Genetic risk for schizophrenia and developmental delay is associated with shape and microstructure of midline white-matter structures

Mark Drakesmith; Greg D. Parker; Jacqueline Smith; Stefanie C. Linden; Elliott Rees; Nigel Williams; Michael J. Owen; Marianne van den Bree; Jeremy Hall; Derek K. Jones; David E. J. Linden

doi:10.1038/s41398-019-0440-7

Genetic risk for schizophrenia and developmental delay is associated with shape and microstructure of midline white-matter structures

Mark Drakesmith^*, Greg D. Parker, Jacqueline Smith, Stefanie C. Linden, Elliott Rees, Nigel Williams, Michael J. Owen, Marianne van den Bree, Jeremy Hall, Derek K. Jones, David E. J. Linden

^*Corresponding author for this work

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

Abstract

Genomic copy number variants (CNVs) are amongst the most highly penetrant genetic risk factors for neuropsychiatric disorders. The scarcity of carriers of individual CNVs and their phenotypical heterogeneity limits investigations of the associated neural mechanisms and endophenotypes. We applied a novel design based on CNV penetrance for schizophrenia (Sz) and developmental delay (DD) that allows us to identify structural sequelae that are most relevant to neuropsychiatric disorders. Our focus on brain structural abnormalities was based on the hypothesis that convergent mechanisms contributing to neurodevelopmental disorders would likely manifest in the macro- and microstructure of white matter and cortical and subcortical grey matter. Twenty one adult participants carrying neuropsychiatric risk CNVs (including those located at 22q11.2, 15q11.2, 1q21.1, 16p11.2 and 17q12) and 15 age- and gender-matched controls underwent T1-weighted structural, diffusion and relaxometry MRI. The macro- and microstructural properties of the cingulum bundles were associated with penetrance for both developmental delay and schizophrenia, in particular curvature along the anterior- posterior axis (Sz: p(corr) = 0.026; DD: p(corr) = 0.035) and intracellular volume fraction (Sz: p(corr) = 0.019; DD: p(corr) = 0.064). Further principal component analysis showed alterations in the interrelationships between the volumes of several midline white-matter structures (Sz: p(corr) = 0.055; DD: p(corr) = 0.027). In particular, the ratio of volumes in the splenium and body of the corpus callosum was significantly associated with both penetrance scores (Sz: p = 0.037; DD; p = 0.006). Our results are consistent with the notion that a significant alteration in developmental trajectories of midline white-matter structures constitutes a common neurodevelopmental aberration contributing to risk for schizophrenia and intellectual disability.

Original language	English
Article number	102
Number of pages	13
Journal	Translational Psychiatry
Volume	9
DOIs	https://doi.org/10.1038/s41398-019-0440-7
Publication status	Published - 25 Feb 2019

Keywords

22Q11.2 DELETION SYNDROME
SURFACE-BASED ANALYSIS
DIFFUSION TENSOR MRI
VELOCARDIOFACIAL SYNDROME
CORPUS-CALLOSUM
CINGULUM BUNDLE
BRAIN
ABNORMALITIES
CHILDREN
SEGMENTATION

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Drakesmith, M., Parker, G. D., Smith, J., Linden, S. C., Rees, E., Williams, N., Owen, M. J., van den Bree, M., Hall, J., Jones, D. K., & Linden, D. E. J. (2019). Genetic risk for schizophrenia and developmental delay is associated with shape and microstructure of midline white-matter structures. Translational Psychiatry, 9, Article 102. https://doi.org/10.1038/s41398-019-0440-7

