EPCT-25. SMO PROTEIN DEPLETION IN SHH MEDULLOBLASTOMAS USING MICROBUBBLE-ENHANCED ULTRASOUND AND SIRNA LOADED CATIONIC NANOPARTICLES

RNA-based therapies offer unique advantages for treating pediatric brain tumors. However, the systemic delivery remains a major problem due to degradation of unmodified RNA in biological fluids, poor brain accumulation, and poor cancer cell uptake or escape from the endosomal lipid bilayer barrier....

Descripción completa

Detalles Bibliográficos
Autores principales: Guo, Yutong, Lee, Hohyun, Fang, Zhou, Velalopoulou, Anastasia, Kim, Jinhwan, Thomas, Midhun Ben, Liu, Jingbo, Abramowitz, Ryan G, Kim, YongTae, Coskun, Ahmet F, Krummel, Daniel Pomeranz, Sengupta, Soma, MacDonald, Tobey J, Arvanitis, Costas
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2021
Materias:
Translational/Early Phase Clinical Trials
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8168192/
http://dx.doi.org/10.1093/neuonc/noab090.211
_version_ 1783701839901884416
author Guo, Yutong
Lee, Hohyun
Fang, Zhou
Velalopoulou, Anastasia
Kim, Jinhwan
Thomas, Midhun Ben
Liu, Jingbo
Abramowitz, Ryan G
Kim, YongTae
Coskun, Ahmet F
Krummel, Daniel Pomeranz
Sengupta, Soma
MacDonald, Tobey J
Arvanitis, Costas
author_facet Guo, Yutong
Lee, Hohyun
Fang, Zhou
Velalopoulou, Anastasia
Kim, Jinhwan
Thomas, Midhun Ben
Liu, Jingbo
Abramowitz, Ryan G
Kim, YongTae
Coskun, Ahmet F
Krummel, Daniel Pomeranz
Sengupta, Soma
MacDonald, Tobey J
Arvanitis, Costas
author_sort Guo, Yutong
collection PubMed
description RNA-based therapies offer unique advantages for treating pediatric brain tumors. However, the systemic delivery remains a major problem due to degradation of unmodified RNA in biological fluids, poor brain accumulation, and poor cancer cell uptake or escape from the endosomal lipid bilayer barrier. While nanoparticle encapsulation can prolong circulation time and facilitate cellular uptake, their accumulation in brain tumor remains particularly poor due to their low permeability across the blood-brain barrier and limited intratumoral penetration. Focused ultrasound, when combined with circulating microbubbles (MB-FUS) provides a physical method to transiently modulate the brain tumor microenvironment (TME) and improve nanoparticle delivery. Here, we have examined the delivery of siRNA targeting the Smoothened (SMO) pathway, packaged in 50 nm cationic lipid-polymer hybrid nanoparticles (cLPH:siRNA-SMO), combined with MB-FUS in murine SmoA2 sonic hedgehog (SHH) medulloblastoma. At 30 hours after treatment, we observed the depletion of the SMO protein target, responsible for driving SHH medulloblastoma formation and growth, in mice that had received treatment with MB-FUS and cLPH:siRNA-SMO, but not with cLPH:siRNA-SMO alone. We also confirmed that SMO protein depletion was spatially achieved in the tumor regions with detected cLPH:siRNA-SMO using FISH assay, and that there was 15 fold induction of tumor cell apoptosis compared to tumors in mice that had received cLPH:siRNA-SMO alone. The limited induction of apoptosis was observed with either cLPH:siRNA (non-targeting) or MB-FUS and cLPH:siRNA (non-targeting), suggest that the observed apoptosis induction in the SmoA2 model was the direct result of SMO depletion rather than nonspecific effects of MB-FUS or cLPH:siRNA. Our findings provide a paradigm shift in drug delivery in brain tumors, where physical methods and nanotechnology are tuned together to develop rational strategies for the effective delivery of nucleic acids in brain tumors.
