Degradable Spirocyclic Polyacetal-Based Core-Amphiphilic Assemblies for Encapsulation and Release of Hydrophobic Cargo

Polymeric nanomaterials that degrade in acidic environments have gained considerable attention in nanomedicine for intracellular drug delivery and cancer therapy. Among various acid-degradable linkages, spirocyclic acetals have rarely been used to fabricate such vehicles. In addition to acid sensiti...

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Main Authors: Brandon Andrade-Gagnon, Marilyne Bélanger-Bouliga, Phuong Trang Nguyen, Thi Hong Diep Nguyen, Steve Bourgault, Ali Nazemi
Format: Article
Language:English
Published: MDPI AG 2021-01-01
Series:Nanomaterials
Subjects:
Online Access:https://www.mdpi.com/2079-4991/11/1/161
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spelling doaj-6c94026bee364f27946715c0bd5748902021-01-11T00:00:45ZengMDPI AGNanomaterials2079-49912021-01-011116116110.3390/nano11010161Degradable Spirocyclic Polyacetal-Based Core-Amphiphilic Assemblies for Encapsulation and Release of Hydrophobic CargoBrandon Andrade-Gagnon0Marilyne Bélanger-Bouliga1Phuong Trang Nguyen2Thi Hong Diep Nguyen3Steve Bourgault4Ali Nazemi5Department of Chemistry, Université du Québec à Montréal, C.P.8888, Succursale Centre-Ville, Montréal, QC H3C 3P8, CanadaDepartment of Chemistry, Université du Québec à Montréal, C.P.8888, Succursale Centre-Ville, Montréal, QC H3C 3P8, CanadaDepartment of Chemistry, Université du Québec à Montréal, C.P.8888, Succursale Centre-Ville, Montréal, QC H3C 3P8, CanadaDepartment of Chemistry, Université du Québec à Montréal, C.P.8888, Succursale Centre-Ville, Montréal, QC H3C 3P8, CanadaDepartment of Chemistry, Université du Québec à Montréal, C.P.8888, Succursale Centre-Ville, Montréal, QC H3C 3P8, CanadaDepartment of Chemistry, Université du Québec à Montréal, C.P.8888, Succursale Centre-Ville, Montréal, QC H3C 3P8, CanadaPolymeric nanomaterials that degrade in acidic environments have gained considerable attention in nanomedicine for intracellular drug delivery and cancer therapy. Among various acid-degradable linkages, spirocyclic acetals have rarely been used to fabricate such vehicles. In addition to acid sensitivity, they benefit from conformational rigidity that is otherwise not attainable by their non-spirocyclic analogs. Herein, amphiphilic spirocyclic polyacetals are synthesized by Cu-catalyzed alkyne–azide “click” polymerization. Unlike conventional block copolymers, which often form core–shell structures, these polymers self-assemble to form core amphiphilic assemblies capable of encapsulating Nile red as a hydrophobic model drug. In vitro experiments show that while release from these materials can occur at neutral pH with preservation of their integrity, acidic pH accelerates efficient cargo release and leads to the complete degradation of assemblies. Moreover, cellular assays reveal that these materials are fully cytocompatible, interact with the plasma membrane, and can be internalized by cells, rendering them as potential candidates for cancer therapy and/or drug delivery.https://www.mdpi.com/2079-4991/11/1/161pH-degradable nanoparticlesspirocyclic polyacetalsdrug deliverycytocompatibilitystimuli-responsive nanomaterials
collection DOAJ
language English
format Article
sources DOAJ
author Brandon Andrade-Gagnon
Marilyne Bélanger-Bouliga
Phuong Trang Nguyen
Thi Hong Diep Nguyen
Steve Bourgault
Ali Nazemi
spellingShingle Brandon Andrade-Gagnon
Marilyne Bélanger-Bouliga
Phuong Trang Nguyen
Thi Hong Diep Nguyen
Steve Bourgault
Ali Nazemi
Degradable Spirocyclic Polyacetal-Based Core-Amphiphilic Assemblies for Encapsulation and Release of Hydrophobic Cargo
Nanomaterials
pH-degradable nanoparticles
spirocyclic polyacetals
drug delivery
cytocompatibility
stimuli-responsive nanomaterials
author_facet Brandon Andrade-Gagnon
Marilyne Bélanger-Bouliga
Phuong Trang Nguyen
Thi Hong Diep Nguyen
Steve Bourgault
Ali Nazemi
author_sort Brandon Andrade-Gagnon
title Degradable Spirocyclic Polyacetal-Based Core-Amphiphilic Assemblies for Encapsulation and Release of Hydrophobic Cargo
title_short Degradable Spirocyclic Polyacetal-Based Core-Amphiphilic Assemblies for Encapsulation and Release of Hydrophobic Cargo
title_full Degradable Spirocyclic Polyacetal-Based Core-Amphiphilic Assemblies for Encapsulation and Release of Hydrophobic Cargo
title_fullStr Degradable Spirocyclic Polyacetal-Based Core-Amphiphilic Assemblies for Encapsulation and Release of Hydrophobic Cargo
title_full_unstemmed Degradable Spirocyclic Polyacetal-Based Core-Amphiphilic Assemblies for Encapsulation and Release of Hydrophobic Cargo
title_sort degradable spirocyclic polyacetal-based core-amphiphilic assemblies for encapsulation and release of hydrophobic cargo
publisher MDPI AG
series Nanomaterials
issn 2079-4991
publishDate 2021-01-01
description Polymeric nanomaterials that degrade in acidic environments have gained considerable attention in nanomedicine for intracellular drug delivery and cancer therapy. Among various acid-degradable linkages, spirocyclic acetals have rarely been used to fabricate such vehicles. In addition to acid sensitivity, they benefit from conformational rigidity that is otherwise not attainable by their non-spirocyclic analogs. Herein, amphiphilic spirocyclic polyacetals are synthesized by Cu-catalyzed alkyne–azide “click” polymerization. Unlike conventional block copolymers, which often form core–shell structures, these polymers self-assemble to form core amphiphilic assemblies capable of encapsulating Nile red as a hydrophobic model drug. In vitro experiments show that while release from these materials can occur at neutral pH with preservation of their integrity, acidic pH accelerates efficient cargo release and leads to the complete degradation of assemblies. Moreover, cellular assays reveal that these materials are fully cytocompatible, interact with the plasma membrane, and can be internalized by cells, rendering them as potential candidates for cancer therapy and/or drug delivery.
topic pH-degradable nanoparticles
spirocyclic polyacetals
drug delivery
cytocompatibility
stimuli-responsive nanomaterials
url https://www.mdpi.com/2079-4991/11/1/161
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