Na+/Ca2+ exchanger-heterozygote knockout mice display increased relaxation in gastric fundus and accelerated gastric transit in vivo

Y. T. Azuma; S. Hayashi; K. Nishiyama; S. Kita; K. Mukai; H. Nakajima; T. Iwamoto; T. Takeuchi

doi:10.1111/nmo.12779

Na⁺/Ca²⁺ exchanger-heterozygote knockout mice display increased relaxation in gastric fundus and accelerated gastric transit in vivo

Y. T. Azuma, S. Hayashi, K. Nishiyama, S. Kita, K. Mukai, H. Nakajima, T. Iwamoto, T. Takeuchi

研究成果: ジャーナルへの寄稿 › 学術誌 › 査読

13 被引用数 (Scopus)

抄録

Background: For the contraction and relaxation of gastric smooth muscles to occur, the intracellular Ca²⁺ concentration must be increased and decreased, respectively. The Na⁺/Ca²⁺ exchanger (NCX) is a plasma membrane transporter that is involved in regulating intracellular Ca²⁺ concentrations. Methods: To determine the role of NCX in gastrointestinal tissues, we examined electric field stimulation (EFS)-induced relaxations in the circular muscles of the gastric fundus in NCX1 and NCX2 heterozygote knockout mice (HET). Key Results: The myenteric plexus layers and the longitudinal and circular muscle layers in the gastric fundus of wild-type mice (WT) were strongly immunoreactive to NCX1 and NCX2. EFS induced a transient relaxation that was apparent during the stimulus and a sustained relaxation that persisted after the end of the stimulus. The amplitudes of EFS-induced transient relaxation and sustained relaxation were greater in NCX1 HET and NCX2 HET than in WT. When an inhibitor of nitric oxide synthase was added following the EFS, neither NCX1 HET nor NCX2 HET exhibited transient relaxation, similar to WT. Furthermore, when a PACAP antagonist was added following the EFS, sustained relaxation in NCX1 HET and NCX2 HET was not observed, similar to WT. Next, we examined the effect of NCX heterozygous deficiency on relaxation in response to NO and PACAP in smooth muscles. The magnitude of NOR-1- and PACAP-induced relaxations in NCX1 HET and NCX2 HET was similar to that of WT. Conclusions & Inferences: In this study, we demonstrate that NCX1 and NCX2 expressed in neurons regulate the motility in the gastric fundus. When an inhibitor of nitric oxide synthase was added following the EFS, neither NCX1 HET nor NCX2 HET exhibited transient relaxation, similar to WT. Furthermore, when a PACAP antagonist was added following the EFS, sustained relaxation in NCX1 HET and NCX2 HET was not observed, similar to WT.

本文言語	英語
ページ（範囲）	827-836
ページ数	10
ジャーナル	Neurogastroenterology and Motility
巻	28
号	6
DOI	https://doi.org/10.1111/nmo.12779
出版ステータス	出版済み - 6月 1 2016
外部発表	はい

!!!All Science Journal Classification (ASJC) codes

生理学
内分泌系および自律システム
消化器病学

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10.1111/nmo.12779

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title = "Na+/Ca2+ exchanger-heterozygote knockout mice display increased relaxation in gastric fundus and accelerated gastric transit in vivo",

abstract = "Background: For the contraction and relaxation of gastric smooth muscles to occur, the intracellular Ca2+ concentration must be increased and decreased, respectively. The Na+/Ca2+ exchanger (NCX) is a plasma membrane transporter that is involved in regulating intracellular Ca2+ concentrations. Methods: To determine the role of NCX in gastrointestinal tissues, we examined electric field stimulation (EFS)-induced relaxations in the circular muscles of the gastric fundus in NCX1 and NCX2 heterozygote knockout mice (HET). Key Results: The myenteric plexus layers and the longitudinal and circular muscle layers in the gastric fundus of wild-type mice (WT) were strongly immunoreactive to NCX1 and NCX2. EFS induced a transient relaxation that was apparent during the stimulus and a sustained relaxation that persisted after the end of the stimulus. The amplitudes of EFS-induced transient relaxation and sustained relaxation were greater in NCX1 HET and NCX2 HET than in WT. When an inhibitor of nitric oxide synthase was added following the EFS, neither NCX1 HET nor NCX2 HET exhibited transient relaxation, similar to WT. Furthermore, when a PACAP antagonist was added following the EFS, sustained relaxation in NCX1 HET and NCX2 HET was not observed, similar to WT. Next, we examined the effect of NCX heterozygous deficiency on relaxation in response to NO and PACAP in smooth muscles. The magnitude of NOR-1- and PACAP-induced relaxations in NCX1 HET and NCX2 HET was similar to that of WT. Conclusions & Inferences: In this study, we demonstrate that NCX1 and NCX2 expressed in neurons regulate the motility in the gastric fundus. When an inhibitor of nitric oxide synthase was added following the EFS, neither NCX1 HET nor NCX2 HET exhibited transient relaxation, similar to WT. Furthermore, when a PACAP antagonist was added following the EFS, sustained relaxation in NCX1 HET and NCX2 HET was not observed, similar to WT.",

