Wnt Signaling Interactor WTIP (Wilms Tumor Interacting Protein) Underlies Novel Mechanism for Cardiac Hypertrophy

Hannah N. De Jong; Frederick E. Dewey; Pablo Cordero; Rachelle A. Victorio; Anna Kirillova; Yong Huang; Roshni Madhvani; Kinya Seo; Andreas A. Werdich; Feng Lan; Mark Orcholski; W. Robert Liu; Ayca Erbilgin; Matthew T. Wheeler; Rui Chen; Stephen Pan; Young M. Kim; Krishna Bommakanti; Cherisse A. Marcou; J. Martijn Bos; Francois Haddad; Michael Ackerman; Ramachandran S. Vasan; Calum Macrae; Joseph C. Wu; Vinicio De Jesus Perez; Michael Snyder; Victoria N. Parikh; Euan A. Ashley

doi:10.1161/CIRCGEN.121.003563

Wnt Signaling Interactor WTIP (Wilms Tumor Interacting Protein) Underlies Novel Mechanism for Cardiac Hypertrophy

Hannah N. De Jong, Frederick E. Dewey, Pablo Cordero, Rachelle A. Victorio, Anna Kirillova, Yong Huang, Roshni Madhvani, Kinya Seo, Andreas A. Werdich, Feng Lan, Mark Orcholski, W. Robert Liu, Ayca Erbilgin, Matthew T. Wheeler, Rui Chen, Stephen Pan, Young M. Kim, Krishna Bommakanti, Cherisse A. Marcou, J. Martijn BosFrancois Haddad, Michael Ackerman, Ramachandran S. Vasan, Calum Macrae, Joseph C. Wu, Vinicio De Jesus Perez, Michael Snyder, Victoria N. Parikh, Euan A. Ashley

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Background: The study of hypertrophic cardiomyopathy (HCM) can yield insight into the mechanisms underlying the complex trait of cardiac hypertrophy. To date, most genetic variants associated with HCM have been found in sarcomeric genes. Here, we describe a novel HCM-associated variant in the noncanonical Wnt signaling interactor WTIP (Wilms tumor interacting protein) and provide evidence of a role for WTIP in complex disease. Methods: In a family affected by HCM, we used exome sequencing and identity-by-descent analysis to identify a novel variant in WTIP (p.Y233F). We knocked down WTIP in isolated neonatal rat ventricular myocytes with lentivirally delivered short hairpin ribonucleic acids and in Danio rerio via morpholino injection. We performed weighted gene coexpression network analysis for WTIP in human cardiac tissue, as well as association analysis for WTIP variation and left ventricular hypertrophy. Finally, we generated induced pluripotent stem cell-derived cardiomyocytes from patient tissue, characterized size and calcium cycling, and determined the effect of verapamil treatment on calcium dynamics. Results: WTIP knockdown caused hypertrophy in neonatal rat ventricular myocytes and increased cardiac hypertrophy, peak calcium, and resting calcium in D rerio. Network analysis of human cardiac tissue indicated WTIP as a central coordinator of prohypertrophic networks, while common variation at the WTIP locus was associated with human left ventricular hypertrophy. Patient-derived WTIP p.Y233F-induced pluripotent stem cell-derived cardiomyocytes recapitulated cellular hypertrophy and increased resting calcium, which was ameliorated by verapamil. Conclusions: We demonstrate that a novel genetic variant found in a family with HCM disrupts binding to a known Wnt signaling protein, misregulating cardiomyocyte calcium dynamics. Further, in orthogonal model systems, we show that expression of the gene WTIP is important in complex cardiac hypertrophy phenotypes. These findings, derived from the observation of a rare Mendelian disease variant, uncover a novel disease mechanism with implications across diverse forms of cardiac hypertrophy.

