Validating layer-specific VASO across species

Laurentius Renzo Huber; Benedikt A. Poser; Amanda L. Kaas; Elizabeth J Fear; Sebastian Dresbach; Jason Berwick; Rainer Goebel; Robert Turner; Aneurin J Kennerley

doi:10.1016/j.neuroimage.2021.118195

Validating layer-specific VASO across species

Laurentius Renzo Huber^*, Benedikt A. Poser, Amanda L. Kaas, Elizabeth J Fear, Sebastian Dresbach, Jason Berwick, Rainer Goebel, Robert Turner, Aneurin J Kennerley^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Cerebral blood volume (CBV) has been shown to be a robust and important physiological parameter for quantitative interpretation of functional (f)MRI, capable of delivering highly localized mapping of neural activity. Indeed, with recent advances in ultra-high-field (≥7T) MRI hardware and associated sequence libraries, it has become possible to capture non-invasive CBV weighted fMRI signals across cortical layers. One of the most widely used approaches to achieve this (in humans) is through vascular-space-occupancy (VASO) fMRI. Unfortunately, the exact contrast mechanisms of layer-dependent VASO fMRI have not been validated for human fMRI and thus interpretation of such data is confounded. Here we validate the signal source of layer-dependent SS-SI VASO fMRI using multi-modal imaging in a rat model in response to neuronal activation (somatosensory cortex) and respiratory challenge (hypercapnia). In particular VASO derived CBV measures are directly compared to concurrent measures of total haemoglobin changes from high resolution intrinsic optical imaging spectroscopy (OIS). Quantified cortical layer profiling is demonstrated to be in agreement between VASO and contrast enhanced fMRI (using monocrystalline iron oxide nanoparticles, MION). Responses show high spatial localisation to layers of cortical processing independent of confounding large draining veins which can hamper BOLD fMRI studies, (depending on slice positioning). Thus, a cross species comparison is enabled using VASO as a common measure. We find increased VASO based CBV reactivity (3.1 ± 1.2 fold increase) in humans compared to rats. Together, our findings confirm that the VASO contrast is indeed a reliable estimate of layer-specific CBV changes. This validation study increases the neuronal interpretability of human layer-dependent VASO fMRI as an appropriate method in neuroscience application studies, in which the presence of large draining intracortical and pial veins limits neuroscientific inference with BOLD fMRI.

Original language	English
Article number	118195
Number of pages	15
Journal	Neuroimage
Volume	237
Early online date	24 May 2021
DOIs	https://doi.org/10.1016/j.neuroimage.2021.118195
Publication status	Published - 15 Aug 2021

Keywords

BOLD POSTSTIMULUS UNDERSHOOT
CEREBRAL BLOOD-VOLUME
Cerebral blood volume
Concurrent imaging
Depth-dependent fMRI
Draining vein
HEMODYNAMIC-RESPONSE
HIGH-RESOLUTION FMRI
HUMAN BRAIN
Laminar
Layer
MION
NEGATIVE BOLD
NEURAL ACTIVITY
OPTICAL IMAGING SPECTROSCOPY
Optical imaging spectroscopy
Pre-clinical
SPIN-ECHO
Somatosensory stimulation
Sub-millimetre
WHISKER STIMULATION
fMRI

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Cite this

@article{7db1feaa7bab4d7488c944a25213f9cc,

title = "Validating layer-specific VASO across species",

abstract = "Cerebral blood volume (CBV) has been shown to be a robust and important physiological parameter for quantitative interpretation of functional (f)MRI, capable of delivering highly localized mapping of neural activity. Indeed, with recent advances in ultra-high-field (≥7T) MRI hardware and associated sequence libraries, it has become possible to capture non-invasive CBV weighted fMRI signals across cortical layers. One of the most widely used approaches to achieve this (in humans) is through vascular-space-occupancy (VASO) fMRI. Unfortunately, the exact contrast mechanisms of layer-dependent VASO fMRI have not been validated for human fMRI and thus interpretation of such data is confounded. Here we validate the signal source of layer-dependent SS-SI VASO fMRI using multi-modal imaging in a rat model in response to neuronal activation (somatosensory cortex) and respiratory challenge (hypercapnia). In particular VASO derived CBV measures are directly compared to concurrent measures of total haemoglobin changes from high resolution intrinsic optical imaging spectroscopy (OIS). Quantified cortical layer profiling is demonstrated to be in agreement between VASO and contrast enhanced fMRI (using monocrystalline iron oxide nanoparticles, MION). Responses show high spatial localisation to layers of cortical processing independent of confounding large draining veins which can hamper BOLD fMRI studies, (depending on slice positioning). Thus, a cross species comparison is enabled using VASO as a common measure. We find increased VASO based CBV reactivity (3.1 ± 1.2 fold increase) in humans compared to rats. Together, our findings confirm that the VASO contrast is indeed a reliable estimate of layer-specific CBV changes. This validation study increases the neuronal interpretability of human layer-dependent VASO fMRI as an appropriate method in neuroscience application studies, in which the presence of large draining intracortical and pial veins limits neuroscientific inference with BOLD fMRI.",

keywords = "BOLD POSTSTIMULUS UNDERSHOOT, CEREBRAL BLOOD-VOLUME, Cerebral blood volume, Concurrent imaging, Depth-dependent fMRI, Draining vein, HEMODYNAMIC-RESPONSE, HIGH-RESOLUTION FMRI, HUMAN BRAIN, Laminar, Layer, MION, NEGATIVE BOLD, NEURAL ACTIVITY, OPTICAL IMAGING SPECTROSCOPY, Optical imaging spectroscopy, Pre-clinical, SPIN-ECHO, Somatosensory stimulation, Sub-millimetre, WHISKER STIMULATION, fMRI",

author = "Huber, {Laurentius Renzo} and Poser, {Benedikt A.} and Kaas, {Amanda L.} and Fear, {Elizabeth J} and Sebastian Dresbach and Jason Berwick and Rainer Goebel and Robert Turner and Kennerley, {Aneurin J}",

note = "Copyright {\textcopyright} 2021. Published by Elsevier Inc.",

year = "2021",

month = aug,

day = "15",

doi = "10.1016/j.neuroimage.2021.118195",

language = "English",

volume = "237",

journal = "Neuroimage",

issn = "1053-8119",

publisher = "Elsevier Science",

}

TY - JOUR

T1 - Validating layer-specific VASO across species

AU - Huber, Laurentius Renzo

AU - Poser, Benedikt A.

