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Alternative polyadenylation: An untapped source for prostate cancer biomarkers and therapeutic targets?

机译:替代多腺苷酸:前列腺癌生物标志物和治疗靶的未开发源泉?

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ObjectiveTo review alternative polyadenylation (APA) as a mechanism of gene regulation and consider potential roles for APA in prostate cancer (PCa) biology and treatment.MethodsAn extensive review of mRNA polyadenylation, APA, and PCa literature was performed. This review article introduces APA and its association with human disease, outlines the mechanisms and components of APA, reviews APA in cancer biology, and considers whether APA may contribute to PCa progression and/or produce novel biomarkers and therapeutic targets for PCa.ResultsEukaryotic mRNA 3′-end cleavage and polyadenylation play a critical role in gene expression. Most human genes encode more than one polyadenylation signal, and produce more than one transcript isoform, through APA. Polyadenylation can occur throughout the gene body to generate transcripts with differing 3′-termini and coding sequence. Differences in 3′-untranslated regions length can modify post-transcriptional gene regulation by microRNAs and RNA binding proteins, and alter mRNA stability, translation efficiency, and subcellular localization. Distinctive APA patterns are associated with human diseases, tissue origins, and changes in cellular proliferation rate and differentiation state. APA events may therefore generate unique mRNA biomarkers or therapeutic targets in certain cancer types or phenotypic states.ConclusionsThe full extent of cancer-associated and tissue-specific APA events have yet to be defined, and the mechanisms and functional consequences of APA in cancer remain incompletely understood. There is evidence that APA is active in PCa, and that it may be an untapped resource for PCa biomarkers or therapeutic targets.
机译:ObjectiveTo评论替代多腺苷酸化(APA)作为基因调控机制,并考虑前列腺癌(PCA)生物学和治疗中APA的潜在作用。方法进行了对mRNA多腺苷酸,APA和PCA文献的广泛审查。本篇文章介绍了APA及其与人类疾病的关联,概述了APA的机制和组成部分,评论APA在癌症生物学中,并考虑APA是否可能有助于PCA进展和/或生产PCA.ResultseuckarycakaryCRNA的新型生物标志物和治疗靶标。 ' - 乳化和多腺苷酸在基因表达中发挥着关键作用。大多数人基因编码多于一种多腺苷酸化信号,并通过APA产生多于一个转录物同种型。聚酰基化可以在整个基因体中发生,以产生具有不同3'-末端和编码序列的转录物。 3' - 未经翻译的区域的差异长度可以通过MicroRNA和RNA结合蛋白改变转录后基因调节,并改变mRNA稳定性,翻译效率和亚细胞定位。独特的APA模式与人类疾病,组织起源和细胞增殖率和分化状态的变化有关。因此,APA事件可能在某些癌症类型或表型状态下产生独特的mRNA生物标志物或治疗靶。尚未确定癌症相关和组织特异性APA事件的全部范围,并且APA在癌症中的机制和功能后果仍然不完全了解。有证据表明APA在PCA中活跃,并且它可能是PCA生物标志物或治疗目标的未开发资源。

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