Dysregulations of sonic hedgehog signaling in MED12-related X-linked intellectual disability disorders

Siddharth Srivastava; Tejasvi Niranjan; Melanie M. May; Patrick Tarpey; William Allen; Anna Hackett; Pierre Simon Jouk; Lucy Raymond; Slyvain Briault; Cindy Skinner; Annick Toutain; Jozef Gecz; William Heath; Roger E. Stevenson; Charles E. Schwartz; Tao Wang

doi:10.1002/mgg3.569

Dysregulations of sonic hedgehog signaling in MED12-related X-linked intellectual disability disorders

Siddharth Srivastava, Tejasvi Niranjan, Melanie M. May, Patrick Tarpey, William Allen, Anna Hackett, Pierre Simon Jouk, Lucy Raymond, Slyvain Briault, Cindy Skinner, Annick Toutain, Jozef Gecz, William Heath, Roger E. Stevenson, Charles E. Schwartz, Tao Wang

School of Medicine

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

7 Scopus citations

Abstract

Background: Mutations in mediator of RNA polymerase II transcription subunit 12 homolog (MED12, OMIM 300188) cause X-linked intellectual disability (XLID) disorders including FG, Lujan, and Ohdo syndromes. The Gli3-dependent Sonic Hedgehog (SHH) signaling pathway has been implicated in the original FG syndrome and Lujan syndrome. How are SHH-signaling defects related to the complex clinical phenotype of MED12-associated XLID syndromes are not fully understood. Methods: Quantitative RT-PCR was used to study expression levels of three SHH-signaling genes in lymophoblast cell lines carrying four MED12 mutations from four unrelated XLID families. Genotype and phenotype correlation studies were performed on these mutations. Results: Three newly identified and one novel MED12 mutations in six affected males from four unrelated XLID families were studied. Three mutations (c.2692A>G; p.N898D, c.3640C>T; p.R1214C, and c.3884G>A; p.R1295H) are located in the LS domain and one (c.617G>A; p.R206Q) is in the L domain of MED12. These mutations involve highly conserved amino acid residues and segregate with ID and related congenital malformations in respective probands families. Patients with the LS-domain mutations share many features of FG syndrome and some features of Lujan syndrome. The patient with the L-domain mutation presented with ID and predominant neuropsychiatric features but little dysmorphic features of either FG or Lujan syndrome. Transcript levels of three Gli3-dependent SHH-signaling genes, CREB5, BMP4, and NEUROG2, were determined by quantitative RT-PCR and found to be significantly elevated in lymphoblasts from patients with three mutations in the MED12-LS domain. Conclusions: These results support a critical role of MED12 in regulating Gli3-dependent SHH signaling and in developing ID and related congenital malformations in XLID syndromes. Differences in the expression profile of SHH-signaling genes potentially contribute to variability in clinical phenotypes in patients with MED12-related XLID disorders.

Original language	English (US)
Article number	e00569
Journal	Molecular Genetics and Genomic Medicine
Volume	7
Issue number	4
DOIs	https://doi.org/10.1002/mgg3.569
State	Published - Apr 2019

Keywords

MED12
Mutation
SHH Signaling
XLID
qRT-PCR

ASJC Scopus subject areas

Molecular Biology
Genetics
Genetics(clinical)

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10.1002/mgg3.569

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Srivastava, S., Niranjan, T., May, M. M., Tarpey, P., Allen, W., Hackett, A., Jouk, P. S., Raymond, L., Briault, S., Skinner, C., Toutain, A., Gecz, J., Heath, W., Stevenson, R. E., Schwartz, C. E., & Wang, T. (2019). Dysregulations of sonic hedgehog signaling in MED12-related X-linked intellectual disability disorders. Molecular Genetics and Genomic Medicine, 7(4), Article e00569. https://doi.org/10.1002/mgg3.569

Srivastava, S, Niranjan, T, May, MM, Tarpey, P, Allen, W, Hackett, A, Jouk, PS, Raymond, L, Briault, S, Skinner, C, Toutain, A, Gecz, J, Heath, W, Stevenson, RE, Schwartz, CE & Wang, T 2019, 'Dysregulations of sonic hedgehog signaling in MED12-related X-linked intellectual disability disorders', Molecular Genetics and Genomic Medicine, vol. 7, no. 4, e00569. https://doi.org/10.1002/mgg3.569

