L‐citrulline inhibits body weight gain and hepatic fat accumulation by improving lipid metabolism in a rat nonalcoholic fatty liver disease model

L‐citrulline inhibits body weight gain and hepatic fat accumulation by improving lipid metabolism in a rat nonalcoholic fatty liver disease model

Abstract Background Body weight gain is a social issue all over the world. When body weight increased, hepatic fat accumulation also increased and it causes fatty liver disease. Therefore, developing a new treatment method and elucidating its mechanism is necessary. L‐citrulline (L‐Cit) is a free am...

Full description

Bibliographic Details
Main Authors: Maya Kudo, Yoshie Yamagishi, Shiori Suguro, Masaaki Nishihara, Hisae Yoshitomi, Misa Hayashi, Ming Gao
Format: Article
Language:English
Published: Wiley 2021-09-01
Series:Food Science & Nutrition
Subjects:
fibrogenesis
hepatic steatosis
L‐citrulline
nonalcoholic fatty liver disease
stroke‐prone spontaneously hypertensive 5/Dmcr
Online Access:https://doi.org/10.1002/fsn3.2439
id doaj-870123373a3742eea2f0c870d77de769
record_format Article
spelling doaj-870123373a3742eea2f0c870d77de7692021-09-15T07:28:34ZengWileyFood Science & Nutrition2048-71772021-09-01994893490410.1002/fsn3.2439L‐citrulline inhibits body weight gain and hepatic fat accumulation by improving lipid metabolism in a rat nonalcoholic fatty liver disease modelMaya Kudo0Yoshie Yamagishi1Shiori Suguro2Masaaki Nishihara3Hisae Yoshitomi4Misa Hayashi5Ming Gao6School of Pharmaceutical Science Mukogawa Women’s University Nishinomiya JapanProtein Chemical Co., Ltd. Tokyo JapanProtein Chemical Co., Ltd. Tokyo JapanProtein Chemical Co., Ltd. Tokyo JapanSchool of Pharmaceutical Science Mukogawa Women’s University Nishinomiya JapanSchool of Pharmaceutical Science Mukogawa Women’s University Nishinomiya JapanSchool of Pharmaceutical Science Mukogawa Women’s University Nishinomiya JapanAbstract Background Body weight gain is a social issue all over the world. When body weight increased, hepatic fat accumulation also increased and it causes fatty liver disease. Therefore, developing a new treatment method and elucidating its mechanism is necessary. L‐citrulline (L‐Cit) is a free amino acid found mainly in watermelon. No reports regarding its effects on the improvement of hepatic steatosis and fibrogenesis are currently available. The aim of this study was to clarify the effect and the mechanism of L‐Cit on inhibition of body weight gain and hepatic fat accumulation in high‐fat and high‐cholesterol fed SHRSP5/Dmcr rats. Methods L‐Cit or water (controls) was administered to six‐week‐old male SHRSP5/Dmcr rats by gavage for nine weeks. We recorded the level of body weight and food intake while performing the administration and sacrificed rats. After that, the blood and lipid metabolism‐related organs and tissues were collected and analyzed. Results L‐Cit treatment reduced body weight gain and hepatic TC and TG levels, and serum levels of AST and ALT. L‐Cit enhanced AMPK, LKB1, PKA, and hormone‐sensitive lipase (HSL) protein phosphorylation levels in the epididymal fat. L‐Cit treatment improved steatosis as revealed by HE staining of liver tissues and enhanced AMPK and LKB1 phosphorylation levels. Moreover, activation of Sirt1 was higher, while the liver fatty acid synthase (FAS) level was lower. Azan staining of liver sections revealed a reduction in fibrogenesis following L‐Cit treatment. Further, the liver levels of TGF‐β, Smad2/3, and α‐SMA, fibrogenesis‐related proteins and genes, were lower in the L‐Cit‐treated group. Conclusions From the results of analysis of the epididymal fat and the liver, L‐Cit inhibits body weight gain and hepatic fat accumulation by activating lipid metabolism and promoting fatty acid β‐oxidation in SHRSP5/Dmcr rats.https://doi.org/10.1002/fsn3.2439fibrogenesishepatic steatosisL‐citrullinenonalcoholic fatty liver diseasestroke‐prone spontaneously hypertensive 5/Dmcr
