Sequence variation in PPP1R13L results in a novel form of cardio-cutaneous syndrome

Tzipora C. Falik-Zaccai; Yiftah Barsheshet; Hanna Mandel; Meital Segev; Avraham Lorber; Shachaf Gelberg; Limor Kalfon; Shani Ben Haroush; Adel Shalata; Liat Gelernter-Yaniv; Sarah Chaim; Dorith Raviv Shay; Morad Khayat; Michal Werbner; Inbar Levi; Yishay Shoval; Galit Tal; Stavit Shalev; Eli Reuveni; Emily Avitan-Hersh; Eugene Vlodavsky; Liat Appl-Sarid; Dorit Goldsher; Reuven Bergman; Zvi Segal; Ora Bitterman-Deutsch; Orly Avni

doi:10.15252/emmm.201606523

Sequence variation in PPP1R13L results in a novel form of cardio-cutaneous syndrome

Tzipora C. Falik-Zaccai, Yiftah Barsheshet, Hanna Mandel, Meital Segev, Avraham Lorber, Shachaf Gelberg, Limor Kalfon, Shani Ben Haroush, Adel Shalata, Liat Gelernter-Yaniv, Sarah Chaim, Dorith Raviv Shay, Morad Khayat, Michal Werbner, Inbar Levi, Yishay Shoval, Galit Tal, Stavit Shalev, Eli Reuveni, Emily Avitan-HershEugene Vlodavsky, Liat Appl-Sarid, Dorit Goldsher, Reuven Bergman, Zvi Segal, Ora Bitterman-Deutsch, Orly Avni

Technion - Israel Institute of Technology, Tel Aviv University

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

Abstract

Dilated cardiomyopathy (DCM) is a life-threatening disorder whose genetic basis is heterogeneous and mostly unknown. Five Arab Christian infants, aged 4–30 months from four families, were diagnosed with DCM associated with mild skin, teeth, and hair abnormalities. All passed away before age 3. A homozygous sequence variation creating a premature stop codon at PPP1R13L encoding the iASPP protein was identified in three infants and in the mother of the other two. Patients’ fibroblasts and PPP1R13L-knocked down human fibroblasts presented higher expression levels of pro-inflammatory cytokine genes in response to lipopolysaccharide, as well as Ppp1r13l-knocked down murine cardiomyocytes and hearts of Ppp1r13l-deficient mice. The hypersensitivity to lipopolysaccharide was NF-κB-dependent, and its inducible binding activity to promoters of pro-inflammatory cytokine genes was elevated in patients’ fibroblasts. RNA sequencing of Ppp1r13l-knocked down murine cardiomyocytes and of hearts derived from different stages of DCM development in Ppp1r13l-deficient mice revealed the crucial role of iASPP in dampening cardiac inflammatory response. Our results determined PPP1R13L as the gene underlying a novel autosomal-recessive cardio-cutaneous syndrome in humans and strongly suggest that the fatal DCM during infancy is a consequence of failure to regulate transcriptional pathways necessary for tuning cardiac threshold response to common inflammatory stressors.

Original language	English
Pages (from-to)	319-336
Number of pages	18
Journal	EMBO Molecular Medicine
Volume	9
Issue number	3
DOIs	https://doi.org/10.15252/emmm.201606523
State	Published - 1 Mar 2017

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

PPP1R13L
dilated cardiomyopathy
genetics
inflammation
myocarditis

All Science Journal Classification (ASJC) codes

Molecular Medicine

Access to Document

10.15252/emmm.201606523

Cite this

Falik-Zaccai, T. C., Barsheshet, Y., Mandel, H., Segev, M., Lorber, A., Gelberg, S., Kalfon, L., Ben Haroush, S., Shalata, A., Gelernter-Yaniv, L., Chaim, S., Raviv Shay, D., Khayat, M., Werbner, M., Levi, I., Shoval, Y., Tal, G., Shalev, S., Reuveni, E., ... Avni, O. (2017). Sequence variation in PPP1R13L results in a novel form of cardio-cutaneous syndrome. EMBO Molecular Medicine, 9(3), 319-336. https://doi.org/10.15252/emmm.201606523

