Beaulieu Normand, Morin Steves, Chute Ian C, Robert Marie-France, Nguyen Hannah, MacLeod A Robert
Department of Molecular Biology, MethylGene Inc., Montreal H4S 2A1, Canada.
J Biol Chem. 2002 Aug 2;277(31):28176-81. doi: 10.1074/jbc.M204734200. Epub 2002 May 15.
Abnormal methylation and associated silencing of tumor suppressor genes is a common feature of many types of cancers. The observation of persistent methylation in human cancer cells lacking the maintenance methyltransferase DNMT1 suggests the involvement of other DNA methyltransferases in gene silencing in cancer. To test this hypothesis, we have evaluated methylation and gene expression in cancer cells specifically depleted of DNMT3A or DNMT3B, de novo methyltransferases that are expressed in adult tissues. Here we have shown that depletion of DNMT3B, but not DNMT3A, induced apoptosis of human cancer cells but not normal cells. DNMT3B depletion reactivated methylation-silenced gene expression but did not induce global or juxtacentromeric satellite demethylation as did specific depletion of DNMT1. Furthermore, the effect of DNMT3B depletion was rescued by exogenous expression of either of the splice variants DNMT3B2 or DNMT3B3 but not DNMT1. These results indicate that DNMT3B has significant site selectivity that is distinct from DNMT1, regulates aberrant gene silencing, and is essential for cancer cell survival.
肿瘤抑制基因的异常甲基化及相关沉默是多种癌症的共同特征。在缺乏维持性甲基转移酶DNMT1的人类癌细胞中观察到持续性甲基化,这表明其他DNA甲基转移酶参与了癌症中的基因沉默。为了验证这一假设,我们评估了在特异性缺失DNMT3A或DNMT3B(在成体组织中表达的从头甲基转移酶)的癌细胞中的甲基化和基因表达。在此我们表明,DNMT3B而非DNMT3A的缺失诱导了人类癌细胞而非正常细胞的凋亡。DNMT3B缺失重新激活了甲基化沉默的基因表达,但并未像DNMT1特异性缺失那样诱导全基因组或着丝粒旁卫星序列去甲基化。此外,通过外源性表达剪接变体DNMT3B2或DNMT3B3而非DNMT1可挽救DNMT3B缺失的影响。这些结果表明,DNMT3B具有与DNMT1不同的显著位点选择性,调节异常基因沉默,并且对癌细胞存活至关重要。
