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前列腺癌患者的循环 RNA。

Circulating RNAs in prostate cancer patients.

机构信息

Department of Cellular, Computational and Integrative Biology (CIBIO), University of Trento, Trento, Italy.

Department of Cellular, Computational and Integrative Biology (CIBIO), University of Trento, Trento, Italy.

出版信息

Cancer Lett. 2022 Jan 1;524:57-69. doi: 10.1016/j.canlet.2021.10.011. Epub 2021 Oct 14.

Abstract

Growing bodies of evidence have demonstrated that the identification of prostate cancer (PCa) biomarkers in the patients' blood and urine may remarkably improve PCa diagnosis and progression monitoring. Among diverse cancer-derived circulating materials, extracellular RNA molecules (exRNAs) represent a compelling component to investigate cancer-related alterations. Once outside the intracellular environment, exRNAs circulate in biofluids either in association with protein complexes or encapsulated inside extracellular vesicles (EVs). Notably, EV-associated RNAs (EV-RNAs) were used for the development of several assays (such as the FDA-approved Progensa Prostate Cancer Antigen 3 (PCA3 test) aiming at improving early PCa detection. EV-RNAs encompass a mixture of species, including small non-coding RNAs (e.g. miRNA and circRNA), lncRNAs and mRNAs. Several methods have been proposed to isolate EVs and relevant RNAs, and to perform RNA-Seq studies to identify potential cancer biomarkers. However, EVs in the circulation of a cancer patient include a multitude of diverse populations that are released by both cancer and normal cells from different tissues, thereby leading to a heterogeneous EV-RNA-associated transcriptional signal. Decrypting the complexity of such a composite signal is nowadays the major challenge faced in the identification of specific tumor-associated RNAs. Multiple deconvolution algorithms have been proposed so far to infer the enrichment of cancer-specific signals from gene expression data. However, novel strategies for EVs sorting and sequencing of RNA associated to single EVs populations will remarkably facilitate the identification of cancer-related molecules. Altogether, the studies summarized here demonstrate the high potential of using EV-RNA biomarkers in PCa and highlight the urgent need of improving technologies and computational approaches to characterize specific EVs populations and their relevant RNA cargo.

摘要

越来越多的证据表明,在患者的血液和尿液中鉴定前列腺癌(PCa)生物标志物可以显著提高 PCa 的诊断和进展监测。在各种癌症来源的循环物质中,细胞外 RNA 分子(exRNAs)是研究与癌症相关变化的一个引人注目的组成部分。一旦离开细胞内环境,exRNAs 就在生物体液中循环,要么与蛋白复合物结合,要么包裹在细胞外囊泡(EVs)中。值得注意的是,EV 相关 RNA(EV-RNAs)被用于开发几种检测方法(如 FDA 批准的 Progensa 前列腺癌抗原 3(PCA3 测试),旨在提高早期 PCa 的检测。EV-RNAs 包含多种物种,包括小非编码 RNA(如 miRNA 和 circRNA)、lncRNAs 和 mRNAs。已经提出了几种方法来分离 EV 和相关的 RNA,并进行 RNA-Seq 研究以鉴定潜在的癌症生物标志物。然而,癌症患者循环中的 EV 包含了由不同组织的癌症和正常细胞释放的多种不同群体,从而导致了异质性的 EV-RNA 相关转录信号。解析这种复杂信号的复杂性是目前在鉴定特定肿瘤相关 RNA 时面临的主要挑战。迄今为止,已经提出了多种去卷积算法来从基因表达数据中推断癌症特异性信号的富集。然而,用于 EV 排序和对与单个 EV 群体相关的 RNA 进行测序的新策略将极大地促进对癌症相关分子的识别。总之,这里总结的研究表明,使用 EV-RNA 生物标志物在 PCa 中的潜力很高,并强调了迫切需要改进技术和计算方法来描述特定的 EV 群体及其相关的 RNA 货物。

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