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Comprehensive Small Animal Imaging Strategies on a Clinical 3 T Dedicated Head MR-Scanner; Adapted Methods and Sequence Protocols in CNS Pathologies

BACKGROUND: Small animal models of human diseases are an indispensable aspect of pre-clinical research. Being dynamic, most pathologies demand extensive longitudinal monitoring to understand disease mechanisms, drug efficacy and side effects. These considerations often demand the concomitant develop...

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Autores principales: Pillai, Deepu R., Heidemann, Robin M., Kumar, Praveen, Shanbhag, Nagesh, Lanz, Titus, Dittmar, Michael S., Sandner, Beatrice, Beier, Christoph P., Weidner, Norbert, Greenlee, Mark W., Schuierer, Gerhard, Bogdahn, Ulrich, Schlachetzki, Felix
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3034718/
https://www.ncbi.nlm.nih.gov/pubmed/21326876
http://dx.doi.org/10.1371/journal.pone.0016091
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author Pillai, Deepu R.
Heidemann, Robin M.
Kumar, Praveen
Shanbhag, Nagesh
Lanz, Titus
Dittmar, Michael S.
Sandner, Beatrice
Beier, Christoph P.
Weidner, Norbert
Greenlee, Mark W.
Schuierer, Gerhard
Bogdahn, Ulrich
Schlachetzki, Felix
author_facet Pillai, Deepu R.
Heidemann, Robin M.
Kumar, Praveen
Shanbhag, Nagesh
Lanz, Titus
Dittmar, Michael S.
Sandner, Beatrice
Beier, Christoph P.
Weidner, Norbert
Greenlee, Mark W.
Schuierer, Gerhard
Bogdahn, Ulrich
Schlachetzki, Felix
author_sort Pillai, Deepu R.
collection PubMed
description BACKGROUND: Small animal models of human diseases are an indispensable aspect of pre-clinical research. Being dynamic, most pathologies demand extensive longitudinal monitoring to understand disease mechanisms, drug efficacy and side effects. These considerations often demand the concomitant development of monitoring systems with sufficient temporal and spatial resolution. METHODOLOGY AND RESULTS: This study attempts to configure and optimize a clinical 3 Tesla magnetic resonance scanner to facilitate imaging of small animal central nervous system pathologies. The hardware of the scanner was complemented by a custom-built, 4-channel phased array coil system. Extensive modification of standard sequence protocols was carried out based on tissue relaxometric calculations. Proton density differences between the gray and white matter of the rodent spinal cord along with transverse relaxation due to magnetic susceptibility differences at the cortex and striatum of both rats and mice demonstrated statistically significant differences. The employed parallel imaging reconstruction algorithms had distinct properties dependent on the sequence type and in the presence of the contrast agent. The attempt to morphologically phenotype a normal healthy rat brain in multiple planes delineated a number of anatomical regions, and all the clinically relevant sequels following acute cerebral ischemia could be adequately characterized. Changes in blood-brain-barrier permeability following ischemia-reperfusion were also apparent at a later time. Typical characteristics of intra-cerebral haemorrhage at acute and chronic stages were also visualized up to one month. Two models of rodent spinal cord injury were adequately characterized and closely mimicked the results of histological studies. In the employed rodent animal handling system a mouse model of glioblastoma was also studied with unequivocal results. CONCLUSIONS: The implemented customizations including extensive sequence protocol modifications resulted in images of high diagnostic quality. These results prove that lack of dedicated animal scanners shouldn't discourage conventional small animal imaging studies.
