4.5 Article

Development of Polyamine Lassos as Polyamine Transport Inhibitors

Journal

ACS MEDICINAL CHEMISTRY LETTERS
Volume 13, Issue 2, Pages 319-326

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acsmedchemlett.1c00557

Keywords

Polyamine transport inhibitor; difluoromethylornithine; triazacyclononane; pancreatic cancer

Funding

  1. UCF College of Medicine
  2. NIH [S10 OD021758-01A1]
  3. Florida Department of Health Bankhead Coley Grant [8BC05]

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In this study, polyamine lassos were synthesized by attaching nine- and twelve-membered triaza-macrocycles to homospermidine. These compounds were found to be potent polyamine transport inhibitors in pancreatic ductal adenocarcinoma cells with high polyamine transport activity. The smaller lasso showed superior inhibition of polyamine uptake and reduced intracellular polyamine levels.
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 3H-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 K-i 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.

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