Karni Rotem, Dor Yuval, Keshet Eli, Meyuhas Oded, Levitzki Alexander
Department of Biological Chemistry, The Alexander Silberman Institute of Life Sciences, The Hebrew University of Jerusalem, Jerusalem 91904, Israel.
J Biol Chem. 2002 Nov 8;277(45):42919-25. doi: 10.1074/jbc.M206141200. Epub 2002 Aug 27.
Hypoxia-inducible factor (HIF)-1 is a master transcription factor, which up-regulates glycolysis, erythropoiesis, and angiogenesis under hypoxia. HIF-1alpha accumulates in normoxic tumor cells, leading to glycolysis under aerobic conditions. This phenomenon, known as the "Warburg effect," is caused by a yet unknown mechanism. Here we show that transformed cells that express constitutively active pp60(c-Src) (Src) express HIF-1alpha protein under normoxia, which results in the expression of multiple HIF-1alpha target genes. We show that this occurrence is due to an enhanced rate of HIF-1alpha protein synthesis and not due to reduced HIF-1alpha degradation. Furthermore, we show that the Src-induced increase in protein synthesis is due to the global increase in the rate of cap-dependent translation and does not involve inhibition of HIF-1alpha degradation.
缺氧诱导因子(HIF)-1是一种主要的转录因子,在缺氧条件下可上调糖酵解、红细胞生成和血管生成。HIF-1α在常氧肿瘤细胞中蓄积,导致有氧条件下的糖酵解。这种被称为“瓦伯格效应”的现象是由一种未知机制引起的。在此我们表明,组成型表达活性pp60(c-Src)(Src)的转化细胞在常氧下表达HIF-1α蛋白,这导致多个HIF-1α靶基因的表达。我们表明,这种情况是由于HIF-1α蛋白合成速率增加,而不是由于HIF-1α降解减少。此外,我们表明Src诱导的蛋白质合成增加是由于帽依赖性翻译速率的整体增加,并且不涉及对HIF-1α降解的抑制。
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