MCTP2 is a dosage-sensitive gene required for cardiac outflow tract development

Seema R. Lalani; Stephanie M. Ware; Xueqing Wang; Gladys Zapata; Qi Tian; Luis M. Franco; Zhengxin Jiang; Kristine Bucasas; Daryl A. Scott; Philippe M. Campeau; Neil Hanchard; Luis Umaña; Ashley Cast; Ankita Patel; Sau W. Cheung; Kim L. McBride; Molly Bray; A. Craig Chinault; Barbara A. Boggs; Miao Huang; Mariah R. Baker; Susan Hamilton; Jeff Towbin; John L. Jefferies; Susan D. Fernbach; Lorraine Potocki; John W. Belmont

doi:10.1093/hmg/ddt283

MCTP2 is a dosage-sensitive gene required for cardiac outflow tract development

Seema R. Lalani, Stephanie M. Ware, Xueqing Wang, Gladys Zapata, Qi Tian, Luis M. Franco, Zhengxin Jiang, Kristine Bucasas, Daryl A. Scott, Philippe M. Campeau, Neil Hanchard, Luis Umaña, Ashley Cast, Ankita Patel, Sau W. Cheung, Kim L. McBride, Molly Bray, A. Craig Chinault, Barbara A. Boggs, Miao HuangMariah R. Baker, Susan Hamilton, Jeff Towbin, John L. Jefferies, Susan D. Fernbach, Lorraine Potocki, John W. Belmont

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Abstract

Coarctation of the aorta (CoA) and hypoplastic left heart syndrome (HLHS) have been reported in rare individuals with large terminal deletions of chromosome15q26.However, nosingle gene important for left ventricularoutflow tract (LVOT) development has been identified in this region. Using array-comparative genomic hybridization, we identified two half-siblings with CoA with a 2.2 Mb deletion on 15q26.2, inherited from their mother, who was mosaic for this deletion. This interval contains an evolutionary conserved, protein-coding gene, MCTP2 (multiple C2-domains with two transmembrane regions 2). Using gene-specific array screening in 146 individualswith nonsyndromic LVOT obstructive defects, another individual with HLHS and CoA was found to have a de novo 41 kb intragenic duplication within MCTP2, predicted to result in premature truncation, p. F697X. Alteration of Mctp2 gene expression in Xenopus laevis embryos by morpholino knockdown and mRNA overexpression resulted in the failure of proper OT development, confirming the functional importance of this dosage-sensitive gene for cardiogenesis. Our results identify MCTP2 as a novel genetic cause of CoA and related cardiac malformations.

Original language	English (US)
Article number	ddt283
Pages (from-to)	4339-4348
Number of pages	10
Journal	Human molecular genetics
Volume	22
Issue number	21
DOIs	https://doi.org/10.1093/hmg/ddt283
State	Published - Nov 2013

ASJC Scopus subject areas

Molecular Biology
Genetics
Genetics(clinical)

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Lalani, S. R., Ware, S. M., Wang, X., Zapata, G., Tian, Q., Franco, L. M., Jiang, Z., Bucasas, K., Scott, D. A., Campeau, P. M., Hanchard, N., Umaña, L., Cast, A., Patel, A., Cheung, S. W., McBride, K. L., Bray, M., Chinault, A. C., Boggs, B. A., ... Belmont, J. W. (2013). MCTP2 is a dosage-sensitive gene required for cardiac outflow tract development. Human molecular genetics, 22(21), 4339-4348. Article ddt283. https://doi.org/10.1093/hmg/ddt283

Lalani, SR, Ware, SM, Wang, X, Zapata, G, Tian, Q, Franco, LM, Jiang, Z, Bucasas, K, Scott, DA, Campeau, PM, Hanchard, N, Umaña, L, Cast, A, Patel, A, Cheung, SW, McBride, KL, Bray, M, Chinault, AC, Boggs, BA, Huang, M, Baker, MR, Hamilton, S, Towbin, J, Jefferies, JL, Fernbach, SD, Potocki, L & Belmont, JW 2013, 'MCTP2 is a dosage-sensitive gene required for cardiac outflow tract development', Human molecular genetics, vol. 22, no. 21, ddt283, pp. 4339-4348. https://doi.org/10.1093/hmg/ddt283

@article{a77425e4185040b7b2c0c2a7627370b3,

title = "MCTP2 is a dosage-sensitive gene required for cardiac outflow tract development",

abstract = "Coarctation of the aorta (CoA) and hypoplastic left heart syndrome (HLHS) have been reported in rare individuals with large terminal deletions of chromosome15q26.However, nosingle gene important for left ventricularoutflow tract (LVOT) development has been identified in this region. Using array-comparative genomic hybridization, we identified two half-siblings with CoA with a 2.2 Mb deletion on 15q26.2, inherited from their mother, who was mosaic for this deletion. This interval contains an evolutionary conserved, protein-coding gene, MCTP2 (multiple C2-domains with two transmembrane regions 2). Using gene-specific array screening in 146 individualswith nonsyndromic LVOT obstructive defects, another individual with HLHS and CoA was found to have a de novo 41 kb intragenic duplication within MCTP2, predicted to result in premature truncation, p. F697X. Alteration of Mctp2 gene expression in Xenopus laevis embryos by morpholino knockdown and mRNA overexpression resulted in the failure of proper OT development, confirming the functional importance of this dosage-sensitive gene for cardiogenesis. Our results identify MCTP2 as a novel genetic cause of CoA and related cardiac malformations.",

