Early alterations in cortical and cerebellar regional brain growth in Down Syndrome: An in vivo fetal and neonatal MRI assessment

doi:10.1016/j.nicl.2019.102139

. 2020:25:102139.

doi: 10.1016/j.nicl.2019.102139. Epub 2019 Dec 23.

Early alterations in cortical and cerebellar regional brain growth in Down Syndrome: An in vivo fetal and neonatal MRI assessment

Affiliations

¹ Centre for the Developing Brain, School of Biomedical Engineering and Imaging Sciences, King's College London, St. Thomas's Hospital, London, SE1 7EH, United Kingdom.
² Centre for the Developing Brain, School of Biomedical Engineering and Imaging Sciences, King's College London, St. Thomas's Hospital, London, SE1 7EH, United Kingdom; Department of Forensic and Neurodevelopmental Science, Sackler Institute for Translational Neurodevelopment, Institute of Psychiatry, Psychology and Neuroscience, King's College London, SE5 8AB, United Kingdom.
³ Department of Forensic and Neurodevelopmental Science, Sackler Institute for Translational Neurodevelopment, Institute of Psychiatry, Psychology and Neuroscience, King's College London, SE5 8AB, United Kingdom.
⁴ Centre for the Developing Brain, School of Biomedical Engineering and Imaging Sciences, King's College London, St. Thomas's Hospital, London, SE1 7EH, United Kingdom. Electronic address: mary.rutherford@kcl.ac.uk.

PMID: 31887718
PMCID: PMC6938981
DOI: 10.1016/j.nicl.2019.102139

Early alterations in cortical and cerebellar regional brain growth in Down Syndrome: An in vivo fetal and neonatal MRI assessment

Prachi A Patkee et al. Neuroimage Clin. 2020.

. 2020:25:102139.

doi: 10.1016/j.nicl.2019.102139. Epub 2019 Dec 23.

Affiliations

¹ Centre for the Developing Brain, School of Biomedical Engineering and Imaging Sciences, King's College London, St. Thomas's Hospital, London, SE1 7EH, United Kingdom.
² Centre for the Developing Brain, School of Biomedical Engineering and Imaging Sciences, King's College London, St. Thomas's Hospital, London, SE1 7EH, United Kingdom; Department of Forensic and Neurodevelopmental Science, Sackler Institute for Translational Neurodevelopment, Institute of Psychiatry, Psychology and Neuroscience, King's College London, SE5 8AB, United Kingdom.
³ Department of Forensic and Neurodevelopmental Science, Sackler Institute for Translational Neurodevelopment, Institute of Psychiatry, Psychology and Neuroscience, King's College London, SE5 8AB, United Kingdom.
⁴ Centre for the Developing Brain, School of Biomedical Engineering and Imaging Sciences, King's College London, St. Thomas's Hospital, London, SE1 7EH, United Kingdom. Electronic address: mary.rutherford@kcl.ac.uk.

PMID: 31887718
PMCID: PMC6938981
DOI: 10.1016/j.nicl.2019.102139

Abstract

Down Syndrome (DS) is the most frequent genetic cause of intellectual disability with a wide spectrum of neurodevelopmental outcomes. At present, the relationship between structural brain morphology and the spectrum of cognitive phenotypes in DS, is not well understood. This study aimed to quantify the development of the fetal and neonatal brain in DS participants, with and without a congenital cardiac defect compared with a control population using dedicated, optimised and motion-corrected in vivo magnetic resonance imaging (MRI). We detected deviations in development and altered regional brain growth in the fetus with DS from 21 weeks' gestation, when compared to age-matched controls. Reduced cerebellar volume was apparent in the second trimester with significant alteration in cortical growth becoming evident during the third trimester. Developmental abnormalities in the cortex and cerebellum are likely substrates for later neurocognitive impairment, and ongoing studies will allow us to confirm the role of antenatal MRI as an early biomarker for subsequent cognitive ability in DS. In the era of rapidly developing technologies, we believe that the results of this study will assist counselling for prospective parents.

Keywords: Brain; Down Syndrome; Fetal; MRI; Neonatal.

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Conflict of interest statement

Declaration of competing interest The authors declare that they have no competing interests.

Figures

Fig 1 — **Fig. 1**
Visual representation of linear measurements in the fetal brain in the axial plane (a: BPD–brain, (b): BPD–skull, (c): OFD–brain, (d): OFD–skull, (e): cavum width, (f): HC, (g): TCD; (h): vermis height; (i): vermis width; (j): vermis surface area).

Fig 2 — **Fig. 2**
Volumetric segmentation of the fetal brain. Segmentation of T2-weighted volumetric MR images in the axial, sagittal and coronal planes showing (a) supratentorial brain tissue (red), (b) cortex (green), (c) lateral ventricles (dark blue), (d) extra cerebral cerebrospinal fluid (light blue); and (e) cerebellar hemispheres (pink), cerebellar vermis (bright green), pons (yellow) and fourth ventricle (blue).

