Biallelic variants in POPDC2 cause a novel autosomal recessive syndrome presenting with cardiac conduction defects and variable hypertrophic cardiomyopathy

Michele Nicastro; Alexa M C Vermeer; Pieter G Postema; Rafik Tadros; Forrest Z Bowling; Hildur M Aegisdottir; Vinicius Tragante; Lukas Mach; Alex V Postma; Elisabeth M Lodder; Karel van Duijvenboden; Rob Zwart; Leander Beekman; Lingshuang Wu; Paul A van der Zwaag; Mariëlle Alders; Mona Allouba; Yasmine Aguib; J Luis Santomel; David de Una; Lorenzo Monserrat; Antonio M A Miranda; Kazumasa Kanemaru; James Cranley; Ingeborg E van Zeggeren; Eleonora M A Aronica; Michela Ripolone; Simona Zanotti; Gardar Sveinbjornsson; Erna V Ivarsdottir; Hilma Hólm; Daníel F Guðbjartsson; Ástrós Th Skúladóttir; Kári Stefánsson; Lincoln Nadauld; Kirk U Knowlton; Sisse Rye Ostrowski; Erik Sørensen; Ole Birger Vesterager Pedersen; Jonas Ghouse; Søren Rand; Henning Bundgaard; Henrik Ullum; Christian Erikstrup; Bitten Aagaard; Mie Topholm Bruun; Mette Christiansen; Henrik K Jensen; Deanna Alexis Carere; Christopher T Cummings; Kristen Fishler; Pernille Mathiesen Tøring; Klaus Brusgaard; Trine Maxel Juul; Lotte Saaby; Bo Gregers Winkel; Jens Mogensen; Francesco Fortunato; Giacomo Pietro Comi; Dario Ronchi; J Peter van Tintelen; Michela Noseda; Michael V Airola; Imke Christiaans; Arthur A M Wilde; Ronald Wilders; Sally-Ann Clur; Arie O Verkerk; Connie R Bezzina; Najim Lahrouchi

doi:10.1101/2024.07.04.24309755

Biallelic variants in POPDC2 cause a novel autosomal recessive syndrome presenting with cardiac conduction defects and variable hypertrophic cardiomyopathy

Michele Nicastro
, Alexa M C Vermeer
, Pieter G Postema
, Rafik Tadros
, Forrest Z Bowling
, Hildur M Aegisdottir
, Vinicius Tragante
, Lukas Mach
, Alex V Postma
, Elisabeth M Lodder
, Karel van Duijvenboden
, Rob Zwart
, Leander Beekman
, Lingshuang Wu
, Paul A van der Zwaag
, Mariëlle Alders
, Mona Allouba
, Yasmine Aguib
, J Luis Santomel
, David de Una

Lorenzo Monserrat, Antonio M A Miranda, Kazumasa Kanemaru, James Cranley, Ingeborg E van Zeggeren, Eleonora M A Aronica, Michela Ripolone, Simona Zanotti, Gardar Sveinbjornsson, Erna V Ivarsdottir, Hilma Hólm, Daníel F Guðbjartsson, Ástrós Th Skúladóttir, Kári Stefánsson, Lincoln Nadauld, Kirk U Knowlton, Sisse Rye Ostrowski, Erik Sørensen, Ole Birger Vesterager Pedersen, Jonas Ghouse, Søren Rand, Henning Bundgaard, Henrik Ullum, Christian Erikstrup, Bitten Aagaard, Mie Topholm Bruun, Mette Christiansen, Henrik K Jensen, Deanna Alexis Carere, Christopher T Cummings, Kristen Fishler, Pernille Mathiesen Tøring, Klaus Brusgaard, Trine Maxel Juul, Lotte Saaby, Bo Gregers Winkel, Jens Mogensen, Francesco Fortunato, Giacomo Pietro Comi, Dario Ronchi, J Peter van Tintelen, Michela Noseda, Michael V Airola, Imke Christiaans, Arthur A M Wilde, Ronald Wilders, Sally-Ann Clur, Arie O Verkerk, Connie R Bezzina, Najim Lahrouchi