author = "Lalani, {Seema R.} and Ware, {Stephanie M.} and Xueqing Wang and Gladys Zapata and Qi Tian and Franco, {Luis M.} and Zhengxin Jiang and Kristine Bucasas and Scott, {Daryl A.} and Campeau, {Philippe M.} and Neil Hanchard and Luis Uma{\~n}a and Ashley Cast and Ankita Patel and Cheung, {Sau W.} and McBride, {Kim L.} and Molly Bray and Chinault, {A. Craig} and Boggs, {Barbara A.} and Miao Huang and Baker, {Mariah R.} and Susan Hamilton and Jeff Towbin and Jefferies, {John L.} and Fernbach, {Susan D.} and Lorraine Potocki and Belmont, {John W.}",

note = "Funding Information: This work was supported by grants to S.R.L. from the Doris Duke Charitable Foundation and the Gillson Logenbaugh Foundation; the NIH RO1-HL091771 grant to J.W.B. and S.R.L.; Burroughs Wellcome Fund Clinical Scientist Award in Translational Research #1008496 to S.M.W.; and March of Dimes #1-FY10-401 grant to S.M.W. and S.R.L. K.L.M. is supported by K23HL70823.",

year = "2013",

month = nov,

doi = "10.1093/hmg/ddt283",

language = "English (US)",

volume = "22",

pages = "4339--4348",

journal = "Human molecular genetics",

issn = "0964-6906",

publisher = "Oxford University Press",

number = "21",

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T1 - MCTP2 is a dosage-sensitive gene required for cardiac outflow tract development

AU - Lalani, Seema R.

AU - Ware, Stephanie M.

AU - Wang, Xueqing

AU - Zapata, Gladys

AU - Tian, Qi

AU - Franco, Luis M.

AU - Jiang, Zhengxin

AU - Bucasas, Kristine

AU - Scott, Daryl A.

AU - Campeau, Philippe M.

AU - Hanchard, Neil

AU - Umaña, Luis

AU - Cast, Ashley

AU - Patel, Ankita

AU - Cheung, Sau W.

AU - McBride, Kim L.

AU - Bray, Molly

AU - Chinault, A. Craig

AU - Boggs, Barbara A.

AU - Huang, Miao

AU - Baker, Mariah R.

AU - Hamilton, Susan

AU - Towbin, Jeff

AU - Jefferies, John L.

AU - Fernbach, Susan D.

AU - Potocki, Lorraine

AU - Belmont, John W.

N1 - Funding Information: This work was supported by grants to S.R.L. from the Doris Duke Charitable Foundation and the Gillson Logenbaugh Foundation; the NIH RO1-HL091771 grant to J.W.B. and S.R.L.; Burroughs Wellcome Fund Clinical Scientist Award in Translational Research #1008496 to S.M.W.; and March of Dimes #1-FY10-401 grant to S.M.W. and S.R.L. K.L.M. is supported by K23HL70823.

PY - 2013/11

Y1 - 2013/11

N2 - Coarctation of the aorta (CoA) and hypoplastic left heart syndrome (HLHS) have been reported in rare individuals with large terminal deletions of chromosome15q26.However, nosingle gene important for left ventricularoutflow tract (LVOT) development has been identified in this region. Using array-comparative genomic hybridization, we identified two half-siblings with CoA with a 2.2 Mb deletion on 15q26.2, inherited from their mother, who was mosaic for this deletion. This interval contains an evolutionary conserved, protein-coding gene, MCTP2 (multiple C2-domains with two transmembrane regions 2). Using gene-specific array screening in 146 individualswith nonsyndromic LVOT obstructive defects, another individual with HLHS and CoA was found to have a de novo 41 kb intragenic duplication within MCTP2, predicted to result in premature truncation, p. F697X. Alteration of Mctp2 gene expression in Xenopus laevis embryos by morpholino knockdown and mRNA overexpression resulted in the failure of proper OT development, confirming the functional importance of this dosage-sensitive gene for cardiogenesis. Our results identify MCTP2 as a novel genetic cause of CoA and related cardiac malformations.

AB - Coarctation of the aorta (CoA) and hypoplastic left heart syndrome (HLHS) have been reported in rare individuals with large terminal deletions of chromosome15q26.However, nosingle gene important for left ventricularoutflow tract (LVOT) development has been identified in this region. Using array-comparative genomic hybridization, we identified two half-siblings with CoA with a 2.2 Mb deletion on 15q26.2, inherited from their mother, who was mosaic for this deletion. This interval contains an evolutionary conserved, protein-coding gene, MCTP2 (multiple C2-domains with two transmembrane regions 2). Using gene-specific array screening in 146 individualswith nonsyndromic LVOT obstructive defects, another individual with HLHS and CoA was found to have a de novo 41 kb intragenic duplication within MCTP2, predicted to result in premature truncation, p. F697X. Alteration of Mctp2 gene expression in Xenopus laevis embryos by morpholino knockdown and mRNA overexpression resulted in the failure of proper OT development, confirming the functional importance of this dosage-sensitive gene for cardiogenesis. Our results identify MCTP2 as a novel genetic cause of CoA and related cardiac malformations.

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MCTP2 is a dosage-sensitive gene required for cardiac outflow tract development

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