TY - JOUR
T1 - Germline and Mosaic Variants in PRKACA and PRKACB Cause a Multiple Congenital Malformation Syndrome
AU - Palencia-Campos, Adrian
AU - Aoto, Phillip C.
AU - Machal, Erik M.F.
AU - Rivera-Barahona, Ana
AU - Soto-Bielicka, Patricia
AU - Bertinetti, Daniela
AU - Baker, Blaine
AU - Vu, Lily
AU - Piceci-Sparascio, Francesca
AU - Torrente, Isabella
AU - Boudin, Eveline
AU - Peeters, Silke
AU - Van Hul, Wim
AU - Huber, Celine
AU - Bonneau, Dominique
AU - Hildebrand, Michael S.
AU - Coleman, Matthew
AU - Bahlo, Melanie
AU - Bennett, Mark F.
AU - Schneider, Amy L.
AU - Scheffer, Ingrid E.
AU - Kibæk, Maria
AU - Kristiansen, Britta S.
AU - Issa, Mahmoud Y.
AU - Mehrez, Mennat I.
AU - Ismail, Samira
AU - Tenorio, Jair
AU - Li, Gaoyang
AU - Skålhegg, Bjørn Steen
AU - Otaify, Ghada A.
AU - Temtamy, Samia
AU - Aglan, Mona
AU - Jønch, Aia E.
AU - De Luca, Alessandro
AU - Mortier, Geert
AU - Cormier-Daire, Valérie
AU - Ziegler, Alban
AU - Wallis, Mathew
AU - Lapunzina, Pablo
AU - Herberg, Friedrich W.
AU - Taylor, Susan S.
AU - Ruiz-Perez, Victor L.
N1 - Funding Information:
We thank all affected individuals, their siblings, and their parents or legal guardians for their participation in this study. Some individuals were included after a GeneMatcher match. 40 This work was partially supported by funding from the Spanish Ministry of Science, Innovation and Universities ( SAF2016 - 75434 - R [AEI/FEDER, UE] and PID2019-105620RB-I00/AEI/10.13039/501100011033 ) to V.L.R.-P. S.S.T. was supported by NIH grant R03TR002947 , E.M.F.M. by Kassel graduate school “Clocks” , and A.D.L. by the Italian Ministry of Health ( RC-2019 ). The University of Antwerp supported G.M. and W.V.H. with Methusalem funding ( FFB190208 ) and S.P. with a predoctoral grant. E.B. was supported by The Research Foundation Flanders with a postdoctoral grant ( 12A3814N ). The study was also funded by a National Health and Medical Research Council Program Grant ( 1091593 ) to I.E.S., a Practitioner Fellowship ( 1006110 ) to I.E.S., a Senior Research Fellowship ( 1102971 ) to M.B., and an R.D. Wright Career Development Fellowship ( 1063799 ) to M.S.H. B.S.S. and G.L. were supported by Throne Holst Foundation UiO (2019-2021) and Strategic PhD fund by UiO/IMB .
Funding Information:
We thank all affected individuals, their siblings, and their parents or legal guardians for their participation in this study. Some individuals were included after a GeneMatcher match.40 This work was partially supported by funding from the Spanish Ministry of Science, Innovation and Universities (SAF2016-75434-R [AEI/FEDER, UE] and PID2019-105620RB-I00/AEI/10.13039/501100011033) to V.L.R.-P. S.S.T. was supported by NIH grant R03TR002947, E.M.F.M. by Kassel graduate school “Clocks”, and A.D.L. by the Italian Ministry of Health (RC-2019). The University of Antwerp supported G.M. and W.V.H. with Methusalem funding (FFB190208) and S.P. with a predoctoral grant. E.B. was supported by The Research Foundation Flanders with a postdoctoral grant (12A3814N). The study was also funded by a National Health and Medical Research Council Program Grant (1091593) to I.E.S. a Practitioner Fellowship (1006110) to I.E.S. a Senior Research Fellowship (1102971) to M.B. and an R.D. Wright Career Development Fellowship (1063799) to M.S.H. B.S.S. and G.L. were supported by Throne Holst Foundation UiO (2019-2021) and Strategic PhD fund by UiO/IMB.
Publisher Copyright:
© 2020 American Society of Human Genetics
PY - 2020/11/5
Y1 - 2020/11/5
N2 - PRKACA and PRKACB code for two catalytic subunits (Cα and Cβ) of cAMP-dependent protein kinase (PKA), a pleiotropic holoenzyme that regulates numerous fundamental biological processes such as metabolism, development, memory, and immune response. We report seven unrelated individuals presenting with a multiple congenital malformation syndrome in whom we identified heterozygous germline or mosaic missense variants in PRKACA or PRKACB. Three affected individuals were found with the same PRKACA variant, and the other four had different PRKACB mutations. In most cases, the mutations arose de novo, and two individuals had offspring with the same condition. Nearly all affected individuals and their affected offspring shared an atrioventricular septal defect or a common atrium along with postaxial polydactyly. Additional features included skeletal abnormalities and ectodermal defects of variable severity in five individuals, cognitive deficit in two individuals, and various unusual tumors in one individual. We investigated the structural and functional consequences of the variants identified in PRKACA and PRKACB through the use of several computational and experimental approaches, and we found that they lead to PKA holoenzymes which are more sensitive to activation by cAMP than are the wild-type proteins. Furthermore, expression of PRKACA or PRKACB variants detected in the affected individuals inhibited hedgehog signaling in NIH 3T3 fibroblasts, thereby providing an underlying mechanism for the developmental defects observed in these cases. Our findings highlight the importance of both Cα and Cβ subunits of PKA during human development.
AB - PRKACA and PRKACB code for two catalytic subunits (Cα and Cβ) of cAMP-dependent protein kinase (PKA), a pleiotropic holoenzyme that regulates numerous fundamental biological processes such as metabolism, development, memory, and immune response. We report seven unrelated individuals presenting with a multiple congenital malformation syndrome in whom we identified heterozygous germline or mosaic missense variants in PRKACA or PRKACB. Three affected individuals were found with the same PRKACA variant, and the other four had different PRKACB mutations. In most cases, the mutations arose de novo, and two individuals had offspring with the same condition. Nearly all affected individuals and their affected offspring shared an atrioventricular septal defect or a common atrium along with postaxial polydactyly. Additional features included skeletal abnormalities and ectodermal defects of variable severity in five individuals, cognitive deficit in two individuals, and various unusual tumors in one individual. We investigated the structural and functional consequences of the variants identified in PRKACA and PRKACB through the use of several computational and experimental approaches, and we found that they lead to PKA holoenzymes which are more sensitive to activation by cAMP than are the wild-type proteins. Furthermore, expression of PRKACA or PRKACB variants detected in the affected individuals inhibited hedgehog signaling in NIH 3T3 fibroblasts, thereby providing an underlying mechanism for the developmental defects observed in these cases. Our findings highlight the importance of both Cα and Cβ subunits of PKA during human development.
KW - Ellis-van Creveld syndrome
KW - GLI transcritpion factors
KW - PKA
KW - PRKACA
KW - PRKACB
KW - cAMP signaling
KW - congenital heart defects
KW - hedgehog signaling
KW - mosaicism
KW - postaxial polydactyly
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U2 - 10.1016/j.ajhg.2020.09.005
DO - 10.1016/j.ajhg.2020.09.005
M3 - Article
C2 - 33058759
AN - SCOPUS:85095455709
SN - 0002-9297
VL - 107
SP - 977
EP - 988
JO - American Journal of Human Genetics
JF - American Journal of Human Genetics
IS - 5
ER -