MKK7 deficiency in mature neurons impairs parental behavior in mice

Tadashi Shin; Yuichi Hiraoka; Tokiwa Yamasaki; Jamey D. Marth; Josef M. Penninger; Masami Kanai-Azuma; Kohichi Tanaka; Satoshi Kofuji; Hiroshi Nishina

doi:10.1111/gtc.12816

MKK7 deficiency in mature neurons impairs parental behavior in mice

Tadashi Shin, Yuichi Hiraoka, Tokiwa Yamasaki, Jamey D. Marth, Josef M. Penninger, Masami Kanai-Azuma, Kohichi Tanaka, Satoshi Kofuji, Hiroshi Nishina

Department of Physiology

Research output: Contribution to journal › Article › peer-review

2 Citations (Scopus)

Abstract

c-Jun N-terminal kinases (JNKs) are constitutively activated in mammalian brains and are indispensable for their development and neural functions. MKK7 is an upstream activator of all JNKs. However, whether the common JNK signaling pathway regulates the brain's control of social behavior remains unclear. Here, we show that female mice in which Mkk7 is deleted specifically in mature neurons (Mkk7^flox/floxSyn-Cre mice) give birth to a normal number of pups but fail to raise them due to a defect in pup retrieval. To explore the mechanism underlying this abnormality, we performed comprehensive behavioral tests. Mkk7^flox/floxSyn-Cre mice showed normal locomotor functions and cognitive ability but exhibited depression-like behavior. cDNA microarray analysis of mutant brain revealed an altered gene expression pattern. Quantitative RT-PCR analysis demonstrated that mRNA expression levels of genes related to neural signaling pathways and a calcium channel were significantly different from controls. In addition, loss of neural MKK7 had unexpected regulatory effects on gene expression patterns in oligodendrocytes. These findings indicate that MKK7 has an important role in regulating the gene expression patterns responsible for promoting normal social behavior and staving off depression.

Original language	English
Pages (from-to)	5-17
Number of pages	13
Journal	Genes to Cells
Volume	26
Issue number	1
DOIs	https://doi.org/10.1111/gtc.12816
Publication status	Published - 2021 Jan

Keywords

JNK
MKK7
mature neuron
parental behavior

ASJC Scopus subject areas

Genetics
Cell Biology

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10.1111/gtc.12816

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@article{335a3da5bc644575b93c68469d23ab77,

title = "MKK7 deficiency in mature neurons impairs parental behavior in mice",

abstract = "c-Jun N-terminal kinases (JNKs) are constitutively activated in mammalian brains and are indispensable for their development and neural functions. MKK7 is an upstream activator of all JNKs. However, whether the common JNK signaling pathway regulates the brain's control of social behavior remains unclear. Here, we show that female mice in which Mkk7 is deleted specifically in mature neurons (Mkk7flox/floxSyn-Cre mice) give birth to a normal number of pups but fail to raise them due to a defect in pup retrieval. To explore the mechanism underlying this abnormality, we performed comprehensive behavioral tests. Mkk7flox/floxSyn-Cre mice showed normal locomotor functions and cognitive ability but exhibited depression-like behavior. cDNA microarray analysis of mutant brain revealed an altered gene expression pattern. Quantitative RT-PCR analysis demonstrated that mRNA expression levels of genes related to neural signaling pathways and a calcium channel were significantly different from controls. In addition, loss of neural MKK7 had unexpected regulatory effects on gene expression patterns in oligodendrocytes. These findings indicate that MKK7 has an important role in regulating the gene expression patterns responsible for promoting normal social behavior and staving off depression.",

keywords = "JNK, MKK7, mature neuron, parental behavior",

author = "Tadashi Shin and Yuichi Hiraoka and Tokiwa Yamasaki and Marth, {Jamey D.} and Penninger, {Josef M.} and Masami Kanai-Azuma and Kohichi Tanaka and Satoshi Kofuji and Hiroshi Nishina",

note = "Funding Information: We thank Dr. S. Shimizu, Dr. K. Kuroda, Dr. K. Homma and numerous members of the Nishina laboratory for their helpful discussions and critical comments on this manuscript. This work was supported by four grants from the Japan Society for the Promotion of Science (JSPS) Grant‐in‐Aid for Scientific Research (JP17H03982, JP20H03381 (H.N.)); a Grant‐in‐Aid for Scientific Research on Innovative Areas (JP17H05996 (H.N.), JP19H04953 (K.H.)); a Nanken‐Kyoten grant from Tokyo Medical and Dental University (TMDU) (H.N.); and a grant from AMED (JP18fk0210042, JP19fk0210042 and JP20fk0210042 (H.N.)) and NIH DK048247 (J.D.M.). Publisher Copyright: {\textcopyright} 2020 The Authors. Genes to Cells published by Molecular Biology Society of Japan and John Wiley & Sons Australia, Ltd",

year = "2021",

month = jan,

doi = "10.1111/gtc.12816",

language = "English",

volume = "26",

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journal = "Genes to Cells",

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T1 - MKK7 deficiency in mature neurons impairs parental behavior in mice

