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Research ArticleNeuroimaging Physics/Functional Neuroimaging/CT and MRI Technology

Whole-Brain Vascular Architecture Mapping Identifies Region-Specific Microvascular Profiles In Vivo

Anja Hohmann, Ke Zhang, Christoph M. Mooshage, Johann M.E. Jende, Lukas T. Rotkopf, Heinz-Peter Schlemmer, Martin Bendszus, Wolfgang Wick and Felix T. Kurz
American Journal of Neuroradiology September 2024, 45 (9) 1346-1354; DOI: https://doi.org/10.3174/ajnr.A8344
Anja Hohmann
aFrom the Department of Neurology (A.H., W.W.), Heidelberg University Hospital, Heidelberg, Germany
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Ke Zhang
bDepartment of Diagnostic and Interventional Radiology (K.Z.), Heidelberg University Hospital, Heidelberg, Germany
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Christoph M. Mooshage
cDepartment of Neuroradiology (C.M.M., J.M.E.J., M.B., F.T.K.), Heidelberg University Hospital, Heidelberg, Germany
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Johann M.E. Jende
cDepartment of Neuroradiology (C.M.M., J.M.E.J., M.B., F.T.K.), Heidelberg University Hospital, Heidelberg, Germany
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Lukas T. Rotkopf
dDivision of Radiology (L.T.R., H.-P.S., F.T.K.) German Cancer Research Center, Heidelberg, Germany
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Heinz-Peter Schlemmer
dDivision of Radiology (L.T.R., H.-P.S., F.T.K.) German Cancer Research Center, Heidelberg, Germany
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Martin Bendszus
cDepartment of Neuroradiology (C.M.M., J.M.E.J., M.B., F.T.K.), Heidelberg University Hospital, Heidelberg, Germany
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Wolfgang Wick
aFrom the Department of Neurology (A.H., W.W.), Heidelberg University Hospital, Heidelberg, Germany
eClinical Cooperation Unit Neurooncology (W.W.), German Cancer Research Center, Heidelberg, Germany
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Felix T. Kurz
cDepartment of Neuroradiology (C.M.M., J.M.E.J., M.B., F.T.K.), Heidelberg University Hospital, Heidelberg, Germany
dDivision of Radiology (L.T.R., H.-P.S., F.T.K.) German Cancer Research Center, Heidelberg, Germany
fDivision of Neuroradiology (F.T.K.), University Hospital Geneva, Geneva, Switzerland
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Abstract

BACKGROUND AND PURPOSE: The novel MR imaging technique of vascular architecture mapping allows in vivo characterization of local changes in cerebral microvasculature, but reference ranges for vascular architecture mapping parameters in healthy brain tissue are lacking, limiting its potential applicability as an MR imaging biomarker in clinical practice. We conducted whole-brain vascular architecture mapping in a large cohort to establish vascular architecture mapping parameter references ranges and identify region-specific cortical and subcortical microvascular profiles.

MATERIALS AND METHODS: This was a single-center examination of adult patients with unifocal, stable low-grade gliomas with multiband spin- and gradient-echo EPI sequence at 3T using parallel imaging. Voxelwise plotting of resulting values for gradient-echo (R2*) versus spin-echo (R2) relaxation rates during contrast agent bolus administration generates vessel vortex curves that allow the extraction of vascular architecture mapping parameters representative of, eg, vessel type, vessel radius, or CBV in the underlying voxel. Averaged whole-brain parametric maps were calculated for 9 parameters, and VOI analysis was conducted on the basis of a standardized brain atlas and individual cortical GM and WM segmentation.

RESULTS: Prevalence of vascular risk factors among subjects (n = 106; mean age, 39.2 [SD, 12.5] years; 56 women) was similar to those in the German population. Compared with WM, we found cortical GM to have larger mean vascular calibers (5.80 [SD, 0.59] versus 4.25 [SD, 0.62] P < .001), increased blood volume fraction (20.40 [SD, 4.49] s−1 versus 11.05 [SD, 2.44] s−1; P < .001), and a dominance of venous vessels. Distinct microvascular profiles emerged for cortical GM, where vascular architecture mapping vessel type indicator differed, eg, between the thalamus and cortical GM (mean, −2.47 [SD, 4.02] s−2 versus −5.41 [SD, 2.84] s−2; P < .001). Intraclass correlation coefficient values indicated overall high test-retest reliability for vascular architecture mapping parameter mean values when comparing multiple scans per subject.

CONCLUSIONS: Whole-brain vascular architecture mapping in the adult brain reveals region-specific microvascular profiles. The obtained parameter reference ranges for distinct anatomic and functional brain areas may be used for future vascular architecture mapping studies on cerebrovascular pathologies and might facilitate early discovery of microvascular changes, in, eg, neurodegeneration and neuro-oncology.

ABBREVIATIONS:

BMI
body mass index
BVF
blood volume fraction
CA
contrast agent
CBI
capillary bed identifier
CGI
caliber gradient indicator
cGM
cortical gray matter
CN
caudate nucleus
GE
gradient-echo
GP
globus pallidus
I
maximum distance between the ascending and descending branches of the vascular hysteresis loop
ICC
intraclass correlation coefficient
KPS
Karnofsky Performance Status
MNI
Montreal Neurological Institute
Q
microvessel density parameter
R2
T2 relaxation rate
rCBV
relative CBV
SAGE
spin-and gradient-echo
SE
spin echo
VAM
vascular architecture mapping
VHL
vascular hysteresis loop
VIPS
vascular-induced bolus peak-time shift
VSI
vessel size index
VTI
vessel type indicator
  • © 2024 by American Journal of Neuroradiology
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American Journal of Neuroradiology: 45 (9)
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Cite this article
Anja Hohmann, Ke Zhang, Christoph M. Mooshage, Johann M.E. Jende, Lukas T. Rotkopf, Heinz-Peter Schlemmer, Martin Bendszus, Wolfgang Wick, Felix T. Kurz
Whole-Brain Vascular Architecture Mapping Identifies Region-Specific Microvascular Profiles In Vivo
American Journal of Neuroradiology Sep 2024, 45 (9) 1346-1354; DOI: 10.3174/ajnr.A8344

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Whole-Brain Vascular Mapping
Anja Hohmann, Ke Zhang, Christoph M. Mooshage, Johann M.E. Jende, Lukas T. Rotkopf, Heinz-Peter Schlemmer, Martin Bendszus, Wolfgang Wick, Felix T. Kurz
American Journal of Neuroradiology Sep 2024, 45 (9) 1346-1354; DOI: 10.3174/ajnr.A8344
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