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在癌细胞系和手术切除的胃癌组织中表达的CDCA1和MSMB基因的癌症相关剪接变体。

Cancer-associated splicing variants of the CDCA1 and MSMB genes expressed in cancer cell lines and surgically resected gastric cancer tissues.

作者信息

Ohnuma Shinobu, Miura Koh, Horii Akira, Fujibuchi Wataru, Kaneko Naoyuki, Gotoh Osamu, Nagasaki Hideki, Mizoi Takayuki, Tsukamoto Nobukazu, Kobayashi Terutada, Kinouchi Makoto, Okabe Mitsunori, Sasaki Hiroyuki, Shiiba Ken-ichi, Miyagawa Kikuo, Sasaki Iwao

机构信息

Department of Surgery, Tohoku University Graduate School of Medicine, Sendai, Japan.

出版信息

Surgery. 2009 Jan;145(1):57-68. doi: 10.1016/j.surg.2008.08.010. Epub 2008 Oct 8.

Abstract

BACKGROUND

Alternative splicing is a molecular mechanism by which different combinations of exons can be alternatively spliced to produce different mRNA isoforms. Recently, several databases have been published to predict the alternative splicing of mRNA; cancer-specific alternative splicing has also been predicted with these databases. Those variants may be potentially useful targets for cancer therapy, however, the accuracy and veracity of these databases have yet to be confirmed.

METHODS

In this study, we analyzed 17 genes by reverse transcriptase-polymerase chain reaction (RT-PCR) that were predicted to have cancer-specific alternative splicing by using the splicing database, the Alternative Splicing Annotation Project (ASAP) by Lee et al, between 38 cancer cell lines from various organs and 9 corresponding normal tissues. By designing 2 types of primer sets for RT-PCR including (1) primers flanking the alternatively spliced exons and (2) primers spanning the exon/exon junctions, cancer-associated splicing variants were investigated.

RESULTS

The alternatively splicing events were detected in 15 of 17 genes (88%); 35 of 43 variants (81%) were detected successfully with RT-PCR. Among these variants, M-RIP, HYAL2, CDCA1, and MSMB genes showed differential expressions between cancer cell lines and corresponding normal tissues. Furthermore, RT-PCR with surgically resected gastric cancer tissues (diffuse type, 6; intestinal type, 4) confirmed that 2 variants of CDCA1 were upregulated in cancer tissues, whereas both variants of MSMB were expressed predominantly in normal tissues.

CONCLUSION

Alternative splicing variants, especially in CDCA1, were detected in this study and may be potentially useful as diagnostic markers and/or novel targets for anticancer therapy.

摘要

背景

可变剪接是一种分子机制,通过该机制外显子的不同组合可被选择性剪接以产生不同的mRNA异构体。最近,已发布了几个数据库来预测mRNA的可变剪接;这些数据库也已用于预测癌症特异性可变剪接。这些变体可能是癌症治疗的潜在有用靶点,然而,这些数据库的准确性和真实性尚未得到证实。

方法

在本研究中,我们通过逆转录聚合酶链反应(RT-PCR)分析了17个基因,这些基因通过使用Lee等人的剪接数据库——可变剪接注释项目(ASAP),被预测具有癌症特异性可变剪接,样本来自38种不同器官的癌细胞系和9种相应的正常组织。通过设计2种用于RT-PCR的引物组,包括(1)位于可变剪接外显子侧翼的引物和(2)跨越外显子/外显子连接点的引物,研究了与癌症相关的剪接变体。

结果

在17个基因中的15个(88%)中检测到可变剪接事件;43个变体中的35个(81%)通过RT-PCR成功检测到。在这些变体中,M-RIP、HYAL2、CDCA1和MSMB基因在癌细胞系和相应正常组织之间表现出差异表达。此外,对手术切除的胃癌组织(弥漫型,6例;肠型,4例)进行的RT-PCR证实,CDCA1的2个变体在癌组织中上调,而MSMB的2个变体主要在正常组织中表达。

结论

在本研究中检测到可变剪接变体,尤其是CDCA1中的变体,它们可能作为诊断标志物和/或抗癌治疗的新靶点具有潜在用途。

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