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甲状腺乳头状癌组织中miR-142的上调:基于计算机模拟和体外分析的报告

Upregulation of miR-142 in papillary thyroid carcinoma tissues: a report based on in silico and in vitro analysis.

作者信息

Valizadeh Sepehr, Zehtabi Mojtaba, Feiziordaklou Neda, Akbarpour Zahra, Khamaneh Amir Mahdi, Raeisi Mortaza

机构信息

Department of Internal Medicine, School of Medicine, Tabriz University of Medical Sciences, Tabriz, Iran.

Hematology and Oncology Research Center, Tabriz University of Medical.

出版信息

Mol Biol Res Commun. 2022;11(3):133-141. doi: 10.22099/mbrc.2022.43947.1757.

Abstract

Papillary thyroid carcinoma (PTC) accounts for approximately 80% of all human thyroid malignancies. Recently, there has been a dramatic rise in the prevalence of thyroid cancer all over the globe. Through analysis of the GEO database, GSE104005, the authors of the current research were able to determine the differential expression of microRNAs (DEMs) as well as their target genes. Real-time PCR was used on a total of 40 samples, 40 of which were from PTC samples and 40 from normal tissues, in order to validate the discovered DEMs and the genes. Gene Ontology (GO) categories were identified, and KEGG was used to conduct pathway enrichment analysis. The multiMiR R package was used to predict target genes of DEMs. Mir-142 was found to be overexpressed in PTC samples, as compared to normal tissues, and this was validated by the identification and validation. In addition, metal ion binding and the cellular response to metal ions were identified as essential pathways in the carcinogenesis of PTC. This demonstrates their significance in the development of this malignancy. The results of our research will serve as the foundation for further research in the area of miRNA-based cancer treatment.

摘要

乳头状甲状腺癌(PTC)约占人类所有甲状腺恶性肿瘤的80%。最近,全球甲状腺癌的患病率急剧上升。通过对GEO数据库GSE104005的分析,本研究的作者能够确定微小RNA(DEM)及其靶基因的差异表达。对总共40个样本进行了实时PCR,其中40个来自PTC样本,40个来自正常组织,以验证发现的DEM和基因。确定了基因本体(GO)类别,并使用KEGG进行通路富集分析。使用multiMiR R包预测DEM的靶基因。与正常组织相比,发现Mir-142在PTC样本中过表达,这一点通过鉴定和验证得到了证实。此外,金属离子结合和细胞对金属离子的反应被确定为PTC致癌过程中的关键通路。这证明了它们在这种恶性肿瘤发展中的重要性。我们的研究结果将为基于miRNA的癌症治疗领域的进一步研究奠定基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1888/9661674/add0196f8a22/mbrc-11-133-g001.jpg

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