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Abstract

POPDC2 encodes for the Popeye domain-containing protein 2 which has an important role in cardiac pacemaking and conduction, due in part to its cAMP-dependent binding and regulation of TREK-1 potassium channels. Loss of Popdc2 in mice results in sinus pauses and bradycardia and morpholino knockdown of popdc2 in zebrafish results in atrioventricular (AV) block. We identified bi-allelic variants in POPDC2 in 4 families that presented with a phenotypic spectrum consisting of sinus node dysfunction, AV conduction defects and hypertrophic cardiomyopathy. Using homology modelling we show that the identified POPDC2 variants are predicted to diminish the ability of POPDC2 to bind cAMP. In in vitro electrophysiological studies we demonstrated that, while co-expression of wild-type POPDC2 with TREK-1 increased TREK-1 current density, POPDC2 variants found in the patients failed to increase TREK-1 current density. While patient muscle biopsy did not show clear myopathic disease, it showed significant reduction of the expression of both POPDC1 and POPDC2, suggesting that stability and/or membrane trafficking of the POPDC1-POPDC2 complex is impaired by pathogenic variants in any of the two proteins. Single-cell RNA sequencing from human hearts demonstrated that co-expression of POPDC1 and 2 was most prevalent in AV node, AV node pacemaker and AV bundle cells. Sinoatrial node cells expressed POPDC2 abundantly, but expression of POPDC1 was sparse. Together, these results concur with predisposition to AV node disease in humans with loss-of-function variants in POPDC1 and POPDC2 and presence of sinus node disease in POPDC2, but not in POPDC1 related disease in human. Using population-level genetic data of more than 1 million individuals we showed that none of the familial variants were associated with clinical outcomes in heterozygous state, suggesting that heterozygous family members are unlikely to develop clinical manifestations and therefore might not necessitate clinical follow-up. Our findings provide evidence for POPDC2 as the cause of a novel Mendelian autosomal recessive cardiac syndrome, consistent with previous work showing that mice and zebrafish deficient in functional POPDC2 display sinus and AV node dysfunction. GRAPHICAL ABSTRACT O_FIG O_LINKSMALLFIG WIDTH=200 HEIGHT=136 SRC="FIGDIR/small/24309755v1_ufig1.gif" ALT="Figure 1"> View larger version (29K): [email protected]@1a89147org.highwire.dtl.DTLVardef@1d9d145org.highwire.dtl.DTLVardef@13a1645_HPS_FORMAT_FIGEXP M_FIG C_FIG

Original language	English
Journal	medRxiv
DOIs	https://doi.org/10.1101/2024.07.04.24309755
Publication status	Published - 5 Jul 2024

Keywords

genetic and genomic medicine

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10.1101/2024.07.04.24309755

Biallelic-variants-in-popdc2-cause-a-novel-autosomal-recessive-syndrome-presenting-with-cardiac-conduction-defects-and-v.pdfFinal published version, 6.63 MBLicence: Taverne

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Nicastro, M., Vermeer, A. M. C., Postema, P. G., Tadros, R., Bowling, F. Z., Aegisdottir, H. M., Tragante, V., Mach, L., Postma, A. V., Lodder, E. M., van Duijvenboden, K., Zwart, R., Beekman, L., Wu, L., van der Zwaag, P. A., Alders, M., Allouba, M., Aguib, Y., Santomel, J. L., ... Lahrouchi, N. (2024). Biallelic variants in POPDC2 cause a novel autosomal recessive syndrome presenting with cardiac conduction defects and variable hypertrophic cardiomyopathy. medRxiv. https://doi.org/10.1101/2024.07.04.24309755

@article{4e0a93bb68444026814fa54ddc74429d,

title = "Biallelic variants in POPDC2 cause a novel autosomal recessive syndrome presenting with cardiac conduction defects and variable hypertrophic cardiomyopathy",

