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Formulation of Metal–Organic Framework-Based Drug Carriers by Controlled Coordination of Methoxy PEG Phosphate: Boosting Colloidal Stability and Redispersibility

[Image: see text] Metal–organic framework nanoparticles (nanoMOFs) have been widely studied in biomedical applications. Although substantial efforts have been devoted to the development of biocompatible approaches, the requirement of tedious synthetic steps, toxic reagents, and limitations on the sh...

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Autores principales: Chen, Xu, Zhuang, Yunhui, Rampal, Nakul, Hewitt, Rachel, Divitini, Giorgio, O’Keefe, Christopher A., Liu, Xiewen, Whitaker, Daniel J., Wills, John W., Jugdaohsingh, Ravin, Powell, Jonathan J., Yu, Han, Grey, Clare P., Scherman, Oren A., Fairen-Jimenez, David
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2021
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8414479/
https://www.ncbi.nlm.nih.gov/pubmed/34357768
http://dx.doi.org/10.1021/jacs.1c03943
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author Chen, Xu
Zhuang, Yunhui
Rampal, Nakul
Hewitt, Rachel
Divitini, Giorgio
O’Keefe, Christopher A.
Liu, Xiewen
Whitaker, Daniel J.
Wills, John W.
Jugdaohsingh, Ravin
Powell, Jonathan J.
Yu, Han
Grey, Clare P.
Scherman, Oren A.
Fairen-Jimenez, David
author_facet Chen, Xu
Zhuang, Yunhui
Rampal, Nakul
Hewitt, Rachel
Divitini, Giorgio
O’Keefe, Christopher A.
Liu, Xiewen
Whitaker, Daniel J.
Wills, John W.
Jugdaohsingh, Ravin
Powell, Jonathan J.
Yu, Han
Grey, Clare P.
Scherman, Oren A.
Fairen-Jimenez, David
author_sort Chen, Xu
collection PubMed
description [Image: see text] Metal–organic framework nanoparticles (nanoMOFs) have been widely studied in biomedical applications. Although substantial efforts have been devoted to the development of biocompatible approaches, the requirement of tedious synthetic steps, toxic reagents, and limitations on the shelf life of nanoparticles in solution are still significant barriers to their translation to clinical use. In this work, we propose a new postsynthetic modification of nanoMOFs with phosphate-functionalized methoxy polyethylene glycol (mPEG–PO(3)) groups which, when combined with lyophilization, leads to the formation of redispersible solid materials. This approach can serve as a facile and general formulation method for the storage of bare or drug-loaded nanoMOFs. The obtained PEGylated nanoMOFs show stable hydrodynamic diameters, improved colloidal stability, and delayed drug-release kinetics compared to their parent nanoMOFs. Ex situ characterization and computational studies reveal that PEGylation of PCN-222 proceeds in a two-step fashion. Most importantly, the lyophilized, PEGylated nanoMOFs can be completely redispersed in water, avoiding common aggregation issues that have limited the use of MOFs in the biomedical field to the wet form—a critical limitation for their translation to clinical use as these materials can now be stored as dried samples. The in vitro performance of the addition of mPEG–PO(3) was confirmed by the improved intracellular stability and delayed drug-release capability, including lower cytotoxicity compared with that of the bare nanoMOFs. Furthermore, z-stack confocal microscopy images reveal the colocalization of bare and PEGylated nanoMOFs. This research highlights a facile PEGylation method with mPEG–PO(3), providing new insights into the design of promising nanocarriers for drug delivery.