AU - Shin, Tadashi

AU - Hiraoka, Yuichi

AU - Yamasaki, Tokiwa

AU - Marth, Jamey D.

AU - Penninger, Josef M.

AU - Kanai-Azuma, Masami

AU - Tanaka, Kohichi

AU - Kofuji, Satoshi

AU - Nishina, Hiroshi

N1 - Funding Information: We thank Dr. S. Shimizu, Dr. K. Kuroda, Dr. K. Homma and numerous members of the Nishina laboratory for their helpful discussions and critical comments on this manuscript. This work was supported by four grants from the Japan Society for the Promotion of Science (JSPS) Grant‐in‐Aid for Scientific Research (JP17H03982, JP20H03381 (H.N.)); a Grant‐in‐Aid for Scientific Research on Innovative Areas (JP17H05996 (H.N.), JP19H04953 (K.H.)); a Nanken‐Kyoten grant from Tokyo Medical and Dental University (TMDU) (H.N.); and a grant from AMED (JP18fk0210042, JP19fk0210042 and JP20fk0210042 (H.N.)) and NIH DK048247 (J.D.M.). Publisher Copyright: © 2020 The Authors. Genes to Cells published by Molecular Biology Society of Japan and John Wiley & Sons Australia, Ltd

PY - 2021/1

Y1 - 2021/1

N2 - c-Jun N-terminal kinases (JNKs) are constitutively activated in mammalian brains and are indispensable for their development and neural functions. MKK7 is an upstream activator of all JNKs. However, whether the common JNK signaling pathway regulates the brain's control of social behavior remains unclear. Here, we show that female mice in which Mkk7 is deleted specifically in mature neurons (Mkk7flox/floxSyn-Cre mice) give birth to a normal number of pups but fail to raise them due to a defect in pup retrieval. To explore the mechanism underlying this abnormality, we performed comprehensive behavioral tests. Mkk7flox/floxSyn-Cre mice showed normal locomotor functions and cognitive ability but exhibited depression-like behavior. cDNA microarray analysis of mutant brain revealed an altered gene expression pattern. Quantitative RT-PCR analysis demonstrated that mRNA expression levels of genes related to neural signaling pathways and a calcium channel were significantly different from controls. In addition, loss of neural MKK7 had unexpected regulatory effects on gene expression patterns in oligodendrocytes. These findings indicate that MKK7 has an important role in regulating the gene expression patterns responsible for promoting normal social behavior and staving off depression.

AB - c-Jun N-terminal kinases (JNKs) are constitutively activated in mammalian brains and are indispensable for their development and neural functions. MKK7 is an upstream activator of all JNKs. However, whether the common JNK signaling pathway regulates the brain's control of social behavior remains unclear. Here, we show that female mice in which Mkk7 is deleted specifically in mature neurons (Mkk7flox/floxSyn-Cre mice) give birth to a normal number of pups but fail to raise them due to a defect in pup retrieval. To explore the mechanism underlying this abnormality, we performed comprehensive behavioral tests. Mkk7flox/floxSyn-Cre mice showed normal locomotor functions and cognitive ability but exhibited depression-like behavior. cDNA microarray analysis of mutant brain revealed an altered gene expression pattern. Quantitative RT-PCR analysis demonstrated that mRNA expression levels of genes related to neural signaling pathways and a calcium channel were significantly different from controls. In addition, loss of neural MKK7 had unexpected regulatory effects on gene expression patterns in oligodendrocytes. These findings indicate that MKK7 has an important role in regulating the gene expression patterns responsible for promoting normal social behavior and staving off depression.

KW - JNK

KW - MKK7

KW - mature neuron

KW - parental behavior

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DO - 10.1111/gtc.12816

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VL - 26

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JO - Genes to Cells

JF - Genes to Cells

IS - 1

ER -

MKK7 deficiency in mature neurons impairs parental behavior in mice

Abstract

Keywords

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