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In Vitro Selection of Cathepsin E-Activity-Enhancing Peptide Aptamers at Neutral pH

机译:在中性pH下组织蛋白酶E活性增强肽适体的体外选择

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摘要

The aspartic protease cathepsin E has been shown to induce apoptosis in cancer cells under physiological conditions. Therefore, cathepsin E-activity-enhancing peptides functioning in the physiological pH range are valuable potential cancer therapeutic candidates. Here, we have used a general in vitro selection method (evolutionary rapid panning analysis system (eRAPANSY)), based on inverse substrate-function link (SF-link) selection to successfully identify cathepsin E-activity-enhancing peptide aptamers at neutral pH. A successive enrichment of peptide activators was attained in the course of selection. One such peptide activated cathepsin E up to 260%, had a high affinity (KD; ∼300 nM), and had physiological activity as demonstrated by its apoptosis-inducing reaction in cancerous cells. This method is expected to be widely applicable for the identification of protease-activity-enhancing peptide aptamers.
机译:已经显示天冬氨酸蛋白酶组织蛋白酶E在生理条件下诱导癌细胞凋亡。因此,在生理pH范围内起作用的组织蛋白酶E活性增强肽是有价值的潜在癌症治疗候选物。在这里,我们使用了一种常规的体外选择方法(进化快速淘选分析系统(eRAPANSY)),它基于逆底物功能连接(SF-link)选择,成功鉴定了中性pH下组织蛋白酶E-活性增强肽的适体。在选择过程中获得了肽激活剂的连续富集。一种这样的肽激活的组织蛋白酶E最高可达260%,具有高亲和力(KD;〜300 nM),并且具有生理活性,如其在癌细胞中诱导细胞凋亡的反应所证明的那样。预期该方法可广泛用于鉴定蛋白酶活性增强肽适体。

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