Fig 3 — **Fig. 3**
Volumetric segmentation of the neonatal brain. (a) Reconstructed T2 neonatal brain, (b) automatic neonatal brain segmentation; supratentorial brain tissue (bright blue + green + gray), cortex (green), lateral ventricles (light blue), extra cerebral cerebrospinal fluid (red), cerebellar hemispheres (pink); and brainstem (deep blue).

Fig 4 — **Fig. 4**
2D and 3D regional measures of the brain in fetuses and neonates with DS and a congenital heart defect (DS + CHD; red circles), DS without a congenital heart defect (DS–CHD; Blue squares), and age-matched normal controls (black triangles). (a) Whole brain volumes, (b) Cortical volumes, (c) Biparietal diameter (BPD)–skull, (d) Biparietal diameter (BPD)–brain, (e) Occipitofrontal diameter (OFD)–skull, (f) Occipitofrontal diameter (OFD)–brain, and (g) Head circumference (HC) (MRI derived).

Fig 5 — **Fig. 5**
2D and 3D measures of the cerebellum in fetuses and neonates with DS and a congenital heart defect (DS+CHD; red circles), DS without a congenital heart defect (DS–CHD; blue squares), and age-matched normal controls (black triangles). (a) Cerebellar volume, (b) Transcerebellar diameter, (c) Vermis height (d) Vermis width, and (e) Vermis surface area.

Fig 6 — **Fig. 6**
2D and 3D measures of the CSF regions in fetuses and neonates with DS and a congenital heart defect (DS + CHD; red circles), DS without a congenital heart defect (DS – CHD; blue squares), and age-matched normal controls (black triangles). (a) Lateral ventricular volume, (b) eCSF volume, and (c) Cavum width.

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References

1. Holtzman D.… The human trisomy 21 brain: insights from mouse models of Down syndrome. Ment. Retard. 1996;72:66–72.
1. Antonarakis S.E., Lyle R., Dermitzakis E.T., Reymond A., Deutsch S. Chromosome 21 and down syndrome: from genomics to pathophysiology. Nat. Rev. Genet. 2004;5:725–738. - PubMed
1. Määttä T., Tervo-Määttä T., Taanila A., Kaski M., Iivanainen M. Mental health, behaviour and intellectual abilities of people with Down syndrome. Down Syndr. Res. Pract. 2006;11:37–43. - PubMed
1. Rachidi M., Lopes C. Mental retardation in Down syndrome: from gene dosage imbalance to molecular and cellular mechanisms. Neurosci. Res. 2007;59:349–369. - PubMed
1. Bartesaghi R., Guidi S., Ciani E. Is it possible to improve neurodevelopmental abnormalities in Down syndrome. Rev. Neurosci. 2011;22:419–455. - PubMed

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[1] Holtzman D.… The human trisomy 21 brain: insights from mouse models of Down syndrome. Ment. Retard. 1996;72:66–72.

[2] Holtzman D.… The human trisomy 21 brain: insights from mouse models of Down syndrome. Ment. Retard. 1996;72:66–72.

[3] Antonarakis S.E., Lyle R., Dermitzakis E.T., Reymond A., Deutsch S. Chromosome 21 and down syndrome: from genomics to pathophysiology. Nat. Rev. Genet. 2004;5:725–738. - PubMed

[4] Antonarakis S.E., Lyle R., Dermitzakis E.T., Reymond A., Deutsch S. Chromosome 21 and down syndrome: from genomics to pathophysiology. Nat. Rev. Genet. 2004;5:725–738. - PubMed

[5] Määttä T., Tervo-Määttä T., Taanila A., Kaski M., Iivanainen M. Mental health, behaviour and intellectual abilities of people with Down syndrome. Down Syndr. Res. Pract. 2006;11:37–43. - PubMed

[6] Määttä T., Tervo-Määttä T., Taanila A., Kaski M., Iivanainen M. Mental health, behaviour and intellectual abilities of people with Down syndrome. Down Syndr. Res. Pract. 2006;11:37–43. - PubMed

[7] Rachidi M., Lopes C. Mental retardation in Down syndrome: from gene dosage imbalance to molecular and cellular mechanisms. Neurosci. Res. 2007;59:349–369. - PubMed

[8] Rachidi M., Lopes C. Mental retardation in Down syndrome: from gene dosage imbalance to molecular and cellular mechanisms. Neurosci. Res. 2007;59:349–369. - PubMed

[9] Bartesaghi R., Guidi S., Ciani E. Is it possible to improve neurodevelopmental abnormalities in Down syndrome. Rev. Neurosci. 2011;22:419–455. - PubMed

[10] Bartesaghi R., Guidi S., Ciani E. Is it possible to improve neurodevelopmental abnormalities in Down syndrome. Rev. Neurosci. 2011;22:419–455. - PubMed

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Early alterations in cortical and cerebellar regional brain growth in Down Syndrome: An in vivo fetal and neonatal MRI assessment

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Early alterations in cortical and cerebellar regional brain growth in Down Syndrome: An in vivo fetal and neonatal MRI assessment

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