@article{b2969a6a2e704ab1b3f10991a881df2e,

title = "Dysregulations of sonic hedgehog signaling in MED12-related X-linked intellectual disability disorders",

abstract = "Background: Mutations in mediator of RNA polymerase II transcription subunit 12 homolog (MED12, OMIM 300188) cause X-linked intellectual disability (XLID) disorders including FG, Lujan, and Ohdo syndromes. The Gli3-dependent Sonic Hedgehog (SHH) signaling pathway has been implicated in the original FG syndrome and Lujan syndrome. How are SHH-signaling defects related to the complex clinical phenotype of MED12-associated XLID syndromes are not fully understood. Methods: Quantitative RT-PCR was used to study expression levels of three SHH-signaling genes in lymophoblast cell lines carrying four MED12 mutations from four unrelated XLID families. Genotype and phenotype correlation studies were performed on these mutations. Results: Three newly identified and one novel MED12 mutations in six affected males from four unrelated XLID families were studied. Three mutations (c.2692A>G; p.N898D, c.3640C>T; p.R1214C, and c.3884G>A; p.R1295H) are located in the LS domain and one (c.617G>A; p.R206Q) is in the L domain of MED12. These mutations involve highly conserved amino acid residues and segregate with ID and related congenital malformations in respective probands families. Patients with the LS-domain mutations share many features of FG syndrome and some features of Lujan syndrome. The patient with the L-domain mutation presented with ID and predominant neuropsychiatric features but little dysmorphic features of either FG or Lujan syndrome. Transcript levels of three Gli3-dependent SHH-signaling genes, CREB5, BMP4, and NEUROG2, were determined by quantitative RT-PCR and found to be significantly elevated in lymphoblasts from patients with three mutations in the MED12-LS domain. Conclusions: These results support a critical role of MED12 in regulating Gli3-dependent SHH signaling and in developing ID and related congenital malformations in XLID syndromes. Differences in the expression profile of SHH-signaling genes potentially contribute to variability in clinical phenotypes in patients with MED12-related XLID disorders.",

keywords = "MED12, Mutation, SHH Signaling, XLID, qRT-PCR",

author = "Siddharth Srivastava and Tejasvi Niranjan and May, {Melanie M.} and Patrick Tarpey and William Allen and Anna Hackett and Jouk, {Pierre Simon} and Lucy Raymond and Slyvain Briault and Cindy Skinner and Annick Toutain and Jozef Gecz and William Heath and Stevenson, {Roger E.} and Schwartz, {Charles E.} and Tao Wang",

note = "Funding Information: This study was supported in part by grants from NIH (HD26202) to C. E. S; (NS73854) to C.E.S. and T.W; NHMRC (1155224 and 1091593) to J.G; Department of Disabilities and Special Needs of South Carolina; and the Greenwood Genetic Center Foundation. We thank Ellen Boyd from Fullerton Genetics, NC for patient data. The cooperation of patients and their families is gratefully acknowledged. Publisher Copyright: {\textcopyright} 2019 The Authors. Molecular Genetics & Genomic Medicine published by Wiley Periodicals, Inc.",

year = "2019",

month = apr,

doi = "10.1002/mgg3.569",

language = "English (US)",

volume = "7",

journal = "Molecular Genetics and Genomic Medicine",

issn = "2324-9269",

publisher = "John Wiley and Sons Inc.",

number = "4",

}

TY - JOUR

T1 - Dysregulations of sonic hedgehog signaling in MED12-related X-linked intellectual disability disorders

AU - Srivastava, Siddharth

AU - Niranjan, Tejasvi

AU - May, Melanie M.

AU - Tarpey, Patrick

AU - Allen, William

AU - Hackett, Anna

AU - Jouk, Pierre Simon

AU - Raymond, Lucy

AU - Briault, Slyvain

AU - Skinner, Cindy

AU - Toutain, Annick

AU - Gecz, Jozef

AU - Heath, William

AU - Stevenson, Roger E.

AU - Schwartz, Charles E.

AU - Wang, Tao

N1 - Funding Information: This study was supported in part by grants from NIH (HD26202) to C. E. S; (NS73854) to C.E.S. and T.W; NHMRC (1155224 and 1091593) to J.G; Department of Disabilities and Special Needs of South Carolina; and the Greenwood Genetic Center Foundation. We thank Ellen Boyd from Fullerton Genetics, NC for patient data. The cooperation of patients and their families is gratefully acknowledged. Publisher Copyright: © 2019 The Authors. Molecular Genetics & Genomic Medicine published by Wiley Periodicals, Inc.

