微小RNA通过个性化药物改善癌症治疗结果。

Saeid Hatam
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引用次数: 0

摘要

微小RNA(miRNA)是一种短的非编码RNA,可抑制或降解mRNA靶点以下调基因。在癌症的发生中,miRNA的表达发生了改变。根据某种miRNA在肿瘤发病生长中的参与程度,它可能上调或下调。miRNA的“致癌”作用与上调相对应,上调导致肿瘤增殖和扩散,同时下调的miRNA带来肿瘤抑制结果。癌基因和抑癌基因是其表达受其控制的基因之一,这表明将它们单独归类为癌基因或抑癌基因不仅阻碍而且不正确。除了基本肿瘤外,miRNA可能存在于几乎所有的体液中,可用于癌症诊断、临床结果预测和对治疗策略的更好反应。这些微小的非编码RNA的总体变异影响抗癌药物的患者特异性药代动力学和药效学,推动了对个性化药物的需求不断增长。到目前为止,来自肿瘤活检或血液的微小RNA作为癌症在时间诊断、预后和进展方面的重要生物标志物正在被广泛研究。随着新冠肺炎的兴起,本文还试图研究与癌症COVID患者死亡有关的miRNA的最新研究。随着单核苷酸多态性的发现,通过微小RNA进行个性化治疗已成为现实。这篇综述文章描述了miRNA在各种癌症中的最新知识,重点是miRNA翻译应用作为创新的潜在诊断和预后指标,以扩大人与人之间的治疗选择。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
MicroRNAs Improve Cancer Treatment Outcomes Through Personalized Medicine.

MicroRNAs (miRNAs) are short non-coding RNAs that repress or degrade mRNA targets to downregulate genes. In cancer occurrence, the expression of miRNAs is altered. Depending on the involvement of a certain miRNA in the pathogenetic growth of a tumor, It may be up or downregulated. The "oncogenic" action of miRNAs corresponds with upregulation, which leads to tumor proliferation and spread meanwhile the miRNAs that have been downregulated bring tumorsuppressive outcomes. Oncogenes and tumor suppressor genes are among the genes whose expression is under their control, demonstrating that classifying them solely as oncogenes or tumor suppressor genes alone is not only hindering but also incorrect. Apart from basic tumors, miRNAs may be found in nearly all human fluids and can be used for cancer diagnosis as well as clinical outcome prognostics and better response to treatment strategies. The overall variance of these tiny noncoding RNAs influences patient-specific pharmacokinetics and pharmacodynamics of anti-cancer medicines, driving a growing demand for personalized medicine. By now, microRNAs from tumor biopsies or blood are being widely investigated as substantial biomarkers for cancer in time diagnosis, prognosis, and, progression. With the rise of COVID-19, this paper also attempts to study recent research on miRNAs involved with deaths in lung cancer COVID patients. With the discovery of single nucleotide polymorphisms, personalized treatment via microRNAs has lately become a reality. The present review article describes the highlights of recent knowledge of miRNAs in various cancers, with a focus on miRNA translational applications as innovative potential diagnostic and prognostic indicators that expand person-to-person therapy options.

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