比较人类结直肠癌中的DNA高甲基化组与基因突变情况。

Comparing the DNA hypermethylome with gene mutations in human colorectal cancer.

作者信息

Schuebel Kornel E, Chen Wei, Cope Leslie, Glöckner Sabine C, Suzuki Hiromu, Yi Joo-Mi, Chan Timothy A, Van Neste Leander, Van Criekinge Wim, van den Bosch Sandra, van Engeland Manon, Ting Angela H, Jair Kamwing, Yu Wayne, Toyota Minoru, Imai Kohzoh, Ahuja Nita, Herman James G, Baylin Stephen B

机构信息

Cancer Biology Division, The Sidney Kimmel Comprehensive Cancer Center at Johns Hopkins, Baltimore, Maryland, USA.

出版信息

PLoS Genet. 2007 Sep;3(9):1709-23. doi: 10.1371/journal.pgen.0030157. Epub 2007 Jul 31.

DOI:10.1371/journal.pgen.0030157

PMID:17892325

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1988850/

Abstract

We have developed a transcriptome-wide approach to identify genes affected by promoter CpG island DNA hypermethylation and transcriptional silencing in colorectal cancer. By screening cell lines and validating tumor-specific hypermethylation in a panel of primary human colorectal cancer samples, we estimate that nearly 5% or more of all known genes may be promoter methylated in an individual tumor. When directly compared to gene mutations, we find larger numbers of genes hypermethylated in individual tumors, and a higher frequency of hypermethylation within individual genes harboring either genetic or epigenetic changes. Thus, to enumerate the full spectrum of alterations in the human cancer genome, and to facilitate the most efficacious grouping of tumors to identify cancer biomarkers and tailor therapeutic approaches, both genetic and epigenetic screens should be undertaken.

摘要

我们已经开发出一种全转录组方法，用于识别在结直肠癌中受启动子CpG岛DNA高甲基化和转录沉默影响的基因。通过筛选细胞系并在一组原发性人类结直肠癌样本中验证肿瘤特异性高甲基化，我们估计在单个肿瘤中，所有已知基因中可能有近5%或更多的基因启动子发生甲基化。当与基因突变直接比较时，我们发现在单个肿瘤中发生高甲基化的基因数量更多，并且在具有遗传或表观遗传变化的单个基因内，高甲基化的频率更高。因此，为了全面列举人类癌症基因组中的改变谱，并促进对肿瘤进行最有效的分组以识别癌症生物标志物并定制治疗方法，应该同时进行遗传和表观遗传筛查。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2234/1994703/d48d4be1da3f/pgen.0030157.g001.jpg

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比较人类结直肠癌中的DNA高甲基化组与基因突变情况。

Comparing the DNA hypermethylome with gene mutations in human colorectal cancer.

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