Identification of a RAI1-associated disease network through integration of exome sequencing, transcriptomics, and 3D genomics

Maria Nicla Loviglio; Christine R. Beck; Janson J. White; Marion Leleu; Tamar Harel; Nicolas Guex; Anne Niknejad; Weimin Bi; Edward S. Chen; Isaac Crespo; Jiong Yan; Wu Lin Charng; Shen Gu; Ping Fang; Zeynep Coban-Akdemir; Chad A. Shaw; Shalini N. Jhangiani; Donna M. Muzny; Richard A. Gibbs; Jacques Rougemont; Ioannis Xenarios; James R. Lupski; Alexandre Reymond

doi:10.1186/s13073-016-0359-z

Identification of a RAI1-associated disease network through integration of exome sequencing, transcriptomics, and 3D genomics

Maria Nicla Loviglio
, Christine R. Beck
, Janson J. White
, Marion Leleu
, Tamar Harel
, Nicolas Guex
, Anne Niknejad
, Weimin Bi
, Edward S. Chen
, Isaac Crespo
, Jiong Yan
, Wu Lin Charng
, Shen Gu
, Ping Fang
, Zeynep Coban-Akdemir
, Chad A. Shaw
, Shalini N. Jhangiani
, Donna M. Muzny
, Richard A. Gibbs
, Jacques Rougemont

Ioannis Xenarios, James R. Lupski, Alexandre Reymond

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

23 Scopus citations

Abstract

Background: Smith-Magenis syndrome (SMS) is a developmental disability/multiple congenital anomaly disorder resulting from haploinsufficiency of RAI1. It is characterized by distinctive facial features, brachydactyly, sleep disturbances, and stereotypic behaviors. Methods: We investigated a cohort of 15 individuals with a clinical suspicion of SMS who showed neither deletion in the SMS critical region nor damaging variants in RAI1 using whole exome sequencing. A combination of network analysis (co-expression and biomedical text mining), transcriptomics, and circularized chromatin conformation capture (4C-seq) was applied to verify whether modified genes are part of the same disease network as known SMS-causing genes. Results: Potentially deleterious variants were identified in nine of these individuals using whole-exome sequencing. Eight of these changes affect KMT2D, ZEB2, MAP2K2, GLDC, CASK, MECP2, KDM5C, and POGZ, known to be associated with Kabuki syndrome 1, Mowat-Wilson syndrome, cardiofaciocutaneous syndrome, glycine encephalopathy, mental retardation and microcephaly with pontine and cerebellar hypoplasia, X-linked mental retardation 13, X-linked mental retardation Claes-Jensen type, and White-Sutton syndrome, respectively. The ninth individual carries a de novo variant in JAKMIP1, a regulator of neuronal translation that was recently found deleted in a patient with autism spectrum disorder. Analyses of co-expression and biomedical text mining suggest that these pathologies and SMS are part of the same disease network. Further support for this hypothesis was obtained from transcriptome profiling that showed that the expression levels of both Zeb2 and Map2k2 are perturbed in Rai1 ^-/- mice. As an orthogonal approach to potentially contributory disease gene variants, we used chromatin conformation capture to reveal chromatin contacts between RAI1 and the loci flanking ZEB2 and GLDC, as well as between RAI1 and human orthologs of the genes that show perturbed expression in our Rai1 ^-/- mouse model. Conclusions: These holistic studies of RAI1 and its interactions allow insights into SMS and other disorders associated with intellectual disability and behavioral abnormalities. Our findings support a pan-genomic approach to the molecular diagnosis of a distinctive disorder.

Original language	English
Article number	105
Journal	Genome Medicine
Volume	8
Issue number	1
DOIs	https://doi.org/10.1186/s13073-016-0359-z
State	Published - 1 Nov 2016
Externally published	Yes

Keywords

Chromatin conformation
Diagnostic
Disease network
Intellectual disability
Text mining

ASJC Scopus subject areas

Molecular Medicine
Molecular Biology
Genetics
Genetics(clinical)

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10.1186/s13073-016-0359-z

Cite this

Loviglio, M. N., Beck, C. R., White, J. J., Leleu, M., Harel, T., Guex, N., Niknejad, A., Bi, W., Chen, E. S., Crespo, I., Yan, J., Charng, W. L., Gu, S., Fang, P., Coban-Akdemir, Z., Shaw, C. A., Jhangiani, S. N., Muzny, D. M., Gibbs, R. A., ... Reymond, A. (2016). Identification of a RAI1-associated disease network through integration of exome sequencing, transcriptomics, and 3D genomics. Genome Medicine, 8(1), Article 105. https://doi.org/10.1186/s13073-016-0359-z

