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首页> 外文期刊>Proteomes >Comprehensive Analysis of Cancer-Proteogenome to Identify Biomarkers for the Early Diagnosis and Prognosis of Cancer
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Comprehensive Analysis of Cancer-Proteogenome to Identify Biomarkers for the Early Diagnosis and Prognosis of Cancer

机译:癌症-蛋白质组学的综合分析,以识别生物标志物,以用于癌症的早期诊断和预后

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During the past century, our understanding of cancer diagnosis and treatment has been based on a monogenic approach, and as a consequence our knowledge of the clinical genetic underpinnings of cancer is incomplete. Since the completion of the human genome in 2003, it has steered us into therapeutic target discovery, enabling us to mine the genome using cutting edge proteogenomics tools. A number of novel and promising cancer targets have emerged from the genome project for diagnostics, therapeutics, and prognostic markers, which are being used to monitor response to cancer treatment. The heterogeneous nature of cancer has hindered progress in understanding the underlying mechanisms that lead to abnormal cellular growth. Since, the start of The Cancer Genome Atlas (TCGA), and the International Genome consortium projects, there has been tremendous progress in genome sequencing and immense numbers of cancer genomes have been completed, and this approach has transformed our understanding of the diagnosis and treatment of different types of cancers. By employing Genomics and proteomics technologies, an immense amount of genomic data is being generated on clinical tumors, which has transformed the cancer landscape and has the potential to transform cancer diagnosis and prognosis. A complete molecular view of the cancer landscape is necessary for understanding the underlying mechanisms of cancer initiation to improve diagnosis and prognosis, which ultimately will lead to personalized treatment. Interestingly, cancer proteome analysis has also allowed us to identify biomarkers to monitor drug and radiation resistance in patients undergoing cancer treatment. Further, TCGA-funded studies have allowed for the genomic and transcriptomic characterization of targeted cancers, this analysis aiding the development of targeted therapies for highly lethal malignancy. High-throughput technologies, such as complete proteome, epigenome, protein?¢????protein interaction, and pharmacogenomics data, are indispensable to glean into the cancer genome and proteome and these approaches have generated multidimensional universal studies of genes and proteins (OMICS) data which has the potential to facilitate precision medicine. However, due to slow progress in computational technologies, the translation of big omics data into their clinical aspects have been slow. In this review, attempts have been made to describe the role of high-throughput genomic and proteomic technologies in identifying a panel of biomarkers which could be used for the early diagnosis and prognosis of cancer.
机译:在过去的一个世纪中,我们对癌症诊断和治疗的理解是基于单基因方法,因此,我们对癌症临床遗传基础的了解还不完善。自从2003年人类基因组完成以来,它引导我们进入了治疗靶标的发现,使我们能够使用最先进的蛋白质组学工具来挖掘基因组。从基因组计划中已经发现了许多新颖且有希望的癌症靶标,用于诊断,治疗和预后标志物,这些标志物被用于监测对癌症治疗的反应。癌症的异质性阻碍了理解导致异常细胞生长的潜在机制的进展。自从癌症基因组图谱(TCGA)的启动以及国际基因组联盟项目开始以来,基因组测序取得了巨大的进展,并且已经完成了众多癌症基因组的构建,这种方法改变了我们对诊断和治疗的理解不同类型的癌症。通过采用基因组学和蛋白质组学技术,正在针对临床肿瘤生成大量的基因组数据,这已改变了癌症格局,并具有改变癌症诊断和预后的潜力。要了解癌症发生的潜在机制以改善诊断和预后,必须全面了解癌症状况的分子观点,最终将导致个性化治疗。有趣的是,癌症蛋白质组分析还使我们能够识别生物标记物,以监测接受癌症治疗的患者的药物和放射线耐药性。此外,TCGA资助的研究已使靶向癌症的基因组和转录组学表征成为可能,该分析有助于开发针对高度致死性恶性肿瘤的靶向疗法。高通量的技术,例如完整的蛋白质组学,表观基因组,蛋白质,蛋白质相互作用以及药物基因组学数据,对于收集癌症基因组和蛋白质组学是必不可少的,这些方法已经产生了基因和蛋白质的多维通用研究(OMICS )有可能促进精密医学发展的数据。但是,由于计算技术的进展缓慢,大组学数据在其临床方面的转换一直很缓慢。在这篇综述中,已经尝试描述高通量基因组学和蛋白质组学技术在鉴定一组可用于癌症的早期诊断和预后的生物标志物中的作用。

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