β-Cyclodextrin-poly (β-Amino Ester) Nanoparticles Are a Generalizable Strategy for High Loading and Sustained Release of HDAC Inhibitors

[Image: see text] Therapeutic development of histone deacetylase inhibitors (HDACi) has been hampered by a number of barriers to drug delivery, including poor solubility and inadequate tissue penetration. Nanoparticle encapsulation could be one approach to improve the delivery of HDACi to target tis...

Descripción completa

Detalles Bibliográficos
Autores principales: Chaudhuri, Sauradip, Fowler, Martha J., Baker, Cassandra, Stopka, Sylwia A., Regan, Michael S., Sablatura, Lindsey, Broughton, Colton W., Knight, Brandon E., Stabenfeldt, Sarah E., Agar, Nathalie Y. R., Sirianni, Rachael W.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2021
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8153536/
https://www.ncbi.nlm.nih.gov/pubmed/33905245
http://dx.doi.org/10.1021/acsami.0c22587
_version_ 1783698820399366144
author Chaudhuri, Sauradip
Fowler, Martha J.
Baker, Cassandra
Stopka, Sylwia A.
Regan, Michael S.
Sablatura, Lindsey
Broughton, Colton W.
Knight, Brandon E.
Stabenfeldt, Sarah E.
Agar, Nathalie Y. R.
Sirianni, Rachael W.
author_facet Chaudhuri, Sauradip
Fowler, Martha J.
Baker, Cassandra
Stopka, Sylwia A.
Regan, Michael S.
Sablatura, Lindsey
Broughton, Colton W.
Knight, Brandon E.
Stabenfeldt, Sarah E.
Agar, Nathalie Y. R.
Sirianni, Rachael W.
author_sort Chaudhuri, Sauradip
collection PubMed
description [Image: see text] Therapeutic development of histone deacetylase inhibitors (HDACi) has been hampered by a number of barriers to drug delivery, including poor solubility and inadequate tissue penetration. Nanoparticle encapsulation could be one approach to improve the delivery of HDACi to target tissues; however, effective and generalizable loading of HDACi within nanoparticle systems remains a long-term challenge. We hypothesized that the common terminally ionizable moiety on many HDACi molecules could be capitalized upon for loading in polymeric nanoparticles. Here, we describe the simple, efficient formulation of a novel library of β-cyclodextrin-poly (β-amino ester) networks (CDN) to achieve this goal. We observed that network architecture was a critical determinant of CDN encapsulation of candidate molecules, with a more hydrophobic core enabling effective self-assembly and a PEGylated surface enabling high loading (up to ∼30% w/w), effective self-assembly of the nanoparticle, and slow release of drug into aqueous media (up to 24 days) for the model HDACi panobinostat. We next constructed a library of CDNs to encapsulate various small, hydrophobic, terminally ionizable molecules (panobinostat, quisinostat, dacinostat, givinostat, bortezomib, camptothecin, nile red, and cytarabine), which yielded important insights into the structural requirements for effective drug loading and CDN self-assembly. Optimized CDN nanoparticles were taken up by GL261 cells in culture and a released panobinostat was confirmed to be bioactive. Panobinostat-loaded CDNs were next administered by convection-enhanced delivery (CED) to mice bearing intracranial GL261 tumors. These studies confirm that CDN encapsulation enables a higher deliverable dose of drug to effectively slow tumor growth. Matrix-assisted laser desorption/ionization (MALDI) analysis on tissue sections confirms higher exposure of tumor to drug, which likely accounts for the therapeutic effects. Taken in sum, these studies present a novel nanocarrier platform for encapsulation of HDACi via both ionic and hydrophobic interactions, which is an important step toward better treatment of disease via HDACi therapy.
format Online
Article
Text
id pubmed-8153536
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher American Chemical Society
record_format MEDLINE/PubMed
spelling pubmed-81535362021-05-27 β-Cyclodextrin-poly (β-Amino Ester) Nanoparticles Are a Generalizable Strategy for High Loading and Sustained Release of HDAC Inhibitors Chaudhuri, Sauradip Fowler, Martha J. Baker, Cassandra Stopka, Sylwia A. Regan, Michael S. Sablatura, Lindsey Broughton, Colton W. Knight, Brandon E. Stabenfeldt, Sarah E. Agar, Nathalie Y. R. Sirianni, Rachael W. ACS Appl Mater Interfaces [Image: see text] Therapeutic development of histone deacetylase inhibitors (HDACi) has been hampered by a number of barriers to drug delivery, including poor solubility and inadequate tissue penetration. Nanoparticle encapsulation could be one approach to improve the delivery of HDACi to target tissues; however, effective and generalizable loading of HDACi within nanoparticle systems remains a long-term challenge. We hypothesized that the common terminally ionizable moiety on many HDACi molecules could be capitalized upon for loading in polymeric nanoparticles. Here, we describe the simple, efficient formulation of a novel library of