@article{08e063028bb74be9925accb019bf404d,

title = "Genetic risk for schizophrenia and developmental delay is associated with shape and microstructure of midline white-matter structures",

abstract = "Genomic copy number variants (CNVs) are amongst the most highly penetrant genetic risk factors for neuropsychiatric disorders. The scarcity of carriers of individual CNVs and their phenotypical heterogeneity limits investigations of the associated neural mechanisms and endophenotypes. We applied a novel design based on CNV penetrance for schizophrenia (Sz) and developmental delay (DD) that allows us to identify structural sequelae that are most relevant to neuropsychiatric disorders. Our focus on brain structural abnormalities was based on the hypothesis that convergent mechanisms contributing to neurodevelopmental disorders would likely manifest in the macro- and microstructure of white matter and cortical and subcortical grey matter. Twenty one adult participants carrying neuropsychiatric risk CNVs (including those located at 22q11.2, 15q11.2, 1q21.1, 16p11.2 and 17q12) and 15 age- and gender-matched controls underwent T1-weighted structural, diffusion and relaxometry MRI. The macro- and microstructural properties of the cingulum bundles were associated with penetrance for both developmental delay and schizophrenia, in particular curvature along the anterior- posterior axis (Sz: p(corr) = 0.026; DD: p(corr) = 0.035) and intracellular volume fraction (Sz: p(corr) = 0.019; DD: p(corr) = 0.064). Further principal component analysis showed alterations in the interrelationships between the volumes of several midline white-matter structures (Sz: p(corr) = 0.055; DD: p(corr) = 0.027). In particular, the ratio of volumes in the splenium and body of the corpus callosum was significantly associated with both penetrance scores (Sz: p = 0.037; DD; p = 0.006). Our results are consistent with the notion that a significant alteration in developmental trajectories of midline white-matter structures constitutes a common neurodevelopmental aberration contributing to risk for schizophrenia and intellectual disability.",

keywords = "22Q11.2 DELETION SYNDROME, SURFACE-BASED ANALYSIS, DIFFUSION TENSOR MRI, VELOCARDIOFACIAL SYNDROME, CORPUS-CALLOSUM, CINGULUM BUNDLE, BRAIN, ABNORMALITIES, CHILDREN, SEGMENTATION",

author = "Mark Drakesmith and Parker, {Greg D.} and Jacqueline Smith and Linden, {Stefanie C.} and Elliott Rees and Nigel Williams and Owen, {Michael J.} and {van den Bree}, Marianne and Jeremy Hall and Jones, {Derek K.} and Linden, {David E. J.}",

note = "Funding Information: This study was funded by two Wellcome Trust Strategic Awards (100202/Z/12/ Z, 104943/Z/14/Z) and a Wellcome Trust New Investigator awarded to DKJ (096646/Z/11/Z). We would also like to thank the members of the field team who assisted in recruitment, assessment and data collection, Ffion Evans, Kali Barawi and Vera Schroeter. Publisher Copyright: {\textcopyright} 2019, The Author(s).",

year = "2019",

month = feb,

day = "25",

doi = "10.1038/s41398-019-0440-7",

language = "English",

volume = "9",

journal = "Translational Psychiatry",

issn = "2158-3188",

publisher = "Nature Publishing Group",

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TY - JOUR

T1 - Genetic risk for schizophrenia and developmental delay is associated with shape and microstructure of midline white-matter structures

AU - Drakesmith, Mark

AU - Parker, Greg D.

AU - Smith, Jacqueline

AU - Linden, Stefanie C.

AU - Rees, Elliott

AU - Williams, Nigel

AU - Owen, Michael J.

AU - van den Bree, Marianne

AU - Hall, Jeremy

AU - Jones, Derek K.

AU - Linden, David E. J.

N1 - Funding Information: This study was funded by two Wellcome Trust Strategic Awards (100202/Z/12/ Z, 104943/Z/14/Z) and a Wellcome Trust New Investigator awarded to DKJ (096646/Z/11/Z). We would also like to thank the members of the field team who assisted in recruitment, assessment and data collection, Ffion Evans, Kali Barawi and Vera Schroeter. Publisher Copyright: © 2019, The Author(s).

