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Dendrimer-based multivalent methotrexates as dual acting nanoconjugates for cancer cell targeting.


ABSTRACT: Cancer-targeting drug delivery can be based on the rational design of a therapeutic platform. This approach is typically achieved by the functionalization of a nanoparticle with two distinct types of molecules, a targeting ligand specific for a cancer cell, and a cytotoxic molecule to kill the cell. The present study aims to evaluate the validity of an alternative simplified approach in the design of cancer-targeting nanotherapeutics: conjugating a single type of molecule with dual activities to nanoparticles, instead of coupling a pair of orthogonal molecules. Herein we investigate whether this strategy can be validated by its application to methotrexate, a dual-acting small molecule that shows cytotoxicity because of its potent inhibitory activity against dihydrofolate reductase and that binds folic acid receptor, a tumor biomarker frequently upregulated on the cancer cell surface. This article describes a series of dendrimer conjugates derived from a generation 5 polyamidoamine (G5 PAMAM) presenting a multivalent array of methotrexate and also demonstrates their dual biological activities by surface plasmon resonance spectroscopy, a cell-free enzyme assay, and cell-based experiments with KB cancer cells.

SUBMITTER: Li MH 

PROVIDER: S-EPMC3243070 | biostudies-literature | 2012 Jan

REPOSITORIES: biostudies-literature

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Dendrimer-based multivalent methotrexates as dual acting nanoconjugates for cancer cell targeting.

Li Ming-Hsin MH   Choi Seok Ki SK   Thomas Thommey P TP   Desai Ankur A   Lee Kyung-Hoon KH   Kotlyar Alina A   Banaszak Holl Mark M MM   Baker James R JR  

European journal of medicinal chemistry 20111123 1


Cancer-targeting drug delivery can be based on the rational design of a therapeutic platform. This approach is typically achieved by the functionalization of a nanoparticle with two distinct types of molecules, a targeting ligand specific for a cancer cell, and a cytotoxic molecule to kill the cell. The present study aims to evaluate the validity of an alternative simplified approach in the design of cancer-targeting nanotherapeutics: conjugating a single type of molecule with dual activities to  ...[more]

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