Department of Molecular Pathology, Tokyo Medical University, Tokyo, Japan.
School of Life Sciences, Tokyo University of Pharmacy and Life Sciences, Tokyo, Japan.
Sci Rep. 2018 Aug 24;8(1):12740. doi: 10.1038/s41598-018-31096-z.
Cell-penetrating peptides (CPPs) including arginine-rich peptides are attracting a lot of attention due to their potential as a novel intracellular drug delivery tool without substantial toxicity. On the other hand, disease-associated arginine-rich CPPs, such as poly-PR and poly-GR translated from C9orf72 gene, also efficiently enter neuronal cells and then kill them. Although both non-harmful CPPs and harmful poly-PR/GR penetrate the plasma membrane using same arginine residues, little is known about the factors which determine the toxicity of the pathogenic CPPs. Here, we show that poly-PR and poly-GR, but not other Arg-rich CPPs, specifically distributed to nucleolus via interaction with RNA. Importantly, C9orf72-dipeptides, but not other Arg-rich CPPs, caused inhibition of protein translation and cell death. Raising extracellular pH enhanced the cell penetration of poly-PR. The repeat number of (PR) affected the secondary structure and determined the intracellular delivery rate and neurotoxicity, and enforced intracellular delivery of non-penetrating short poly-PR peptide caused cell death, suggesting that modulation of extracellular environment to inhibit the uptake of Arg-rich dipeptides might be a drug target against poly-PR/GR-mediated neurotoxicity.
细胞穿透肽(CPPs),包括富含精氨酸的肽,由于其作为一种新型细胞内药物递送工具的潜力而受到广泛关注,而没有实质性的毒性。另一方面,与疾病相关的富含精氨酸的 CPPs,如从 C9orf72 基因翻译的多-PR 和多-GR,也能有效地进入神经元细胞并杀死它们。虽然非有害 CPPs 和有害的多-PR/GR 都使用相同的精氨酸残基穿透质膜,但对于决定致病 CPPs 毒性的因素知之甚少。在这里,我们表明多-PR 和多-GR 但不是其他富含精氨酸的 CPPs ,而是通过与 RNA 的相互作用特异性分布到核仁。重要的是,C9orf72 二肽,但不是其他富含精氨酸的 CPPs ,会抑制蛋白质翻译和细胞死亡。提高细胞外 pH 值增强了多-PR 的细胞穿透性。(PR)的重复次数影响二级结构,并决定细胞内递送率和神经毒性,强制非穿透性短多-PR 肽的细胞内递送导致细胞死亡,这表明调节细胞外环境以抑制富含精氨酸二肽的摄取可能是针对多-PR/GR 介导的神经毒性的药物靶点。
