Alpha-CaMKII deficiency causes immature dentate gyrus, a novel candidate endophenotype of psychiatric disorders

Elucidating the neural and genetic factors underlying psychiatric illness is hampered by current methods of clinical diagnosis. The identification and investigation of clinical endophenotypes may be one solution, but represents a considerable challenge in human subjects. Here we report that mice het...

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Autores principales: Yamasaki, Nobuyuki, Maekawa, Motoko, Kobayashi, Katsunori, Kajii, Yasushi, Maeda, Jun, Soma, Miho, Takao, Keizo, Tanda, Koichi, Ohira, Koji, Toyama, Keiko, Kanzaki, Kouji, Fukunaga, Kohji, Sudo, Yusuke, Ichinose, Hiroshi, Ikeda, Masashi, Iwata, Nakao, Ozaki, Norio, Suzuki, Hidenori, Higuchi, Makoto, Suhara, Tetsuya, Yuasa, Shigeki, Miyakawa, Tsuyoshi
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2008
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2562999/
https://www.ncbi.nlm.nih.gov/pubmed/18803808
http://dx.doi.org/10.1186/1756-6606-1-6
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author Yamasaki, Nobuyuki
Maekawa, Motoko
Kobayashi, Katsunori
Kajii, Yasushi
Maeda, Jun
Soma, Miho
Takao, Keizo
Tanda, Koichi
Ohira, Koji
Toyama, Keiko
Kanzaki, Kouji
Fukunaga, Kohji
Sudo, Yusuke
Ichinose, Hiroshi
Ikeda, Masashi
Iwata, Nakao
Ozaki, Norio
Suzuki, Hidenori
Higuchi, Makoto
Suhara, Tetsuya
Yuasa, Shigeki
Miyakawa, Tsuyoshi
author_facet Yamasaki, Nobuyuki
Maekawa, Motoko
Kobayashi, Katsunori
Kajii, Yasushi
Maeda, Jun
Soma, Miho
Takao, Keizo
Tanda, Koichi
Ohira, Koji
Toyama, Keiko
Kanzaki, Kouji
Fukunaga, Kohji
Sudo, Yusuke
Ichinose, Hiroshi
Ikeda, Masashi
Iwata, Nakao
Ozaki, Norio
Suzuki, Hidenori
Higuchi, Makoto
Suhara, Tetsuya
Yuasa, Shigeki
Miyakawa, Tsuyoshi
author_sort Yamasaki, Nobuyuki
collection PubMed
description Elucidating the neural and genetic factors underlying psychiatric illness is hampered by current methods of clinical diagnosis. The identification and investigation of clinical endophenotypes may be one solution, but represents a considerable challenge in human subjects. Here we report that mice heterozygous for a null mutation of the alpha-isoform of calcium/calmodulin-dependent protein kinase II (alpha-CaMKII+/-) have profoundly dysregulated behaviours and impaired neuronal development in the dentate gyrus (DG). The behavioral abnormalities include a severe working memory deficit and an exaggerated infradian rhythm, which are similar to symptoms seen in schizophrenia, bipolar mood disorder and other psychiatric disorders. Transcriptome analysis of the hippocampus of these mutants revealed that the expression levels of more than 2000 genes were significantly changed. Strikingly, among the 20 most downregulated genes, 5 had highly selective expression in the DG. Whereas BrdU incorporated cells in the mutant mouse DG was increased by more than 50 percent, the number of mature neurons in the DG was dramatically decreased. Morphological and physiological features of the DG neurons in the mutants were strikingly similar to those of immature DG neurons in normal rodents. Moreover, c-Fos expression in the DG after electric footshock was almost completely and selectively abolished in the mutants. Statistical clustering of human post-mortem brains using 10 genes differentially-expressed in the mutant mice were used to classify individuals into two clusters, one of which contained 16 of 18 schizophrenic patients. Nearly half of the differentially-expressed probes in the schizophrenia-enriched cluster encoded genes that are involved in neurogenesis or in neuronal migration/maturation, including calbindin, a marker for mature DG neurons. Based on these results, we propose that an "immature DG" in adulthood might induce alterations in behavior and serve as a promising candidate endophenotype of schizophrenia and other human psychiatric disorders.
