Serotonin signals through a gut-liver axis to regulate hepatic steatosis

Choi, Wonsuk; Namkung, Jun; Hwang, Inseon; Kim, Hyeongseok; Lim, Ajin; Park, Hye Jung; Lee, Hye Won; Han, Kwang Hyub; Park, Seongyeol; Jeong, Ji Seon; Bang, Geul; Kim, Young Hwan; Yadav, Vijay K.; Karsenty, G.; Ju, Young Seok; Choi, Chan; Suh, Jae Myoung; Park, Jun Yong; Park, Sang-Kyu; Kim, Hail

doi:10.1038/s41467-018-07287-7

Cited by 108 publications

(132 citation statements)

References 46 publications

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“…High fat fed mice have increased levels of 5-HT in serum 76 and in BAT, 54 and inhibition of peripheral 5-HT synthesis reduces their adiposity, metabolic dysfunction, 54,77 and hepatic steatosis. 78 This effect was at least partially attributed to increased β3-adrenergic induction of UCP1mediated, BAT thermogenesis. 54 BAT SNA is impaired in rats maintained chronically on a high fat diet, 79,80 similar to the reduction in BAT thermogenesis in obese humans.…”

Section: Discussionmentioning

confidence: 99%

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Systemic serotonin inhibits brown adipose tissue sympathetic nerve activity via a GABA input to the dorsomedial hypothalamus, not via 5HT_1A receptor activation in raphe pallidus

et al. 2019

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Aim Serotonin (5‐hydroxytryptamine, 5‐HT), an important neurotransmitter and hormone, modulates many physiological functions including body temperature. We investigated neural mechanisms involved in the inhibition of brown adipose tissue (BAT) sympathetic nerve activity (SNA) and BAT thermogenesis evoked by 5‐HT. Methods Electrophysiological recordings, intravenous (iv) injections and nanoinjections in the brains of anaesthetized rats. Results Cooling‐evoked increases in BAT SNA were inhibited by the intra‐rostral raphé pallidus (rRPa) and the iv administration of the 5‐HT1A receptor agonist, 8‐OH‐DPAT or 5‐HT. The intra‐rRPa 5‐HT, the intra‐rRPa and the iv 8‐OH‐DPAT, but not the iv 5‐HT‐induced inhibition of BAT SNA were prevented by nanoinjection of a 5‐HT1A receptor antagonist in the rRPa. The increase in BAT SNA evoked by nanoinjection of NMDA in the rRPa was not inhibited by iv 5‐HT, indicating that iv 5‐HT does not inhibit BAT SNA by acting in the rRPa or in the sympathetic pathway distal to the rRPa. In contrast, under a warm condition, blockade of 5HT1A receptors in the rRPa increased BAT SNA and BAT thermogenesis, suggesting that endogenous 5‐HT in the rRPa contributes to the suppression of BAT SNA and BAT thermogenesis. The increases in BAT SNA and BAT thermogenesis evoked by nanoinjection of NMDA in the dorsomedial hypothalamus (DMH) were inhibited by iv 5‐HT, but those following bicuculline nanoinjection in the DMH were not inhibited. Conclusions The systemic 5‐HT‐induced inhibition of BAT SNA requires a GABAergic inhibition of BAT sympathoexcitatory neurones in the DMH. In addition, during warming, 5‐HT released endogenously in rRPa inhibits BAT SNA.

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Section: Discussionmentioning

confidence: 99%

“…High fat fed mice have increased levels of 5‐HT in serum and in BAT, and inhibition of peripheral 5‐HT synthesis reduces their adiposity, metabolic dysfunction, and hepatic steatosis . This effect was at least partially attributed to increased β3‐adrenergic induction of UCP1‐mediated, BAT thermogenesis .…”

Section: Discussionmentioning

confidence: 99%

Systemic serotonin inhibits brown adipose tissue sympathetic nerve activity via a GABA input to the dorsomedial hypothalamus, not via 5HT_1A receptor activation in raphe pallidus

et al. 2019

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“…Choi et al [65] demonstrated that the portal blood serotonin concentrations are selectively increased by high-fat diet feeding in mice, and they have endocrine effects on the liver. In fact, nutrient infusion induces 5-HT production in the human gut while the liver is the first organ to encounter gut-derived serotonin via the portal vein.…”

Section: Gut-microbiota and Serotonin Metabolismmentioning

confidence: 99%

The Relationship Between the Serotonin Metabolism, Gut-Microbiota and the Gut-Brain Axis

