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侵袭性前列腺癌中缺氧反应基因的超诱导性,无p53/p21依赖的细胞周期检查点。

Hyperinducibility of hypoxia-responsive genes without p53/p21-dependent checkpoint in aggressive prostate cancer.

作者信息

Salnikow K, Costa M, Figg W D, Blagosklonny M V

机构信息

Nelson Institute of Environmental Medicine, and Kaplan Comprehensive Cancer Center, New York University School of Medicine, New York 10016, USA.

出版信息

Cancer Res. 2000 Oct 15;60(20):5630-4.

Abstract

Hypoxia limits tumor growth but selects for higher metastatic potential. We tested the functional activity of hypoxia-inducible factor-1 (HIF-1) in prostate cell lines ranging from normal epithelial cells (PrEC), hormone-dependent LNCaP, hormone-independent DU145, PC-3 to highly metastatic PC-3M cancer cell lines. We found that HIF-1-stimulated transcription was the lowest in PrEC and LNCaP cells and the highest in PC-3M cells. The induction by hypoxia of the HIF-1 dependent genes Cap43 and GAPDH was the highest in the most aggressive PC-3M cancer cells. Because these advanced prostate cancer cell lines have lost p53 function, this further shifts a balance from p53 to HIF-1 transcriptional regulation, and a high ratio of HIF-1-dependent:p53-dependent transcription was a marker of the advanced malignant phenotype. Transient transfection of HIF-1alpha expression vector induced transcription from p21 promoter construct in prostate cancer cell lines. Furthermore, hypoxia slightly induced p21 mRNA in these cells. However, neither expression of p21 nor hypoxia caused growth arrest in PC-3M cells. Therefore, high inducibility of HIF-1-dependent genes, loss of p53 functions with high ratio of HIF-1-dependent:p53-dependent transcription, and loss of sensitivity to p21 inhibition is a part of hypoxic phenotype associated with aggressive cancer behavior.

摘要

缺氧限制肿瘤生长,但会选择具有更高转移潜能的细胞。我们检测了缺氧诱导因子-1(HIF-1)在一系列前列腺细胞系中的功能活性,这些细胞系包括正常上皮细胞(PrEC)、激素依赖型LNCaP、激素非依赖型DU145、PC-3以及高转移性PC-3M癌细胞系。我们发现,HIF-1刺激的转录在PrEC和LNCaP细胞中最低,而在PC-3M细胞中最高。缺氧对HIF-1依赖基因Cap43和GAPDH的诱导在最具侵袭性的PC-3M癌细胞中最高。由于这些晚期前列腺癌细胞系已丧失p53功能,这进一步使平衡从p53转录调控转向HIF-1转录调控,且HIF-1依赖型转录与p53依赖型转录的高比例是晚期恶性表型的一个标志。在前列腺癌细胞系中瞬时转染HIF-1α表达载体可诱导p21启动子构建体的转录。此外,缺氧在这些细胞中轻微诱导p21 mRNA表达。然而,p21的表达和缺氧均未导致PC-3M细胞生长停滞。因此,HIF-1依赖基因的高诱导性、p53功能丧失以及HIF-1依赖型转录与p53依赖型转录的高比例,以及对p21抑制的敏感性丧失,是与侵袭性癌症行为相关的缺氧表型的一部分。

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