CNNM2 Mutations Cause Impaired Brain Development and Seizures in Patients with Hypomagnesemia

Intellectual disability and seizures are frequently associated with hypomagnesemia and have an important genetic component. However, to find the genetic origin of intellectual disability and seizures often remains challenging because of considerable genetic heterogeneity and clinical variability. In...

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Autores principales: Arjona, Francisco J., de Baaij, Jeroen H. F., Schlingmann, Karl P., Lameris, Anke L. L., van Wijk, Erwin, Flik, Gert, Regele, Sabrina, Korenke, G. Christoph, Neophytou, Birgit, Rust, Stephan, Reintjes, Nadine, Konrad, Martin, Bindels, René J. M., Hoenderop, Joost G. J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3974678/
https://www.ncbi.nlm.nih.gov/pubmed/24699222
http://dx.doi.org/10.1371/journal.pgen.1004267
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author Arjona, Francisco J.
de Baaij, Jeroen H. F.
Schlingmann, Karl P.
Lameris, Anke L. L.
van Wijk, Erwin
Flik, Gert
Regele, Sabrina
Korenke, G. Christoph
Neophytou, Birgit
Rust, Stephan
Reintjes, Nadine
Konrad, Martin
Bindels, René J. M.
Hoenderop, Joost G. J.
author_facet Arjona, Francisco J.
de Baaij, Jeroen H. F.
Schlingmann, Karl P.
Lameris, Anke L. L.
van Wijk, Erwin
Flik, Gert
Regele, Sabrina
Korenke, G. Christoph
Neophytou, Birgit
Rust, Stephan
Reintjes, Nadine
Konrad, Martin
Bindels, René J. M.
Hoenderop, Joost G. J.
author_sort Arjona, Francisco J.
collection PubMed
description Intellectual disability and seizures are frequently associated with hypomagnesemia and have an important genetic component. However, to find the genetic origin of intellectual disability and seizures often remains challenging because of considerable genetic heterogeneity and clinical variability. In this study, we have identified new mutations in CNNM2 in five families suffering from mental retardation, seizures, and hypomagnesemia. For the first time, a recessive mode of inheritance of CNNM2 mutations was observed. Importantly, patients with recessive CNNM2 mutations suffer from brain malformations and severe intellectual disability. Additionally, three patients with moderate mental disability were shown to carry de novo heterozygous missense mutations in the CNNM2 gene. To elucidate the physiological role of CNNM2 and explain the pathomechanisms of disease, we studied CNNM2 function combining in vitro activity assays and the zebrafish knockdown model system. Using stable Mg(2+) isotopes, we demonstrated that CNNM2 increases cellular Mg(2+) uptake in HEK293 cells and that this process occurs through regulation of the Mg(2+)-permeable cation channel TRPM7. In contrast, cells expressing mutated CNNM2 proteins did not show increased Mg(2+) uptake. Knockdown of cnnm2 isoforms in zebrafish resulted in disturbed brain development including neurodevelopmental impairments such as increased embryonic spontaneous contractions and weak touch-evoked escape behaviour, and reduced body Mg content, indicative of impaired renal Mg(2+) absorption. These phenotypes were rescued by injection of mammalian wild-type Cnnm2 cRNA, whereas mammalian mutant Cnnm2 cRNA did not improve the zebrafish knockdown phenotypes. We therefore concluded that CNNM2 is fundamental for brain development, neurological functioning and Mg(2+) homeostasis. By establishing the loss-of-function zebrafish model for CNNM2 genetic disease, we provide a unique system for testing therapeutic drugs targeting CNNM2 and for monitoring their effects on the brain and kidney phenotype.
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spelling pubmed-39746782014-04-08 CNNM2 Mutations Cause Impaired Brain Development and Seizures in Patients with Hypomagnesemia Arjona, Francisco J. de Baaij, Jeroen H. F. Schlingmann, Karl P. Lameris, Anke L. L. van Wijk, Erwin Flik, Gert Regele, Sabrina Korenke, G. Christoph Neophytou, Birgit Rust, Stephan Reintjes, Nadine Konrad, Martin Bindels, René J. M. Hoenderop, Joost G. J. PLoS Genet Research Article Intellectual disability and seizures are frequently associated with hypomagnesemia and have an important genetic component. However, to find the genetic origin of intellectual disability and seizures often remains challenging because of considerable genetic heterogeneity and clinical variability. In this study, we have identified new mutations in CNNM2 in five families suffering from mental retardation, seizures, and hypomagnesemia. For the first time, a recessive mode of inheritance of CNNM2 mutations was observed. Importantly, patients with recessive CNNM2 mutations suffer from brain malformations and severe intellectual disability. Additionally, three patients with moderate mental disability were shown to carry de novo heterozygous missense mutations in the CNNM2 gene. To elucidate the physiological role of CNNM2 and explain the pathomechanisms of disease, we studied CNNM2 function combining in vitro activity assays and the zebrafish knockdown model system. Using stable Mg(2+) isotopes, we demonstrated that CNNM2 increases cellular Mg(2+) uptake in HEK293 cells and that this process occurs through regulation of the Mg(2+)-permeable cation channel TRPM7. In contrast, cells expressing mutated CNNM2 proteins did not show increased Mg(2+) uptake. Knockdown of cnnm2 isoforms in zebrafish resulted in disturbed brain development including neurodevelopmental impairments such as increased embryonic spontaneous contractions and weak touch-evoked escape behaviour, and reduced body Mg content, indicative of impaired renal Mg(2+) absorption. These phenotypes were rescued by injection of mammalian wild-type Cnnm2 cRNA, whereas mammalian mutant Cnnm2 cRNA did not improve the zebrafish knockdown phenotypes. We therefore concluded that CNNM2 is fundamental for brain development, neurological functioning and Mg(2+) homeostasis. By establishing the loss-of-function zebrafish model for CNNM2 genetic disease, we provide a unique system for testing therapeutic drugs targeting CNNM2 and for monitoring their effects on the brain and kidney phenotype. Public Library of Science 2014-04-03 /pmc/articles/PMC3974678/ /pubmed/24699222 http://dx.doi.org/10.1371/journal.pgen.1004267 Text en © 2014 Arjona et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Arjona, Francisco J.
de Baaij, Jeroen H. F.
Schlingmann, Karl P.
Lameris, Anke L. L.
van Wijk, Erwin
Flik, Gert
Regele, Sabrina
Korenke, G. Christoph
Neophytou, Birgit
Rust, Stephan
Reintjes, Nadine
Konrad, Martin
Bindels, René J. M.
Hoenderop, Joost G. J.
CNNM2 Mutations Cause Impaired Brain Development and Seizures in Patients with Hypomagnesemia
title CNNM2 Mutations Cause Impaired Brain Development and Seizures in Patients with Hypomagnesemia
title_full CNNM2 Mutations Cause Impaired Brain Development and Seizures in Patients with Hypomagnesemia
title_fullStr CNNM2 Mutations Cause Impaired Brain Development and Seizures in Patients with Hypomagnesemia
title_full_unstemmed CNNM2 Mutations Cause Impaired Brain Development and Seizures in Patients with Hypomagnesemia
title_short CNNM2 Mutations Cause Impaired Brain Development and Seizures in Patients with Hypomagnesemia
title_sort cnnm2 mutations cause impaired brain development and seizures in patients with hypomagnesemia
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3974678/
https://www.ncbi.nlm.nih.gov/pubmed/24699222
http://dx.doi.org/10.1371/journal.pgen.1004267
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