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Anticancer peptide PNC-27 adopts an HDM-2-binding conformation and kills cancer cells by binding to HDM-2 in their membranes

机译:抗癌肽PNC-27具有HDM-2结合构象,并通过与膜中的HDM-2结合来杀死癌细胞

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摘要

The anticancer peptide PNC-27, which contains an HDM-2-binding domain corresponding to residues 12-26 of p53 and a transmembrane-penetrating domain, has been found to kill cancer cells (but not normal cells) by inducing membranolysis. We find that our previously determined 3D structure of the p53 residues of PNC-27 is directly superimposable on the structure for the same residues bound to HDM-2, suggesting that the peptide may target HDM-2 in the membranes of cancer cells. We now find significant levels of HDM-2 in the membranes of a variety of cancer cells but not in the membranes of several untransformed cell lines. In colocalization experiments, we find that PNC-27 binds to cell membrane-bound HDM-2. We further transfected a plasmid expressing full-length HDM-2 with a membrane-localization signal into untransformed MCF-10-2A cells not susceptible to PNC-27 and found that these cells expressing full-length HDM-2 on their cell surface became susceptible to PNC-27. We conclude that PNC-27 targets HDM-2 in the membranes of cancer cells, allowing it to induce membranolysis of these cells selectively.
机译:已经发现抗癌肽PNC-27包含对应于p53残基12-26的HDM-2结合结构域和跨膜穿透结构域,可通过诱导膜分解杀死癌细胞(但不杀死正常细胞)。我们发现,我们先前确定的PNC-27 p53残基的3D结构在与HDM-2结合的相同残基的结构上可以直接叠加,这表明该肽可能靶向癌细胞膜中的HDM-2。现在,我们在多种癌细胞的膜中发现了高水平的HDM-2,但在几种未转化的细胞系的膜中却未发现。在共定位实验中,我们发现PNC-27与细胞膜结合的HDM-2结合。我们进一步将表达带有膜定位信号的全长HDM-2的质粒转染到对PNC-27不敏感的未转化的MCF-10-2A细胞中,发现这些在细胞表面表达全长HDM-2的细胞变得易感到PNC-27。我们得出的结论是,PNC-27靶向癌细胞膜中的HDM-2,使其能够选择性地诱导这些细胞的膜溶解。

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