DNA 高甲基化生物标志物预测顺铂治疗、放疗或放化疗反应：现状。

DNA hypermethylation biomarkers to predict response to cisplatin treatment, radiotherapy or chemoradiation: the present state of art.

机构信息

Department of Gynecologic Oncology, University of Groningen, University Medical Center Groningen, The Netherlands.

出版信息

Cell Oncol (Dordr). 2012 Aug;35(4):231-41. doi: 10.1007/s13402-012-0091-7. Epub 2012 Jul 27.

DOI:10.1007/s13402-012-0091-7

PMID:22836879

Abstract

BACKGROUND

Concurrent platinum-based chemoradiation significantly improved survival of advanced stage cervical patients over radiotherapy alone. However, the 5-year overall survival is still only 66%. Presently, no biomarkers are available to select those cervical cancer patients that might benefit from concurrent platinum-based chemoradiation therapy. DNA methylation is a well-established contributor to the regulation of gene transcription, predominantly causing transcriptional silencing. Differences in promoter hypermethylation patterns and subsequent silencing, could contribute to the variety of responses observed in clinical practice. Several clinical trials on various malignancies reported a better response when Decitabine was administered prior to or in combination with standard therapy. This sensitization is thought to be due to re-expression of tumor suppressor genes. However, not all patients might benefit from demethylating agents, since re-expression of oncogenes could render patients more resistant.

AIM

In this review, we summarized the present state of art regarding hypermethylated genes and their affected signaling pathways that are associated with outcome after cisplatin treatment, radiotherapy or chemoradiation. Since only few studies were reported in cervical cancer, other malignancies were reviewed as well.

CONCLUSIONS

From the data presented in this review, we conclude that, in order to select patients that benefit most optimally from demethylating strategies, a comprehensive screening of a large panel of methylation markers, associated with both good as well as poor clinical outcome have to be investigated. Since such panels are not available at this moment, global methylation screening approaches are required to profile such methylated genes. Such methylated gene profiles might be very useful to optimize personalized treatment planning not only in cervical cancer but also in other malignancies.

摘要

背景

与单独放疗相比，同步铂类放化疗显著提高了晚期宫颈癌患者的生存率。然而，5 年总生存率仍只有 66%。目前，尚无生物标志物可用于选择那些可能受益于同步铂类放化疗的宫颈癌患者。DNA 甲基化是调节基因转录的一种成熟机制，主要导致转录沉默。启动子超甲基化模式和随后的沉默差异可能导致临床实践中观察到的各种反应。几项针对各种恶性肿瘤的临床试验报告称，在标准治疗前或联合使用地西他滨时，反应更好。这种增敏作用被认为是由于肿瘤抑制基因的重新表达。然而，并非所有患者都可能受益于去甲基化剂，因为癌基因的重新表达可能使患者更具耐药性。

目的

在这篇综述中，我们总结了目前关于与顺铂治疗、放疗或放化疗后结局相关的高甲基化基因及其受影响的信号通路的研究现状。由于宫颈癌的报道较少，因此还对其他恶性肿瘤进行了综述。

结论

根据本综述中提供的数据，我们得出结论，为了选择最能从去甲基化策略中受益的患者，必须对与良好和不良临床结局相关的大量甲基化标记物进行综合筛选。由于目前还没有这样的标志物，因此需要进行全基因组甲基化筛选方法来对这些甲基化基因进行分析。这些甲基化基因图谱可能非常有助于优化不仅在宫颈癌而且在其他恶性肿瘤中的个体化治疗计划。

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DNA 高甲基化生物标志物预测顺铂治疗、放疗或放化疗反应：现状。

DNA hypermethylation biomarkers to predict response to cisplatin treatment, radiotherapy or chemoradiation: the present state of art.

机构信息

出版信息

BACKGROUND

AIM

CONCLUSIONS

背景

目的

结论

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