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全球组蛋白修饰模式可预测前列腺癌复发风险。

Global histone modification patterns predict risk of prostate cancer recurrence.

作者信息

Seligson David B, Horvath Steve, Shi Tao, Yu Hong, Tze Sheila, Grunstein Michael, Kurdistani Siavash K

机构信息

Department of Pathology and Laboratory Medicine, David Geffen School of Medicine, University of California, Los Angeles, California 90095, USA.

出版信息

Nature. 2005 Jun 30;435(7046):1262-6. doi: 10.1038/nature03672.

Abstract

Aberrations in post-translational modifications of histones have been shown to occur in cancer cells but only at individual promoters; they have not been related to clinical outcome. Other than being targeted to promoters, modifications of histones, such as acetylation and methylation of lysine and arginine residues, also occur over large regions of chromatin including coding regions and non-promoter sequences, which are referred to as global histone modifications. Here we show that changes in global levels of individual histone modifications are also associated with cancer and that these changes are predictive of clinical outcome. Through immunohistochemical staining of primary prostatectomy tissue samples, we determined the percentage of cells that stained for the histone acetylation and dimethylation of five residues in histones H3 and H4. Grouping of samples with similar patterns of modifications identified two disease subtypes with distinct risks of tumour recurrence in patients with low-grade prostate cancer. These histone modification patterns were predictors of outcome independently of tumour stage, preoperative prostate-specific antigen levels, and capsule invasion. Thus, widespread changes in specific histone modifications indicate previously undescribed molecular heterogeneity in prostate cancer and might underlie the broad range of clinical behaviour in cancer patients.

摘要

组蛋白翻译后修饰的异常已被证明在癌细胞中存在,但仅发生在个别启动子上;它们与临床结果并无关联。除了作用于启动子外,组蛋白的修饰,如赖氨酸和精氨酸残基的乙酰化和甲基化,也发生在包括编码区和非启动子序列在内的大片染色质区域,这些被称为整体组蛋白修饰。在此我们表明,个别组蛋白修饰的整体水平变化也与癌症相关,并且这些变化可预测临床结果。通过对原发性前列腺切除组织样本进行免疫组织化学染色,我们确定了对组蛋白H3和H4中五个残基的组蛋白乙酰化和二甲基化呈阳性染色的细胞百分比。对具有相似修饰模式的样本进行分组,识别出了两种疾病亚型,它们在低级别前列腺癌患者中具有不同的肿瘤复发风险。这些组蛋白修饰模式是独立于肿瘤分期、术前前列腺特异性抗原水平和包膜侵犯的预后预测指标。因此,特定组蛋白修饰的广泛变化表明前列腺癌中存在先前未描述的分子异质性,并且可能是癌症患者广泛临床行为的基础。

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