Stasi

Sadalla

Milani

2019

CDM

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Background:: Serotonin (5-HT) has a pleiotropic function in gastrointestinal, neurological/psychiatric and liver diseases. The aim of this review was to elucidate whether the gut-microbiota played a critical role in regulating peripheral serotonin levels. Methods:: We searched for relevant studies published in English using the PubMed database from 1993 to the present. Results: : Several studies suggested that alterations in the gut-microbiota may contribute to a modulation of serotonin signalling. The first indication regarded the changes in the composition of the commensal bacteria and the intestinal transit time caused by antibiotic treatment. The second indication regarded the changes in serotonin levels correlated to specific bacteria. The third indication regarded the fact that decreased serotonin transporter expression was associated with a shift in gut-microbiota from homeostasis to inflammatory type microbiota. Serotonin plays a key role in the regulation of visceral pain, secretion, and initiation of the peristaltic reflex; however, its altered levels are also detected in many different psychiatric disorders. Symptoms of some gastrointestinal functional disorders may be due to deregulation in central nervous system activity, dysregulation at the peripheral level (intestine), or a combination of both (brain-gut axis) by means of neuro-endocrine-immune stimuli. Moreover, several studies have demonstrated the profibrogenic role of 5-HT in the liver, showing that it works synergistically with platelet-derived growth factor in stimulating hepatic stellate cell proliferation. Conclusion:: Although the specific interaction mechanisms are still unclear, some studies have suggested that there is a correlation between the gut-microbiota, some gastrointestinal and liver diseases and the serotonin metabolism.

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“…У роботі J. Namkung et al за допомогою генетичних і фармакологічних моделей інгібування серотоніну у мишей досліджувались функціональні зв'язки між стеатозом печінки і гормоном. Було показано, що серотонін має прямий вплив на накопичення ліпідів в печінці, а пригнічення його синтезу в кишечнику полегшує прояви стеатозу печінки [28,29]. Однак, досліджень в цьому напрямку у людей ще [30].…”

Section: серотонінunclassified

“…Отже, збільшення рівня гормону в ЦНС сприяє зменшенню споживання їжі і маси тіла, а гіперпродукція серотоніну в кишечнику, як вважають, призводить до ожиріння [27]. У дослідженнях на мишах концентра ція серотоніну в портальній вені підвищувалася при харчуванні продуктами з високим вмістом жиру [28]. У роботі A. Ojeda-Rodríguez et.…”

Section: серотонінunclassified

Influence of Gastrointestinal Hormones on the Development of Obesity and Non-Alcoholic Fatty Liver Disease in Children

Parkhomenko¹,

Strashok²,

Khomenko³

2019

PEP

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Obesity is becoming a global epidemic among children, and the social significance of this problem is determined by the threat of disability of young patients, reducing life expectancy and the development of severe comorbidities. As a result of the increasing number of studies on energy homeostasis, it has been suggested that obesity is a multifactorial and more complex disease than previously thought. In recent years, the attention of researchers is increasingly attracted to the study of intestinal microbiota and its impact on human health, due to the development of new technologies and methods of studying the microbiome. Recent studies have shown that there is a mutual influence of the brain and intestines on each other, and there is increasing evidence that confirms the role of this complex relationship in the regulation of hunger, satiation and energy balance. It is proved that there is a direct impact on these processes of intestinal microbiota, and mediated through its intervention in the synthesis and metabolism of hormones and biologically active compounds of the digestive system. Today it is known that the gastrointestinal tract is one of the human organs where the most hormones are synthesized. At the present stage of development of science, it is known that there are more than 30 gastrointestinal hormones and biologically active substances that regulate the processes of digestion and participate in the regulation of general homeostasis. The most important role in the development of obesity and non-alcoholic fatty liver disease belongs to hormones such as ghrelin, peptide YY and glucagon-like peptide 1. The literature review presents current data that demonstrate the role of gastrointestinal hormones in the formation and development of obesity and non-alcoholic fatty liver disease in children as well as data of own research.

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Serotonin signals through a gut-liver axis to regulate hepatic steatosis

Cited by 108 publications

References 46 publications

Systemic serotonin inhibits brown adipose tissue sympathetic nerve activity via a GABA input to the dorsomedial hypothalamus, not via 5HT_1A receptor activation in raphe pallidus

Systemic serotonin inhibits brown adipose tissue sympathetic nerve activity via a GABA input to the dorsomedial hypothalamus, not via 5HT_1A receptor activation in raphe pallidus

The Relationship Between the Serotonin Metabolism, Gut-Microbiota and the Gut-Brain Axis

Influence of Gastrointestinal Hormones on the Development of Obesity and Non-Alcoholic Fatty Liver Disease in Children

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Serotonin signals through a gut-liver axis to regulate hepatic steatosis

Cited by 108 publications

References 46 publications

Systemic serotonin inhibits brown adipose tissue sympathetic nerve activity via a GABA input to the dorsomedial hypothalamus, not via 5HT1A receptor activation in raphe pallidus

Systemic serotonin inhibits brown adipose tissue sympathetic nerve activity via a GABA input to the dorsomedial hypothalamus, not via 5HT1A receptor activation in raphe pallidus

The Relationship Between the Serotonin Metabolism, Gut-Microbiota and the Gut-Brain Axis

Influence of Gastrointestinal Hormones on the Development of Obesity and Non-Alcoholic Fatty Liver Disease in Children

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Product

Resources

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Systemic serotonin inhibits brown adipose tissue sympathetic nerve activity via a GABA input to the dorsomedial hypothalamus, not via 5HT_1A receptor activation in raphe pallidus

Systemic serotonin inhibits brown adipose tissue sympathetic nerve activity via a GABA input to the dorsomedial hypothalamus, not via 5HT_1A receptor activation in raphe pallidus