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      Fluorogenic reaction-based prodrug conjugates as targeted cancer theranostics

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          Abstract

          This Tutorial Review will describe various fluorogenic reaction-based prodrug strategies used for targeted theranostic drug delivery.

          Abstract

          Theranostic systems are receiving ever-increasing attention due to their potential therapeutic utility, imaging enhancement capability, and promise for advancing the field of personalized medicine, particularly as it relates to the diagnosis, staging, and treatment of cancer. In this Tutorial Review, we provide an introduction to the concepts of theranostic drug delivery effected via use of conjugates that are able to target cancer cells selectively, provide cytotoxic chemotherapeutics, and produce readily monitored imaging signals in vitro and in vivo. The underlying design concepts, requiring the synthesis of conjugates composed of imaging reporters, masked chemotherapeutic drugs, cleavable linkers, and cancer targeting ligands, are discussed. Particular emphasis is placed on highlighting the potential benefits of fluorogenic reaction-based targeted systems that are activated for both imaging and therapy by cellular entities, e.g., thiols, reactive oxygen species and enzymes, which are present at relatively elevated levels in tumour environments, physiological characteristics of cancer, e.g., hypoxia and acidic pH. Also discussed are systems activated by an external stimulus, such as light. The work summarized in this Tutorial Review will help define the role fluorogenic reaction-based, cancer-targeting theranostics may have in advancing drug discovery efforts, as well as improving our understanding of cellular uptake and drug release mechanisms.

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          Most cited references39

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          Nanomaterials for theranostics: recent advances and future challenges.

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            Ligand-targeted therapeutics in anticancer therapy.

            Cytotoxic chemotherapy or radiotherapy of cancer is limited by serious, sometimes life-threatening, side effects that arise from toxicities to sensitive normal cells because the therapies are not selective for malignant cells. So how can selectivity be improved? One strategy is to couple the therapeutics to antibodies or other ligands that recognize tumour-associated antigens. This increases the exposure of the malignant cells, and reduces the exposure of normal cells, to the ligand-targeted therapeutics.
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              Disulfide-cleavage-triggered chemosensors and their biological applications.

                Author and article information

                Journal
                CSRVBR
                Chemical Society Reviews
                Chem. Soc. Rev.
                Royal Society of Chemistry (RSC)
                0306-0012
                1460-4744
                2018
                2018
                : 47
                : 1
                : 28-52
                Affiliations
                [1 ]Department of Chemistry
                [2 ]Sookmyung Women's University
                [3 ]Seoul 04310
                [4 ]Korea
                [5 ]Korea University
                [6 ]Seoul 02841
                [7 ]The University of Texas at Austin
                [8 ]Austin
                [9 ]USA
                [10 ]The School of East-West Medical Science
                [11 ]Kyung Hee University
                [12 ]Yongin 17104
                Article
                10.1039/C7CS00557A
                5750141
                29057403
                66764af2-0c28-435f-9b7e-13d6d67f8da4
                © 2018

                http://rsc.li/journals-terms-of-use

                History

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