PY - 2019/2/25

Y1 - 2019/2/25

N2 - Genomic copy number variants (CNVs) are amongst the most highly penetrant genetic risk factors for neuropsychiatric disorders. The scarcity of carriers of individual CNVs and their phenotypical heterogeneity limits investigations of the associated neural mechanisms and endophenotypes. We applied a novel design based on CNV penetrance for schizophrenia (Sz) and developmental delay (DD) that allows us to identify structural sequelae that are most relevant to neuropsychiatric disorders. Our focus on brain structural abnormalities was based on the hypothesis that convergent mechanisms contributing to neurodevelopmental disorders would likely manifest in the macro- and microstructure of white matter and cortical and subcortical grey matter. Twenty one adult participants carrying neuropsychiatric risk CNVs (including those located at 22q11.2, 15q11.2, 1q21.1, 16p11.2 and 17q12) and 15 age- and gender-matched controls underwent T1-weighted structural, diffusion and relaxometry MRI. The macro- and microstructural properties of the cingulum bundles were associated with penetrance for both developmental delay and schizophrenia, in particular curvature along the anterior- posterior axis (Sz: p(corr) = 0.026; DD: p(corr) = 0.035) and intracellular volume fraction (Sz: p(corr) = 0.019; DD: p(corr) = 0.064). Further principal component analysis showed alterations in the interrelationships between the volumes of several midline white-matter structures (Sz: p(corr) = 0.055; DD: p(corr) = 0.027). In particular, the ratio of volumes in the splenium and body of the corpus callosum was significantly associated with both penetrance scores (Sz: p = 0.037; DD; p = 0.006). Our results are consistent with the notion that a significant alteration in developmental trajectories of midline white-matter structures constitutes a common neurodevelopmental aberration contributing to risk for schizophrenia and intellectual disability.

AB - Genomic copy number variants (CNVs) are amongst the most highly penetrant genetic risk factors for neuropsychiatric disorders. The scarcity of carriers of individual CNVs and their phenotypical heterogeneity limits investigations of the associated neural mechanisms and endophenotypes. We applied a novel design based on CNV penetrance for schizophrenia (Sz) and developmental delay (DD) that allows us to identify structural sequelae that are most relevant to neuropsychiatric disorders. Our focus on brain structural abnormalities was based on the hypothesis that convergent mechanisms contributing to neurodevelopmental disorders would likely manifest in the macro- and microstructure of white matter and cortical and subcortical grey matter. Twenty one adult participants carrying neuropsychiatric risk CNVs (including those located at 22q11.2, 15q11.2, 1q21.1, 16p11.2 and 17q12) and 15 age- and gender-matched controls underwent T1-weighted structural, diffusion and relaxometry MRI. The macro- and microstructural properties of the cingulum bundles were associated with penetrance for both developmental delay and schizophrenia, in particular curvature along the anterior- posterior axis (Sz: p(corr) = 0.026; DD: p(corr) = 0.035) and intracellular volume fraction (Sz: p(corr) = 0.019; DD: p(corr) = 0.064). Further principal component analysis showed alterations in the interrelationships between the volumes of several midline white-matter structures (Sz: p(corr) = 0.055; DD: p(corr) = 0.027). In particular, the ratio of volumes in the splenium and body of the corpus callosum was significantly associated with both penetrance scores (Sz: p = 0.037; DD; p = 0.006). Our results are consistent with the notion that a significant alteration in developmental trajectories of midline white-matter structures constitutes a common neurodevelopmental aberration contributing to risk for schizophrenia and intellectual disability.

KW - 22Q11.2 DELETION SYNDROME

KW - SURFACE-BASED ANALYSIS

KW - DIFFUSION TENSOR MRI

KW - VELOCARDIOFACIAL SYNDROME

KW - CORPUS-CALLOSUM

KW - CINGULUM BUNDLE

KW - BRAIN

KW - ABNORMALITIES

KW - CHILDREN

KW - SEGMENTATION

U2 - 10.1038/s41398-019-0440-7

DO - 10.1038/s41398-019-0440-7

M3 - Article

C2 - 30804328

SN - 2158-3188

VL - 9

JO - Translational Psychiatry

JF - Translational Psychiatry

M1 - 102

ER -