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Circulating biomarkers in renal cell carcinoma: the link between microRNAs and extracellular vesicles, where are we now?

机译:肾细胞癌中的循环生物标志物:MicroRNA和细胞外囊泡之间的联系,我们现在在哪里?

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摘要

Renal cell carcinoma (RCC) is a lethal urological cancer, with incidence and mortality rates increasing by 2-3% per decade. The lack of   standard screening tests contributes to the fact that one-third of patients are diagnosed with locally invasive or metastatic disease. Moreover, 20-40% of RCC patients submitted to surgical nephrectomy will develop metastasis. MicroRNAs (miRNAs) are small non-coding RNAs responsible for gene regulation at a post-transcriptional level.  It is accepted that they are deregulated in cancer and can influence tumor development. Thus, miRNAs are promising RCC biomarkers, since they can be detected using non-invasive methods. They are highly stable and easier to quantify in circulating biofluids. The elevated miRNA stability in circulating samples may be the consequence of their capacity to circulate inside of extracellular microvesicles (EMVs), for example, the exosomes.  The EMVs are bilayered membrane vesicles secreted by all cell types. They can be released in the interstitial space or into circulating biofluids, which allows the travelling, binding and entrance of these vesicles in receptor cells. This type of cell communication can shuttle bioactive molecules between cells, allowing the horizontal transference of genetic material. In this review, we focus on circulating miRNAs (miR-210, miR-1233, miR-221, miR-15a, miR-451, miR-508, miR-378) in the biofluids of RCC patients and attempt to establish the diagnostic and prognostic accuracy, their synergic effects, and the pathways involved in RCC biology.
机译:肾细胞癌(RCC)是一种致命的泌尿外癌,发病率和死亡率每十年增加2-3%。缺乏标准筛查测试有助于患者诊断患有局部侵入性或转移性疾病的患者的事实。此外,20-40%的RCC患者提交给外科肾切除术将产生转移。 MicroRNAS(miRNA)是在转录后水平的基因调节中的小非编码RNA。它被认为它们在癌症中造成危险,可以影响肿瘤发育。因此,miRNA是有前途的RCC生物标志物,因为可以使用非侵入性方法检测它们。它们在循环生物流体中非常稳定,更容易定量。循环样品中的升高的miRNA稳定性可能是它们在细胞外微泡(EMV)内部循环的能力的结果,例如外泌体。 EMV是由所有细胞类型分泌的双层膜囊泡。它们可以在间质空间或循环生物流体中释放,这允许在受体细胞中允许这些囊泡的行进,结合和入口。这种类型的细胞通信可以在细胞之间穿梭生物活性分子,允许遗传物质的水平转移。在本次综述中,我们专注于RCC患者生物流体的循环miRNA(miR-210,miR-1233,miR-221,miR-15a,miR-451,miR-508,miR-378),并试图建立诊断和预后的准确性,它们的协同效应和参与RCC生物学的途径。

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