Potentiating the cellular targeting and anti-tumor activity of Dp44mT via binding to human serum albumin: two saturable mechanisms of Dp44mT uptake by cells
Angelica M. Merlot, Sumit Sahni, Darius J.R. Lane, Ashleigh M. Fordham, Namfon Pantarat, David E. Hibbs, Vera Richardson, Munikumar R. Doddareddy, Jennifer A. Ong, Michael L.H. Huang, Des R. Richardson, Danuta S. Kalinowski

TL;DR
This study shows how human serum albumin enhances the cancer cell targeting and effectiveness of a drug called Dp44mT through two specific uptake mechanisms.
Contribution
The discovery of two saturable mechanisms for Dp44mT uptake, with one being HSA-dependent, is a novel finding.
Findings
HSA significantly increases Dp44mT uptake by cancer cells through a second saturable mechanism.
The HSA-mediated uptake mechanism has lower affinity but higher capacity compared to the first mechanism.
Enhanced Dp44mT targeting by HSA increases apoptosis in cancer cells.
Abstract
Di-2-pyridylketone 4,4-dimethyl-3-thiosemicarbazone (Dp44mT) demonstrates potent anti-cancer activity. We previously demonstrated that 14C-Dp44mT enters and targets cells through a carrier/receptor-mediated uptake process. Despite structural similarity, 2-benzoylpyridine 4-ethyl-3-thiosemicarbazone (Bp4eT) and pyridoxal isonicotinoyl hydrazone (PIH) enter cells via passive diffusion. Considering albumin alters the uptake of many drugs, we examined the effect of human serum albumin (HSA) on the cellular uptake of Dp44mT, Bp4eT and PIH. Chelator-HSA binding studies demonstrated the following order of relative affinity: Bp4eT≈PIH>Dp44mT. Interestingly, HSA decreased Bp4eT and PIH uptake, potentially due to its high affinity for the ligands. In contrast, HSA markedly stimulated Dp44mT uptake by cells, with two saturable uptake mechanisms identified. The first mechanism saturated at 5-10 μM…
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Taxonomy
TopicsPolitical Economy and Marxism