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title = "Identification of a RAI1-associated disease network through integration of exome sequencing, transcriptomics, and 3D genomics",

abstract = "Background: Smith-Magenis syndrome (SMS) is a developmental disability/multiple congenital anomaly disorder resulting from haploinsufficiency of RAI1. It is characterized by distinctive facial features, brachydactyly, sleep disturbances, and stereotypic behaviors. Methods: We investigated a cohort of 15 individuals with a clinical suspicion of SMS who showed neither deletion in the SMS critical region nor damaging variants in RAI1 using whole exome sequencing. A combination of network analysis (co-expression and biomedical text mining), transcriptomics, and circularized chromatin conformation capture (4C-seq) was applied to verify whether modified genes are part of the same disease network as known SMS-causing genes. Results: Potentially deleterious variants were identified in nine of these individuals using whole-exome sequencing. Eight of these changes affect KMT2D, ZEB2, MAP2K2, GLDC, CASK, MECP2, KDM5C, and POGZ, known to be associated with Kabuki syndrome 1, Mowat-Wilson syndrome, cardiofaciocutaneous syndrome, glycine encephalopathy, mental retardation and microcephaly with pontine and cerebellar hypoplasia, X-linked mental retardation 13, X-linked mental retardation Claes-Jensen type, and White-Sutton syndrome, respectively. The ninth individual carries a de novo variant in JAKMIP1, a regulator of neuronal translation that was recently found deleted in a patient with autism spectrum disorder. Analyses of co-expression and biomedical text mining suggest that these pathologies and SMS are part of the same disease network. Further support for this hypothesis was obtained from transcriptome profiling that showed that the expression levels of both Zeb2 and Map2k2 are perturbed in Rai1 -/- mice. As an orthogonal approach to potentially contributory disease gene variants, we used chromatin conformation capture to reveal chromatin contacts between RAI1 and the loci flanking ZEB2 and GLDC, as well as between RAI1 and human orthologs of the genes that show perturbed expression in our Rai1 -/- mouse model. Conclusions: These holistic studies of RAI1 and its interactions allow insights into SMS and other disorders associated with intellectual disability and behavioral abnormalities. Our findings support a pan-genomic approach to the molecular diagnosis of a distinctive disorder.",

keywords = "Chromatin conformation, Diagnostic, Disease network, Intellectual disability, Text mining",

author = "Loviglio, \{Maria Nicla\} and Beck, \{Christine R.\} and White, \{Janson J.\} and Marion Leleu and Tamar Harel and Nicolas Guex and Anne Niknejad and Weimin Bi and Chen, \{Edward S.\} and Isaac Crespo and Jiong Yan and Charng, \{Wu Lin\} and Shen Gu and Ping Fang and Zeynep Coban-Akdemir and Shaw, \{Chad A.\} and Jhangiani, \{Shalini N.\} and Muzny, \{Donna M.\} and Gibbs, \{Richard A.\} and Jacques Rougemont and Ioannis Xenarios and Lupski, \{James R.\} and Alexandre Reymond",

note = "Publisher Copyright: {\textcopyright} 2016 The Author(s).",

year = "2016",

month = nov,

day = "1",

doi = "10.1186/s13073-016-0359-z",

language = "English",

volume = "8",

journal = "Genome Medicine",

issn = "1756-994X",

publisher = "BioMed Central Ltd.",

number = "1",

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Loviglio, MN, Beck, CR, White, JJ, Leleu, M, Harel, T, Guex, N, Niknejad, A, Bi, W, Chen, ES, Crespo, I, Yan, J, Charng, WL, Gu, S, Fang, P, Coban-Akdemir, Z, Shaw, CA, Jhangiani, SN, Muzny, DM, Gibbs, RA, Rougemont, J, Xenarios, I, Lupski, JR & Reymond, A 2016, 'Identification of a RAI1-associated disease network through integration of exome sequencing, transcriptomics, and 3D genomics', Genome Medicine, vol. 8, no. 1, 105. https://doi.org/10.1186/s13073-016-0359-z

TY - JOUR

T1 - Identification of a RAI1-associated disease network through integration of exome sequencing, transcriptomics, and 3D genomics

AU - Loviglio, Maria Nicla

AU - Beck, Christine R.

AU - White, Janson J.

AU - Leleu, Marion

AU - Harel, Tamar

AU - Guex, Nicolas

AU - Niknejad, Anne

AU - Bi, Weimin

AU - Chen, Edward S.

AU - Crespo, Isaac

AU - Yan, Jiong

AU - Charng, Wu Lin

AU - Gu, Shen

AU - Fang, Ping

AU - Coban-Akdemir, Zeynep

AU - Shaw, Chad A.

AU - Jhangiani, Shalini N.

AU - Muzny, Donna M.

AU - Gibbs, Richard A.

AU - Rougemont, Jacques

AU - Xenarios, Ioannis

AU - Lupski, James R.