format Online
Article
Text
id pubmed-8168192
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Oxford University Press
record_format MEDLINE/PubMed
spelling pubmed-81681922021-06-02 EPCT-25. SMO PROTEIN DEPLETION IN SHH MEDULLOBLASTOMAS USING MICROBUBBLE-ENHANCED ULTRASOUND AND SIRNA LOADED CATIONIC NANOPARTICLES Guo, Yutong Lee, Hohyun Fang, Zhou Velalopoulou, Anastasia Kim, Jinhwan Thomas, Midhun Ben Liu, Jingbo Abramowitz, Ryan G Kim, YongTae Coskun, Ahmet F Krummel, Daniel Pomeranz Sengupta, Soma MacDonald, Tobey J Arvanitis, Costas Neuro Oncol Translational/Early Phase Clinical Trials RNA-based therapies offer unique advantages for treating pediatric brain tumors. However, the systemic delivery remains a major problem due to degradation of unmodified RNA in biological fluids, poor brain accumulation, and poor cancer cell uptake or escape from the endosomal lipid bilayer barrier. While nanoparticle encapsulation can prolong circulation time and facilitate cellular uptake, their accumulation in brain tumor remains particularly poor due to their low permeability across the blood-brain barrier and limited intratumoral penetration. Focused ultrasound, when combined with circulating microbubbles (MB-FUS) provides a physical method to transiently modulate the brain tumor microenvironment (TME) and improve nanoparticle delivery. Here, we have examined the delivery of siRNA targeting the Smoothened (SMO) pathway, packaged in 50 nm cationic lipid-polymer hybrid nanoparticles (cLPH:siRNA-SMO), combined with MB-FUS in murine SmoA2 sonic hedgehog (SHH) medulloblastoma. At 30 hours after treatment, we observed the depletion of the SMO protein target, responsible for driving SHH medulloblastoma formation and growth, in mice that had received treatment with MB-FUS and cLPH:siRNA-SMO, but not with cLPH:siRNA-SMO alone. We also confirmed that SMO protein depletion was spatially achieved in the tumor regions with detected cLPH:siRNA-SMO using FISH assay, and that there was 15 fold induction of tumor cell apoptosis compared to tumors in mice that had received cLPH:siRNA-SMO alone. The limited induction of apoptosis was observed with either cLPH:siRNA (non-targeting) or MB-FUS and cLPH:siRNA (non-targeting), suggest that the observed apoptosis induction in the SmoA2 model was the direct result of SMO depletion rather than nonspecific effects of MB-FUS or cLPH:siRNA. Our findings provide a paradigm shift in drug delivery in brain tumors, where physical methods and nanotechnology are tuned together to develop rational strategies for the effective delivery of nucleic acids in brain tumors. Oxford University Press 2021-06-01 /pmc/articles/PMC8168192/ http://dx.doi.org/10.1093/neuonc/noab090.211 Text en © The Author(s) 2021. Published by Oxford University Press on behalf of the Society for Neuro-Oncology. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com. https://creativecommons.org/licenses/by-nc/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/4.0/ (https://creativecommons.org/licenses/by-nc/4.0/) ), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Translational/Early Phase Clinical Trials
Guo, Yutong
Lee, Hohyun
Fang, Zhou
Velalopoulou, Anastasia
Kim, Jinhwan
