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  1. J-3. 子どものこころの発達研究センター
  2. j-3 10. 学術雑誌掲載論文
  3. 1. 査読済論文

Cyclic ADP-ribose and heat regulate oxytocin release via CD38 and TRPM2 in the hypothalamus during social or psychological stress in mice

https://doi.org/10.24517/00030974
https://doi.org/10.24517/00030974
d2ee9338-d2ca-427d-9329-90b279e5938c
名前 / ファイル ライセンス アクション
CH-PR-HIGASHIDA-H-304.pdf CH-PR-HIGASHIDA-H-304.pdf (3.0 MB)
license.icon
Item type 学術雑誌論文 / Journal Article(1)
公開日 2017-10-05
タイトル
タイトル Cyclic ADP-ribose and heat regulate oxytocin release via CD38 and TRPM2 in the hypothalamus during social or psychological stress in mice
言語
言語 eng
資源タイプ
資源タイプ識別子 http://purl.org/coar/resource_type/c_6501
資源タイプ journal article
ID登録
ID登録 10.24517/00030974
ID登録タイプ JaLC
著者 Zhong, Jing

× Zhong, Jing

WEKO 52621

Zhong, Jing

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Amina, Sarwat

× Amina, Sarwat

WEKO 52622

Amina, Sarwat

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Liang, Mingkun

× Liang, Mingkun

WEKO 52623

Liang, Mingkun

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Akther, Shirin

× Akther, Shirin

WEKO 52624

Akther, Shirin

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Yuhi, Teruko

× Yuhi, Teruko

WEKO 52625

Yuhi, Teruko

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Nishimura, Tomoko

× Nishimura, Tomoko

WEKO 52626

Nishimura, Tomoko

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Tsuji, Chiharu

× Tsuji, Chiharu

WEKO 52627

Tsuji, Chiharu

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Tsuji, Takahiro

× Tsuji, Takahiro

WEKO 52628

Tsuji, Takahiro

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Liu, Hong-Xiang

× Liu, Hong-Xiang

WEKO 52629

Liu, Hong-Xiang

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Hashii, Minako

× Hashii, Minako

WEKO 52630

Hashii, Minako

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Furuhara, Kazumi

× Furuhara, Kazumi

WEKO 52631

Furuhara, Kazumi

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Yokoyama, Shigeru

× Yokoyama, Shigeru

WEKO 69
e-Rad 00210633
金沢大学研究者情報 00210633
研究者番号 00210633

Yokoyama, Shigeru

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Yamamoto, Yasuhiko

× Yamamoto, Yasuhiko

WEKO 100
e-Rad 20313637
金沢大学研究者情報 20313637
研究者番号 20313637

Yamamoto, Yasuhiko

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Okamoto, Hiroshi

× Okamoto, Hiroshi

WEKO 20142
e-Rad 60025632

Okamoto, Hiroshi

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Zhao, Yong Juan

× Zhao, Yong Juan

WEKO 52633

Zhao, Yong Juan

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Lee, Hon Cheung

× Lee, Hon Cheung

WEKO 52634

Lee, Hon Cheung

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Tominaga, Makoto

× Tominaga, Makoto

WEKO 52635

Tominaga, Makoto

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Lopatina, Olga

× Lopatina, Olga

WEKO 52636

Lopatina, Olga

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Higashida, Haruhiro

× Higashida, Haruhiro

WEKO 36
e-Rad 30093066
金沢大学研究者情報 30093066
研究者番号 30093066

Higashida, Haruhiro

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著者別表示 横山, 茂

× 横山, 茂

横山, 茂

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山本, 靖彦

× 山本, 靖彦

山本, 靖彦

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岡本, 宏

× 岡本, 宏

岡本, 宏

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東田, 陽博

× 東田, 陽博

東田, 陽博

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書誌情報 Frontiers in Neuroscience

巻 10, 号 JUL, p. 304, 発行日 2016-07-01
ISSN
収録物識別子タイプ ISSN
収録物識別子 1662-4548
DOI
関連タイプ isIdenticalTo
識別子タイプ DOI
関連識別子 10.3389/fnins.2016.00304
出版者
出版者 Frontiers Research Foundation
抄録
内容記述タイプ Abstract
内容記述 Hypothalamic oxytocin (OT) is released into the brain by cyclic ADP-ribose (cADPR) with or without depolarizing stimulation. Previously, we showed that the intracellular free calcium concentration ([Ca2+]i) that seems to trigger OT release can be elevated by β-NAD+, cADPR, and ADP in mouse oxytocinergic neurons. As these β-NAD+ metabolites activate warm-sensitive TRPM2 cation channels, when the incubation temperature is increased, the [Ca2+]i in hypothalamic neurons is elevated. However, it has not been determined whether OT release is facilitated by heat in vitro or hyperthermia in vivo in combination with cADPR. Furthermore, it has not been examined whether CD38 and TRPM2 exert their functions on OT release during stress or stress-induced hyperthermia in relation to the anxiolytic roles and social behaviors of OT under stress conditions. Here, we report that OT release from the isolated hypothalami of male mice in culture was enhanced by extracellular application of cADPR or increasing the incubation temperature from 35°C to 38.5°C, and simultaneous stimulation showed a greater effect. This release was inhibited by a cADPR-dependent ryanodine receptor inhibitor and a nonspecific TRPM2 inhibitor. The facilitated release by heat and cADPR was suppressed in the hypothalamus isolated from CD38 knockout mice and CD38-or TRPM2-knockdown mice. In the course of these experiments, we noted that OT release differed markedly between individual mice under stress with group housing. That is, when male mice received cage-switch stress and eliminated due to their social subclass, significantly higher levels of OT release were found in subordinates compared with ordinates. In mice exposed to anxiety stress in an open field, the cerebrospinal fluid (CSF) OT level increased transiently at 5 min after exposure, and the rectal temperature also increased from 36.6°C to 37.8°C. OT levels in the CSF of mice with lipopolysaccharide-induced fever (+0.8°C) were higher than those of control mice. The TRPM2 mRNA levels and immunoreactivities increased in the subordinate group with cage-switch stress. These results showed that cADPR/CD38 and heat/TRPM2 are co-regulators of OT secretion and suggested that CD38 and TRPM2 are potential therapeutic targets for OT release in psychiatric diseases caused by social stress. © 2016 Zhong, Amina, Liang, Akther, Yuhi, Nishimura, Tsuji, Tsuji, Liu, Hashii, Furuhara, Yokoyama, Yamamoto, Okamoto, Zhao, Lee, Tominaga, Lopatina and Higashida.
著者版フラグ
出版タイプ VoR
出版タイプResource http://purl.org/coar/version/c_970fb48d4fbd8a85
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