AU - Reymond, Alexandre

PY - 2016/11/1

Y1 - 2016/11/1

N2 - Background: Smith-Magenis syndrome (SMS) is a developmental disability/multiple congenital anomaly disorder resulting from haploinsufficiency of RAI1. It is characterized by distinctive facial features, brachydactyly, sleep disturbances, and stereotypic behaviors. Methods: We investigated a cohort of 15 individuals with a clinical suspicion of SMS who showed neither deletion in the SMS critical region nor damaging variants in RAI1 using whole exome sequencing. A combination of network analysis (co-expression and biomedical text mining), transcriptomics, and circularized chromatin conformation capture (4C-seq) was applied to verify whether modified genes are part of the same disease network as known SMS-causing genes. Results: Potentially deleterious variants were identified in nine of these individuals using whole-exome sequencing. Eight of these changes affect KMT2D, ZEB2, MAP2K2, GLDC, CASK, MECP2, KDM5C, and POGZ, known to be associated with Kabuki syndrome 1, Mowat-Wilson syndrome, cardiofaciocutaneous syndrome, glycine encephalopathy, mental retardation and microcephaly with pontine and cerebellar hypoplasia, X-linked mental retardation 13, X-linked mental retardation Claes-Jensen type, and White-Sutton syndrome, respectively. The ninth individual carries a de novo variant in JAKMIP1, a regulator of neuronal translation that was recently found deleted in a patient with autism spectrum disorder. Analyses of co-expression and biomedical text mining suggest that these pathologies and SMS are part of the same disease network. Further support for this hypothesis was obtained from transcriptome profiling that showed that the expression levels of both Zeb2 and Map2k2 are perturbed in Rai1 -/- mice. As an orthogonal approach to potentially contributory disease gene variants, we used chromatin conformation capture to reveal chromatin contacts between RAI1 and the loci flanking ZEB2 and GLDC, as well as between RAI1 and human orthologs of the genes that show perturbed expression in our Rai1 -/- mouse model. Conclusions: These holistic studies of RAI1 and its interactions allow insights into SMS and other disorders associated with intellectual disability and behavioral abnormalities. Our findings support a pan-genomic approach to the molecular diagnosis of a distinctive disorder.

AB - Background: Smith-Magenis syndrome (SMS) is a developmental disability/multiple congenital anomaly disorder resulting from haploinsufficiency of RAI1. It is characterized by distinctive facial features, brachydactyly, sleep disturbances, and stereotypic behaviors. Methods: We investigated a cohort of 15 individuals with a clinical suspicion of SMS who showed neither deletion in the SMS critical region nor damaging variants in RAI1 using whole exome sequencing. A combination of network analysis (co-expression and biomedical text mining), transcriptomics, and circularized chromatin conformation capture (4C-seq) was applied to verify whether modified genes are part of the same disease network as known SMS-causing genes. Results: Potentially deleterious variants were identified in nine of these individuals using whole-exome sequencing. Eight of these changes affect KMT2D, ZEB2, MAP2K2, GLDC, CASK, MECP2, KDM5C, and POGZ, known to be associated with Kabuki syndrome 1, Mowat-Wilson syndrome, cardiofaciocutaneous syndrome, glycine encephalopathy, mental retardation and microcephaly with pontine and cerebellar hypoplasia, X-linked mental retardation 13, X-linked mental retardation Claes-Jensen type, and White-Sutton syndrome, respectively. The ninth individual carries a de novo variant in JAKMIP1, a regulator of neuronal translation that was recently found deleted in a patient with autism spectrum disorder. Analyses of co-expression and biomedical text mining suggest that these pathologies and SMS are part of the same disease network. Further support for this hypothesis was obtained from transcriptome profiling that showed that the expression levels of both Zeb2 and Map2k2 are perturbed in Rai1 -/- mice. As an orthogonal approach to potentially contributory disease gene variants, we used chromatin conformation capture to reveal chromatin contacts between RAI1 and the loci flanking ZEB2 and GLDC, as well as between RAI1 and human orthologs of the genes that show perturbed expression in our Rai1 -/- mouse model. Conclusions: These holistic studies of RAI1 and its interactions allow insights into SMS and other disorders associated with intellectual disability and behavioral abnormalities. Our findings support a pan-genomic approach to the molecular diagnosis of a distinctive disorder.

KW - Chromatin conformation

KW - Diagnostic

KW - Disease network

KW - Intellectual disability

KW - Text mining

UR - https://www.scopus.com/pages/publications/84994504658

U2 - 10.1186/s13073-016-0359-z

DO - 10.1186/s13073-016-0359-z

M3 - Article

C2 - 27799067

AN - SCOPUS:84994504658

SN - 1756-994X

VL - 8

JO - Genome Medicine

JF - Genome Medicine

IS - 1

M1 - 105

ER -

Identification of a RAI1-associated disease network through integration of exome sequencing, transcriptomics, and 3D genomics

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