Peripheral serotonin enhances lipid metabolism by accelerating bile acid turnover

Hitoshi Watanabe; Daisuke Akasaka; Hideki Ogasawara; Kan Sato; Masato Miyake; Kazuki Saito; Yu Takahashi; Takashi Kanaya; Ikuro Takakura; Tetsuya Hondo; Guozheng Chao; Michael Terence Rose; Shyuichi Ohwada; Kouichi Watanabe; Takahiro Yamaguchi; Hisashi Aso

doi:10.1210/en.2009-1349

Peripheral serotonin enhances lipid metabolism by accelerating bile acid turnover

Hitoshi Watanabe, Daisuke Akasaka, Hideki Ogasawara, Kan Sato, Masato Miyake, Kazuki Saito, Yu Takahashi, Takashi Kanaya, Ikuro Takakura, Tetsuya Hondo, Guozheng Chao, Michael Terence Rose, Shyuichi Ohwada, Kouichi Watanabe, Takahiro Yamaguchi, Hisashi Aso

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Serotonin is synthesized by two distinct tryptophan hydroxylases, one in the brain and one in the periphery. The latter is known to be unable to cross the blood-brain barrier. These two serotonin systems have apparently independent functions, although the functions of peripheral serotonin have yet to be fully elucidated. In this study, we have investigated the physiological effect of peripheral serotonin on the concentrations of metabolites in the circulation and in the liver. After fasting, mice were ip injected with 1 mg serotonin. The plasma glucose concentration was significantly elevated between 60 and 270 min after the injection. In contrast, plasma triglyceride, cholesterol, and nonesterified fatty acid concentrations were decreased. The hepatic glycogen synthesis and concentrations were significantly higher at 240 min. At the same time, the hepatic triglyceride content was significantly lower than the basal levels noted before the serotonin injection, whereas the hepatic cholesterol content was significantly higher by 60 min after the injection. Furthermore, serotonin stimulated the contraction of the gallbladder and the excretion of bile. After the serotonin injection, there was a significant induction of apical sodium-dependent bile acid transporter expression, resulting in a decrease in the concentration of bile acids in the feces. Additionally, data are presented to show that the functions of serotonin are mediated through diverse serotonin receptor subtypes. These data indicate that peripheral serotonin accelerates the metabolism of lipid by increasing the concentration of bile acids in circulation.

Iaith wreiddiol	Saesneg
Tudalennau (o-i)	4776-4786
Nifer y tudalennau	11
Cyfnodolyn	Endocrinology
Cyfrol	151
Rhif cyhoeddi	10
Dyddiad ar-lein cynnar	04 Awst 2010
Dynodwyr Gwrthrych Digidol (DOIs)	https://doi.org/10.1210/en.2009-1349
Statws	Cyhoeddwyd - 01 Hyd 2010

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10.1210/en.2009-1349

http://hdl.handle.net/2160/6899

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@article{4dc63a6e5e934dfaa62519cb23dd9941,

title = "Peripheral serotonin enhances lipid metabolism by accelerating bile acid turnover",

abstract = "Serotonin is synthesized by two distinct tryptophan hydroxylases, one in the brain and one in the periphery. The latter is known to be unable to cross the blood-brain barrier. These two serotonin systems have apparently independent functions, although the functions of peripheral serotonin have yet to be fully elucidated. In this study, we have investigated the physiological effect of peripheral serotonin on the concentrations of metabolites in the circulation and in the liver. After fasting, mice were ip injected with 1 mg serotonin. The plasma glucose concentration was significantly elevated between 60 and 270 min after the injection. In contrast, plasma triglyceride, cholesterol, and nonesterified fatty acid concentrations were decreased. The hepatic glycogen synthesis and concentrations were significantly higher at 240 min. At the same time, the hepatic triglyceride content was significantly lower than the basal levels noted before the serotonin injection, whereas the hepatic cholesterol content was significantly higher by 60 min after the injection. Furthermore, serotonin stimulated the contraction of the gallbladder and the excretion of bile. After the serotonin injection, there was a significant induction of apical sodium-dependent bile acid transporter expression, resulting in a decrease in the concentration of bile acids in the feces. Additionally, data are presented to show that the functions of serotonin are mediated through diverse serotonin receptor subtypes. These data indicate that peripheral serotonin accelerates the metabolism of lipid by increasing the concentration of bile acids in circulation.",

author = "Hitoshi Watanabe and Daisuke Akasaka and Hideki Ogasawara and Kan Sato and Masato Miyake and Kazuki Saito and Yu Takahashi and Takashi Kanaya and Ikuro Takakura and Tetsuya Hondo and Guozheng Chao and Rose, {Michael Terence} and Shyuichi Ohwada and Kouichi Watanabe and Takahiro Yamaguchi and Hisashi Aso",

