Magel2 truncation alters select behavioral and physiological outcomes in a rat model of Schaaf-Yang syndrome

Previous studies in mice have utilized Magel2 gene deletion models to examine the consequences of its absence. We report the generation, molecular validation and phenotypic characterization of a novel rat model with a truncating Magel2 mutation modeling variants associated with Schaaf-Yang syndrome-...

Descripción completa

Detalles Bibliográficos
Autores principales: Reznik, Derek L., Yang, Mingxiao V., Albelda de la Haza, Pedro, Jain, Antrix, Spanjaard, Melanie, Theiss, Susanne, Schaaf, Christian P., Malovannaya, Anna, Strong, Theresa V., Veeraragavan, Surabi, Samaco, Rodney C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Company of Biologists Ltd 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9922728/
https://www.ncbi.nlm.nih.gov/pubmed/36637363
http://dx.doi.org/10.1242/dmm.049829
_version_ 1784887589122080768
author Reznik, Derek L.
Yang, Mingxiao V.
Albelda de la Haza, Pedro
Jain, Antrix
Spanjaard, Melanie
Theiss, Susanne
Schaaf, Christian P.
Malovannaya, Anna
Strong, Theresa V.
Veeraragavan, Surabi
Samaco, Rodney C.
author_facet Reznik, Derek L.
Yang, Mingxiao V.
Albelda de la Haza, Pedro
Jain, Antrix
Spanjaard, Melanie
Theiss, Susanne
Schaaf, Christian P.
Malovannaya, Anna
Strong, Theresa V.
Veeraragavan, Surabi
Samaco, Rodney C.
author_sort Reznik, Derek L.
collection PubMed
description Previous studies in mice have utilized Magel2 gene deletion models to examine the consequences of its absence. We report the generation, molecular validation and phenotypic characterization of a novel rat model with a truncating Magel2 mutation modeling variants associated with Schaaf-Yang syndrome-causing mutations. Within the hypothalamus, a brain region in which human MAGEL2 is paternally expressed, we demonstrated, at the level of transcript and peptide detection, that rat Magel2 exhibits a paternal, parent-of-origin effect. In evaluations of behavioral features across several domains, juvenile Magel2 mutant rats displayed alterations in anxiety-like behavior and sociability measures. Moreover, the analysis of peripheral organ systems detected alterations in body composition, cardiac structure and function, and breathing irregularities in Magel2 mutant rats. Several of these findings are concordant with reported mouse phenotypes, indicating the conservation of MAGEL2 function across rodent species. Our comprehensive analysis revealing impairments across multiple domains demonstrates the tractability of this model system for the study of truncating MAGEL2 mutations.
format Online
Article
Text
id pubmed-9922728
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher The Company of Biologists Ltd
record_format MEDLINE/PubMed
spelling pubmed-99227282023-02-13 Magel2 truncation alters select behavioral and physiological outcomes in a rat model of Schaaf-Yang syndrome Reznik, Derek L. Yang, Mingxiao V. Albelda de la Haza, Pedro Jain, Antrix Spanjaard, Melanie Theiss, Susanne Schaaf, Christian P. Malovannaya, Anna Strong, Theresa V. Veeraragavan, Surabi Samaco, Rodney C. Dis Model Mech Research Article Previous studies in mice have utilized Magel2 gene deletion models to examine the consequences of its absence. We report the generation, molecular validation and phenotypic characterization of a novel rat model with a truncating Magel2 mutation modeling variants associated with Schaaf-Yang syndrome-causing mutations. Within the hypothalamus, a brain region in which human MAGEL2 is paternally expressed, we demonstrated, at the level of transcript and peptide detection, that rat Magel2 exhibits a paternal, parent-of-origin effect. In evaluations of behavioral features across several domains, juvenile Magel2 mutant rats displayed alterations in anxiety-like behavior and sociability measures. Moreover, the analysis of peripheral organ systems detected alterations in body composition, cardiac structure and function, and breathing irregularities in Magel2 mutant rats. Several of these findings are concordant with reported mouse phenotypes, indicating the conservation of MAGEL2 function across rodent species. Our comprehensive analysis revealing impairments across multiple domains demonstrates the tractability of this model system for the study of truncating MAGEL2 mutations. The Company of Biologists Ltd 2023-02-03 /pmc/articles/PMC9922728/ /pubmed/36637363 http://dx.doi.org/10.1242/dmm.049829 Text en © 2023. Published by The Company of Biologists Ltd https://creativecommons.org/licenses/by/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0), which permits unrestricted use, distribution and reproduction in any medium provided that the original work is properly attributed.
spellingShingle Research Article
Reznik, Derek L.
Yang, Mingxiao V.
Albelda de la Haza, Pedro
Jain, Antrix
Spanjaard, Melanie
Theiss, Susanne
Schaaf, Christian P.
Malovannaya, Anna
Strong, Theresa V.
Veeraragavan, Surabi
Samaco, Rodney C.
Magel2 truncation alters select behavioral and physiological outcomes in a rat model of Schaaf-Yang syndrome
title Magel2 truncation alters select behavioral and physiological outcomes in a rat model of Schaaf-Yang syndrome
title_full Magel2 truncation alters select behavioral and physiological outcomes in a rat model of Schaaf-Yang syndrome
title_fullStr Magel2 truncation alters select behavioral and physiological outcomes in a rat model of Schaaf-Yang syndrome
title_full_unstemmed Magel2 truncation alters select behavioral and physiological outcomes in a rat model of Schaaf-Yang syndrome
title_short Magel2 truncation alters select behavioral and physiological outcomes in a rat model of Schaaf-Yang syndrome
title_sort magel2 truncation alters select behavioral and physiological outcomes in a rat model of schaaf-yang syndrome
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9922728/
https://www.ncbi.nlm.nih.gov/pubmed/36637363
http://dx.doi.org/10.1242/dmm.049829
work_keys_str_mv AT reznikderekl magel2truncationaltersselectbehavioralandphysiologicaloutcomesinaratmodelofschaafyangsyndrome
AT yangmingxiaov magel2truncationaltersselectbehavioralandphysiologicaloutcomesinaratmodelofschaafyangsyndrome
AT albeldadelahazapedro magel2truncationaltersselectbehavioralandphysiologicaloutcomesinaratmodelofschaafyangsyndrome
AT jainantrix magel2truncationaltersselectbehavioralandphysiologicaloutcomesinaratmodelofschaafyangsyndrome
AT spanjaardmelanie magel2truncationaltersselectbehavioralandphysiologicaloutcomesinaratmodelofschaafyangsyndrome
AT theisssusanne magel2truncationaltersselectbehavioralandphysiologicaloutcomesinaratmodelofschaafyangsyndrome
AT schaafchristianp magel2truncationaltersselectbehavioralandphysiologicaloutcomesinaratmodelofschaafyangsyndrome
AT malovannayaanna magel2truncationaltersselectbehavioralandphysiologicaloutcomesinaratmodelofschaafyangsyndrome
AT strongtheresav magel2truncationaltersselectbehavioralandphysiologicaloutcomesinaratmodelofschaafyangsyndrome
AT veeraragavansurabi magel2truncationaltersselectbehavioralandphysiologicaloutcomesinaratmodelofschaafyangsyndrome
AT samacorodneyc magel2truncationaltersselectbehavioralandphysiologicaloutcomesinaratmodelofschaafyangsyndrome

Ejemplares similares