AU - Kaas, Amanda L.

AU - Fear, Elizabeth J

AU - Dresbach, Sebastian

AU - Berwick, Jason

AU - Goebel, Rainer

AU - Turner, Robert

AU - Kennerley, Aneurin J

PY - 2021/8/15

Y1 - 2021/8/15

N2 - Cerebral blood volume (CBV) has been shown to be a robust and important physiological parameter for quantitative interpretation of functional (f)MRI, capable of delivering highly localized mapping of neural activity. Indeed, with recent advances in ultra-high-field (≥7T) MRI hardware and associated sequence libraries, it has become possible to capture non-invasive CBV weighted fMRI signals across cortical layers. One of the most widely used approaches to achieve this (in humans) is through vascular-space-occupancy (VASO) fMRI. Unfortunately, the exact contrast mechanisms of layer-dependent VASO fMRI have not been validated for human fMRI and thus interpretation of such data is confounded. Here we validate the signal source of layer-dependent SS-SI VASO fMRI using multi-modal imaging in a rat model in response to neuronal activation (somatosensory cortex) and respiratory challenge (hypercapnia). In particular VASO derived CBV measures are directly compared to concurrent measures of total haemoglobin changes from high resolution intrinsic optical imaging spectroscopy (OIS). Quantified cortical layer profiling is demonstrated to be in agreement between VASO and contrast enhanced fMRI (using monocrystalline iron oxide nanoparticles, MION). Responses show high spatial localisation to layers of cortical processing independent of confounding large draining veins which can hamper BOLD fMRI studies, (depending on slice positioning). Thus, a cross species comparison is enabled using VASO as a common measure. We find increased VASO based CBV reactivity (3.1 ± 1.2 fold increase) in humans compared to rats. Together, our findings confirm that the VASO contrast is indeed a reliable estimate of layer-specific CBV changes. This validation study increases the neuronal interpretability of human layer-dependent VASO fMRI as an appropriate method in neuroscience application studies, in which the presence of large draining intracortical and pial veins limits neuroscientific inference with BOLD fMRI.

AB - Cerebral blood volume (CBV) has been shown to be a robust and important physiological parameter for quantitative interpretation of functional (f)MRI, capable of delivering highly localized mapping of neural activity. Indeed, with recent advances in ultra-high-field (≥7T) MRI hardware and associated sequence libraries, it has become possible to capture non-invasive CBV weighted fMRI signals across cortical layers. One of the most widely used approaches to achieve this (in humans) is through vascular-space-occupancy (VASO) fMRI. Unfortunately, the exact contrast mechanisms of layer-dependent VASO fMRI have not been validated for human fMRI and thus interpretation of such data is confounded. Here we validate the signal source of layer-dependent SS-SI VASO fMRI using multi-modal imaging in a rat model in response to neuronal activation (somatosensory cortex) and respiratory challenge (hypercapnia). In particular VASO derived CBV measures are directly compared to concurrent measures of total haemoglobin changes from high resolution intrinsic optical imaging spectroscopy (OIS). Quantified cortical layer profiling is demonstrated to be in agreement between VASO and contrast enhanced fMRI (using monocrystalline iron oxide nanoparticles, MION). Responses show high spatial localisation to layers of cortical processing independent of confounding large draining veins which can hamper BOLD fMRI studies, (depending on slice positioning). Thus, a cross species comparison is enabled using VASO as a common measure. We find increased VASO based CBV reactivity (3.1 ± 1.2 fold increase) in humans compared to rats. Together, our findings confirm that the VASO contrast is indeed a reliable estimate of layer-specific CBV changes. This validation study increases the neuronal interpretability of human layer-dependent VASO fMRI as an appropriate method in neuroscience application studies, in which the presence of large draining intracortical and pial veins limits neuroscientific inference with BOLD fMRI.

KW - BOLD POSTSTIMULUS UNDERSHOOT

KW - CEREBRAL BLOOD-VOLUME

KW - Cerebral blood volume

KW - Concurrent imaging

KW - Depth-dependent fMRI

KW - Draining vein

KW - HEMODYNAMIC-RESPONSE

KW - HIGH-RESOLUTION FMRI

KW - HUMAN BRAIN

KW - Laminar

KW - Layer

KW - MION

KW - NEGATIVE BOLD

KW - NEURAL ACTIVITY

KW - OPTICAL IMAGING SPECTROSCOPY

KW - Optical imaging spectroscopy

KW - Pre-clinical

KW - SPIN-ECHO

KW - Somatosensory stimulation

KW - Sub-millimetre

KW - WHISKER STIMULATION

KW - fMRI

U2 - 10.1016/j.neuroimage.2021.118195

DO - 10.1016/j.neuroimage.2021.118195

M3 - Article

C2 - 34038769

SN - 1053-8119

VL - 237

JO - Neuroimage

JF - Neuroimage

M1 - 118195

ER -