abstract = "POPDC2 encodes for the Popeye domain-containing protein 2 which has an important role in cardiac pacemaking and conduction, due in part to its cAMP-dependent binding and regulation of TREK-1 potassium channels. Loss of Popdc2 in mice results in sinus pauses and bradycardia and morpholino knockdown of popdc2 in zebrafish results in atrioventricular (AV) block. We identified bi-allelic variants in POPDC2 in 4 families that presented with a phenotypic spectrum consisting of sinus node dysfunction, AV conduction defects and hypertrophic cardiomyopathy. Using homology modelling we show that the identified POPDC2 variants are predicted to diminish the ability of POPDC2 to bind cAMP. In in vitro electrophysiological studies we demonstrated that, while co-expression of wild-type POPDC2 with TREK-1 increased TREK-1 current density, POPDC2 variants found in the patients failed to increase TREK-1 current density. While patient muscle biopsy did not show clear myopathic disease, it showed significant reduction of the expression of both POPDC1 and POPDC2, suggesting that stability and/or membrane trafficking of the POPDC1-POPDC2 complex is impaired by pathogenic variants in any of the two proteins. Single-cell RNA sequencing from human hearts demonstrated that co-expression of POPDC1 and 2 was most prevalent in AV node, AV node pacemaker and AV bundle cells. Sinoatrial node cells expressed POPDC2 abundantly, but expression of POPDC1 was sparse. Together, these results concur with predisposition to AV node disease in humans with loss-of-function variants in POPDC1 and POPDC2 and presence of sinus node disease in POPDC2, but not in POPDC1 related disease in human. Using population-level genetic data of more than 1 million individuals we showed that none of the familial variants were associated with clinical outcomes in heterozygous state, suggesting that heterozygous family members are unlikely to develop clinical manifestations and therefore might not necessitate clinical follow-up. Our findings provide evidence for POPDC2 as the cause of a novel Mendelian autosomal recessive cardiac syndrome, consistent with previous work showing that mice and zebrafish deficient in functional POPDC2 display sinus and AV node dysfunction. GRAPHICAL ABSTRACT O\_FIG O\_LINKSMALLFIG WIDTH=200 HEIGHT=136 SRC={"}FIGDIR/small/24309755v1\_ufig1.gif{"} ALT={"}Figure 1{"}> View larger version (29K): [email protected]@1a89147org.highwire.dtl.DTLVardef@1d9d145org.highwire.dtl.DTLVardef@13a1645\_HPS\_FORMAT\_FIGEXP M\_FIG C\_FIG",

keywords = "genetic and genomic medicine",

author = "Michele Nicastro and Vermeer, \{Alexa M C\} and Postema, \{Pieter G\} and Rafik Tadros and Bowling, \{Forrest Z\} and Aegisdottir, \{Hildur M\} and Vinicius Tragante and Lukas Mach and Postma, \{Alex V\} and Lodder, \{Elisabeth M\} and \{van Duijvenboden\}, Karel and Rob Zwart and Leander Beekman and Lingshuang Wu and \{van der Zwaag\}, \{Paul A\} and Mari{\"e}lle Alders and Mona Allouba and Yasmine Aguib and Santomel, \{J Luis\} and \{de Una\}, David and Lorenzo Monserrat and Miranda, \{Antonio M A\} and Kazumasa Kanemaru and James Cranley and \{van Zeggeren\}, \{Ingeborg E\} and Aronica, \{Eleonora M A\} and Michela Ripolone and Simona Zanotti and Gardar Sveinbjornsson and Ivarsdottir, \{Erna V\} and Hilma H{\'o}lm and Gu{\dh}bjartsson, \{Dan{\'i}el F\} and Sk{\'u}lad{\'o}ttir, \{{\'A}str{\'o}s Th\} and K{\'a}ri Stef{\'a}nsson and Lincoln Nadauld and Knowlton, \{Kirk U\} and Ostrowski, \{Sisse Rye\} and Erik S{\o}rensen and \{Vesterager Pedersen\}, \{Ole Birger\} and Jonas Ghouse and S{\o}ren Rand and Henning Bundgaard and Henrik Ullum and Christian Erikstrup and Bitten Aagaard and Bruun, \{Mie Topholm\} and Mette Christiansen and Jensen, \{Henrik K\} and Carere, \{Deanna Alexis\} and Cummings, \{Christopher T\} and Kristen Fishler and T{\o}ring, \{Pernille Mathiesen\} and Klaus Brusgaard and Juul, \{Trine Maxel\} and Lotte Saaby and Winkel, \{Bo Gregers\} and Jens Mogensen and Francesco Fortunato and Comi, \{Giacomo Pietro\} and Dario Ronchi and \{van Tintelen\}, \{J Peter\} and Michela Noseda and Airola, \{Michael V\} and Imke Christiaans and Wilde, \{Arthur A M\} and Ronald Wilders and Sally-Ann Clur and Verkerk, \{Arie O\} and Bezzina, \{Connie R\} and Najim Lahrouchi",

