Calmodulin Methyltransferase Is Required for Growth, Muscle Strength, Somatosensory Development and Brain Function

Calmodulin lysine methyl transferase (CaM KMT) is ubiquitously expressed and highly conserved from plants to vertebrates. CaM is frequently trimethylated at Lys-115, however, the role of CaM methylation in vertebrates has not been studied. CaM KMT was found to be homozygously deleted in the 2P21 del...

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Autores principales: Haziza, Sitvanit, Magnani, Roberta, Lan, Dima, Keinan, Omer, Saada, Ann, Hershkovitz, Eli, Yanay, Nurit, Cohen, Yoram, Nevo, Yoram, Houtz, Robert L., Sheffield, Val C., Golan, Hava, Parvari, Ruti
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4527749/
https://www.ncbi.nlm.nih.gov/pubmed/26247364
http://dx.doi.org/10.1371/journal.pgen.1005388
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author Haziza, Sitvanit
Magnani, Roberta
Lan, Dima
Keinan, Omer
Saada, Ann
Hershkovitz, Eli
Yanay, Nurit
Cohen, Yoram
Nevo, Yoram
Houtz, Robert L.
Sheffield, Val C.
Golan, Hava
Parvari, Ruti
author_facet Haziza, Sitvanit
Magnani, Roberta
Lan, Dima
Keinan, Omer
Saada, Ann
Hershkovitz, Eli
Yanay, Nurit
Cohen, Yoram
Nevo, Yoram
Houtz, Robert L.
Sheffield, Val C.
Golan, Hava
Parvari, Ruti
author_sort Haziza, Sitvanit
collection PubMed
description Calmodulin lysine methyl transferase (CaM KMT) is ubiquitously expressed and highly conserved from plants to vertebrates. CaM is frequently trimethylated at Lys-115, however, the role of CaM methylation in vertebrates has not been studied. CaM KMT was found to be homozygously deleted in the 2P21 deletion syndrome that includes 4 genes. These patients present with cystinuria, severe intellectual disabilities, hypotonia, mitochondrial disease and facial dysmorphism. Two siblings with deletion of three of the genes included in the 2P21 deletion syndrome presented with cystinuria, hypotonia, a mild/moderate mental retardation and a respiratory chain complex IV deficiency. To be able to attribute the functional significance of the methylation of CaM in the mouse and the contribution of CaM KMT to the clinical presentation of the 2p21deletion patients, we produced a mouse model lacking only CaM KMT with deletion borders as in the human 2p21deletion syndrome. No compensatory activity for CaM methylation was found. Impairment of complexes I and IV, and less significantly III, of the mitochondrial respiratory chain was more pronounced in the brain than in muscle. CaM KMT is essential for normal body growth and somatosensory development, as well as for the proper functioning of the adult mouse brain. Developmental delay was demonstrated for somatosensory function and for complex behavior, which involved both basal motor function and motivation. The mutant mice also had deficits in motor learning, complex coordination and learning of aversive stimuli. The mouse model contributes to the evaluation of the role of methylated CaM. CaM methylation appears to have a role in growth, muscle strength, somatosensory development and brain function. The current study has clinical implications for human patients. Patients presenting slow growth and muscle weakness that could result from a mitochondrial impairment and mental retardation should be considered for sequence analysis of the CaM KMT gene.
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spelling pubmed-45277492015-08-12 Calmodulin Methyltransferase Is Required for Growth, Muscle Strength, Somatosensory Development and Brain Function Haziza, Sitvanit Magnani, Roberta Lan, Dima Keinan, Omer Saada, Ann Hershkovitz, Eli Yanay, Nurit Cohen, Yoram Nevo, Yoram Houtz, Robert L. Sheffield, Val C. Golan, Hava Parvari, Ruti PLoS Genet Research Article Calmodulin lysine methyl transferase (CaM KMT) is ubiquitously expressed and highly conserved from plants to vertebrates. CaM is frequently trimethylated at Lys-115, however, the role of CaM methylation in vertebrates has not been studied. CaM KMT was found to be homozygously deleted in the 2P21 deletion syndrome that includes 4 genes. These patients present with cystinuria, severe intellectual disabilities, hypotonia, mitochondrial disease and facial dysmorphism. Two siblings with deletion of three of the genes included in the 2P21 deletion syndrome presented with cystinuria, hypotonia, a mild/moderate mental retardation and a respiratory chain complex IV deficiency. To be able to attribute the functional significance of the methylation of CaM in the mouse and the contribution of CaM KMT to the clinical presentation of the 2p21deletion patients, we produced a mouse model lacking only CaM KMT with deletion borders as in the human 2p21deletion syndrome. No compensatory activity for CaM methylation was found. Impairment of complexes I and IV, and less significantly III, of the mitochondrial respiratory chain was more pronounced in the brain than in muscle. CaM KMT is essential for normal body growth and somatosensory development, as well as for the proper functioning of the adult mouse brain. Developmental delay was demonstrated for somatosensory function and for complex behavior, which involved both basal motor function and motivation. The mutant mice also had deficits in motor learning, complex coordination and learning of aversive stimuli. The mouse model contributes to the evaluation of the role of methylated CaM. CaM methylation appears to have a role in growth, muscle strength, somatosensory development and brain function. The current study has clinical implications for human patients. Patients presenting slow growth and muscle weakness that could result from a mitochondrial impairment and mental retardation should be considered for sequence analysis of the CaM KMT gene. Public Library of Science 2015-08-06 /pmc/articles/PMC4527749/ /pubmed/26247364 http://dx.doi.org/10.1371/journal.pgen.1005388 Text en © 2015 Haziza 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
Haziza, Sitvanit
Magnani, Roberta
Lan, Dima
Keinan, Omer
Saada, Ann
Hershkovitz, Eli
Yanay, Nurit
Cohen, Yoram
Nevo, Yoram
Houtz, Robert L.
Sheffield, Val C.
Golan, Hava
Parvari, Ruti
Calmodulin Methyltransferase Is Required for Growth, Muscle Strength, Somatosensory Development and Brain Function
title Calmodulin Methyltransferase Is Required for Growth, Muscle Strength, Somatosensory Development and Brain Function
title_full Calmodulin Methyltransferase Is Required for Growth, Muscle Strength, Somatosensory Development and Brain Function
title_fullStr Calmodulin Methyltransferase Is Required for Growth, Muscle Strength, Somatosensory Development and Brain Function
title_full_unstemmed Calmodulin Methyltransferase Is Required for Growth, Muscle Strength, Somatosensory Development and Brain Function
title_short Calmodulin Methyltransferase Is Required for Growth, Muscle Strength, Somatosensory Development and Brain Function
title_sort calmodulin methyltransferase is required for growth, muscle strength, somatosensory development and brain function
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4527749/
https://www.ncbi.nlm.nih.gov/pubmed/26247364
http://dx.doi.org/10.1371/journal.pgen.1005388
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