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PLCD1 is a functional tumor suppressor inducing G(2)/M arrest and frequently methylated in breast cancer.

机译:PLCD1是一种功能性肿瘤抑制因子,可诱导G(2)/ M停滞,并经常在乳腺癌中甲基化。

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摘要

Chromosome 3p harbors multiple tumor-suppressor genes. PLCD1, located at 3p22, encodes an enzyme that mediates regulatory signaling of energy metabolism, calcium homeostasis and intracellular movement. We investigated the epigenetic alterations of PLCD1 and its tumor suppressor function in breast cancer. Frequent downregulation/silencing of PLCD1 was shown in most breast cancer cell lines by using semi-quantitative PCR. Promoter methylation of PLCD1 was detected in 78% (7/9) of cell lines and 52% (13/25) of primary tumors by Methylation-specific PCR (MSP), but not in any tumor adjacent breast tissues and normal breast tissues, which was further confirmed by bisulfite genomic sequencing (BGS). The silencing of PLCD1 could be reversed by pharmacological demethylation, indicating a methylation-mediated mechanism. Ectopic expression of PLCD1 in silenced breast cancer cells significantly inhibited their colony formation. In addition, PLCD1 inhibited tumor cell migration and induced cell cycle G(2)/M arrest. Thus, this study for the first time demonstrates the frequent inactivation of PLCD1 by promoter methylation and its tumor inhibitory function in breast cancer. Tumor-specific methylation of PLCD1 might serve as a biomarker for possible early detection and prognosis prediction of breast cancer.
机译:染色体3p包含多个肿瘤抑制基因。位于3p22的PLCD1编码一种酶,该酶介导能量代谢,钙稳态和细胞内运动的调控信号。我们调查了PLCD1在乳腺癌中的表观遗传学改变及其抑癌功能。通过使用半定量PCR,在大多数乳腺癌细胞系中PLCD1频繁下调/沉默。通过甲基化特异性PCR(MSP)在78%(7/9)的细胞系和52%(13/25)的原发性肿瘤中检测到PLCD1的启动子甲基化,但在邻近乳腺组织和正常乳腺组织的任何肿瘤中均未检测到,亚硫酸氢盐基因组测序(BGS)进一步证实了这一点。 PLCD1的沉默可以通过药理学去甲基化逆转,表明甲基化介导的机制。 PLCD1在沉默的乳腺癌细胞中的异位表达显着抑制了其集落形成。此外,PLCD1抑制肿瘤细胞迁移并诱导细胞周期G(2)/ M逮捕。因此,本研究首次证明了启动子甲基化导致PLCD1频繁失活及其在乳腺癌中的肿瘤抑制功能。 PLCD1的肿瘤特异性甲基化可能作为生物标志物,用于乳腺癌的早期检测和预后预测。

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