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Efficient Prostate Cancer Therapy with Tissue-Specific Homing Peptides Identified by Advanced Phage Display Technology

机译:通过先进的噬菌体展示技术鉴定的具有组织特异性归巢肽的高效前列腺癌治疗

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摘要

Selective targeting of drugs to tumor cells is a key goal in oncology. Here, we performed an in vivo phage display to identify peptides that specifically target xenografted prostate cancer cells. This yielded three peptide candidates, LN1 (C-TGTPARQ-C), LN2 (C-KNSMFAT-C), and LN3 (C-TNKHSPK-C); each of these peptides was synthesized and evaluated for binding and biological activity. LN1 showed the highest avidity for LNCaP prostate cancer cells in vitro and was thus administered to tumor-bearing mice to evaluate in vivo binding. Strikingly, LN1 specifically bound to the tumor tissue and exhibited very low reactivity with normal liver and kidney tissues. To demonstrate that LN1 could specifically deliver drugs to prostate cancer tissue, a therapeutic peptide, LN1-KLA (C-TGTPARQ-C-GGG-D[KLAKLAK]2), was prepared and used to treat LNCaP cells in vitro and was also administered to tumor-bearing mice. The therapeutic peptide significantly suppressed growth of the cells both in vitro and in vivo. Our study shows that a selective homing peptide strategy could facilitate cell-specific targeting of therapeutics while avoiding adverse reactions in normal tissues.
机译:药物对肿瘤细胞的选择性靶向是肿瘤学的关键目标。在这里,我们进行了体内噬菌体展示以鉴定特异性靶向异种移植前列腺癌细胞的肽。这产生了三个候选肽,LN1(C-TGTPARQ-C),LN2(C-KNSMFAT-C)和LN3(C-TNKHSPK-C);合成这些肽中的每一个并评估其结合和生物学活性。 LN1在体外对LNCaP前列腺癌细胞显示出最高的亲和力,因此被施用于荷瘤小鼠以评估其体内结合。令人惊讶的是,LN1与肿瘤组织特异性结合,并且与正常肝和肾组织的反应性非常低。为了证明LN1可以特异性地将药物递送至前列腺癌组织,制备了一种治疗性肽LN1-KLA(C-TGTPARQ-C-GGG-D [KLAKLAK] 2),并用于体外处理LNCaP细胞,并进行了给药给荷瘤小鼠。治疗性肽在体外和体内均可显着抑制细胞的生长。我们的研究表明,选择性归巢肽策略可以促进针对细胞的靶向治疗,同时避免正常组织发生不良反应。

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