PY - 2019/4

Y1 - 2019/4

N2 - Background: Mutations in mediator of RNA polymerase II transcription subunit 12 homolog (MED12, OMIM 300188) cause X-linked intellectual disability (XLID) disorders including FG, Lujan, and Ohdo syndromes. The Gli3-dependent Sonic Hedgehog (SHH) signaling pathway has been implicated in the original FG syndrome and Lujan syndrome. How are SHH-signaling defects related to the complex clinical phenotype of MED12-associated XLID syndromes are not fully understood. Methods: Quantitative RT-PCR was used to study expression levels of three SHH-signaling genes in lymophoblast cell lines carrying four MED12 mutations from four unrelated XLID families. Genotype and phenotype correlation studies were performed on these mutations. Results: Three newly identified and one novel MED12 mutations in six affected males from four unrelated XLID families were studied. Three mutations (c.2692A>G; p.N898D, c.3640C>T; p.R1214C, and c.3884G>A; p.R1295H) are located in the LS domain and one (c.617G>A; p.R206Q) is in the L domain of MED12. These mutations involve highly conserved amino acid residues and segregate with ID and related congenital malformations in respective probands families. Patients with the LS-domain mutations share many features of FG syndrome and some features of Lujan syndrome. The patient with the L-domain mutation presented with ID and predominant neuropsychiatric features but little dysmorphic features of either FG or Lujan syndrome. Transcript levels of three Gli3-dependent SHH-signaling genes, CREB5, BMP4, and NEUROG2, were determined by quantitative RT-PCR and found to be significantly elevated in lymphoblasts from patients with three mutations in the MED12-LS domain. Conclusions: These results support a critical role of MED12 in regulating Gli3-dependent SHH signaling and in developing ID and related congenital malformations in XLID syndromes. Differences in the expression profile of SHH-signaling genes potentially contribute to variability in clinical phenotypes in patients with MED12-related XLID disorders.

AB - Background: Mutations in mediator of RNA polymerase II transcription subunit 12 homolog (MED12, OMIM 300188) cause X-linked intellectual disability (XLID) disorders including FG, Lujan, and Ohdo syndromes. The Gli3-dependent Sonic Hedgehog (SHH) signaling pathway has been implicated in the original FG syndrome and Lujan syndrome. How are SHH-signaling defects related to the complex clinical phenotype of MED12-associated XLID syndromes are not fully understood. Methods: Quantitative RT-PCR was used to study expression levels of three SHH-signaling genes in lymophoblast cell lines carrying four MED12 mutations from four unrelated XLID families. Genotype and phenotype correlation studies were performed on these mutations. Results: Three newly identified and one novel MED12 mutations in six affected males from four unrelated XLID families were studied. Three mutations (c.2692A>G; p.N898D, c.3640C>T; p.R1214C, and c.3884G>A; p.R1295H) are located in the LS domain and one (c.617G>A; p.R206Q) is in the L domain of MED12. These mutations involve highly conserved amino acid residues and segregate with ID and related congenital malformations in respective probands families. Patients with the LS-domain mutations share many features of FG syndrome and some features of Lujan syndrome. The patient with the L-domain mutation presented with ID and predominant neuropsychiatric features but little dysmorphic features of either FG or Lujan syndrome. Transcript levels of three Gli3-dependent SHH-signaling genes, CREB5, BMP4, and NEUROG2, were determined by quantitative RT-PCR and found to be significantly elevated in lymphoblasts from patients with three mutations in the MED12-LS domain. Conclusions: These results support a critical role of MED12 in regulating Gli3-dependent SHH signaling and in developing ID and related congenital malformations in XLID syndromes. Differences in the expression profile of SHH-signaling genes potentially contribute to variability in clinical phenotypes in patients with MED12-related XLID disorders.

KW - MED12

KW - Mutation

KW - SHH Signaling

KW - XLID

KW - qRT-PCR

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U2 - 10.1002/mgg3.569

DO - 10.1002/mgg3.569

M3 - Article

C2 - 30729724

AN - SCOPUS:85064444849

SN - 2324-9269

VL - 7

JO - Molecular Genetics and Genomic Medicine

JF - Molecular Genetics and Genomic Medicine

IS - 4

M1 - e00569

ER -

Dysregulations of sonic hedgehog signaling in MED12-related X-linked intellectual disability disorders

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