@article{c61b830289014a7d8f4da0cb556b2190,

title = "Sequence variation in PPP1R13L results in a novel form of cardio-cutaneous syndrome",

abstract = "Dilated cardiomyopathy (DCM) is a life-threatening disorder whose genetic basis is heterogeneous and mostly unknown. Five Arab Christian infants, aged 4–30 months from four families, were diagnosed with DCM associated with mild skin, teeth, and hair abnormalities. All passed away before age 3. A homozygous sequence variation creating a premature stop codon at PPP1R13L encoding the iASPP protein was identified in three infants and in the mother of the other two. Patients{\textquoteright} fibroblasts and PPP1R13L-knocked down human fibroblasts presented higher expression levels of pro-inflammatory cytokine genes in response to lipopolysaccharide, as well as Ppp1r13l-knocked down murine cardiomyocytes and hearts of Ppp1r13l-deficient mice. The hypersensitivity to lipopolysaccharide was NF-κB-dependent, and its inducible binding activity to promoters of pro-inflammatory cytokine genes was elevated in patients{\textquoteright} fibroblasts. RNA sequencing of Ppp1r13l-knocked down murine cardiomyocytes and of hearts derived from different stages of DCM development in Ppp1r13l-deficient mice revealed the crucial role of iASPP in dampening cardiac inflammatory response. Our results determined PPP1R13L as the gene underlying a novel autosomal-recessive cardio-cutaneous syndrome in humans and strongly suggest that the fatal DCM during infancy is a consequence of failure to regulate transcriptional pathways necessary for tuning cardiac threshold response to common inflammatory stressors.",

keywords = "PPP1R13L, dilated cardiomyopathy, genetics, inflammation, myocarditis",

author = "Falik-Zaccai, \{Tzipora C.\} and Yiftah Barsheshet and Hanna Mandel and Meital Segev and Avraham Lorber and Shachaf Gelberg and Limor Kalfon and \{Ben Haroush\}, Shani and Adel Shalata and Liat Gelernter-Yaniv and Sarah Chaim and \{Raviv Shay\}, Dorith and Morad Khayat and Michal Werbner and Inbar Levi and Yishay Shoval and Galit Tal and Stavit Shalev and Eli Reuveni and Emily Avitan-Hersh and Eugene Vlodavsky and Liat Appl-Sarid and Dorit Goldsher and Reuven Bergman and Zvi Segal and Ora Bitterman-Deutsch and Orly Avni",

note = "Publisher Copyright: {\textcopyright} 2017 The Authors. Published under the terms of the CC BY 4.0 license",

year = "2017",

month = mar,

day = "1",

doi = "10.15252/emmm.201606523",

language = "الإنجليزيّة",

volume = "9",

pages = "319--336",

journal = "EMBO Molecular Medicine",

issn = "1757-4676",

publisher = "Springer Science and Business Media Deutschland GmbH",

number = "3",

}

Falik-Zaccai, TC, Barsheshet, Y, Mandel, H, Segev, M, Lorber, A, Gelberg, S, Kalfon, L, Ben Haroush, S, Shalata, A, Gelernter-Yaniv, L, Chaim, S, Raviv Shay, D, Khayat, M, Werbner, M, Levi, I, Shoval, Y, Tal, G, Shalev, S, Reuveni, E, Avitan-Hersh, E, Vlodavsky, E, Appl-Sarid, L, Goldsher, D, Bergman, R, Segal, Z, Bitterman-Deutsch, O & Avni, O 2017, 'Sequence variation in PPP1R13L results in a novel form of cardio-cutaneous syndrome', EMBO Molecular Medicine, vol. 9, no. 3, pp. 319-336. https://doi.org/10.15252/emmm.201606523

TY - JOUR

T1 - Sequence variation in PPP1R13L results in a novel form of cardio-cutaneous syndrome

AU - Falik-Zaccai, Tzipora C.