year = "2024",

month = jul,

day = "5",

doi = "10.1101/2024.07.04.24309755",

language = "English",

journal = "medRxiv",

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Nicastro, M , Vermeer, AMC , Postema, PG, Tadros, R, Bowling, FZ, Aegisdottir, HM, Tragante, V, Mach, L, Postma, AV , Lodder, EM , van Duijvenboden, K , Zwart, R , Beekman, L, Wu, L, van der Zwaag, PA, Alders, M, Allouba, M, Aguib, Y, Santomel, JL, de Una, D, Monserrat, L, Miranda, AMA, Kanemaru, K, Cranley, J, van Zeggeren, IE , Aronica, EMA, Ripolone, M, Zanotti, S, Sveinbjornsson, G, Ivarsdottir, EV, Hólm, H, Guðbjartsson, DF, Skúladóttir, ÁT, Stefánsson, K, Nadauld, L, Knowlton, KU, Ostrowski, SR, Sørensen, E, Vesterager Pedersen, OB, Ghouse, J, Rand, S, Bundgaard, H, Ullum, H, Erikstrup, C, Aagaard, B, Bruun, MT, Christiansen, M, Jensen, HK, Carere, DA, Cummings, CT, Fishler, K, Tøring, PM, Brusgaard, K, Juul, TM, Saaby, L, Winkel, BG, Mogensen, J, Fortunato, F, Comi, GP, Ronchi, D, van Tintelen, JP, Noseda, M, Airola, MV, Christiaans, I, Wilde, AAM , Wilders, R , Clur, S-A , Verkerk, AO , Bezzina, CR & Lahrouchi, N 2024, 'Biallelic variants in POPDC2 cause a novel autosomal recessive syndrome presenting with cardiac conduction defects and variable hypertrophic cardiomyopathy', medRxiv. https://doi.org/10.1101/2024.07.04.24309755

TY - JOUR

T1 - Biallelic variants in POPDC2 cause a novel autosomal recessive syndrome presenting with cardiac conduction defects and variable hypertrophic cardiomyopathy

