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自组装烷基化聚胺类似物作为超分子抗癌剂。

Self-Assembled Alkylated Polyamine Analogs as Supramolecular Anticancer Agents.

机构信息

Department of Pharmaceutical Sciences, Center for Drug Delivery and Nanomedicine, University of Nebraska Medical Center, Omaha, NE 68198, USA.

Sidney Kimmel Comprehensive Cancer Center, Johns Hopkins School of Medicine, Baltimore, MD 21231, USA.

出版信息

Molecules. 2022 Apr 10;27(8):2441. doi: 10.3390/molecules27082441.

Abstract

Conformationally restrained polyamine analog PG11047 is a well-known drug candidate that modulates polyamine metabolism and inhibits cancer cell growth in a broad spectrum of cancers. Here, we report a structure-activity relationship study of the PG11047 analogs (HPGs) containing alkyl chains of varying length, while keeping the unsaturated spermine backbone unchanged. Synthesis of higher symmetrical homologues was achieved through a synthetic route with fewer steps than the previous route to PG11047. The amphiphilic HPG analogs underwent self-assembly and formed spherically shaped nanoparticles whose size increased with the hydrophobic alkyl group's increasing chain length. Assessment of the in vitro anticancer activity showed more than an eight-fold increase in the cancer cell inhibition activity of the analogs with longer alkyl chains compared to PG11047 in human colon cancer cell line HCT116, and a more than ten-fold increase in human lung cancer cell line A549. Evaluation of the inhibition of spermine oxidase (SMOX) showed no activity for PG11047, but activity was observed for its higher symmetrical homologues. Comparison with a reference SMOX inhibitor MDL72527 showed nine-fold better activity for the best performing HPG analog.

摘要

构象受限的聚胺类似物 PG11047 是一种众所周知的候选药物,可调节多胺代谢并抑制多种癌症中的癌细胞生长。在这里,我们报告了含有不同长度烷基链的 PG11047 类似物(HPGs)的构效关系研究,同时保持不饱和精脒骨架不变。通过比以前到 PG11047 的路线具有更少步骤的合成路线实现了更高对称性同系物的合成。两亲性 HPG 类似物自组装形成具有球形的纳米颗粒,其粒径随疏水性烷基链的增加而增加。体外抗癌活性评估表明,与 PG11047 相比,具有较长烷基链的类似物在人结肠癌细胞系 HCT116 中的癌细胞抑制活性增加了八倍以上,在人肺癌细胞系 A549 中增加了十倍以上。对亚精胺氧化酶(SMOX)抑制作用的评估表明 PG11047 没有活性,但它的更高对称性同系物有活性。与参考 SMOX 抑制剂 MDL72527 相比,表现最佳的 HPG 类似物的活性高出九倍。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/39c0/9032695/96d6024cd142/molecules-27-02441-sch001.jpg

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