Down Syndrome Developmental Brain Transcriptome Reveals Defective Oligodendrocyte Differentiation and Myelination

Jose Luis Olmos-Serrano; Hyo Jung Kang; William A. Tyler; John C. Silbereis; Feng Cheng; Ying Zhu; Mihovil Pletikos; Lucija Jankovic-Rapan; Nathan P. Cramer; Zygmunt Galdzicki; Joseph Goodliffe; Alan Peters; Claire Sethares; Ivana Delalle; Jeffrey A. Golden; Tarik F. Haydar; Nenad Sestan

doi:10.1016/j.neuron.2016.01.042

Down Syndrome Developmental Brain Transcriptome Reveals Defective Oligodendrocyte Differentiation and Myelination

Jose Luis Olmos-Serrano, Hyo Jung Kang, William A. Tyler, John C. Silbereis, Feng Cheng, Ying Zhu, Mihovil Pletikos, Lucija Jankovic-Rapan, Nathan P. Cramer, Zygmunt Galdzicki, Joseph Goodliffe, Alan Peters, Claire Sethares, Ivana Delalle, Jeffrey A. Golden, Tarik F. Haydar^*, Nenad Sestan

^*Corresponding author for this work

Anatomy, Physiology, and Genetics

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

196 Scopus citations

Abstract

Trisomy 21, or Down syndrome (DS), is the most common genetic cause of developmental delay and intellectual disability. To gain insight into the underlying molecular and cellular pathogenesis, we conducted a multi-region transcriptome analysis of DS and euploid control brains spanning from mid-fetal development to adulthood. We found genome-wide alterations in the expression of a large number of genes, many of which exhibited temporal and spatial specificity and were associated with distinct biological processes. In particular, we uncovered co-dysregulation of genes associated with oligodendrocyte differentiation and myelination that were validated via cross-species comparison to Ts65Dn trisomy mice. Furthermore, we show that hypomyelination present in Ts65Dn mice is in part due to cell-autonomous effects of trisomy on oligodendrocyte differentiation and results in slower neocortical action potential transmission. Together, these results identify defects in white matter development and function in DS, and they provide a transcriptional framework for further investigating DS neuropathogenesis.

Original language	English
Pages (from-to)	1208-1222
Number of pages	15
Journal	Neuron
Volume	89
Issue number	6
DOIs	https://doi.org/10.1016/j.neuron.2016.01.042
State	Published - 16 Mar 2016

Keywords

Brain development
Gene expression
Genomics
Glia
Neocortex
Neurodevelopmental disorders
White matter

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10.1016/j.neuron.2016.01.042

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Olmos-Serrano, J. L., Kang, H. J., Tyler, W. A., Silbereis, J. C., Cheng, F., Zhu, Y., Pletikos, M., Jankovic-Rapan, L., Cramer, N. P., Galdzicki, Z., Goodliffe, J., Peters, A., Sethares, C., Delalle, I., Golden, J. A., Haydar, T. F., & Sestan, N. (2016). Down Syndrome Developmental Brain Transcriptome Reveals Defective Oligodendrocyte Differentiation and Myelination. Neuron, 89(6), 1208-1222. https://doi.org/10.1016/j.neuron.2016.01.042

@article{fdf56564d5094b90b62c5d27ea14e1f1,

title = "Down Syndrome Developmental Brain Transcriptome Reveals Defective Oligodendrocyte Differentiation and Myelination",

abstract = "Trisomy 21, or Down syndrome (DS), is the most common genetic cause of developmental delay and intellectual disability. To gain insight into the underlying molecular and cellular pathogenesis, we conducted a multi-region transcriptome analysis of DS and euploid control brains spanning from mid-fetal development to adulthood. We found genome-wide alterations in the expression of a large number of genes, many of which exhibited temporal and spatial specificity and were associated with distinct biological processes. In particular, we uncovered co-dysregulation of genes associated with oligodendrocyte differentiation and myelination that were validated via cross-species comparison to Ts65Dn trisomy mice. Furthermore, we show that hypomyelination present in Ts65Dn mice is in part due to cell-autonomous effects of trisomy on oligodendrocyte differentiation and results in slower neocortical action potential transmission. Together, these results identify defects in white matter development and function in DS, and they provide a transcriptional framework for further investigating DS neuropathogenesis.",

keywords = "Brain development, Gene expression, Genomics, Glia, Neocortex, Neurodevelopmental disorders, White matter",

