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Phage Display-Based Homing Peptide-Daunomycin Conjugates for Selective Drug Targeting to PANC-1 Pancreatic Cancer

机译:噬菌体展示型归硝肽 - Daunomycin缀合物,用于选择性药物靶向Panc-1胰腺癌

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The Pancreatic Ductal Adenocarcinoma (PDAC) is one of the most aggressive and dangerous cancerous diseases, leading to a high rate of mortality. Therefore, the development of new, more efficient treatment approaches is necessary to cure this illness. Peptide-based drug targeting provides a new tool for this purpose. Previously, a hexapeptide Cys-Lys-Ala-Ala-Lys-Asn (CKAAKN) was applied efficiently as the homing device for drug-loaded nanostructures in PDAC cells. In this research, Cys was replaced by Ser in the sequence and this new SKAAKN targeting moiety was used in conjugates containing daunomycin (Dau). Five different structures were developed and tested. The results indicated that linear versions with one Dau were not effective on PANC-1 cells in vitro; however, branched conjugates with two Dau molecules showed significant antitumor activity. Differences in the antitumor effect of the conjugates could be explained with the different cellular uptake and lysosomal degradation. The most efficient conjugate was Dau=Aoa -GFLG-K( Dau=Aoa )SKAAKN- OH (conjugate 4 ) that also showed significant tumor growth inhibition on s.c. implanted PANC-1 tumor-bearing mice with negligible side effects. Our novel results suggest that peptide-based drug delivery systems could be a promising tool for the treatment of pancreatic cancers.
机译:胰腺导管腺癌(PDAC)是最具侵略性和危险的癌症疾病之一,导致死亡率高。因此,制定新的,更有效的治疗方法是治愈这种疾病所必需的。基于肽的药物靶向为此提供了一种新工具。以前,作为PDAC细胞中的用于药物负载纳米结构的归巢装置,有效地施加六肽Cys-Lys-Ala-Ala-Lys-ASN(CKAAKN)。在本研究中,Cys被Ser在序列中取代,并且这种新的Skaakn靶向部分用于含有Daunomycin(DAU)的缀合物。开发并测试了五种不同的结构。结果表明,具有一个DAU的线性型号在体外Panc-1细胞没有有效;然而,具有两个DAU分子的支链缀合物显示出显着的抗肿瘤活性。可以用不同的细胞摄取和溶酶体降解解释缀合物的抗肿瘤效应的差异。最有效的缀合物是DAU = AOA-GFLG-K(DAU = AOA)SKAAKN-OH(缀合4),也表现出对S.C的显着肿瘤生长抑制作用。植入Panc-1携带肿瘤的小鼠可忽略不计的副作用。我们的新结果表明,基于肽的药物递送系统可能是治疗胰腺癌的有希望的工具。

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