note = "Watanabe, H., Akasaka, D., Ogasawara, H., Sato, K., Miyake, M., Saito, K., Takahashi, Y., Kanaya, T., Takakura, I., Hondo, T., Chao, G., Rose, M. T., Ohwada, S., Watanabe, K., Yamaguchi, T., Aso, H. (2010). Peripheral serotonin enhances lipid metabolism by accelerating bile acid turnover. Endocrinology, 151, (10), 4776-4786. IMPF: 04.99 ",

year = "2010",

month = oct,

day = "1",

doi = "10.1210/en.2009-1349",

language = "English",

volume = "151",

pages = "4776--4786",

journal = "Endocrinology",

issn = "0013-7227",

publisher = "The Endocrine Society",

number = "10",

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TY - JOUR

T1 - Peripheral serotonin enhances lipid metabolism by accelerating bile acid turnover

AU - Watanabe, Hitoshi

AU - Akasaka, Daisuke

AU - Ogasawara, Hideki

AU - Sato, Kan

AU - Miyake, Masato

AU - Saito, Kazuki

AU - Takahashi, Yu

AU - Kanaya, Takashi

AU - Takakura, Ikuro

AU - Hondo, Tetsuya

AU - Chao, Guozheng

AU - Rose, Michael Terence

AU - Ohwada, Shyuichi

AU - Watanabe, Kouichi

AU - Yamaguchi, Takahiro

AU - Aso, Hisashi

N1 - Watanabe, H., Akasaka, D., Ogasawara, H., Sato, K., Miyake, M., Saito, K., Takahashi, Y., Kanaya, T., Takakura, I., Hondo, T., Chao, G., Rose, M. T., Ohwada, S., Watanabe, K., Yamaguchi, T., Aso, H. (2010). Peripheral serotonin enhances lipid metabolism by accelerating bile acid turnover. Endocrinology, 151, (10), 4776-4786. IMPF: 04.99

PY - 2010/10/1

Y1 - 2010/10/1

N2 - Serotonin is synthesized by two distinct tryptophan hydroxylases, one in the brain and one in the periphery. The latter is known to be unable to cross the blood-brain barrier. These two serotonin systems have apparently independent functions, although the functions of peripheral serotonin have yet to be fully elucidated. In this study, we have investigated the physiological effect of peripheral serotonin on the concentrations of metabolites in the circulation and in the liver. After fasting, mice were ip injected with 1 mg serotonin. The plasma glucose concentration was significantly elevated between 60 and 270 min after the injection. In contrast, plasma triglyceride, cholesterol, and nonesterified fatty acid concentrations were decreased. The hepatic glycogen synthesis and concentrations were significantly higher at 240 min. At the same time, the hepatic triglyceride content was significantly lower than the basal levels noted before the serotonin injection, whereas the hepatic cholesterol content was significantly higher by 60 min after the injection. Furthermore, serotonin stimulated the contraction of the gallbladder and the excretion of bile. After the serotonin injection, there was a significant induction of apical sodium-dependent bile acid transporter expression, resulting in a decrease in the concentration of bile acids in the feces. Additionally, data are presented to show that the functions of serotonin are mediated through diverse serotonin receptor subtypes. These data indicate that peripheral serotonin accelerates the metabolism of lipid by increasing the concentration of bile acids in circulation.

AB - Serotonin is synthesized by two distinct tryptophan hydroxylases, one in the brain and one in the periphery. The latter is known to be unable to cross the blood-brain barrier. These two serotonin systems have apparently independent functions, although the functions of peripheral serotonin have yet to be fully elucidated. In this study, we have investigated the physiological effect of peripheral serotonin on the concentrations of metabolites in the circulation and in the liver. After fasting, mice were ip injected with 1 mg serotonin. The plasma glucose concentration was significantly elevated between 60 and 270 min after the injection. In contrast, plasma triglyceride, cholesterol, and nonesterified fatty acid concentrations were decreased. The hepatic glycogen synthesis and concentrations were significantly higher at 240 min. At the same time, the hepatic triglyceride content was significantly lower than the basal levels noted before the serotonin injection, whereas the hepatic cholesterol content was significantly higher by 60 min after the injection. Furthermore, serotonin stimulated the contraction of the gallbladder and the excretion of bile. After the serotonin injection, there was a significant induction of apical sodium-dependent bile acid transporter expression, resulting in a decrease in the concentration of bile acids in the feces. Additionally, data are presented to show that the functions of serotonin are mediated through diverse serotonin receptor subtypes. These data indicate that peripheral serotonin accelerates the metabolism of lipid by increasing the concentration of bile acids in circulation.

U2 - 10.1210/en.2009-1349

DO - 10.1210/en.2009-1349

M3 - Article

C2 - 20685881

SN - 0013-7227

VL - 151

SP - 4776

EP - 4786

JO - Endocrinology

JF - Endocrinology

IS - 10

ER -

Peripheral serotonin enhances lipid metabolism by accelerating bile acid turnover

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