author = "Olmos-Serrano, \{Jose Luis\} and Kang, \{Hyo Jung\} and Tyler, \{William A.\} and Silbereis, \{John C.\} and Feng Cheng and Ying Zhu and Mihovil Pletikos and Lucija Jankovic-Rapan and Cramer, \{Nathan P.\} and Zygmunt Galdzicki and Joseph Goodliffe and Alan Peters and Claire Sethares and Ivana Delalle and Golden, \{Jeffrey A.\} and Haydar, \{Tarik F.\} and Nenad Sestan",

note = "Publisher Copyright: {\textcopyright} 2016 Elsevier Inc.",

year = "2016",

month = mar,

day = "16",

doi = "10.1016/j.neuron.2016.01.042",

language = "English",

volume = "89",

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Olmos-Serrano, JL, Kang, HJ, Tyler, WA, Silbereis, JC, Cheng, F, Zhu, Y, Pletikos, M, Jankovic-Rapan, L, Cramer, NP, Galdzicki, Z, Goodliffe, J, Peters, A, Sethares, C, Delalle, I, Golden, JA, Haydar, TF & Sestan, N 2016, 'Down Syndrome Developmental Brain Transcriptome Reveals Defective Oligodendrocyte Differentiation and Myelination', Neuron, vol. 89, no. 6, pp. 1208-1222. https://doi.org/10.1016/j.neuron.2016.01.042

TY - JOUR

T1 - Down Syndrome Developmental Brain Transcriptome Reveals Defective Oligodendrocyte Differentiation and Myelination

AU - Olmos-Serrano, Jose Luis

AU - Kang, Hyo Jung

AU - Tyler, William A.

AU - Silbereis, John C.

AU - Cheng, Feng

AU - Zhu, Ying

AU - Pletikos, Mihovil

AU - Jankovic-Rapan, Lucija

AU - Cramer, Nathan P.

AU - Galdzicki, Zygmunt

AU - Goodliffe, Joseph

AU - Peters, Alan

AU - Sethares, Claire

AU - Delalle, Ivana

AU - Golden, Jeffrey A.

AU - Haydar, Tarik F.

AU - Sestan, Nenad

PY - 2016/3/16

Y1 - 2016/3/16

N2 - Trisomy 21, or Down syndrome (DS), is the most common genetic cause of developmental delay and intellectual disability. To gain insight into the underlying molecular and cellular pathogenesis, we conducted a multi-region transcriptome analysis of DS and euploid control brains spanning from mid-fetal development to adulthood. We found genome-wide alterations in the expression of a large number of genes, many of which exhibited temporal and spatial specificity and were associated with distinct biological processes. In particular, we uncovered co-dysregulation of genes associated with oligodendrocyte differentiation and myelination that were validated via cross-species comparison to Ts65Dn trisomy mice. Furthermore, we show that hypomyelination present in Ts65Dn mice is in part due to cell-autonomous effects of trisomy on oligodendrocyte differentiation and results in slower neocortical action potential transmission. Together, these results identify defects in white matter development and function in DS, and they provide a transcriptional framework for further investigating DS neuropathogenesis.

AB - Trisomy 21, or Down syndrome (DS), is the most common genetic cause of developmental delay and intellectual disability. To gain insight into the underlying molecular and cellular pathogenesis, we conducted a multi-region transcriptome analysis of DS and euploid control brains spanning from mid-fetal development to adulthood. We found genome-wide alterations in the expression of a large number of genes, many of which exhibited temporal and spatial specificity and were associated with distinct biological processes. In particular, we uncovered co-dysregulation of genes associated with oligodendrocyte differentiation and myelination that were validated via cross-species comparison to Ts65Dn trisomy mice. Furthermore, we show that hypomyelination present in Ts65Dn mice is in part due to cell-autonomous effects of trisomy on oligodendrocyte differentiation and results in slower neocortical action potential transmission. Together, these results identify defects in white matter development and function in DS, and they provide a transcriptional framework for further investigating DS neuropathogenesis.

KW - Brain development

KW - Gene expression

KW - Genomics

KW - Glia

KW - Neocortex

KW - Neurodevelopmental disorders

KW - White matter

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DO - 10.1016/j.neuron.2016.01.042

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AN - SCOPUS:84960802950

SN - 0896-6273

VL - 89

SP - 1208

EP - 1222

JO - Neuron

JF - Neuron

IS - 6

ER -

Down Syndrome Developmental Brain Transcriptome Reveals Defective Oligodendrocyte Differentiation and Myelination

Abstract

Keywords

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