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CD24 是 HIF-1 驱动的原发性肿瘤生长和转移的效应因子。

CD24 is an effector of HIF-1-driven primary tumor growth and metastasis.

机构信息

Departments of Urology, University of Virginia, Charlottesville, Virginia, USA.

出版信息

Cancer Res. 2012 Nov 1;72(21):5600-12. doi: 10.1158/0008-5472.CAN-11-3666. Epub 2012 Aug 27.

Abstract

Hypoxia drives malignant progression in part by promoting accumulation of the oncogenic transcription factor hypoxia inducible factor-1α (HIF-1α) in tumor cells. Tumor aggressiveness also relates to elevation of the cancer stem cell-associated membrane protein CD24, which has been causally implicated in tumor formation and metastasis in experimental models. Here, we link these two elements by showing that hypoxia induces CD24 expression through a functional hypoxia responsive element in the CD24 promoter. HIF-1α overexpression induced CD24 mRNA and protein under normoxic conditions, with this effect traced to a recruitment of endogenous HIF-1α to the CD24 promoter. Short hairpin RNA-mediated attenuation of HIF-1α or CD24 expression reduced cancer cell survival in vitro and in vivo at the levels of primary and metastatic tumor growth. CD24 overexpression in HIF-1α-depleted cancer cells rescued this decrease, whereas HIF-1α overexpression in CD24-depleted cells did not. Analysis of clinical tumor specimens revealed a correlation between HIF-1α and CD24 levels and an association of their coexpression to decreased patient survival. Our results establish a mechanistic linkage between 2 critically important molecules in cancer, identifying CD24 as a critical HIF-1α transcriptional target and biologic effector, strengthening the rationale to target CD24 for cancer therapy.

摘要

缺氧在一定程度上通过促进肿瘤细胞中致癌转录因子缺氧诱导因子-1α(HIF-1α)的积累来驱动恶性进展。肿瘤侵袭性也与癌症干细胞相关的膜蛋白 CD24 的升高有关,在实验模型中,CD24 已被因果关系牵连到肿瘤形成和转移中。在这里,我们通过显示缺氧通过 CD24 启动子中的功能性缺氧反应元件诱导 CD24 表达将这两个元素联系起来。HIF-1α 在常氧条件下过表达诱导 CD24 mRNA 和蛋白,这种效应可追溯到内源性 HIF-1α 募集到 CD24 启动子。短发夹 RNA 介导的 HIF-1α 或 CD24 表达衰减可降低体外和体内原代和转移性肿瘤生长水平的癌细胞存活。在 HIF-1α 耗尽的癌细胞中过表达 CD24 可挽救这种减少,而在 CD24 耗尽的细胞中过表达 HIF-1α 则不行。对临床肿瘤标本的分析揭示了 HIF-1α 和 CD24 水平之间的相关性,以及它们共表达与患者生存时间缩短之间的关联。我们的结果确立了癌症中两个至关重要的分子之间的机制联系,将 CD24 鉴定为 HIF-1α 的关键转录靶标和生物学效应物,为针对 CD24 进行癌症治疗提供了更强的理论依据。

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