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spelling pubmed-30347182011-02-15 Comprehensive Small Animal Imaging Strategies on a Clinical 3 T Dedicated Head MR-Scanner; Adapted Methods and Sequence Protocols in CNS Pathologies Pillai, Deepu R. Heidemann, Robin M. Kumar, Praveen Shanbhag, Nagesh Lanz, Titus Dittmar, Michael S. Sandner, Beatrice Beier, Christoph P. Weidner, Norbert Greenlee, Mark W. Schuierer, Gerhard Bogdahn, Ulrich Schlachetzki, Felix PLoS One Research Article BACKGROUND: Small animal models of human diseases are an indispensable aspect of pre-clinical research. Being dynamic, most pathologies demand extensive longitudinal monitoring to understand disease mechanisms, drug efficacy and side effects. These considerations often demand the concomitant development of monitoring systems with sufficient temporal and spatial resolution. METHODOLOGY AND RESULTS: This study attempts to configure and optimize a clinical 3 Tesla magnetic resonance scanner to facilitate imaging of small animal central nervous system pathologies. The hardware of the scanner was complemented by a custom-built, 4-channel phased array coil system. Extensive modification of standard sequence protocols was carried out based on tissue relaxometric calculations. Proton density differences between the gray and white matter of the rodent spinal cord along with transverse relaxation due to magnetic susceptibility differences at the cortex and striatum of both rats and mice demonstrated statistically significant differences. The employed parallel imaging reconstruction algorithms had distinct properties dependent on the sequence type and in the presence of the contrast agent. The attempt to morphologically phenotype a normal healthy rat brain in multiple planes delineated a number of anatomical regions, and all the clinically relevant sequels following acute cerebral ischemia could be adequately characterized. Changes in blood-brain-barrier permeability following ischemia-reperfusion were also apparent at a later time. Typical characteristics of intra-cerebral haemorrhage at acute and chronic stages were also visualized up to one month. Two models of rodent spinal cord injury were adequately characterized and closely mimicked the results of histological studies. In the employed rodent animal handling system a mouse model of glioblastoma was also studied with unequivocal results. CONCLUSIONS: The implemented customizations including extensive sequence protocol modifications resulted in images of high diagnostic quality. These results prove that lack of dedicated animal scanners shouldn't discourage conventional small animal imaging studies. Public Library of Science 2011-02-07 /pmc/articles/PMC3034718/ /pubmed/21326876 http://dx.doi.org/10.1371/journal.pone.0016091 Text en Pillai et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Pillai, Deepu R.
Heidemann, Robin M.
Kumar, Praveen
Shanbhag, Nagesh
Lanz, Titus
Dittmar, Michael S.
Sandner, Beatrice
Beier, Christoph P.
Weidner, Norbert
Greenlee, Mark W.
Schuierer, Gerhard
Bogdahn, Ulrich
Schlachetzki, Felix
Comprehensive Small Animal Imaging Strategies on a Clinical 3 T Dedicated Head MR-Scanner; Adapted Methods and Sequence Protocols in CNS Pathologies
title Comprehensive Small Animal Imaging Strategies on a Clinical 3 T Dedicated Head MR-Scanner; Adapted Methods and Sequence Protocols in CNS Pathologies
title_full Comprehensive Small Animal Imaging Strategies on a Clinical 3 T Dedicated Head MR-Scanner; Adapted Methods and Sequence Protocols in CNS Pathologies
title_fullStr Comprehensive Small Animal Imaging Strategies on a Clinical 3 T Dedicated Head MR-Scanner; Adapted Methods and Sequence Protocols in CNS Pathologies
title_full_unstemmed Comprehensive Small Animal Imaging Strategies on a Clinical 3 T Dedicated Head MR-Scanner; Adapted Methods and Sequence Protocols in CNS Pathologies
title_short Comprehensive Small Animal Imaging Strategies on a Clinical 3 T Dedicated Head MR-Scanner; Adapted Methods and Sequence Protocols in CNS Pathologies
title_sort comprehensive small animal imaging strategies on a clinical 3 t dedicated head mr-scanner; adapted methods and sequence protocols in cns pathologies
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3034718/
https://www.ncbi.nlm.nih.gov/pubmed/21326876
http://dx.doi.org/10.1371/journal.pone.0016091
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