Thomas, Midhun Ben
Liu, Jingbo
Abramowitz, Ryan G
Kim, YongTae
Coskun, Ahmet F
Krummel, Daniel Pomeranz
Sengupta, Soma
MacDonald, Tobey J
Arvanitis, Costas
EPCT-25. SMO PROTEIN DEPLETION IN SHH MEDULLOBLASTOMAS USING MICROBUBBLE-ENHANCED ULTRASOUND AND SIRNA LOADED CATIONIC NANOPARTICLES
title EPCT-25. SMO PROTEIN DEPLETION IN SHH MEDULLOBLASTOMAS USING MICROBUBBLE-ENHANCED ULTRASOUND AND SIRNA LOADED CATIONIC NANOPARTICLES
title_full EPCT-25. SMO PROTEIN DEPLETION IN SHH MEDULLOBLASTOMAS USING MICROBUBBLE-ENHANCED ULTRASOUND AND SIRNA LOADED CATIONIC NANOPARTICLES
title_fullStr EPCT-25. SMO PROTEIN DEPLETION IN SHH MEDULLOBLASTOMAS USING MICROBUBBLE-ENHANCED ULTRASOUND AND SIRNA LOADED CATIONIC NANOPARTICLES
title_full_unstemmed EPCT-25. SMO PROTEIN DEPLETION IN SHH MEDULLOBLASTOMAS USING MICROBUBBLE-ENHANCED ULTRASOUND AND SIRNA LOADED CATIONIC NANOPARTICLES
title_short EPCT-25. SMO PROTEIN DEPLETION IN SHH MEDULLOBLASTOMAS USING MICROBUBBLE-ENHANCED ULTRASOUND AND SIRNA LOADED CATIONIC NANOPARTICLES
title_sort epct-25. smo protein depletion in shh medulloblastomas using microbubble-enhanced ultrasound and sirna loaded cationic nanoparticles
topic Translational/Early Phase Clinical Trials
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8168192/
http://dx.doi.org/10.1093/neuonc/noab090.211
work_keys_str_mv AT guoyutong epct25smoproteindepletioninshhmedulloblastomasusingmicrobubbleenhancedultrasoundandsirnaloadedcationicnanoparticles
AT leehohyun epct25smoproteindepletioninshhmedulloblastomasusingmicrobubbleenhancedultrasoundandsirnaloadedcationicnanoparticles
AT fangzhou epct25smoproteindepletioninshhmedulloblastomasusingmicrobubbleenhancedultrasoundandsirnaloadedcationicnanoparticles
AT velalopoulouanastasia epct25smoproteindepletioninshhmedulloblastomasusingmicrobubbleenhancedultrasoundandsirnaloadedcationicnanoparticles
AT kimjinhwan epct25smoproteindepletioninshhmedulloblastomasusingmicrobubbleenhancedultrasoundandsirnaloadedcationicnanoparticles
AT thomasmidhunben epct25smoproteindepletioninshhmedulloblastomasusingmicrobubbleenhancedultrasoundandsirnaloadedcationicnanoparticles
AT liujingbo epct25smoproteindepletioninshhmedulloblastomasusingmicrobubbleenhancedultrasoundandsirnaloadedcationicnanoparticles
AT abramowitzryang epct25smoproteindepletioninshhmedulloblastomasusingmicrobubbleenhancedultrasoundandsirnaloadedcationicnanoparticles
AT kimyongtae epct25smoproteindepletioninshhmedulloblastomasusingmicrobubbleenhancedultrasoundandsirnaloadedcationicnanoparticles
AT coskunahmetf epct25smoproteindepletioninshhmedulloblastomasusingmicrobubbleenhancedultrasoundandsirnaloadedcationicnanoparticles
AT krummeldanielpomeranz epct25smoproteindepletioninshhmedulloblastomasusingmicrobubbleenhancedultrasoundandsirnaloadedcationicnanoparticles
AT senguptasoma epct25smoproteindepletioninshhmedulloblastomasusingmicrobubbleenhancedultrasoundandsirnaloadedcationicnanoparticles
AT macdonaldtobeyj epct25smoproteindepletioninshhmedulloblastomasusingmicrobubbleenhancedultrasoundandsirnaloadedcationicnanoparticles
AT arvanitiscostas epct25smoproteindepletioninshhmedulloblastomasusingmicrobubbleenhancedultrasoundandsirnaloadedcationicnanoparticles

Ejemplares similares