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来自缺氧诱导因子-1α(HIF-1α)的两个序列基序与p53的DNA结合位点结合。

Two sequence motifs from HIF-1alpha bind to the DNA-binding site of p53.

作者信息

Hansson Lars O, Friedler Assaf, Freund Stefan, Rudiger Stefan, Fersht Alan R

机构信息

Cambridge Centre for Protein Engineering, Medical Research Council Centre, Hills Road, Cambridge CB2 2QH, United Kingdom.

出版信息

Proc Natl Acad Sci U S A. 2002 Aug 6;99(16):10305-9. doi: 10.1073/pnas.122347199. Epub 2002 Jul 17.

Abstract

There is evidence that hypoxia-inducible factor-1alpha (HIF-1alpha) interacts with the tumor suppressor p53. To characterize the putative interaction, we mapped the binding of the core domain of p53 (p53c) to an array of immobilized HIF-1alpha-derived peptides and found two peptide-sequence motifs that bound to p53c with micromolar affinity in solution. One sequence was adjacent to and the other coincided with the two proline residues of the oxygen-dependent degradation domain (P402 and P564) that act as switches for the oxygen-dependent regulation of HIF-1alpha. The binding affinity was independent of the hydroxylation state of P564. We found from NMR spectroscopy that these sequence motifs bind to the DNA-binding site of p53c. Because the two sequences are homologous and separated by 120 residues, and one is in a largely unstructured transactivation domain, we speculate that each sequence motif in HIF-1alpha binds to a different subunit of the p53 tetramer, leading to very tight binding. The binding data support the proposal that p53 provides a route for the degradation in hypoxic tumor cells of HIF-1alpha that is not hydroxylated at the two proline residues.

摘要

有证据表明低氧诱导因子-1α(HIF-1α)与肿瘤抑制因子p53相互作用。为了表征这种假定的相互作用,我们将p53核心结构域(p53c)与一系列固定化的HIF-1α衍生肽段的结合情况进行了定位,发现有两个肽段序列基序在溶液中以微摩尔亲和力与p53c结合。一个序列与氧依赖性降解结构域的两个脯氨酸残基(P402和P564)相邻,另一个与之重合,这两个脯氨酸残基作为HIF-1α氧依赖性调节的开关。结合亲和力与P564的羟基化状态无关。我们通过核磁共振光谱发现,这些序列基序与p53c的DNA结合位点结合。由于这两个序列是同源的,且相隔120个残基,并且其中一个位于很大程度上无结构的反式激活结构域中,我们推测HIF-1α中的每个序列基序与p53四聚体的不同亚基结合,从而导致非常紧密的结合。这些结合数据支持了这样的提议,即p53为缺氧肿瘤细胞中未在两个脯氨酸残基处羟基化的HIF-1α的降解提供了一条途径。

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