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Dual-mode US/MRI nanoparticles delivering siRNA and Pt(iv) for ovarian cancer treatment

As known to all, ovarian cancer ranks the most lethal of the gynecological malignancies. The antitumor drugs based on platinum are first-line chemotherapy drugs for ovarian cancer. However, their therapeutic efficiency is severely limited owing to dose-limiting toxicities of platinum. New theranosti...

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Autores principales: Zhang, Yanhua, Huang, Hui, Fu, Hao, Zhao, Meng, Wu, Zhihua, Dong, Yang, Li, He, Duan, Yourong, Sun, Ying
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Royal Society of Chemistry 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9073344/
https://www.ncbi.nlm.nih.gov/pubmed/35529112
http://dx.doi.org/10.1039/c9ra03681d
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author Zhang, Yanhua
Huang, Hui
Fu, Hao
Zhao, Meng
Wu, Zhihua
Dong, Yang
Li, He
Duan, Yourong
Sun, Ying
author_facet Zhang, Yanhua
Huang, Hui
Fu, Hao
Zhao, Meng
Wu, Zhihua
Dong, Yang
Li, He
Duan, Yourong
Sun, Ying
author_sort Zhang, Yanhua
collection PubMed
description As known to all, ovarian cancer ranks the most lethal of the gynecological malignancies. The antitumor drugs based on platinum are first-line chemotherapy drugs for ovarian cancer. However, their therapeutic efficiency is severely limited owing to dose-limiting toxicities of platinum. New theranostic strategies to overcome chemotherapy toxicity is highly desirable. Meanwhile, the real-time treating effect is not visible for doctors. Herein, we constructed PFH/siRNA/Fe(3)O(4)@Pt(iv) NPs-cRGD (NPs-cRGD) for precise theranostics against ovarian tumors with real-time imaging. The NPs-cRGD had a good storage stability and resisted the serum-induced aggregation, which was beneficial for drug delivery. Additionally, gel-retardation assay demonstrated that the NPs-cRGD exhibited great protection to siRNA to resist nuclease degradation. In vitro, the NPs-cRGD showed good dual-mode US/MRI imaging and the relative imaging research was also discussed. Moreover, the in vitro experiments indicated that the NPs-cRGD with US exhibited excellent antitumor therapeutic efficiency, resulting from the cRGD ligands and US exposure enhanced the cellular uptake efficiency. Thus, the dual-mode nanoparticles in this work may provide precious insight into the development of various multi-mode nanoplatforms delivering drugs or genes for precise theranostics against various cancer.
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spelling pubmed-90733442022-05-06 Dual-mode US/MRI nanoparticles delivering siRNA and Pt(iv) for ovarian cancer treatment Zhang, Yanhua Huang, Hui Fu, Hao Zhao, Meng Wu, Zhihua Dong, Yang Li, He Duan, Yourong Sun, Ying RSC Adv Chemistry As known to all, ovarian cancer ranks the most lethal of the gynecological malignancies. The antitumor drugs based on platinum are first-line chemotherapy drugs for ovarian cancer. However, their therapeutic efficiency is severely limited owing to dose-limiting toxicities of platinum. New theranostic strategies to overcome chemotherapy toxicity is highly desirable. Meanwhile, the real-time treating effect is not visible for doctors. Herein, we constructed PFH/siRNA/Fe(3)O(4)@Pt(iv) NPs-cRGD (NPs-cRGD) for precise theranostics against ovarian tumors with real-time imaging. The NPs-cRGD had a good storage stability and resisted the serum-induced aggregation, which was beneficial for drug delivery. Additionally, gel-retardation assay demonstrated that the NPs-cRGD exhibited great protection to siRNA to resist nuclease degradation. In vitro, the NPs-cRGD showed good dual-mode US/MRI imaging and the relative imaging research was also discussed. Moreover, the in vitro experiments indicated that the NPs-cRGD with US exhibited excellent antitumor therapeutic efficiency, resulting from the cRGD ligands and US exposure enhanced the cellular uptake efficiency. Thus, the dual-mode nanoparticles in this work may provide precious insight into the development of various multi-mode nanoplatforms delivering drugs or genes for precise theranostics against various cancer. The Royal Society of Chemistry 2019-10-17 /pmc/articles/PMC9073344/ /pubmed/35529112 http://dx.doi.org/10.1039/c9ra03681d Text en This journal is © The Royal Society of Chemistry https://creativecommons.org/licenses/by-nc/3.0/
spellingShingle Chemistry
Zhang, Yanhua
Huang, Hui
Fu, Hao
Zhao, Meng
Wu, Zhihua
Dong, Yang
Li, He
Duan, Yourong
Sun, Ying
Dual-mode US/MRI nanoparticles delivering siRNA and Pt(iv) for ovarian cancer treatment
title Dual-mode US/MRI nanoparticles delivering siRNA and Pt(iv) for ovarian cancer treatment
title_full Dual-mode US/MRI nanoparticles delivering siRNA and Pt(iv) for ovarian cancer treatment
title_fullStr Dual-mode US/MRI nanoparticles delivering siRNA and Pt(iv) for ovarian cancer treatment
title_full_unstemmed Dual-mode US/MRI nanoparticles delivering siRNA and Pt(iv) for ovarian cancer treatment
title_short Dual-mode US/MRI nanoparticles delivering siRNA and Pt(iv) for ovarian cancer treatment
title_sort dual-mode us/mri nanoparticles delivering sirna and pt(iv) for ovarian cancer treatment
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9073344/
https://www.ncbi.nlm.nih.gov/pubmed/35529112
http://dx.doi.org/10.1039/c9ra03681d
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