Idioma original	English (US)
Páginas (desde-hasta)	E003563
Publicación	Circulation. Genomic and precision medicine
Volumen	15
N.º	4
DOI	https://doi.org/10.1161/CIRCGEN.121.003563
Estado	Published - ago 1 2022
Publicado de forma externa	Sí

ASJC Scopus subject areas

Genetics
Cardiology and Cardiovascular Medicine
Genetics(clinical)

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10.1161/CIRCGEN.121.003563

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De Jong, H. N., Dewey, F. E., Cordero, P., Victorio, R. A., Kirillova, A., Huang, Y., Madhvani, R., Seo, K., Werdich, A. A., Lan, F., Orcholski, M., Liu, W. R., Erbilgin, A., Wheeler, M. T., Chen, R., Pan, S., Kim, Y. M., Bommakanti, K., Marcou, C. A., ... Ashley, E. A. (2022). Wnt Signaling Interactor WTIP (Wilms Tumor Interacting Protein) Underlies Novel Mechanism for Cardiac Hypertrophy. Circulation. Genomic and precision medicine, 15(4), E003563. https://doi.org/10.1161/CIRCGEN.121.003563

De Jong, HN, Dewey, FE, Cordero, P, Victorio, RA, Kirillova, A, Huang, Y, Madhvani, R, Seo, K, Werdich, AA, Lan, F, Orcholski, M, Liu, WR, Erbilgin, A, Wheeler, MT, Chen, R, Pan, S, Kim, YM, Bommakanti, K, Marcou, CA, Bos, JM, Haddad, F, Ackerman, M, Vasan, RS, Macrae, C, Wu, JC, De Jesus Perez, V, Snyder, M, Parikh, VN & Ashley, EA 2022, 'Wnt Signaling Interactor WTIP (Wilms Tumor Interacting Protein) Underlies Novel Mechanism for Cardiac Hypertrophy', Circulation. Genomic and precision medicine, vol. 15, n.º 4, pp. E003563. https://doi.org/10.1161/CIRCGEN.121.003563

@article{f6433f11a3d440569d765fceb21b3b6a,

title = "Wnt Signaling Interactor WTIP (Wilms Tumor Interacting Protein) Underlies Novel Mechanism for Cardiac Hypertrophy",

abstract = "Background: The study of hypertrophic cardiomyopathy (HCM) can yield insight into the mechanisms underlying the complex trait of cardiac hypertrophy. To date, most genetic variants associated with HCM have been found in sarcomeric genes. Here, we describe a novel HCM-associated variant in the noncanonical Wnt signaling interactor WTIP (Wilms tumor interacting protein) and provide evidence of a role for WTIP in complex disease. Methods: In a family affected by HCM, we used exome sequencing and identity-by-descent analysis to identify a novel variant in WTIP (p.Y233F). We knocked down WTIP in isolated neonatal rat ventricular myocytes with lentivirally delivered short hairpin ribonucleic acids and in Danio rerio via morpholino injection. We performed weighted gene coexpression network analysis for WTIP in human cardiac tissue, as well as association analysis for WTIP variation and left ventricular hypertrophy. Finally, we generated induced pluripotent stem cell-derived cardiomyocytes from patient tissue, characterized size and calcium cycling, and determined the effect of verapamil treatment on calcium dynamics. Results: WTIP knockdown caused hypertrophy in neonatal rat ventricular myocytes and increased cardiac hypertrophy, peak calcium, and resting calcium in D rerio. Network analysis of human cardiac tissue indicated WTIP as a central coordinator of prohypertrophic networks, while common variation at the WTIP locus was associated with human left ventricular hypertrophy. Patient-derived WTIP p.Y233F-induced pluripotent stem cell-derived cardiomyocytes recapitulated cellular hypertrophy and increased resting calcium, which was ameliorated by verapamil. Conclusions: We demonstrate that a novel genetic variant found in a family with HCM disrupts binding to a known Wnt signaling protein, misregulating cardiomyocyte calcium dynamics. Further, in orthogonal model systems, we show that expression of the gene WTIP is important in complex cardiac hypertrophy phenotypes. These findings, derived from the observation of a rare Mendelian disease variant, uncover a novel disease mechanism with implications across diverse forms of cardiac hypertrophy.",

