C>G 基因型作为 BC 复发指标的可能性。根据 rs2910164 SNP 的基因型,将 170 例 BC 患者分为不同组。绘制 Kaplan-Meier 生存曲线以比较这些组之间的无复发生存率。进行实时 PCR、Western Blot、生物信息学分析、荧光素酶测定和 IHC 测定以研究 rs2910164 SNP 在 BC 进展中的作用。相应地,与 GG 基因型患者相比,GC/CC 基因型患者的复发风险更高,而 BC 调节剂的表达受 rs2910164 的影响。COX2 mRNA 和 YAP1 mRNA 分别被验证为 miR-146a 的直接靶基因,miR-146a 前体抑制 YAP1 和 COX2 mRNA/蛋白的表达。下调 YAP1 抑制 ALDH1A1 mRNA/蛋白的表达,而下调 COX2 抑制 let7 和 SOX2 mRNA/蛋白的表达。总之,miR-146a 调节了两条信号通路,miR-146a/YAP1/ALDH1A1 和 miR-146a/COX2/PGE2/let7/SOX2。作为调节 miR-146a 表达的 SNP,rs2910164 G>C SNP 可作为 BC 复发的生物标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7e74/7412697/807350078603/JCMM-24-8545-g001.jpg

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