AU - Nicastro, Michele

AU - Vermeer, Alexa M C

AU - Postema, Pieter G

AU - Tadros, Rafik

AU - Bowling, Forrest Z

AU - Aegisdottir, Hildur M

AU - Tragante, Vinicius

AU - Mach, Lukas

AU - Postma, Alex V

AU - Lodder, Elisabeth M

AU - van Duijvenboden, Karel

AU - Zwart, Rob

AU - Beekman, Leander

AU - Wu, Lingshuang

AU - van der Zwaag, Paul A

AU - Alders, Mariëlle

AU - Allouba, Mona

AU - Aguib, Yasmine

AU - Santomel, J Luis

AU - de Una, David

AU - Monserrat, Lorenzo

AU - Miranda, Antonio M A

AU - Kanemaru, Kazumasa

AU - Cranley, James

AU - van Zeggeren, Ingeborg E

AU - Aronica, Eleonora M A

AU - Ripolone, Michela

AU - Zanotti, Simona

AU - Sveinbjornsson, Gardar

AU - Ivarsdottir, Erna V

AU - Hólm, Hilma

AU - Guðbjartsson, Daníel F

AU - Skúladóttir, Ástrós Th

AU - Stefánsson, Kári

AU - Nadauld, Lincoln

AU - Knowlton, Kirk U

AU - Ostrowski, Sisse Rye

AU - Sørensen, Erik

AU - Vesterager Pedersen, Ole Birger

AU - Ghouse, Jonas

AU - Rand, Søren

AU - Bundgaard, Henning

AU - Ullum, Henrik

AU - Erikstrup, Christian

AU - Aagaard, Bitten

AU - Bruun, Mie Topholm

AU - Christiansen, Mette

AU - Jensen, Henrik K

AU - Carere, Deanna Alexis

AU - Cummings, Christopher T

AU - Fishler, Kristen

AU - Tøring, Pernille Mathiesen

AU - Brusgaard, Klaus

AU - Juul, Trine Maxel

AU - Saaby, Lotte

AU - Winkel, Bo Gregers

AU - Mogensen, Jens

AU - Fortunato, Francesco

AU - Comi, Giacomo Pietro

AU - Ronchi, Dario

AU - van Tintelen, J Peter

AU - Noseda, Michela

AU - Airola, Michael V

AU - Christiaans, Imke

AU - Wilde, Arthur A M

AU - Wilders, Ronald

AU - Clur, Sally-Ann

AU - Verkerk, Arie O

AU - Bezzina, Connie R

AU - Lahrouchi, Najim

PY - 2024/7/5

Y1 - 2024/7/5

N2 - POPDC2 encodes for the Popeye domain-containing protein 2 which has an important role in cardiac pacemaking and conduction, due in part to its cAMP-dependent binding and regulation of TREK-1 potassium channels. Loss of Popdc2 in mice results in sinus pauses and bradycardia and morpholino knockdown of popdc2 in zebrafish results in atrioventricular (AV) block. We identified bi-allelic variants in POPDC2 in 4 families that presented with a phenotypic spectrum consisting of sinus node dysfunction, AV conduction defects and hypertrophic cardiomyopathy. Using homology modelling we show that the identified POPDC2 variants are predicted to diminish the ability of POPDC2 to bind cAMP. In in vitro electrophysiological studies we demonstrated that, while co-expression of wild-type POPDC2 with TREK-1 increased TREK-1 current density, POPDC2 variants found in the patients failed to increase TREK-1 current density. While patient muscle biopsy did not show clear myopathic disease, it showed significant reduction of the expression of both POPDC1 and POPDC2, suggesting that stability and/or membrane trafficking of the POPDC1-POPDC2 complex is impaired by pathogenic variants in any of the two proteins. Single-cell RNA sequencing from human hearts demonstrated that co-expression of POPDC1 and 2 was most prevalent in AV node, AV node pacemaker and AV bundle cells. Sinoatrial node cells expressed POPDC2 abundantly, but expression of POPDC1 was sparse. Together, these results concur with predisposition to AV node disease in humans with loss-of-function variants in POPDC1 and POPDC2 and presence of sinus node disease in POPDC2, but not in POPDC1 related disease in human. Using population-level genetic data of more than 1 million individuals we showed that none of the familial variants were associated with clinical outcomes in heterozygous state, suggesting that heterozygous family members are unlikely to develop clinical manifestations and therefore might not necessitate clinical follow-up. Our findings provide evidence for POPDC2 as the cause of a novel Mendelian autosomal recessive cardiac syndrome, consistent with previous work showing that mice and zebrafish deficient in functional POPDC2 display sinus and AV node dysfunction. GRAPHICAL ABSTRACT O_FIG O_LINKSMALLFIG WIDTH=200 HEIGHT=136 SRC="FIGDIR/small/24309755v1_ufig1.gif" ALT="Figure 1"> View larger version (29K): [email protected]@1a89147org.highwire.dtl.DTLVardef@1d9d145org.highwire.dtl.DTLVardef@13a1645_HPS_FORMAT_FIGEXP M_FIG C_FIG

AB - POPDC2 encodes for the Popeye domain-containing protein 2 which has an important role in cardiac pacemaking and conduction, due in part to its cAMP-dependent binding and regulation of TREK-1 potassium channels. Loss of Popdc2 in mice results in sinus pauses and bradycardia and morpholino knockdown of popdc2 in zebrafish results in atrioventricular (AV) block. We identified bi-allelic variants in POPDC2 in 4 families that presented with a phenotypic spectrum consisting of sinus node dysfunction, AV conduction defects and hypertrophic cardiomyopathy. Using homology modelling we show that the identified POPDC2 variants are predicted to diminish the ability of POPDC2 to bind cAMP. In in vitro electrophysiological studies we demonstrated that, while co-expression of wild-type POPDC2 with TREK-1 increased TREK-1 current density, POPDC2 variants found in the patients failed to increase TREK-1 current density. While patient muscle biopsy did not show clear myopathic disease, it showed significant reduction of the expression of both POPDC1 and POPDC2, suggesting that stability and/or membrane trafficking of the POPDC1-POPDC2 complex is impaired by pathogenic variants in any of the two proteins. Single-cell RNA sequencing from human hearts demonstrated that co-expression of POPDC1 and 2 was most prevalent in AV node, AV node pacemaker and AV bundle cells. Sinoatrial node cells expressed POPDC2 abundantly, but expression of POPDC1 was sparse. Together, these results concur with predisposition to AV node disease in humans with loss-of-function variants in POPDC1 and POPDC2 and presence of sinus node disease in POPDC2, but not in POPDC1 related disease in human. Using population-level genetic data of more than 1 million individuals we showed that none of the familial variants were associated with clinical outcomes in heterozygous state, suggesting that heterozygous family members are unlikely to develop clinical manifestations and therefore might not necessitate clinical follow-up. Our findings provide evidence for POPDC2 as the cause of a novel Mendelian autosomal recessive cardiac syndrome, consistent with previous work showing that mice and zebrafish deficient in functional POPDC2 display sinus and AV node dysfunction. GRAPHICAL ABSTRACT O_FIG O_LINKSMALLFIG WIDTH=200 HEIGHT=136 SRC="FIGDIR/small/24309755v1_ufig1.gif" ALT="Figure 1"> View larger version (29K): [email protected]@1a89147org.highwire.dtl.DTLVardef@1d9d145org.highwire.dtl.DTLVardef@13a1645_HPS_FORMAT_FIGEXP M_FIG C_FIG

KW - genetic and genomic medicine

U2 - 10.1101/2024.07.04.24309755

DO - 10.1101/2024.07.04.24309755

M3 - Article

C2 - 39006410

JO - medRxiv

JF - medRxiv

ER -

Biallelic variants in POPDC2 cause a novel autosomal recessive syndrome presenting with cardiac conduction defects and variable hypertrophic cardiomyopathy

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