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Selective Intratumoral Drug Release and Simultaneous Inhibition of Oxidative Stress by a Highly Reductive Nanosystem and Its Application as an Anti-tumor Agent

Excessive oxidative stress is always associated with the serious side effects of chemotherapy. In the current study, we developed a vitamin E based strongly reductive nanosystem to increase the loading efficiency of docetaxel (DTX, DTX-VNS), reduce its side toxicity and enhance the antitumor effect....

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Autores principales: Zhu, Chunqi, Luo, Lihua, jiang, Xindong, Jiang, Mengshi, Luo, Zhenyu, Li, Xiang, Qiu, Weigen, Jin, Zhaolei, Shen, Tianxiang, Li, Chunlong, Li, Qingpo, Qiu, Yunqing, You, Jian
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6956823/
https://www.ncbi.nlm.nih.gov/pubmed/31938058
http://dx.doi.org/10.7150/thno.38627
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author Zhu, Chunqi
Luo, Lihua
jiang, Xindong
Jiang, Mengshi
Luo, Zhenyu
Li, Xiang
Qiu, Weigen
Jin, Zhaolei
Shen, Tianxiang
Li, Chunlong
Li, Qingpo
Qiu, Yunqing
You, Jian
author_facet Zhu, Chunqi
Luo, Lihua
jiang, Xindong
Jiang, Mengshi
Luo, Zhenyu
Li, Xiang
Qiu, Weigen
Jin, Zhaolei
Shen, Tianxiang
Li, Chunlong
Li, Qingpo
Qiu, Yunqing
You, Jian
author_sort Zhu, Chunqi
collection PubMed
description Excessive oxidative stress is always associated with the serious side effects of chemotherapy. In the current study, we developed a vitamin E based strongly reductive nanosystem to increase the loading efficiency of docetaxel (DTX, DTX-VNS), reduce its side toxicity and enhance the antitumor effect. Methods: We used Förster Resonance Energy Transfer (FRET) to reveal the in vivo and in vitro fate of DTX-VNS over time. All FRET images were observed using the Maestro imaging system (CRI, Inc., Woburn, MA) and Fluo-View software (Olympus LX83-FV3000). Results: Through FRET analyzing, we found that our nanosystem showed a selective rapider release of drugs in tumors compared to normal organs due to the higher levels of ROS in tumor cells than normal cells, and the accumulation of DTX at tumor sites in the DTX-VNS group was also notably more than that in the Taxotere group after 24 h injection. Meanwhile, DTX-VNS had a prominently stronger anti-tumor effect in various models than Taxotere, and had a synergistic effect of immunotherapy. Conclusions: Our work presented a useful reference for clinical exploration of the in vivo behavior of nanocarriers (DTX-VNS), inhibition oxidative stress and selective release of drugs at tumor sites, thus reducing the side effects and enhancing the anti-tumor effects.
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spelling pubmed-69568232020-01-14 Selective Intratumoral Drug Release and Simultaneous Inhibition of Oxidative Stress by a Highly Reductive Nanosystem and Its Application as an Anti-tumor Agent Zhu, Chunqi Luo, Lihua jiang, Xindong Jiang, Mengshi Luo, Zhenyu Li, Xiang Qiu, Weigen Jin, Zhaolei Shen, Tianxiang Li, Chunlong Li, Qingpo Qiu, Yunqing You, Jian Theranostics Research Paper Excessive oxidative stress is always associated with the serious side effects of chemotherapy. In the current study, we developed a vitamin E based strongly reductive nanosystem to increase the loading efficiency of docetaxel (DTX, DTX-VNS), reduce its side toxicity and enhance the antitumor effect. Methods: We used Förster Resonance Energy Transfer (FRET) to reveal the in vivo and in vitro fate of DTX-VNS over time. All FRET images were observed using the Maestro imaging system (CRI, Inc., Woburn, MA) and Fluo-View software (Olympus LX83-FV3000). Results: Through FRET analyzing, we found that our nanosystem showed a selective rapider release of drugs in tumors compared to normal organs due to the higher levels of ROS in tumor cells than normal cells, and the accumulation of DTX at tumor sites in the DTX-VNS group was also notably more than that in the Taxotere group after 24 h injection. Meanwhile, DTX-VNS had a prominently stronger anti-tumor effect in various models than Taxotere, and had a synergistic effect of immunotherapy. Conclusions: Our work presented a useful reference for clinical exploration of the in vivo behavior of nanocarriers (DTX-VNS), inhibition oxidative stress and selective release of drugs at tumor sites, thus reducing the side effects and enhancing the anti-tumor effects. Ivyspring International Publisher 2020-01-01 /pmc/articles/PMC6956823/ /pubmed/31938058 http://dx.doi.org/10.7150/thno.38627 Text en © The author(s) This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Zhu, Chunqi
Luo, Lihua
jiang, Xindong
Jiang, Mengshi
Luo, Zhenyu
Li, Xiang
Qiu, Weigen
Jin, Zhaolei
Shen, Tianxiang
Li, Chunlong
Li, Qingpo
Qiu, Yunqing
You, Jian
Selective Intratumoral Drug Release and Simultaneous Inhibition of Oxidative Stress by a Highly Reductive Nanosystem and Its Application as an Anti-tumor Agent
title Selective Intratumoral Drug Release and Simultaneous Inhibition of Oxidative Stress by a Highly Reductive Nanosystem and Its Application as an Anti-tumor Agent
title_full Selective Intratumoral Drug Release and Simultaneous Inhibition of Oxidative Stress by a Highly Reductive Nanosystem and Its Application as an Anti-tumor Agent
title_fullStr Selective Intratumoral Drug Release and Simultaneous Inhibition of Oxidative Stress by a Highly Reductive Nanosystem and Its Application as an Anti-tumor Agent
title_full_unstemmed Selective Intratumoral Drug Release and Simultaneous Inhibition of Oxidative Stress by a Highly Reductive Nanosystem and Its Application as an Anti-tumor Agent
title_short Selective Intratumoral Drug Release and Simultaneous Inhibition of Oxidative Stress by a Highly Reductive Nanosystem and Its Application as an Anti-tumor Agent
title_sort selective intratumoral drug release and simultaneous inhibition of oxidative stress by a highly reductive nanosystem and its application as an anti-tumor agent
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6956823/
https://www.ncbi.nlm.nih.gov/pubmed/31938058
http://dx.doi.org/10.7150/thno.38627
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