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The pH-triggered drug release and simultaneous carrier decomposition of effervescent SiO(2)–drug–Na(2)CO(3) composite nanoparticles: to improve the antitumor activity of hydrophobic drugs

To achieve a better release effect of hydrophobic drugs and spontaneous nanocarrier disintegration by dissolution as well as the CO(2) production of Na(2)CO(3) further, improving the therapeutic effect of hydrophobic drugs, and thereby avoiding the accumulation of the nanocarrier in vivo to produce...

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Autores principales: Chen, Tianyu, Jiang, Yichun, Wang, Changmao, Cai, Zhengxue, Chen, Hui, Zhu, Junliang, Tao, Pinrun, Wu, Min
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Royal Society of Chemistry 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8694630/
https://www.ncbi.nlm.nih.gov/pubmed/35423073
http://dx.doi.org/10.1039/d0ra07896d
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author Chen, Tianyu
Jiang, Yichun
Wang, Changmao
Cai, Zhengxue
Chen, Hui
Zhu, Junliang
Tao, Pinrun
Wu, Min
author_facet Chen, Tianyu
Jiang, Yichun
Wang, Changmao
Cai, Zhengxue
Chen, Hui
Zhu, Junliang
Tao, Pinrun
Wu, Min
author_sort Chen, Tianyu
collection PubMed
description To achieve a better release effect of hydrophobic drugs and spontaneous nanocarrier disintegration by dissolution as well as the CO(2) production of Na(2)CO(3) further, improving the therapeutic effect of hydrophobic drugs, and thereby avoiding the accumulation of the nanocarrier in vivo to produce organ toxicity, effervescent SiO(2)–drug–Na(2)CO(3) composite nanoparticles (ESNs) were prepared in this study using a tetraethyl orthosilicate hydrolysis method. Sodium carbonate was used as the effervescent disintegrant to respond to the acidic microenvironment of the tumor. The properties of ESNs were assessed and TEM images were taken to verify the self-disintegration characteristics of nanocarrier materials. The in vitro anticancer efficacy of ESNs was evaluated in human breast cancer MCF-7 cells. ESNs loaded with hydrophobic drugs were successfully constructed, and showed high entrapment efficiency and drug loading. The nanocarrier successfully achieved self-disintegration in a PBS environment of pH value at 5.0, and showed excellent antitumor effect in vitro. ESNs can effectively load hydrophobic drugs and achieve self-disintegration, while avoiding toxicity from the accumulation of the nanocarrier. These results suggest that ESNs are a promising drug delivery system capable of maximizing the anticancer therapeutic efficacy and minimizing the systemic toxicity.
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spelling pubmed-86946302022-04-13 The pH-triggered drug release and simultaneous carrier decomposition of effervescent SiO(2)–drug–Na(2)CO(3) composite nanoparticles: to improve the antitumor activity of hydrophobic drugs Chen, Tianyu Jiang, Yichun Wang, Changmao Cai, Zhengxue Chen, Hui Zhu, Junliang Tao, Pinrun Wu, Min RSC Adv Chemistry To achieve a better release effect of hydrophobic drugs and spontaneous nanocarrier disintegration by dissolution as well as the CO(2) production of Na(2)CO(3) further, improving the therapeutic effect of hydrophobic drugs, and thereby avoiding the accumulation of the nanocarrier in vivo to produce organ toxicity, effervescent SiO(2)–drug–Na(2)CO(3) composite nanoparticles (ESNs) were prepared in this study using a tetraethyl orthosilicate hydrolysis method. Sodium carbonate was used as the effervescent disintegrant to respond to the acidic microenvironment of the tumor. The properties of ESNs were assessed and TEM images were taken to verify the self-disintegration characteristics of nanocarrier materials. The in vitro anticancer efficacy of ESNs was evaluated in human breast cancer MCF-7 cells. ESNs loaded with hydrophobic drugs were successfully constructed, and showed high entrapment efficiency and drug loading. The nanocarrier successfully achieved self-disintegration in a PBS environment of pH value at 5.0, and showed excellent antitumor effect in vitro. ESNs can effectively load hydrophobic drugs and achieve self-disintegration, while avoiding toxicity from the accumulation of the nanocarrier. These results suggest that ESNs are a promising drug delivery system capable of maximizing the anticancer therapeutic efficacy and minimizing the systemic toxicity. The Royal Society of Chemistry 2021-01-28 /pmc/articles/PMC8694630/ /pubmed/35423073 http://dx.doi.org/10.1039/d0ra07896d Text en This journal is © The Royal Society of Chemistry https://creativecommons.org/licenses/by-nc/3.0/
spellingShingle Chemistry
Chen, Tianyu
Jiang, Yichun
Wang, Changmao
Cai, Zhengxue
Chen, Hui
Zhu, Junliang
Tao, Pinrun
Wu, Min
The pH-triggered drug release and simultaneous carrier decomposition of effervescent SiO(2)–drug–Na(2)CO(3) composite nanoparticles: to improve the antitumor activity of hydrophobic drugs
title The pH-triggered drug release and simultaneous carrier decomposition of effervescent SiO(2)–drug–Na(2)CO(3) composite nanoparticles: to improve the antitumor activity of hydrophobic drugs
title_full The pH-triggered drug release and simultaneous carrier decomposition of effervescent SiO(2)–drug–Na(2)CO(3) composite nanoparticles: to improve the antitumor activity of hydrophobic drugs
title_fullStr The pH-triggered drug release and simultaneous carrier decomposition of effervescent SiO(2)–drug–Na(2)CO(3) composite nanoparticles: to improve the antitumor activity of hydrophobic drugs
title_full_unstemmed The pH-triggered drug release and simultaneous carrier decomposition of effervescent SiO(2)–drug–Na(2)CO(3) composite nanoparticles: to improve the antitumor activity of hydrophobic drugs
title_short The pH-triggered drug release and simultaneous carrier decomposition of effervescent SiO(2)–drug–Na(2)CO(3) composite nanoparticles: to improve the antitumor activity of hydrophobic drugs
title_sort ph-triggered drug release and simultaneous carrier decomposition of effervescent sio(2)–drug–na(2)co(3) composite nanoparticles: to improve the antitumor activity of hydrophobic drugs
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8694630/
https://www.ncbi.nlm.nih.gov/pubmed/35423073
http://dx.doi.org/10.1039/d0ra07896d
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