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spelling pubmed-84144792021-09-03 Formulation of Metal–Organic Framework-Based Drug Carriers by Controlled Coordination of Methoxy PEG Phosphate: Boosting Colloidal Stability and Redispersibility Chen, Xu Zhuang, Yunhui Rampal, Nakul Hewitt, Rachel Divitini, Giorgio O’Keefe, Christopher A. Liu, Xiewen Whitaker, Daniel J. Wills, John W. Jugdaohsingh, Ravin Powell, Jonathan J. Yu, Han Grey, Clare P. Scherman, Oren A. Fairen-Jimenez, David J Am Chem Soc [Image: see text] Metal–organic framework nanoparticles (nanoMOFs) have been widely studied in biomedical applications. Although substantial efforts have been devoted to the development of biocompatible approaches, the requirement of tedious synthetic steps, toxic reagents, and limitations on the shelf life of nanoparticles in solution are still significant barriers to their translation to clinical use. In this work, we propose a new postsynthetic modification of nanoMOFs with phosphate-functionalized methoxy polyethylene glycol (mPEG–PO(3)) groups which, when combined with lyophilization, leads to the formation of redispersible solid materials. This approach can serve as a facile and general formulation method for the storage of bare or drug-loaded nanoMOFs. The obtained PEGylated nanoMOFs show stable hydrodynamic diameters, improved colloidal stability, and delayed drug-release kinetics compared to their parent nanoMOFs. Ex situ characterization and computational studies reveal that PEGylation of PCN-222 proceeds in a two-step fashion. Most importantly, the lyophilized, PEGylated nanoMOFs can be completely redispersed in water, avoiding common aggregation issues that have limited the use of MOFs in the biomedical field to the wet form—a critical limitation for their translation to clinical use as these materials can now be stored as dried samples. The in vitro performance of the addition of mPEG–PO(3) was confirmed by the improved intracellular stability and delayed drug-release capability, including lower cytotoxicity compared with that of the bare nanoMOFs. Furthermore, z-stack confocal microscopy images reveal the colocalization of bare and PEGylated nanoMOFs. This research highlights a facile PEGylation method with mPEG–PO(3), providing new insights into the design of promising nanocarriers for drug delivery. American Chemical Society 2021-08-06 2021-09-01 /pmc/articles/PMC8414479/ /pubmed/34357768 http://dx.doi.org/10.1021/jacs.1c03943 Text en © 2021 The Authors. Published by American Chemical Society https://creativecommons.org/licenses/by/4.0/Permits the broadest form of re-use including for commercial purposes, provided that author attribution and integrity are maintained (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Chen, Xu
Zhuang, Yunhui
Rampal, Nakul
Hewitt, Rachel
Divitini, Giorgio
O’Keefe, Christopher A.
Liu, Xiewen
Whitaker, Daniel J.
Wills, John W.
Jugdaohsingh, Ravin
Powell, Jonathan J.
Yu, Han
Grey, Clare P.
Scherman, Oren A.
Fairen-Jimenez, David
Formulation of Metal–Organic Framework-Based Drug Carriers by Controlled Coordination of Methoxy PEG Phosphate: Boosting Colloidal Stability and Redispersibility
title Formulation of Metal–Organic Framework-Based Drug Carriers by Controlled Coordination of Methoxy PEG Phosphate: Boosting Colloidal Stability and Redispersibility
title_full Formulation of Metal–Organic Framework-Based Drug Carriers by Controlled Coordination of Methoxy PEG Phosphate: Boosting Colloidal Stability and Redispersibility
title_fullStr Formulation of Metal–Organic Framework-Based Drug Carriers by Controlled Coordination of Methoxy PEG Phosphate: Boosting Colloidal Stability and Redispersibility
title_full_unstemmed Formulation of Metal–Organic Framework-Based Drug Carriers by Controlled Coordination of Methoxy PEG Phosphate: Boosting Colloidal Stability and Redispersibility
title_short Formulation of Metal–Organic Framework-Based Drug Carriers by Controlled Coordination of Methoxy PEG Phosphate: Boosting Colloidal Stability and Redispersibility
title_sort formulation of metal–organic framework-based drug carriers by controlled coordination of methoxy peg phosphate: boosting colloidal stability and redispersibility
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8414479/
https://www.ncbi.nlm.nih.gov/pubmed/34357768
http://dx.doi.org/10.1021/jacs.1c03943
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