keywords = "calcium, cardiomyopathy, hypertrophic, humans, induced pluripotent stem cells, myocytes, cardiac, zebra fish",

author = "{De Jong}, {Hannah N.} and Dewey, {Frederick E.} and Pablo Cordero and Victorio, {Rachelle A.} and Anna Kirillova and Yong Huang and Roshni Madhvani and Kinya Seo and Werdich, {Andreas A.} and Feng Lan and Mark Orcholski and Liu, {W. Robert} and Ayca Erbilgin and Wheeler, {Matthew T.} and Rui Chen and Stephen Pan and Kim, {Young M.} and Krishna Bommakanti and Marcou, {Cherisse A.} and Bos, {J. Martijn} and Francois Haddad and Michael Ackerman and Vasan, {Ramachandran S.} and Calum Macrae and Wu, {Joseph C.} and {De Jesus Perez}, Vinicio and Michael Snyder and Parikh, {Victoria N.} and Ashley, {Euan A.}",

note = "Funding Information: This work was supported, in part, by the National Institutes of Health grants 1R01HL144843-01 (H.N.D., V.N.P., and E.A.A.), 1U01HG010218-01 (M.T.W. and E.A.A.), and NHLBI K08 HL143185 (V.N.P.), the US Department of Energy Computational Science Graduate Fellowship (H.N.D.), the US National Heart, Lung, and Blood Institute grants N01-HL-25195 (R.S.V.) and R01HL 093328 (R.S.V.), the Sarnoff Foundation (V.N.P.), and the John Taylor Babbitt Foundation (V.N.P.). Funding Information: Dr Madhvani is currently an employee at Cytokinetics. Dr Chen is currently an employee at Personalis, Inc. Dr Ackerman is a consultant for Abbott, Audentes Therapeutics, Boston Scientific, Daiichi Sankyo, Invitae, LQT Therapeutics, Medtronic, MyoKardia, and UpToDate. Dr Ackerman and Mayo Clinic have an equity/royalty relationship with Alive Cor and Anumana. Dr MacRae has the following disclosures: Bayer, Merck, Affinia Tx, Design Tx, DiNAQor, Dewpoint, Myokardia, Atman Health, BioSymetrics, Foresite Labs, Dr Evidence, Apple, Verily, AstraZeneca, Bodyport, gWell, NeuCures, Clarify Health Solutions, Pfizer, and Quest Diagnostics. E.A. Ashley has the following financial disclosures: Personalis (founder and advisor), Deepcell (founder and advisor), Silicon Valley Exercise Analytics (founder and advisor), AstraZeneca (nonexecutive director), Gilead (advisor, clinical trial site PI), MyoKardia (academic grant, clinical trial site PI), Amgen (advisor, academic grant), Takeda (academic grant), Genome Medical (advisor), Avive (founding advisor), Samsung (scientific collaboration), Apple (advisor, scientific collaboration), Google (academic grants), Verily (scientific collaboration), Disney (advisor), Illumina (collaborative support in kind), Pacific Biosciences (collaborative support in kind), Oxford Nanopore (collaborative support in kind), Foresite Capital (advisor), and Sequence Bio (advisor). The other authors report no conflicts. Publisher Copyright: {\textcopyright} 2022 Lippincott Williams and Wilkins. All rights reserved.",

year = "2022",

month = aug,

day = "1",

doi = "10.1161/CIRCGEN.121.003563",

language = "English (US)",

volume = "15",

pages = "E003563",

journal = "Circulation. Genomic and precision medicine",

issn = "1942-325X",

publisher = "Lippincott Williams and Wilkins Ltd.",

number = "4",

}

TY - JOUR

T1 - Wnt Signaling Interactor WTIP (Wilms Tumor Interacting Protein) Underlies Novel Mechanism for Cardiac Hypertrophy

AU - De Jong, Hannah N.

AU - Dewey, Frederick E.

AU - Cordero, Pablo

AU - Victorio, Rachelle A.