AU - Barsheshet, Yiftah

AU - Mandel, Hanna

AU - Segev, Meital

AU - Lorber, Avraham

AU - Gelberg, Shachaf

AU - Kalfon, Limor

AU - Ben Haroush, Shani

AU - Shalata, Adel

AU - Gelernter-Yaniv, Liat

AU - Chaim, Sarah

AU - Raviv Shay, Dorith

AU - Khayat, Morad

AU - Werbner, Michal

AU - Levi, Inbar

AU - Shoval, Yishay

AU - Tal, Galit

AU - Shalev, Stavit

AU - Reuveni, Eli

AU - Avitan-Hersh, Emily

AU - Vlodavsky, Eugene

AU - Appl-Sarid, Liat

AU - Goldsher, Dorit

AU - Bergman, Reuven

AU - Segal, Zvi

AU - Bitterman-Deutsch, Ora

AU - Avni, Orly

PY - 2017/3/1

Y1 - 2017/3/1

N2 - Dilated cardiomyopathy (DCM) is a life-threatening disorder whose genetic basis is heterogeneous and mostly unknown. Five Arab Christian infants, aged 4–30 months from four families, were diagnosed with DCM associated with mild skin, teeth, and hair abnormalities. All passed away before age 3. A homozygous sequence variation creating a premature stop codon at PPP1R13L encoding the iASPP protein was identified in three infants and in the mother of the other two. Patients’ fibroblasts and PPP1R13L-knocked down human fibroblasts presented higher expression levels of pro-inflammatory cytokine genes in response to lipopolysaccharide, as well as Ppp1r13l-knocked down murine cardiomyocytes and hearts of Ppp1r13l-deficient mice. The hypersensitivity to lipopolysaccharide was NF-κB-dependent, and its inducible binding activity to promoters of pro-inflammatory cytokine genes was elevated in patients’ fibroblasts. RNA sequencing of Ppp1r13l-knocked down murine cardiomyocytes and of hearts derived from different stages of DCM development in Ppp1r13l-deficient mice revealed the crucial role of iASPP in dampening cardiac inflammatory response. Our results determined PPP1R13L as the gene underlying a novel autosomal-recessive cardio-cutaneous syndrome in humans and strongly suggest that the fatal DCM during infancy is a consequence of failure to regulate transcriptional pathways necessary for tuning cardiac threshold response to common inflammatory stressors.

AB - Dilated cardiomyopathy (DCM) is a life-threatening disorder whose genetic basis is heterogeneous and mostly unknown. Five Arab Christian infants, aged 4–30 months from four families, were diagnosed with DCM associated with mild skin, teeth, and hair abnormalities. All passed away before age 3. A homozygous sequence variation creating a premature stop codon at PPP1R13L encoding the iASPP protein was identified in three infants and in the mother of the other two. Patients’ fibroblasts and PPP1R13L-knocked down human fibroblasts presented higher expression levels of pro-inflammatory cytokine genes in response to lipopolysaccharide, as well as Ppp1r13l-knocked down murine cardiomyocytes and hearts of Ppp1r13l-deficient mice. The hypersensitivity to lipopolysaccharide was NF-κB-dependent, and its inducible binding activity to promoters of pro-inflammatory cytokine genes was elevated in patients’ fibroblasts. RNA sequencing of Ppp1r13l-knocked down murine cardiomyocytes and of hearts derived from different stages of DCM development in Ppp1r13l-deficient mice revealed the crucial role of iASPP in dampening cardiac inflammatory response. Our results determined PPP1R13L as the gene underlying a novel autosomal-recessive cardio-cutaneous syndrome in humans and strongly suggest that the fatal DCM during infancy is a consequence of failure to regulate transcriptional pathways necessary for tuning cardiac threshold response to common inflammatory stressors.

KW - PPP1R13L

KW - dilated cardiomyopathy

KW - genetics

KW - inflammation

KW - myocarditis

UR - http://www.scopus.com/inward/record.url?scp=85010515216&partnerID=8YFLogxK

U2 - 10.15252/emmm.201606523

DO - 10.15252/emmm.201606523

M3 - مقالة

C2 - 28069640

SN - 1757-4676

VL - 9

SP - 319

EP - 336

JO - EMBO Molecular Medicine

JF - EMBO Molecular Medicine

IS - 3

ER -

Sequence variation in PPP1R13L results in a novel form of cardio-cutaneous syndrome

Abstract

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Keywords

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