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spelling pubmed-25629992008-10-08 Alpha-CaMKII deficiency causes immature dentate gyrus, a novel candidate endophenotype of psychiatric disorders Yamasaki, Nobuyuki Maekawa, Motoko Kobayashi, Katsunori Kajii, Yasushi Maeda, Jun Soma, Miho Takao, Keizo Tanda, Koichi Ohira, Koji Toyama, Keiko Kanzaki, Kouji Fukunaga, Kohji Sudo, Yusuke Ichinose, Hiroshi Ikeda, Masashi Iwata, Nakao Ozaki, Norio Suzuki, Hidenori Higuchi, Makoto Suhara, Tetsuya Yuasa, Shigeki Miyakawa, Tsuyoshi Mol Brain Research Elucidating the neural and genetic factors underlying psychiatric illness is hampered by current methods of clinical diagnosis. The identification and investigation of clinical endophenotypes may be one solution, but represents a considerable challenge in human subjects. Here we report that mice heterozygous for a null mutation of the alpha-isoform of calcium/calmodulin-dependent protein kinase II (alpha-CaMKII+/-) have profoundly dysregulated behaviours and impaired neuronal development in the dentate gyrus (DG). The behavioral abnormalities include a severe working memory deficit and an exaggerated infradian rhythm, which are similar to symptoms seen in schizophrenia, bipolar mood disorder and other psychiatric disorders. Transcriptome analysis of the hippocampus of these mutants revealed that the expression levels of more than 2000 genes were significantly changed. Strikingly, among the 20 most downregulated genes, 5 had highly selective expression in the DG. Whereas BrdU incorporated cells in the mutant mouse DG was increased by more than 50 percent, the number of mature neurons in the DG was dramatically decreased. Morphological and physiological features of the DG neurons in the mutants were strikingly similar to those of immature DG neurons in normal rodents. Moreover, c-Fos expression in the DG after electric footshock was almost completely and selectively abolished in the mutants. Statistical clustering of human post-mortem brains using 10 genes differentially-expressed in the mutant mice were used to classify individuals into two clusters, one of which contained 16 of 18 schizophrenic patients. Nearly half of the differentially-expressed probes in the schizophrenia-enriched cluster encoded genes that are involved in neurogenesis or in neuronal migration/maturation, including calbindin, a marker for mature DG neurons. Based on these results, we propose that an "immature DG" in adulthood might induce alterations in behavior and serve as a promising candidate endophenotype of schizophrenia and other human psychiatric disorders. BioMed Central 2008-09-10 /pmc/articles/PMC2562999/ /pubmed/18803808 http://dx.doi.org/10.1186/1756-6606-1-6 Text en Copyright © 2008 Yamasaki et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Yamasaki, Nobuyuki
Maekawa, Motoko
Kobayashi, Katsunori
Kajii, Yasushi
Maeda, Jun
Soma, Miho
Takao, Keizo
Tanda, Koichi
Ohira, Koji
Toyama, Keiko
Kanzaki, Kouji
Fukunaga, Kohji
Sudo, Yusuke
Ichinose, Hiroshi
Ikeda, Masashi
Iwata, Nakao
Ozaki, Norio
Suzuki, Hidenori
Higuchi, Makoto
Suhara, Tetsuya
Yuasa, Shigeki
Miyakawa, Tsuyoshi
Alpha-CaMKII deficiency causes immature dentate gyrus, a novel candidate endophenotype of psychiatric disorders
title Alpha-CaMKII deficiency causes immature dentate gyrus, a novel candidate endophenotype of psychiatric disorders
title_full Alpha-CaMKII deficiency causes immature dentate gyrus, a novel candidate endophenotype of psychiatric disorders
title_fullStr Alpha-CaMKII deficiency causes immature dentate gyrus, a novel candidate endophenotype of psychiatric disorders
title_full_unstemmed Alpha-CaMKII deficiency causes immature dentate gyrus, a novel candidate endophenotype of psychiatric disorders
title_short Alpha-CaMKII deficiency causes immature dentate gyrus, a novel candidate endophenotype of psychiatric disorders
title_sort alpha-camkii deficiency causes immature dentate gyrus, a novel candidate endophenotype of psychiatric disorders
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2562999/
https://www.ncbi.nlm.nih.gov/pubmed/18803808
http://dx.doi.org/10.1186/1756-6606-1-6
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