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人类癌症中 let-7 家族的基因组 DNA 拷贝数改变。

Genomic DNA copy-number alterations of the let-7 family in human cancers.

机构信息

Department of Obstetrics and Gynecology; University of Pennsylvania, Philadelphia, Pennsylvania, United States of America.

出版信息

PLoS One. 2012;7(9):e44399. doi: 10.1371/journal.pone.0044399. Epub 2012 Sep 6.

Abstract

In human cancer, expression of the let-7 family is significantly reduced, and this is associated with shorter survival times in patients. However, the mechanisms leading to let-7 downregulation in cancer are still largely unclear. Since an alteration in copy-number is one of the causes of gene deregulation in cancer, we examined copy number alterations of the let-7 family in 2,969 cancer specimens from a high-resolution SNP array dataset. We found that there was a reduction in the copy number of let-7 genes in a cancer-type specific manner. Importantly, focal deletion of four let-7 family members was found in three cancer types: medulloblastoma (let-7a-2 and let-7e), breast cancer (let-7a-2), and ovarian cancer (let-7a-3/let-7b). For example, the genomic locus harboring let-7a-3/let-7b was deleted in 44% of the specimens from ovarian cancer patients. We also found a positive correlation between the copy number of let-7b and mature let-7b expression in ovarian cancer. Finally, we showed that restoration of let-7b expression dramatically reduced ovarian tumor growth in vitro and in vivo. Our results indicate that copy number deletion is an important mechanism leading to the downregulation of expression of specific let-7 family members in medulloblastoma, breast, and ovarian cancers. Restoration of let-7 expression in tumor cells could provide a novel therapeutic strategy for the treatment of cancer.

摘要

在人类癌症中,let-7 家族的表达显著降低,这与患者的生存时间较短有关。然而,导致癌症中 let-7 下调的机制在很大程度上仍不清楚。由于拷贝数的改变是癌症中基因失调的原因之一,我们在一个高分辨率 SNP 阵列数据集的 2969 个癌症样本中检查了 let-7 家族的拷贝数改变。我们发现 let-7 基因的拷贝数以癌症类型特异性的方式减少。重要的是,在三种癌症类型中发现了四个 let-7 家族成员的焦点缺失:髓母细胞瘤(let-7a-2 和 let-7e)、乳腺癌(let-7a-2)和卵巢癌(let-7a-3/let-7b)。例如,卵巢癌患者标本中约 44%的 let-7a-3/let-7b 基因组位点缺失。我们还发现卵巢癌中 let-7b 的拷贝数与成熟 let-7b 表达之间存在正相关。最后,我们表明 let-7b 表达的恢复显著降低了体外和体内卵巢肿瘤的生长。我们的结果表明,拷贝数缺失是导致髓母细胞瘤、乳腺癌和卵巢癌中特定 let-7 家族成员表达下调的重要机制。恢复肿瘤细胞中的 let-7 表达可能为癌症治疗提供一种新的治疗策略。

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