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Title: | New Insight into a Cancer Theranostic Probe: Efficient Cell-Specific Delivery of SN-38 Guided by Biotinylated Poly(vinyl alcohol) |
Authors: | Debabrata, Dutta Susan, M. Alex Kondapa Naidu Bobba, Bobba Maiti, Kaustabh Kumar Sankarprasad, Bhuniya |
Keywords: | heranostic, poly(vinyl alcohol), biocompatible blood serum SN-38 antiproliferative |
Issue Date: | 18-Nov-2016 |
Publisher: | ACS publication |
Citation: | ACS Appl. Mater. Interfaces,8:33430−33438 |
Abstract: | An optically modulated “turn-on” theranostic prodrug TP1 has been explored and formulated with biotinylated poly(vinyl alcohol) (biotinPVA) to obtain desired pharmacokinetics. TP1, consisting of the antineoplastic camptothecin analogue SN-38, and the fluorescent dye rhodol green have been covalently conjugated through a disulfide bond. Glutathione triggering the release of drug and fluorophore has been well established by UV−vis measurements through mass spectral analysis in physiological conditions. The biocompatible biotinPVA formulated prodrug (PTP1) showed remarkably higher stability against blood serum and cell-specific activation in contrast to that of TP1. Significantly, PTP1 permits monitoring of the delivery and release of well-known topoisomerase I inhibitor SN-38 by modulating fluorescence signal at λem 550 nm within intracellular milieus. Moreover, theranostic probe PTP1 exhibited dose-dependent antiproliferative activity against receptor-positive HeLa cells, whereas it did not show such an effect against receptor-negative NIH3T3 cells. Finally, the cellspecific antiproliferative activity of PTP1 via the apoptotic pathway is an efficient approach in cancer theranostics. Thus, futuristic PTP1 could be a promising agent in which diagnostic and prognostic data will be monitored synergistically |
URI: | http://hdl.handle.net/123456789/2746 |
Appears in Collections: | 2016 |
Files in This Item:
File | Description | Size | Format | |
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new insight-debabatra dutta-applied materials interface.pdf Restricted Access | 3.91 MB | Adobe PDF | View/Open Request a copy |
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