首页> 外文期刊>Biochimica et Biophysica Acta. General Subjects >Transducing properties of a pre-structured α-helical DPT-peptide containing a short canine adenovirus type 2 E4orf4 PP2A1-binding sequence
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Transducing properties of a pre-structured α-helical DPT-peptide containing a short canine adenovirus type 2 E4orf4 PP2A1-binding sequence

机译:包含短犬腺病毒2型E4orf4 PP2A1结合序列的预结构化α-螺旋DPT肽的转导特性

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Background Induction of the death pathway resulting from the specific interaction of the PP2A1 phosphatase with adenoviral E4orf4 protein is a promising approach for cancer therapy. With the aim of deregulating tumor pathways, and mimicking E4orf4 anti-cancer signal, we have previously proposed the DPT technology concept, based on design of specific PP1/PP2A interacting penetrating peptides. Methods Using biochemical, structural and cell survival experiments, we have characterized new DPT-peptides containing short PP2A binding sequences. Results We identified overlapping sequences, located within the N-terminal domain E4orf423-46 of canine adenoviral E4orf4 protein, that interact with the PP2A-Bα subunit of PP2A1 holoenzyme. We characterized DPT-E4orf44 and TAT-E4orf44, two bi-partite cell penetrating peptides containing the 12 PP2A1 binding residues of the canine type 2 E4orf427-38 sequence, respectively fused to the DPT-sh1 and TAT shuttle sequences. Surprisingly DPT-E4orf44, in contrast to inactive TAT-E4orf44, adopted a well defined α-helical structure and co-precipitated PP2A1 from HeLa cell extracts. DPT-E4orf44 also internalized streptavidin-HRP and inhibited survival of HeLa cells more efficiently than TAT, TAT-E4orf44 or the previously published anti-tumor TAT-derived peptide shepherdin. DPT-E4orf44 also efficiently inhibited the survival of human adherent transformed cells, including wild type and p53 mutated colonic HCT116 cells, without affecting survival of human non-transformed fibroblasts. Conclusions We characterized the transducing properties of a new α-helical DPT-E4orf44 peptide containing a short PP2A-interacting sequence from canine Adenoviral E4orf4 protein. General significance Our results suggest that α-helical structured DPT peptides specifically interacting with PP2A could be a valuable anti-cancer drug design scaffold.
机译:背景技术由PP2A1磷酸酶与腺病毒E4orf4蛋白的特异性相互作用导致的死亡途径的诱导是一种有前途的癌症治疗方法。为了放松肿瘤通路并模仿E4orf4抗癌信号,我们先前基于特定的PP1 / PP2A相互作用渗透肽的设计提出了DPT技术概念。方法使用生化,结构和细胞存活实验,我们鉴定了含有短PP2A结合序列的新DPT肽。结果我们确定了位于犬腺病毒E4orf4蛋白N端结构域E4orf423-46内的重叠序列,这些序列与PP2A1全酶的PP2A-Bα亚基相互作用。我们表征了DPT-E4orf44和TAT-E4orf44,这是两个双向分子穿透肽,包含犬2型E4orf427-38序列的12个PP2A1结合残基,分别与DPT-sh1和TAT穿梭序列融合。令人惊讶的是,与无活性的TAT-E4orf44相比,DPT-E4orf44采用了明确定义的α螺旋结构,并从HeLa细胞提取物中共沉淀了PP2A1。与TAT,TAT-E4orf44或先前发表的抗肿瘤TAT衍生肽shepherdin相比,DPT-E4orf44还内化了链霉亲和素-HRP,并更有效地抑制HeLa细胞的存活。 DPT-E4orf44还有效抑制了人类粘附的转化细胞(包括野生型和p53突变的结肠HCT116细胞)的存活,而没有影响人类未转化的成纤维细胞的存活。结论我们表征了一种新的α-螺旋DPT-E4orf44肽的转导特性,该肽包含来自犬腺病毒E4orf4蛋白的短PP2A相互作用序列。一般意义我们的结果表明,与PP2A特异性相互作用的α螺旋结构DPT肽可能是有价值的抗癌药物设计支架。

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