AU - Kirillova, Anna

AU - Huang, Yong

AU - Madhvani, Roshni

AU - Seo, Kinya

AU - Werdich, Andreas A.

AU - Lan, Feng

AU - Orcholski, Mark

AU - Liu, W. Robert

AU - Erbilgin, Ayca

AU - Wheeler, Matthew T.

AU - Chen, Rui

AU - Pan, Stephen

AU - Kim, Young M.

AU - Bommakanti, Krishna

AU - Marcou, Cherisse A.

AU - Bos, J. Martijn

AU - Haddad, Francois

AU - Ackerman, Michael

AU - Vasan, Ramachandran S.

AU - Macrae, Calum

AU - Wu, Joseph C.

AU - De Jesus Perez, Vinicio

AU - Snyder, Michael

AU - Parikh, Victoria N.

AU - Ashley, Euan A.

N1 - Funding Information: This work was supported, in part, by the National Institutes of Health grants 1R01HL144843-01 (H.N.D., V.N.P., and E.A.A.), 1U01HG010218-01 (M.T.W. and E.A.A.), and NHLBI K08 HL143185 (V.N.P.), the US Department of Energy Computational Science Graduate Fellowship (H.N.D.), the US National Heart, Lung, and Blood Institute grants N01-HL-25195 (R.S.V.) and R01HL 093328 (R.S.V.), the Sarnoff Foundation (V.N.P.), and the John Taylor Babbitt Foundation (V.N.P.). Funding Information: Dr Madhvani is currently an employee at Cytokinetics. Dr Chen is currently an employee at Personalis, Inc. Dr Ackerman is a consultant for Abbott, Audentes Therapeutics, Boston Scientific, Daiichi Sankyo, Invitae, LQT Therapeutics, Medtronic, MyoKardia, and UpToDate. Dr Ackerman and Mayo Clinic have an equity/royalty relationship with Alive Cor and Anumana. Dr MacRae has the following disclosures: Bayer, Merck, Affinia Tx, Design Tx, DiNAQor, Dewpoint, Myokardia, Atman Health, BioSymetrics, Foresite Labs, Dr Evidence, Apple, Verily, AstraZeneca, Bodyport, gWell, NeuCures, Clarify Health Solutions, Pfizer, and Quest Diagnostics. E.A. Ashley has the following financial disclosures: Personalis (founder and advisor), Deepcell (founder and advisor), Silicon Valley Exercise Analytics (founder and advisor), AstraZeneca (nonexecutive director), Gilead (advisor, clinical trial site PI), MyoKardia (academic grant, clinical trial site PI), Amgen (advisor, academic grant), Takeda (academic grant), Genome Medical (advisor), Avive (founding advisor), Samsung (scientific collaboration), Apple (advisor, scientific collaboration), Google (academic grants), Verily (scientific collaboration), Disney (advisor), Illumina (collaborative support in kind), Pacific Biosciences (collaborative support in kind), Oxford Nanopore (collaborative support in kind), Foresite Capital (advisor), and Sequence Bio (advisor). The other authors report no conflicts. Publisher Copyright: © 2022 Lippincott Williams and Wilkins. All rights reserved.

