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Analysis of structural effects of sickle cell disease on brain vasculature of mice using three-dimensional quantitative phase imaging

SIGNIFICANCE: Although the molecular origins of sickle cell disease (SCD) have been extensively studied, the effects of SCD on the vasculature—which can influence blood clotting mechanisms, pain crises, and strokes—are not well understood. Improving this understanding can yield insight into the mech...

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Autores principales: Filan, Caroline, Song, Hannah, Platt, Manu O., Robles, Francisco E.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Society of Photo-Optical Instrumentation Engineers 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10491933/
https://www.ncbi.nlm.nih.gov/pubmed/37692563
http://dx.doi.org/10.1117/1.JBO.28.9.096501
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author Filan, Caroline
Song, Hannah
Platt, Manu O.
Robles, Francisco E.
author_facet Filan, Caroline
Song, Hannah
Platt, Manu O.
Robles, Francisco E.
author_sort Filan, Caroline
collection PubMed
description SIGNIFICANCE: Although the molecular origins of sickle cell disease (SCD) have been extensively studied, the effects of SCD on the vasculature—which can influence blood clotting mechanisms, pain crises, and strokes—are not well understood. Improving this understanding can yield insight into the mechanisms and wide-ranging effects of this devastating disease. AIM: We aim to demonstrate the ability of a label-free 3D quantitative phase imaging technology, called quantitative oblique back-illumination microscopy (qOBM), to provide insight into the effects of SCD on brain vasculature. APPROACH: Using qOBM, we quantitatively analyze the vasculature of freshly excised, but otherwise unaltered, whole mouse brains. We use Townes sickle transgenic mice, which closely recapitulate the pathophysiology of human SCD, and sickle cell trait mice as controls. Two developmental time points are studied: 6-week-old mice and 20-week-old mice. Quantitative structural and biophysical parameters of the vessels (including the refractive index (RI), which is linearly proportional to dry mass) are extracted from the high-resolution images and analyzed. RESULTS: qOBM reveals structural differences in the brain blood vessel thickness (thinner for SCD in particular brain regions) and the RI of the vessel wall (higher and containing a larger variation throughout the brain for SCD). These changes were only significant in 20-week-old mice. Further, vessel breakages are observed in SCD mice at both time points. The vessel wall RI distribution near these breaks, up to [Formula: see text] away from the breaking point, shows an erratic behavior characterized by wide RI variations. Vessel diameter, tortuosity, texture within the vessel, and structural fractal patterns are found to not be statistically different. As with vessel breaks, we also observe blood vessel blockages only in mice brains with SCD. CONCLUSIONS: qOBM provides insight into the biophysical and structural composition of brain blood vessels in mice with SCD. Data suggest that the RI may be an indirect indicator of vessel rigidity, vessel strength, and/or tensions, which change with SCD. Future ex vivo and in vivo studies with qOBM could improve our understanding of SCD.
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spelling pubmed-104919332023-09-10 Analysis of structural effects of sickle cell disease on brain vasculature of mice using three-dimensional quantitative phase imaging Filan, Caroline Song, Hannah Platt, Manu O. Robles, Francisco E. J Biomed Opt Microscopy SIGNIFICANCE: Although the molecular origins of sickle cell disease (SCD) have been extensively studied, the effects of SCD on the vasculature—which can influence blood clotting mechanisms, pain crises, and strokes—are not well understood. Improving this understanding can yield insight into the mechanisms and wide-ranging effects of this devastating disease. AIM: We aim to demonstrate the ability of a label-free 3D quantitative phase imaging technology, called quantitative oblique back-illumination microscopy (qOBM), to provide insight into the effects of SCD on brain vasculature. APPROACH: Using qOBM, we quantitatively analyze the vasculature of freshly excised, but otherwise unaltered, whole mouse brains. We use Townes sickle transgenic mice, which closely recapitulate the pathophysiology of human SCD, and sickle cell trait mice as controls. Two developmental time points are studied: 6-week-old mice and 20-week-old mice. Quantitative structural and biophysical parameters of the vessels (including the refractive index (RI), which is linearly proportional to dry mass) are extracted from the high-resolution images and analyzed. RESULTS: qOBM reveals structural differences in the brain blood vessel thickness (thinner for SCD in particular brain regions) and the RI of the vessel wall (higher and containing a larger variation throughout the brain for SCD). These changes were only significant in 20-week-old mice. Further, vessel breakages are observed in SCD mice at both time points. The vessel wall RI distribution near these breaks, up to [Formula: see text] away from the breaking point, shows an erratic behavior characterized by wide RI variations. Vessel diameter, tortuosity, texture within the vessel, and structural fractal patterns are found to not be statistically different. As with vessel breaks, we also observe blood vessel blockages only in mice brains with SCD. CONCLUSIONS: qOBM provides insight into the biophysical and structural composition of brain blood vessels in mice with SCD. Data suggest that the RI may be an indirect indicator of vessel rigidity, vessel strength, and/or tensions, which change with SCD. Future ex vivo and in vivo studies with qOBM could improve our understanding of SCD. Society of Photo-Optical Instrumentation Engineers 2023-09-09 2023-09 /pmc/articles/PMC10491933/ /pubmed/37692563 http://dx.doi.org/10.1117/1.JBO.28.9.096501 Text en © 2023 The Authors https://creativecommons.org/licenses/by/4.0/Published by SPIE under a Creative Commons Attribution 4.0 International License. Distribution or reproduction of this work in whole or in part requires full attribution of the original publication, including its DOI.
spellingShingle Microscopy
Filan, Caroline
Song, Hannah
Platt, Manu O.
Robles, Francisco E.
Analysis of structural effects of sickle cell disease on brain vasculature of mice using three-dimensional quantitative phase imaging
title Analysis of structural effects of sickle cell disease on brain vasculature of mice using three-dimensional quantitative phase imaging
title_full Analysis of structural effects of sickle cell disease on brain vasculature of mice using three-dimensional quantitative phase imaging
title_fullStr Analysis of structural effects of sickle cell disease on brain vasculature of mice using three-dimensional quantitative phase imaging
title_full_unstemmed Analysis of structural effects of sickle cell disease on brain vasculature of mice using three-dimensional quantitative phase imaging
title_short Analysis of structural effects of sickle cell disease on brain vasculature of mice using three-dimensional quantitative phase imaging
title_sort analysis of structural effects of sickle cell disease on brain vasculature of mice using three-dimensional quantitative phase imaging
topic Microscopy
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10491933/
https://www.ncbi.nlm.nih.gov/pubmed/37692563
http://dx.doi.org/10.1117/1.JBO.28.9.096501
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