| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2042349 | Cell Reports | 2014 | 14 Pages |
•p53 is downregulated in tumorigenesis-associated iron/heme excess•The C terminus of p53 specifically binds to heme•Heme excess destabilizes p53 by promoting its nuclear export and cytosolic degradation•Tumor suppression by iron deprivation relies on wild-type p53 signaling
SummaryIron excess is closely associated with tumorigenesis in multiple types of human cancers, with underlying mechanisms yet unclear. Recently, iron deprivation has emerged as a major strategy for chemotherapy, but it exerts tumor suppression only on select human malignancies. Here, we report that the tumor suppressor protein p53 is downregulated during iron excess. Strikingly, the iron polyporphyrin heme binds to p53 protein, interferes with p53-DNA interactions, and triggers both nuclear export and cytosolic degradation of p53. Moreover, in a tumorigenicity assay, iron deprivation suppressed wild-type p53-dependent tumor growth, suggesting that upregulation of wild-type p53 signaling underlies the selective efficacy of iron deprivation. Our findings thus identify a direct link between iron/heme homeostasis and the regulation of p53 signaling, which not only provides mechanistic insights into iron-excess-associated tumorigenesis but may also help predict and improve outcomes in iron-deprivation-based chemotherapy.
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