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Heterozygosity for Nuclear Factor One X Affects Hippocampal-Dependent Behaviour in Mice

Identification of the genes that regulate the development and subsequent functioning of the hippocampus is pivotal to understanding the role of this cortical structure in learning and memory. One group of genes that has been shown to be critical for the early development of the hippocampus is the Nu...

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Autores principales: Harris, Lachlan, Dixon, Chantelle, Cato, Kathleen, Heng, Yee Hsieh Evelyn, Kurniawan, Nyoman D., Ullmann, Jeremy F. P., Janke, Andrew L., Gronostajski, Richard M., Richards, Linda J., Burne, Thomas H. J., Piper, Michael
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3679126/
https://www.ncbi.nlm.nih.gov/pubmed/23776487
http://dx.doi.org/10.1371/journal.pone.0065478
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author Harris, Lachlan
Dixon, Chantelle
Cato, Kathleen
Heng, Yee Hsieh Evelyn
Kurniawan, Nyoman D.
Ullmann, Jeremy F. P.
Janke, Andrew L.
Gronostajski, Richard M.
Richards, Linda J.
Burne, Thomas H. J.
Piper, Michael
author_facet Harris, Lachlan
Dixon, Chantelle
Cato, Kathleen
Heng, Yee Hsieh Evelyn
Kurniawan, Nyoman D.
Ullmann, Jeremy F. P.
Janke, Andrew L.
Gronostajski, Richard M.
Richards, Linda J.
Burne, Thomas H. J.
Piper, Michael
author_sort Harris, Lachlan
collection PubMed
description Identification of the genes that regulate the development and subsequent functioning of the hippocampus is pivotal to understanding the role of this cortical structure in learning and memory. One group of genes that has been shown to be critical for the early development of the hippocampus is the Nuclear factor one (Nfi) family, which encodes four site-specific transcription factors, NFIA, NFIB, NFIC and NFIX. In mice lacking Nfia, Nfib or Nfix, aspects of early hippocampal development, including neurogenesis within the dentate gyrus, are delayed. However, due to the perinatal lethality of these mice, it is not clear whether this hippocampal phenotype persists to adulthood and affects hippocampal-dependent behaviour. To address this we examined the hippocampal phenotype of mice heterozygous for Nfix (Nfix (+/−)), which survive to adulthood. We found that Nfix (+/−) mice had reduced expression of NFIX throughout the brain, including the hippocampus, and that early hippocampal development in these mice was disrupted, producing a phenotype intermediate to that of wild-type mice and Nfix(−/−) mice. The abnormal hippocampal morphology of Nfix (+/−) mice persisted to adulthood, and these mice displayed a specific performance deficit in the Morris water maze learning and memory task. These findings demonstrate that the level of Nfix expression during development and within the adult is essential for the function of the hippocampus during learning and memory.
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spelling pubmed-36791262013-06-17 Heterozygosity for Nuclear Factor One X Affects Hippocampal-Dependent Behaviour in Mice Harris, Lachlan Dixon, Chantelle Cato, Kathleen Heng, Yee Hsieh Evelyn Kurniawan, Nyoman D. Ullmann, Jeremy F. P. Janke, Andrew L. Gronostajski, Richard M. Richards, Linda J. Burne, Thomas H. J. Piper, Michael PLoS One Research Article Identification of the genes that regulate the development and subsequent functioning of the hippocampus is pivotal to understanding the role of this cortical structure in learning and memory. One group of genes that has been shown to be critical for the early development of the hippocampus is the Nuclear factor one (Nfi) family, which encodes four site-specific transcription factors, NFIA, NFIB, NFIC and NFIX. In mice lacking Nfia, Nfib or Nfix, aspects of early hippocampal development, including neurogenesis within the dentate gyrus, are delayed. However, due to the perinatal lethality of these mice, it is not clear whether this hippocampal phenotype persists to adulthood and affects hippocampal-dependent behaviour. To address this we examined the hippocampal phenotype of mice heterozygous for Nfix (Nfix (+/−)), which survive to adulthood. We found that Nfix (+/−) mice had reduced expression of NFIX throughout the brain, including the hippocampus, and that early hippocampal development in these mice was disrupted, producing a phenotype intermediate to that of wild-type mice and Nfix(−/−) mice. The abnormal hippocampal morphology of Nfix (+/−) mice persisted to adulthood, and these mice displayed a specific performance deficit in the Morris water maze learning and memory task. These findings demonstrate that the level of Nfix expression during development and within the adult is essential for the function of the hippocampus during learning and memory. Public Library of Science 2013-06-11 /pmc/articles/PMC3679126/ /pubmed/23776487 http://dx.doi.org/10.1371/journal.pone.0065478 Text en © 2013 Harris 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
Harris, Lachlan
Dixon, Chantelle
Cato, Kathleen
Heng, Yee Hsieh Evelyn
Kurniawan, Nyoman D.
Ullmann, Jeremy F. P.
Janke, Andrew L.
Gronostajski, Richard M.
Richards, Linda J.
Burne, Thomas H. J.
Piper, Michael
Heterozygosity for Nuclear Factor One X Affects Hippocampal-Dependent Behaviour in Mice
title Heterozygosity for Nuclear Factor One X Affects Hippocampal-Dependent Behaviour in Mice
title_full Heterozygosity for Nuclear Factor One X Affects Hippocampal-Dependent Behaviour in Mice
title_fullStr Heterozygosity for Nuclear Factor One X Affects Hippocampal-Dependent Behaviour in Mice
title_full_unstemmed Heterozygosity for Nuclear Factor One X Affects Hippocampal-Dependent Behaviour in Mice
title_short Heterozygosity for Nuclear Factor One X Affects Hippocampal-Dependent Behaviour in Mice
title_sort heterozygosity for nuclear factor one x affects hippocampal-dependent behaviour in mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3679126/
https://www.ncbi.nlm.nih.gov/pubmed/23776487
http://dx.doi.org/10.1371/journal.pone.0065478
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