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Selective brain entry of lipid nanoparticles in haemorrhagic stroke is linked to biphasic blood-brain barrier disruption

Haemorrhagic stroke represents a significant public health burden, yet our knowledge and ability to treat this type of stroke are lacking. Previously we showed that we can target ischaemic-stroke lesions by selective translocation of lipid nanoparticles through the site of blood-brain barrier (BBB)...

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Autores principales: Al-Ahmady, Zahraa S., Dickie, Ben R., Aldred, Isabelle, Jasim, Dhifaf A., Barrington, Jack, Haley, Michael, Lemarchand, Eloise, Coutts, Graham, Kaur, Satinderdeep, Bates, Jessica, Curran, Sarah, Goddard, Ruth, Walker, Megan, Parry-jones, Adrian, Kostarelos, Kostas, Allan, Stuart M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9254235/
https://www.ncbi.nlm.nih.gov/pubmed/35832077
http://dx.doi.org/10.7150/thno.72167
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author Al-Ahmady, Zahraa S.
Dickie, Ben R.
Aldred, Isabelle
Jasim, Dhifaf A.
Barrington, Jack
Haley, Michael
Lemarchand, Eloise
Coutts, Graham
Kaur, Satinderdeep
Bates, Jessica
Curran, Sarah
Goddard, Ruth
Walker, Megan
Parry-jones, Adrian
Kostarelos, Kostas
Allan, Stuart M.
author_facet Al-Ahmady, Zahraa S.
Dickie, Ben R.
Aldred, Isabelle
Jasim, Dhifaf A.
Barrington, Jack
Haley, Michael
Lemarchand, Eloise
Coutts, Graham
Kaur, Satinderdeep
Bates, Jessica
Curran, Sarah
Goddard, Ruth
Walker, Megan
Parry-jones, Adrian
Kostarelos, Kostas
Allan, Stuart M.
author_sort Al-Ahmady, Zahraa S.
collection PubMed
description Haemorrhagic stroke represents a significant public health burden, yet our knowledge and ability to treat this type of stroke are lacking. Previously we showed that we can target ischaemic-stroke lesions by selective translocation of lipid nanoparticles through the site of blood-brain barrier (BBB) disruption. The data we presented in this study provide compelling evidence that haemorrhagic stroke in mice induces BBB injury that mimics key features of the human pathology and, more importantly, provides a gate for entry of lipid nanoparticles-based therapeutics selectively to the bleeding site. Methods: Haemorrhagic stroke was induced in mice by intra-striatal collagenase injection. lipid nanoparticles were injected intravenously at 3 h, 24 h & 48 h post-haemorrhagic stroke and accumulation in the brain studied using in-vivo optical imaging and histology. BBB integrity, brain water content and iron accumulation were characterised using dynamic contrast-enhanced MRI, quantitative T(1) mapping, and gradient echo MRI. Results: Using in-vivo SPECT/CT imaging and optical imaging revealed biphasic lipid nanoparticles entry into the bleeding site, with an early phase of increased uptake at 3-24 h post-haemorrhagic stroke, followed by a second phase at 48-72 h. Lipid nanoparticles entry into the brain post-haemorrhage showed an identical entry pattern to the trans-BBB leakage rate (K(trans) [min(-1)]) of Gd-DOTA, a biomarker for BBB disruption, measured using dynamic contrast-enhanced MRI. Discussion: Our findings suggest that selective accumulation of liposomes into the lesion site is linked to a biphasic pattern of BBB hyper-permeability. This approach provides a unique opportunity to selectively and efficiently deliver therapeutic molecules across the BBB, an approach that has not been utilised for haemorrhagic stroke therapy and is not achievable using free small drug molecules.
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spelling pubmed-92542352022-07-12 Selective brain entry of lipid nanoparticles in haemorrhagic stroke is linked to biphasic blood-brain barrier disruption Al-Ahmady, Zahraa S. Dickie, Ben R. Aldred, Isabelle Jasim, Dhifaf A. Barrington, Jack Haley, Michael Lemarchand, Eloise Coutts, Graham Kaur, Satinderdeep Bates, Jessica Curran, Sarah Goddard, Ruth Walker, Megan Parry-jones, Adrian Kostarelos, Kostas Allan, Stuart M. Theranostics Research Paper Haemorrhagic stroke represents a significant public health burden, yet our knowledge and ability to treat this type of stroke are lacking. Previously we showed that we can target ischaemic-stroke lesions by selective translocation of lipid nanoparticles through the site of blood-brain barrier (BBB) disruption. The data we presented in this study provide compelling evidence that haemorrhagic stroke in mice induces BBB injury that mimics key features of the human pathology and, more importantly, provides a gate for entry of lipid nanoparticles-based therapeutics selectively to the bleeding site. Methods: Haemorrhagic stroke was induced in mice by intra-striatal collagenase injection. lipid nanoparticles were injected intravenously at 3 h, 24 h & 48 h post-haemorrhagic stroke and accumulation in the brain studied using in-vivo optical imaging and histology. BBB integrity, brain water content and iron accumulation were characterised using dynamic contrast-enhanced MRI, quantitative T(1) mapping, and gradient echo MRI. Results: Using in-vivo SPECT/CT imaging and optical imaging revealed biphasic lipid nanoparticles entry into the bleeding site, with an early phase of increased uptake at 3-24 h post-haemorrhagic stroke, followed by a second phase at 48-72 h. Lipid nanoparticles entry into the brain post-haemorrhage showed an identical entry pattern to the trans-BBB leakage rate (K(trans) [min(-1)]) of Gd-DOTA, a biomarker for BBB disruption, measured using dynamic contrast-enhanced MRI. Discussion: Our findings suggest that selective accumulation of liposomes into the lesion site is linked to a biphasic pattern of BBB hyper-permeability. This approach provides a unique opportunity to selectively and efficiently deliver therapeutic molecules across the BBB, an approach that has not been utilised for haemorrhagic stroke therapy and is not achievable using free small drug molecules. Ivyspring International Publisher 2022-05-26 /pmc/articles/PMC9254235/ /pubmed/35832077 http://dx.doi.org/10.7150/thno.72167 Text en © The author(s) https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Al-Ahmady, Zahraa S.
Dickie, Ben R.
Aldred, Isabelle
Jasim, Dhifaf A.
Barrington, Jack
Haley, Michael
Lemarchand, Eloise
Coutts, Graham
Kaur, Satinderdeep
Bates, Jessica
Curran, Sarah
Goddard, Ruth
Walker, Megan
Parry-jones, Adrian
Kostarelos, Kostas
Allan, Stuart M.
Selective brain entry of lipid nanoparticles in haemorrhagic stroke is linked to biphasic blood-brain barrier disruption
title Selective brain entry of lipid nanoparticles in haemorrhagic stroke is linked to biphasic blood-brain barrier disruption
title_full Selective brain entry of lipid nanoparticles in haemorrhagic stroke is linked to biphasic blood-brain barrier disruption
title_fullStr Selective brain entry of lipid nanoparticles in haemorrhagic stroke is linked to biphasic blood-brain barrier disruption
title_full_unstemmed Selective brain entry of lipid nanoparticles in haemorrhagic stroke is linked to biphasic blood-brain barrier disruption
title_short Selective brain entry of lipid nanoparticles in haemorrhagic stroke is linked to biphasic blood-brain barrier disruption
title_sort selective brain entry of lipid nanoparticles in haemorrhagic stroke is linked to biphasic blood-brain barrier disruption
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9254235/
https://www.ncbi.nlm.nih.gov/pubmed/35832077
http://dx.doi.org/10.7150/thno.72167
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