PY - 2022/8/1

Y1 - 2022/8/1

N2 - Background: The study of hypertrophic cardiomyopathy (HCM) can yield insight into the mechanisms underlying the complex trait of cardiac hypertrophy. To date, most genetic variants associated with HCM have been found in sarcomeric genes. Here, we describe a novel HCM-associated variant in the noncanonical Wnt signaling interactor WTIP (Wilms tumor interacting protein) and provide evidence of a role for WTIP in complex disease. Methods: In a family affected by HCM, we used exome sequencing and identity-by-descent analysis to identify a novel variant in WTIP (p.Y233F). We knocked down WTIP in isolated neonatal rat ventricular myocytes with lentivirally delivered short hairpin ribonucleic acids and in Danio rerio via morpholino injection. We performed weighted gene coexpression network analysis for WTIP in human cardiac tissue, as well as association analysis for WTIP variation and left ventricular hypertrophy. Finally, we generated induced pluripotent stem cell-derived cardiomyocytes from patient tissue, characterized size and calcium cycling, and determined the effect of verapamil treatment on calcium dynamics. Results: WTIP knockdown caused hypertrophy in neonatal rat ventricular myocytes and increased cardiac hypertrophy, peak calcium, and resting calcium in D rerio. Network analysis of human cardiac tissue indicated WTIP as a central coordinator of prohypertrophic networks, while common variation at the WTIP locus was associated with human left ventricular hypertrophy. Patient-derived WTIP p.Y233F-induced pluripotent stem cell-derived cardiomyocytes recapitulated cellular hypertrophy and increased resting calcium, which was ameliorated by verapamil. Conclusions: We demonstrate that a novel genetic variant found in a family with HCM disrupts binding to a known Wnt signaling protein, misregulating cardiomyocyte calcium dynamics. Further, in orthogonal model systems, we show that expression of the gene WTIP is important in complex cardiac hypertrophy phenotypes. These findings, derived from the observation of a rare Mendelian disease variant, uncover a novel disease mechanism with implications across diverse forms of cardiac hypertrophy.

AB - Background: The study of hypertrophic cardiomyopathy (HCM) can yield insight into the mechanisms underlying the complex trait of cardiac hypertrophy. To date, most genetic variants associated with HCM have been found in sarcomeric genes. Here, we describe a novel HCM-associated variant in the noncanonical Wnt signaling interactor WTIP (Wilms tumor interacting protein) and provide evidence of a role for WTIP in complex disease. Methods: In a family affected by HCM, we used exome sequencing and identity-by-descent analysis to identify a novel variant in WTIP (p.Y233F). We knocked down WTIP in isolated neonatal rat ventricular myocytes with lentivirally delivered short hairpin ribonucleic acids and in Danio rerio via morpholino injection. We performed weighted gene coexpression network analysis for WTIP in human cardiac tissue, as well as association analysis for WTIP variation and left ventricular hypertrophy. Finally, we generated induced pluripotent stem cell-derived cardiomyocytes from patient tissue, characterized size and calcium cycling, and determined the effect of verapamil treatment on calcium dynamics. Results: WTIP knockdown caused hypertrophy in neonatal rat ventricular myocytes and increased cardiac hypertrophy, peak calcium, and resting calcium in D rerio. Network analysis of human cardiac tissue indicated WTIP as a central coordinator of prohypertrophic networks, while common variation at the WTIP locus was associated with human left ventricular hypertrophy. Patient-derived WTIP p.Y233F-induced pluripotent stem cell-derived cardiomyocytes recapitulated cellular hypertrophy and increased resting calcium, which was ameliorated by verapamil. Conclusions: We demonstrate that a novel genetic variant found in a family with HCM disrupts binding to a known Wnt signaling protein, misregulating cardiomyocyte calcium dynamics. Further, in orthogonal model systems, we show that expression of the gene WTIP is important in complex cardiac hypertrophy phenotypes. These findings, derived from the observation of a rare Mendelian disease variant, uncover a novel disease mechanism with implications across diverse forms of cardiac hypertrophy.

KW - calcium

KW - cardiomyopathy, hypertrophic

KW - humans

KW - induced pluripotent stem cells

KW - myocytes, cardiac

KW - zebra fish

UR - http://www.scopus.com/inward/record.url?scp=85136311055&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85136311055&partnerID=8YFLogxK

U2 - 10.1161/CIRCGEN.121.003563

DO - 10.1161/CIRCGEN.121.003563

M3 - Article

C2 - 35671065

AN - SCOPUS:85136311055

SN - 1942-325X

VL - 15

SP - E003563

JO - Circulation. Genomic and precision medicine

JF - Circulation. Genomic and precision medicine

IS - 4

ER -

Wnt Signaling Interactor WTIP (Wilms Tumor Interacting Protein) Underlies Novel Mechanism for Cardiac Hypertrophy

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