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前列腺癌中EFEMP1的表观遗传调控:生物学相关性及临床潜力

Epigenetic regulation of EFEMP1 in prostate cancer: biological relevance and clinical potential.

作者信息

Almeida Mafalda, Costa Vera L, Costa Natália R, Ramalho-Carvalho João, Baptista Tiago, Ribeiro Franclim R, Paulo Paula, Teixeira Manuel R, Oliveira Jorge, Lothe Ragnhild A, Lind Guro E, Henrique Rui, Jerónimo Carmen

机构信息

Cancer Biology and Epigenetics Group, Research Center of the Portuguese Oncology Institute - Porto, Porto, Portugal.

出版信息

J Cell Mol Med. 2014 Nov;18(11):2287-97. doi: 10.1111/jcmm.12394. Epub 2014 Sep 11.

Abstract

Epigenetic alterations are common in prostate cancer (PCa) and seem to contribute decisively to its initiation and progression. Moreover, aberrant promoter methylation is a promising biomarker for non-invasive screening. Herein, we sought to characterize EFEMP1 as biomarker for PCa, unveiling its biological relevance in prostate carcinogenesis. Microarray analyses of treated PCa cell lines and primary tissues enabled the selection of differentially methylated genes, among which EFEMP1 was further validated by MSP and bisulfite sequencing. Assessment of biomarker performance was accomplished by qMSP. Expression analysis of EFEMP1 and characterization of histone marks were performed in tissue samples and cancer cell lines to determine the impact of epigenetic mechanisms on EFEMP1 transcriptional regulation. Phenotypic assays, using transfected cell lines, permitted the evaluation of EFEMP1's role in PCa development. EFEMP1 methylation assay discriminated PCa from normal prostate tissue (NPT; P < 0.001, Kruskall-Wallis test) and renal and bladder cancers (96% sensitivity and 98% specificity). EFEMP1 transcription levels inversely correlated with promoter methylation and histone deacetylation, suggesting that both epigenetic mechanisms are involved in gene regulation. Phenotypic assays showed that EFEMP1 de novo expression reduces malignant phenotype of PCa cells. EFEMP1 promoter methylation is prevalent in PCa and accurately discriminates PCa from non-cancerous prostate tissues and other urological neoplasms. This epigenetic alteration occurs early in prostate carcinogenesis and, in association with histone deacetylation, progressively leads to gene down-regulation, fostering cell proliferation, invasion and evasion of apoptosis.

摘要

表观遗传改变在前列腺癌(PCa)中很常见,似乎对其发生和发展起决定性作用。此外,异常的启动子甲基化是一种有前景的非侵入性筛查生物标志物。在此,我们试图将EFEMP1鉴定为PCa的生物标志物,揭示其在前列腺癌发生中的生物学相关性。对处理过的PCa细胞系和原发性组织进行微阵列分析,从而筛选出差异甲基化基因,其中EFEMP1通过甲基化特异性PCR(MSP)和亚硫酸氢盐测序进一步验证。通过定量甲基化特异性PCR(qMSP)评估生物标志物性能。在组织样本和癌细胞系中进行EFEMP1的表达分析和组蛋白标记特征分析,以确定表观遗传机制对EFEMP1转录调控的影响。使用转染细胞系进行表型分析,以评估EFEMP1在PCa发展中的作用。EFEMP1甲基化检测可区分PCa与正常前列腺组织(NPT;P < 0.001,克鲁斯卡尔-沃利斯检验)以及肾癌和膀胱癌(敏感性96%,特异性98%)。EFEMP1转录水平与启动子甲基化和组蛋白去乙酰化呈负相关,表明这两种表观遗传机制均参与基因调控。表型分析表明,EFEMP1的从头表达可降低PCa细胞的恶性表型。EFEMP1启动子甲基化在PCa中普遍存在,可准确区分PCa与非癌性前列腺组织及其他泌尿系统肿瘤。这种表观遗传改变在前列腺癌发生早期就会出现,并与组蛋白去乙酰化一起,逐渐导致基因下调,促进细胞增殖、侵袭和逃避凋亡。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8eca/4224561/3210d41ec725/jcmm0018-2287-f1.jpg

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