β-cyclodextrin-poly (β-amino ester) networks (CDN) to achieve this goal. We observed that network architecture was a critical determinant of CDN encapsulation of candidate molecules, with a more hydrophobic core enabling effective self-assembly and a PEGylated surface enabling high loading (up to ∼30% w/w), effective self-assembly of the nanoparticle, and slow release of drug into aqueous media (up to 24 days) for the model HDACi panobinostat. We next constructed a library of CDNs to encapsulate various small, hydrophobic, terminally ionizable molecules (panobinostat, quisinostat, dacinostat, givinostat, bortezomib, camptothecin, nile red, and cytarabine), which yielded important insights into the structural requirements for effective drug loading and CDN self-assembly. Optimized CDN nanoparticles were taken up by GL261 cells in culture and a released panobinostat was confirmed to be bioactive. Panobinostat-loaded CDNs were next administered by convection-enhanced delivery (CED) to mice bearing intracranial GL261 tumors. These studies confirm that CDN encapsulation enables a higher deliverable dose of drug to effectively slow tumor growth. Matrix-assisted laser desorption/ionization (MALDI) analysis on tissue sections confirms higher exposure of tumor to drug, which likely accounts for the therapeutic effects. Taken in sum, these studies present a novel nanocarrier platform for encapsulation of HDACi via both ionic and hydrophobic interactions, which is an important step toward better treatment of disease via HDACi therapy. American Chemical Society 2021-04-27 2021-05-12 /pmc/articles/PMC8153536/ /pubmed/33905245 http://dx.doi.org/10.1021/acsami.0c22587 Text en © 2021 The Authors. Published by American Chemical Society Permits non-commercial access and re-use, provided that author attribution and integrity are maintained; but does not permit creation of adaptations or other derivative works (https://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Chaudhuri, Sauradip
Fowler, Martha J.
Baker, Cassandra
Stopka, Sylwia A.
Regan, Michael S.
Sablatura, Lindsey
Broughton, Colton W.
Knight, Brandon E.
Stabenfeldt, Sarah E.
Agar, Nathalie Y. R.
Sirianni, Rachael W.
β-Cyclodextrin-poly (β-Amino Ester) Nanoparticles Are a Generalizable Strategy for High Loading and Sustained Release of HDAC Inhibitors
title β-Cyclodextrin-poly (β-Amino Ester) Nanoparticles Are a Generalizable Strategy for High Loading and Sustained Release of HDAC Inhibitors
title_full β-Cyclodextrin-poly (β-Amino Ester) Nanoparticles Are a Generalizable Strategy for High Loading and Sustained Release of HDAC Inhibitors
title_fullStr β-Cyclodextrin-poly (β-Amino Ester) Nanoparticles Are a Generalizable Strategy for High Loading and Sustained Release of HDAC Inhibitors
title_full_unstemmed β-Cyclodextrin-poly (β-Amino Ester) Nanoparticles Are a Generalizable Strategy for High Loading and Sustained Release of HDAC Inhibitors
title_short β-Cyclodextrin-poly (β-Amino Ester) Nanoparticles Are a Generalizable Strategy for High Loading and Sustained Release of HDAC Inhibitors
title_sort β-cyclodextrin-poly (β-amino ester) nanoparticles are a generalizable strategy for high loading and sustained release of hdac inhibitors
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8153536/
https://www.ncbi.nlm.nih.gov/pubmed/33905245
http://dx.doi.org/10.1021/acsami.0c22587
work_keys_str_mv AT chaudhurisauradip bcyclodextrinpolybaminoesternanoparticlesareageneralizablestrategyforhighloadingandsustainedreleaseofhdacinhibitors
AT fowlermarthaj bcyclodextrinpolybaminoesternanoparticlesareageneralizablestrategyforhighloadingandsustainedreleaseofhdacinhibitors
AT bakercassandra bcyclodextrinpolybaminoesternanoparticlesareageneralizablestrategyforhighloadingandsustainedreleaseofhdacinhibitors
AT stopkasylwiaa bcyclodextrinpolybaminoesternanoparticlesareageneralizablestrategyforhighloadingandsustainedreleaseofhdacinhibitors
AT reganmichaels bcyclodextrinpolybaminoesternanoparticlesareageneralizablestrategyforhighloadingandsustainedreleaseofhdacinhibitors
AT sablaturalindsey bcyclodextrinpolybaminoesternanoparticlesareageneralizablestrategyforhighloadingandsustainedreleaseofhdacinhibitors
AT broughtoncoltonw bcyclodextrinpolybaminoesternanoparticlesareageneralizablestrategyforhighloadingandsustainedreleaseofhdacinhibitors
AT knightbrandone bcyclodextrinpolybaminoesternanoparticlesareageneralizablestrategyforhighloadingandsustainedreleaseofhdacinhibitors
AT stabenfeldtsarahe bcyclodextrinpolybaminoesternanoparticlesareageneralizablestrategyforhighloadingandsustainedreleaseofhdacinhibitors
AT agarnathalieyr bcyclodextrinpolybaminoesternanoparticlesareageneralizablestrategyforhighloadingandsustainedreleaseofhdacinhibitors
AT siriannirachaelw bcyclodextrinpolybaminoesternanoparticlesareageneralizablestrategyforhighloadingandsustainedreleaseofhdacinhibitors

Ejemplares similares