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Research ArticlePediatric Neuroimaging

Mapping Human Fetal Brain Maturation In Vivo Using Quantitative MRI

V.U. Schmidbauer, G.O. Dovjak, M.S. Yildirim, G. Mayr-Geisl, M. Weber, M.C. Diogo, G.M. Gruber, F. Prayer, R.-I. Milos, M. Stuempflen, B. Ulm, J. Binder, D. Bettelheim, H. Kiss, D. Prayer and G. Kasprian
American Journal of Neuroradiology November 2021, 42 (11) 2086-2093; DOI: https://doi.org/10.3174/ajnr.A7286
V.U. Schmidbauer
aFrom the Departments of Biomedical Imaging and Image-Guided Therapy (V.U.S., G.O.D., M.S.Y., M.W., M.C.D., F.P., R.-I.M., M.S., D.P. G.K)
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G.O. Dovjak
aFrom the Departments of Biomedical Imaging and Image-Guided Therapy (V.U.S., G.O.D., M.S.Y., M.W., M.C.D., F.P., R.-I.M., M.S., D.P. G.K)
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M.S. Yildirim
aFrom the Departments of Biomedical Imaging and Image-Guided Therapy (V.U.S., G.O.D., M.S.Y., M.W., M.C.D., F.P., R.-I.M., M.S., D.P. G.K)
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G. Mayr-Geisl
bNeurosurgery (G.M.-G.)
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M. Weber
aFrom the Departments of Biomedical Imaging and Image-Guided Therapy (V.U.S., G.O.D., M.S.Y., M.W., M.C.D., F.P., R.-I.M., M.S., D.P. G.K)
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M.C. Diogo
aFrom the Departments of Biomedical Imaging and Image-Guided Therapy (V.U.S., G.O.D., M.S.Y., M.W., M.C.D., F.P., R.-I.M., M.S., D.P. G.K)
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G.M. Gruber
dDepartment of Anatomy and Biomechanics (G.M.G.), Karl Landsteiner University of Health Sciences, Krems an der Donau, Austria
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F. Prayer
aFrom the Departments of Biomedical Imaging and Image-Guided Therapy (V.U.S., G.O.D., M.S.Y., M.W., M.C.D., F.P., R.-I.M., M.S., D.P. G.K)
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R.-I. Milos
aFrom the Departments of Biomedical Imaging and Image-Guided Therapy (V.U.S., G.O.D., M.S.Y., M.W., M.C.D., F.P., R.-I.M., M.S., D.P. G.K)
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M. Stuempflen
aFrom the Departments of Biomedical Imaging and Image-Guided Therapy (V.U.S., G.O.D., M.S.Y., M.W., M.C.D., F.P., R.-I.M., M.S., D.P. G.K)
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B. Ulm
cObstetrics and Gynecology (B.U., J.B., D.B., H.K.), Medical University of Vienna, Vienna, Austria
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J. Binder
cObstetrics and Gynecology (B.U., J.B., D.B., H.K.), Medical University of Vienna, Vienna, Austria
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D. Bettelheim
cObstetrics and Gynecology (B.U., J.B., D.B., H.K.), Medical University of Vienna, Vienna, Austria
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H. Kiss
cObstetrics and Gynecology (B.U., J.B., D.B., H.K.), Medical University of Vienna, Vienna, Austria
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D. Prayer
aFrom the Departments of Biomedical Imaging and Image-Guided Therapy (V.U.S., G.O.D., M.S.Y., M.W., M.C.D., F.P., R.-I.M., M.S., D.P. G.K)
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G. Kasprian
aFrom the Departments of Biomedical Imaging and Image-Guided Therapy (V.U.S., G.O.D., M.S.Y., M.W., M.C.D., F.P., R.-I.M., M.S., D.P. G.K)
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Abstract

BACKGROUND AND PURPOSE: On the basis of a single multidynamic multiecho sequence acquisition, SyMRI generates a variety of quantitative image data that can characterize tissue-specific properties. The aim of this retrospective study was to evaluate the feasibility of SyMRI for the qualitative and quantitative assessment of fetal brain maturation.

MATERIALS AND METHODS: In 52 fetuses, multidynamic multiecho sequence acquisitions were available. SyMRI was used to perform multidynamic multiecho–based postprocessing. Fetal brain maturity was scored qualitatively on the basis of SyMRI-generated MR imaging data. The results were compared with conventionally acquired T1-weighted/T2-weighted contrasts as a standard of reference. Myelin-related changes in T1-/T2-relaxation time/relaxation rate, proton density, and MR imaging signal intensity of the developing fetal brain stem were measured. A Pearson correlation analysis was used to detect correlations between the following: 1) the gestational age at MR imaging and the fetal brain maturity score, and 2) the gestational age at MR imaging and the quantitative measurements.

RESULTS: SyMRI provided images of sufficient quality in 12/52 (23.08%) (range, 23 + 6–34 + 0) fetal multidynamic multiecho sequence acquisitions. The fetal brain maturity score positively correlated with gestational age at MR imaging (SyMRI: r = 0.915, P < .001/standard of reference: r = 0.966, P < .001). Myelination-related changes in the T2 relaxation time/T2 relaxation rate of the medulla oblongata significantly correlated with gestational age at MR imaging (T2-relaxation time: r = –0.739, P = .006/T2-relaxation rate: r = 0.790, P = .002).

CONCLUSIONS: Fetal motion limits the applicability of multidynamic multiecho–based postprocessing. However, SyMRI-generated image data of sufficient quality enable the qualitative assessment of maturity-related changes of the fetal brain. In addition, quantitative T2 relaxation time/T2 relaxation rate mapping characterizes myelin-related changes of the brain stem prenatally. This approach, if successful, opens novel possibilities for the evaluation of structural and biochemical aspects of fetal brain maturation.

ABBREVIATIONS:

GA
gestational age
MDME
multidynamic multiecho
PD
proton density
R1
T1-relaxation rate
R2
T2-relaxation rate
SI
signal intensity
T1R
T1-relaxation time
T2R
T2-relaxation time
  • © 2021 by American Journal of Neuroradiology
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American Journal of Neuroradiology: 42 (11)
American Journal of Neuroradiology
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V.U. Schmidbauer, G.O. Dovjak, M.S. Yildirim, G. Mayr-Geisl, M. Weber, M.C. Diogo, G.M. Gruber, F. Prayer, R.-I. Milos, M. Stuempflen, B. Ulm, J. Binder, D. Bettelheim, H. Kiss, D. Prayer, G. Kasprian
Mapping Human Fetal Brain Maturation In Vivo Using Quantitative MRI
American Journal of Neuroradiology Nov 2021, 42 (11) 2086-2093; DOI: 10.3174/ajnr.A7286

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Mapping Human Fetal Brain Maturation In Vivo Using Quantitative MRI
V.U. Schmidbauer, G.O. Dovjak, M.S. Yildirim, G. Mayr-Geisl, M. Weber, M.C. Diogo, G.M. Gruber, F. Prayer, R.-I. Milos, M. Stuempflen, B. Ulm, J. Binder, D. Bettelheim, H. Kiss, D. Prayer, G. Kasprian
American Journal of Neuroradiology Nov 2021, 42 (11) 2086-2093; DOI: 10.3174/ajnr.A7286
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