血清小rna深度测序鉴定与乳腺癌相关的5' tRNA半和YRNA片段表达模式

Biomarkers in cancer Pub Date : 2014-12-08 eCollection Date: 2014-01-01 DOI:10.4137/BIC.S20764
Joseph M Dhahbi, Stephen R Spindler, Hani Atamna, Dario Boffelli, David Ik Martin
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引用次数: 145

摘要

血液中循环的小非编码rna可以作为信号分子,因为它们具有执行各种细胞功能的能力。我们之前已经描述了tRNA和yrna衍生的小rna作为人类和小鼠血液中较大复合物的组成部分循环;这些小rna的特性意味着特定的加工、分泌和生理调节。在这项研究中,我们询问了这些tRNA和YRNA片段的血清丰度的变化是否与癌症的诊断有关。我们使用深度测序和信息学分析对乳腺癌病例和正常对照血清中的小rna进行分类。5' tRNA半段和YRNA片段在两组中都很丰富,但我们发现乳腺癌的诊断与特定亚型水平的变化有关。这促使我们查看现有的42例乳腺癌病例的血清小rna序列数据集,这些数据是在诊断时采集的。我们发现与癌症临床病理特征相关的特定5' tRNA半和YRNA片段水平的显著变化。虽然这些发现没有建立因果关系,但它们表明循环的5' tRNA一半和具有已知细胞功能的YRNA片段可能参与乳腺癌综合征,并具有作为循环生物标志物的潜力。需要对多种类型的癌症进行更大规模的研究,以充分评估它们在发展非侵入性癌症筛查方面的潜在用途。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Deep Sequencing of Serum Small RNAs Identifies Patterns of 5' tRNA Half and YRNA Fragment Expression Associated with Breast Cancer.

Deep Sequencing of Serum Small RNAs Identifies Patterns of 5' tRNA Half and YRNA Fragment Expression Associated with Breast Cancer.

Deep Sequencing of Serum Small RNAs Identifies Patterns of 5' tRNA Half and YRNA Fragment Expression Associated with Breast Cancer.

Deep Sequencing of Serum Small RNAs Identifies Patterns of 5' tRNA Half and YRNA Fragment Expression Associated with Breast Cancer.

Small noncoding RNAs circulating in the blood may serve as signaling molecules because of their ability to carry out a variety of cellular functions. We have previously described tRNA- and YRNA-derived small RNAs circulating as components of larger complexes in the blood of humans and mice; the characteristics of these small RNAs imply specific processing, secretion, and physiological regulation. In this study, we have asked if changes in the serum abundance of these tRNA and YRNA fragments are associated with a diagnosis of cancer. We used deep sequencing and informatics analysis to catalog small RNAs in the sera of breast cancer cases and normal controls. 5' tRNA halves and YRNA fragments are abundant in both groups, but we found that a breast cancer diagnosis is associated with changes in levels of specific subtypes. This prompted us to look at existing sequence datasets of serum small RNAs from 42 breast cancer cases, taken at the time of diagnosis. We find significant changes in the levels of specific 5' tRNA halves and YRNA fragments associated with clinicopathologic characteristics of the cancer. Although these findings do not establish causality, they suggest that circulating 5' tRNA halves and YRNA fragments with known cellular functions may participate in breast cancer syndromes and have potential as circulating biomarkers. Larger studies with multiple types of cancer are needed to adequately evaluate their potential use for the development of noninvasive cancer screening.

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