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      Diverse gatekeepers for mesoporous silica nanoparticle based drug delivery systems

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          Abstract

          Progress on the design of diverse gatekeepers for mesoporous silica nanoparticle based drug delivery systems is summarized.

          Abstract

          Conventional cancer chemotherapy is often associated with toxicity issues. Thus, new drug delivery systems (DDSs) are developed as alternatives owing to their potential to selectively target affected cells while sparing normal tissues. Among them, noninvasive and biocompatible mesoporous silica nanoparticle (MSN)-based targeted DDSs have developed rapidly. In particular, controlled gatekeepers capping the pore entrances of MSNs play prominent and crucial roles in achieving specific drug release and avoiding premature leakage in the delivery process before the target is reached, and perfect gatekeepers can only be removed under specific internal or external stimuli, such as pH, redox potential, temperature, biomolecules, light, magnetic field and ultrasound, or a combination of these stimuli, which is significant for precise therapeutic treatments and potential applications in human bodies. Thus, the main focus of this review is to highlight the most recent progress on the design of various controlled MSN gatekeepers to achieve ‘zero premature release’ drug delivery. The diverse gatekeepers are categorised into the following kinds according to their types and characteristics: (1) polymers; (2) inorganic nanomaterials; (3) host–guest assemblies; and (4) biomacromolecules. This review will offer a broad palette of opportunities for researchers with interests including nanomaterial fabrication and modification, targeted drug delivery and stimuli-responsive drug release.

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          Most cited references191

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          A new family of mesoporous molecular sieves prepared with liquid crystal templates

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            para-Bridged symmetrical pillar[5]arenes: their Lewis acid catalyzed synthesis and host-guest property.

            Condensation of 1,4-dimethoxybenzene (DMB) with paraformaldehyde in the presence of BF3.O(C2H5)2 gave novel para-bridged pentacyclic pillar DMB (DMpillar[5]arene). Moreover, para-bridged pentacyclic hydroquinone (pillar[5]arene) was prepared. Pillar[5]arene formed 1:1 host-guest complexes with dialkyl viologen and alkyl pyridinium derivatives. However, pillar[5]arene did not form complexes with the diadamantyl viologen derivative since a bulky adamantyl group was unable to thread the cavity of pillar[5]arene.
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              A New Property of MCM-41:  Drug Delivery System

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                Author and article information

                Journal
                CSRVBR
                Chemical Society Reviews
                Chem. Soc. Rev.
                Royal Society of Chemistry (RSC)
                0306-0012
                1460-4744
                2017
                2017
                : 46
                : 19
                : 6024-6045
                Affiliations
                [1 ]Shaanxi Key Laboratory of Natural Products & Chemical Biology
                [2 ]College of Chemistry & Pharmacy
                [3 ]Northwest A&F University
                [4 ]Yangling
                [5 ]P. R. China
                [6 ]State Key Laboratory of Fine Chemicals
                [7 ]School of Chemistry
                [8 ]Dalian University of Technology
                [9 ]Dalian 116023
                [10 ]China
                Article
                10.1039/C7CS00219J
                28848978
                a411e712-800a-4182-857c-d4c2598e9dc3
                © 2017
                History

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