Department of Surgery, Division of Surgical Oncology, University of Illinois at Chicago College of Medicine, Chicago, IL, USA.
Br J Cancer. 2013 Jun 25;108(12):2495-504. doi: 10.1038/bjc.2013.266. Epub 2013 Jun 4.
A 28 amino-acid (aa) cell-penetrating peptide (p28) derived from azurin, a redox protein secreted from the opportunistic pathogen Pseudomonas aeruginosa, produces a post-translational increase in p53 in cancer cells by inhibiting its ubiquitination.
In silico computational simulations were used to predict motifs within the p53 DNA-binding domain (DBD) as potential sites for p28 binding. In vitro direct and competitive pull-down studies as well as western blot and RT-PCR analyses were used to validate predictions.
The L1 loop (aa 112-124), a region within the S7-S8 loop (aa 214-236) and T140, P142, Q144, W146, R282 and L289 of the p53DBD were identified as potential sites for p28 binding. p28 decreased the level of the E3 ligase COP1 >80%, in p53wt and p53mut cells with no decrease in COP1 in p53dom/neg or p53null cells. Brief increases in the expression of the E3 ligases, TOPORS, Pirh2 and HDM2 (human double minute 2) in p53wt and p53mut cells were in response to sustained increases in p53.
These data identify the specific motifs within the DBD of p53 that bind p28 and suggest that p28 inhibition of COP1 binding results in the sustained, post-translational increase in p53 levels and subsequent inhibition of cancer cell growth independent of an HDM2 pathway.
一种来自铜蓝蛋白(一种由机会性病原体铜绿假单胞菌分泌的氧化还原蛋白)的 28 个氨基酸(aa)细胞穿透肽(p28)通过抑制其泛素化来增加癌细胞中的 p53 后翻译。
使用计算机模拟来预测 p53 DNA 结合域(DBD)内的模体作为 p28 结合的潜在位点。进行体外直接和竞争下拉研究以及 Western blot 和 RT-PCR 分析以验证预测。
L1 环(aa112-124)、S7-S8 环(aa214-236)内的 L1 环(aa112-124)内的区域以及 p53DBD 的 T140、P142、Q144、W146、R282 和 L289 被鉴定为 p28 结合的潜在位点。p28 在 p53wt 和 p53mut 细胞中使 E3 连接酶 COP1 的水平降低了 >80%,而在 p53dom/neg 或 p53null 细胞中 COP1 没有降低。在 p53wt 和 p53mut 细胞中,E3 连接酶 TOPORS、Pirh2 和 HDM2(人双微体 2)的表达短暂增加是对 p53 持续增加的反应。
这些数据确定了 p53 DBD 内与 p28 结合的特定模体,并表明 p28 抑制 COP1 结合导致 p53 水平的持续后翻译增加,并随后抑制独立于 HDM2 途径的癌细胞生长。
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