Carbon-dot-mediated co-administration of chemotherapeutic agents for reversing cisplatin resistance in cancer therapy

Carbon-dot-mediated co-administration of chemotherapeutic agents for reversing cisplatin resistance in cancer therapy

Chemotherapeutic DNA-modifying cisplatin and topoisomerase II (TOP2)-inhibiting doxorubicin (DOX) were co-administrated by full-color emissive carbon dots (CDs−Pt(IV)−DOX) through tumor intracellular environment responsive covalent bonds to successfully reverse the resistance of cisplatin in cancer...

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Main Authors: Feng, Tao, Chua, Huoy Jing, Zhao, Yanli
Other Authors: School of Materials Science & Engineering
Format: Article
Language:English
Published: 2020
Subjects:
Science::Chemistry
Cancer
Carbon Dots
Online Access:https://hdl.handle.net/10356/140629
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Institution: Nanyang Technological University
Language: English
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spelling sg-ntu-dr.10356-1406292020-06-01T10:43:37Z Carbon-dot-mediated co-administration of chemotherapeutic agents for reversing cisplatin resistance in cancer therapy Feng, Tao Chua, Huoy Jing Zhao, Yanli School of Materials Science & Engineering School of Physical and Mathematical Sciences Division of Chemistry and Biological Chemistry Science::Chemistry Cancer Carbon Dots Chemotherapeutic DNA-modifying cisplatin and topoisomerase II (TOP2)-inhibiting doxorubicin (DOX) were co-administrated by full-color emissive carbon dots (CDs−Pt(IV)−DOX) through tumor intracellular environment responsive covalent bonds to successfully reverse the resistance of cisplatin in cancer therapy. Cisplatin was loaded in the form of cisplatin(IV) prodrug and DOX was conjugated via a pH-sensitive hydrazone bond. The internalization process of CDs−Pt(IV)−DOX by cancer cells could be monitored through multicolor emission from CDs and DOX. Upon uptake, cisplatin(IV) prodrug was activated to cytotoxic cisplatin under intracellular reductive condition, and the hydrazone bond was hydrolyzed to release DOX in intracellular weakly acidic environment. The released cisplatin and DOX exhibited combined anticancer effects via different mechanisms of action. Fluorescence imaging, a cytotoxicity study, and an apoptosis assay using CDs−Pt(IV)−DOX were performed to demonstrate the effective uptake and potent therapeutic efficacy toward A2780 and A2780cis cancer cells with cisplatin resistance. The developed CDs−Pt(IV)−DOX offers a promising fluorescent CD-based co-administration system for combating cisplatin resistance in cancer treatment. 2020-06-01T02:50:06Z 2020-06-01T02:50:06Z 2018 Journal Article Feng, T., Chua, H. J., & Zhao, Y. (2018). Carbon-dot-mediated co-administration of chemotherapeutic agents for reversing cisplatin resistance in cancer therapy. ChemNanoMat, 4(8), 801-806. doi:10.1002/cnma.201700367 2199-692X https://hdl.handle.net/10356/140629 10.1002/cnma.201700367 2-s2.0-85042453547 8 4 801 806 en ChemNanoMat © 2018 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim. All rights reserved.
institution Nanyang Technological University
building NTU Library
country Singapore
collection DR-NTU
language English
topic Science::Chemistry
Cancer
Carbon Dots
spellingShingle Science::Chemistry
Cancer
Carbon Dots
Feng, Tao
Chua, Huoy Jing
Zhao, Yanli
Carbon-dot-mediated co-administration of chemotherapeutic agents for reversing cisplatin resistance in cancer therapy
description Chemotherapeutic DNA-modifying cisplatin and topoisomerase II (TOP2)-inhibiting doxorubicin (DOX) were co-administrated by full-color emissive carbon dots (CDs−Pt(IV)−DOX) through tumor intracellular environment responsive covalent bonds to successfully reverse the resistance of cisplatin in cancer therapy. Cisplatin was loaded in the form of cisplatin(IV) prodrug and DOX was conjugated via a pH-sensitive hydrazone bond. The internalization process of CDs−Pt(IV)−DOX by cancer cells could be monitored through multicolor emission from CDs and DOX. Upon uptake, cisplatin(IV) prodrug was activated to cytotoxic cisplatin under intracellular reductive condition, and the hydrazone bond was hydrolyzed to release DOX in intracellular weakly acidic environment. The released cisplatin and DOX exhibited combined anticancer effects via different mechanisms of action. Fluorescence imaging, a cytotoxicity study, and an apoptosis assay using CDs−Pt(IV)−DOX were performed to demonstrate the effective uptake and potent therapeutic efficacy toward A2780 and A2780cis cancer cells with cisplatin resistance. The developed CDs−Pt(IV)−DOX offers a promising fluorescent CD-based co-administration system for combating cisplatin resistance in cancer treatment.
author2 School of Materials Science & Engineering
author_facet School of Materials Science & Engineering
Feng, Tao
Chua, Huoy Jing
Zhao, Yanli
format Article
author Feng, Tao
Chua, Huoy Jing
Zhao, Yanli
author_sort Feng, Tao
title Carbon-dot-mediated co-administration of chemotherapeutic agents for reversing cisplatin resistance in cancer therapy
title_short Carbon-dot-mediated co-administration of chemotherapeutic agents for reversing cisplatin resistance in cancer therapy
title_full Carbon-dot-mediated co-administration of chemotherapeutic agents for reversing cisplatin resistance in cancer therapy
title_fullStr Carbon-dot-mediated co-administration of chemotherapeutic agents for reversing cisplatin resistance in cancer therapy
title_full_unstemmed Carbon-dot-mediated co-administration of chemotherapeutic agents for reversing cisplatin resistance in cancer therapy
title_sort carbon-dot-mediated co-administration of chemotherapeutic agents for reversing cisplatin resistance in cancer therapy
publishDate 2020
url https://hdl.handle.net/10356/140629
_version_ 1681056077138886656

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