author = "Azuma, {Y. T.} and S. Hayashi and K. Nishiyama and S. Kita and K. Mukai and H. Nakajima and T. Iwamoto and T. Takeuchi",

note = "Publisher Copyright: {\textcopyright} 2016 John Wiley & Sons Ltd.",

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month = jun,

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T1 - Na+/Ca2+ exchanger-heterozygote knockout mice display increased relaxation in gastric fundus and accelerated gastric transit in vivo

AU - Azuma, Y. T.

AU - Hayashi, S.

AU - Nishiyama, K.

AU - Kita, S.

AU - Mukai, K.

AU - Nakajima, H.

AU - Iwamoto, T.

AU - Takeuchi, T.

PY - 2016/6/1

Y1 - 2016/6/1

N2 - Background: For the contraction and relaxation of gastric smooth muscles to occur, the intracellular Ca2+ concentration must be increased and decreased, respectively. The Na+/Ca2+ exchanger (NCX) is a plasma membrane transporter that is involved in regulating intracellular Ca2+ concentrations. Methods: To determine the role of NCX in gastrointestinal tissues, we examined electric field stimulation (EFS)-induced relaxations in the circular muscles of the gastric fundus in NCX1 and NCX2 heterozygote knockout mice (HET). Key Results: The myenteric plexus layers and the longitudinal and circular muscle layers in the gastric fundus of wild-type mice (WT) were strongly immunoreactive to NCX1 and NCX2. EFS induced a transient relaxation that was apparent during the stimulus and a sustained relaxation that persisted after the end of the stimulus. The amplitudes of EFS-induced transient relaxation and sustained relaxation were greater in NCX1 HET and NCX2 HET than in WT. When an inhibitor of nitric oxide synthase was added following the EFS, neither NCX1 HET nor NCX2 HET exhibited transient relaxation, similar to WT. Furthermore, when a PACAP antagonist was added following the EFS, sustained relaxation in NCX1 HET and NCX2 HET was not observed, similar to WT. Next, we examined the effect of NCX heterozygous deficiency on relaxation in response to NO and PACAP in smooth muscles. The magnitude of NOR-1- and PACAP-induced relaxations in NCX1 HET and NCX2 HET was similar to that of WT. Conclusions & Inferences: In this study, we demonstrate that NCX1 and NCX2 expressed in neurons regulate the motility in the gastric fundus. When an inhibitor of nitric oxide synthase was added following the EFS, neither NCX1 HET nor NCX2 HET exhibited transient relaxation, similar to WT. Furthermore, when a PACAP antagonist was added following the EFS, sustained relaxation in NCX1 HET and NCX2 HET was not observed, similar to WT.

AB - Background: For the contraction and relaxation of gastric smooth muscles to occur, the intracellular Ca2+ concentration must be increased and decreased, respectively. The Na+/Ca2+ exchanger (NCX) is a plasma membrane transporter that is involved in regulating intracellular Ca2+ concentrations. Methods: To determine the role of NCX in gastrointestinal tissues, we examined electric field stimulation (EFS)-induced relaxations in the circular muscles of the gastric fundus in NCX1 and NCX2 heterozygote knockout mice (HET). Key Results: The myenteric plexus layers and the longitudinal and circular muscle layers in the gastric fundus of wild-type mice (WT) were strongly immunoreactive to NCX1 and NCX2. EFS induced a transient relaxation that was apparent during the stimulus and a sustained relaxation that persisted after the end of the stimulus. The amplitudes of EFS-induced transient relaxation and sustained relaxation were greater in NCX1 HET and NCX2 HET than in WT. When an inhibitor of nitric oxide synthase was added following the EFS, neither NCX1 HET nor NCX2 HET exhibited transient relaxation, similar to WT. Furthermore, when a PACAP antagonist was added following the EFS, sustained relaxation in NCX1 HET and NCX2 HET was not observed, similar to WT. Next, we examined the effect of NCX heterozygous deficiency on relaxation in response to NO and PACAP in smooth muscles. The magnitude of NOR-1- and PACAP-induced relaxations in NCX1 HET and NCX2 HET was similar to that of WT. Conclusions & Inferences: In this study, we demonstrate that NCX1 and NCX2 expressed in neurons regulate the motility in the gastric fundus. When an inhibitor of nitric oxide synthase was added following the EFS, neither NCX1 HET nor NCX2 HET exhibited transient relaxation, similar to WT. Furthermore, when a PACAP antagonist was added following the EFS, sustained relaxation in NCX1 HET and NCX2 HET was not observed, similar to WT.

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