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作为多胺转运抑制剂的多胺套索的开发。

Development of Polyamine Lassos as Polyamine Transport Inhibitors.

作者信息

Dobrovolskaite Aiste, Gardner Richard Andrew, Delcros Jean-Guy, Phanstiel Otto

机构信息

Department of Medical Education, College of Medicine, University of Central Florida, Orlando, Florida 32826, United States.

Ludger Ltd., Culham Science Centre, Abingdon, Oxfordshire OX14 3EB, United Kingdom.

出版信息

ACS Med Chem Lett. 2022 Jan 20;13(2):319-326. doi: 10.1021/acsmedchemlett.1c00557. eCollection 2022 Feb 10.

Abstract

Nine- and twelve-membered triaza-macrocycles were appended to one end of homospermidine to make polyamine lassos. These compounds were shown to be potent polyamine transport inhibitors (PTIs) using pancreatic ductal adenocarcinoma L3.6pl cells, which have high polyamine transport activity. The smaller triazacyclononane-based lasso significantly reduced the uptake of a fluorescent polyamine probe and inhibited spermidine uptake and reduced intracellular polyamine levels in difluoromethylornithine (DFMO)-treated L3.6pl cells. Both designs were shown to be effective inhibitors of H-spermidine uptake, with the smaller lasso outperforming the larger lasso. When the smaller lasso was challenged to inhibit each of the three radiolabeled native polyamines, it had similar values as those of the known PTIs, Trimer44NMe and AMXT1501. Because of these promising properties, these materials may have future anticancer applications in polyamine blocking therapy, an approach that couples a polyamine biosynthesis inhibitor (DFMO) with a PTI to lower intracellular polyamines and suppress cell growth.

摘要

将九元环和十二元环三氮杂大环连接到高亚精胺的一端以制备多胺套索。使用具有高多胺转运活性的胰腺导管腺癌L3.6pl细胞,这些化合物被证明是有效的多胺转运抑制剂(PTIs)。基于较小的三氮杂环壬烷的套索显著降低了荧光多胺探针的摄取,并抑制了亚精胺摄取,并降低了经二氟甲基鸟氨酸(DFMO)处理的L3.6pl细胞中的细胞内多胺水平。两种设计均显示为H-亚精胺摄取的有效抑制剂,较小的套索性能优于较大的套索。当用较小的套索抑制三种放射性标记的天然多胺中的每一种时,其值与已知的PTIs Trimer44NMe和AMXT1501相似。由于这些有前景的特性,这些材料在多胺阻断疗法中可能具有未来的抗癌应用,该方法将多胺生物合成抑制剂(DFMO)与PTI相结合以降低细胞内多胺并抑制细胞生长。

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Development of Polyamine Lassos as Polyamine Transport Inhibitors.作为多胺转运抑制剂的多胺套索的开发。
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