collection DOAJ
language English
format Article
sources DOAJ
author Maya Kudo
Yoshie Yamagishi
Shiori Suguro
Masaaki Nishihara
Hisae Yoshitomi
Misa Hayashi
Ming Gao
spellingShingle Maya Kudo
Yoshie Yamagishi
Shiori Suguro
Masaaki Nishihara
Hisae Yoshitomi
Misa Hayashi
Ming Gao
L‐citrulline inhibits body weight gain and hepatic fat accumulation by improving lipid metabolism in a rat nonalcoholic fatty liver disease model
Food Science & Nutrition
fibrogenesis
hepatic steatosis
L‐citrulline
nonalcoholic fatty liver disease
stroke‐prone spontaneously hypertensive 5/Dmcr
author_facet Maya Kudo
Yoshie Yamagishi
Shiori Suguro
Masaaki Nishihara
Hisae Yoshitomi
Misa Hayashi
Ming Gao
author_sort Maya Kudo
title L‐citrulline inhibits body weight gain and hepatic fat accumulation by improving lipid metabolism in a rat nonalcoholic fatty liver disease model
title_short L‐citrulline inhibits body weight gain and hepatic fat accumulation by improving lipid metabolism in a rat nonalcoholic fatty liver disease model
title_full L‐citrulline inhibits body weight gain and hepatic fat accumulation by improving lipid metabolism in a rat nonalcoholic fatty liver disease model
title_fullStr L‐citrulline inhibits body weight gain and hepatic fat accumulation by improving lipid metabolism in a rat nonalcoholic fatty liver disease model
title_full_unstemmed L‐citrulline inhibits body weight gain and hepatic fat accumulation by improving lipid metabolism in a rat nonalcoholic fatty liver disease model
title_sort l‐citrulline inhibits body weight gain and hepatic fat accumulation by improving lipid metabolism in a rat nonalcoholic fatty liver disease model
publisher Wiley
series Food Science & Nutrition
issn 2048-7177
publishDate 2021-09-01
description Abstract Background Body weight gain is a social issue all over the world. When body weight increased, hepatic fat accumulation also increased and it causes fatty liver disease. Therefore, developing a new treatment method and elucidating its mechanism is necessary. L‐citrulline (L‐Cit) is a free amino acid found mainly in watermelon. No reports regarding its effects on the improvement of hepatic steatosis and fibrogenesis are currently available. The aim of this study was to clarify the effect and the mechanism of L‐Cit on inhibition of body weight gain and hepatic fat accumulation in high‐fat and high‐cholesterol fed SHRSP5/Dmcr rats. Methods L‐Cit or water (controls) was administered to six‐week‐old male SHRSP5/Dmcr rats by gavage for nine weeks. We recorded the level of body weight and food intake while performing the administration and sacrificed rats. After that, the blood and lipid metabolism‐related organs and tissues were collected and analyzed. Results L‐Cit treatment reduced body weight gain and hepatic TC and TG levels, and serum levels of AST and ALT. L‐Cit enhanced AMPK, LKB1, PKA, and hormone‐sensitive lipase (HSL) protein phosphorylation levels in the epididymal fat. L‐Cit treatment improved steatosis as revealed by HE staining of liver tissues and enhanced AMPK and LKB1 phosphorylation levels. Moreover, activation of Sirt1 was higher, while the liver fatty acid synthase (FAS) level was lower. Azan staining of liver sections revealed a reduction in fibrogenesis following L‐Cit treatment. Further, the liver levels of TGF‐β, Smad2/3, and α‐SMA, fibrogenesis‐related proteins and genes, were lower in the L‐Cit‐treated group. Conclusions From the results of analysis of the epididymal fat and the liver, L‐Cit inhibits body weight gain and hepatic fat accumulation by activating lipid metabolism and promoting fatty acid β‐oxidation in SHRSP5/Dmcr rats.
topic fibrogenesis
hepatic steatosis
L‐citrulline
nonalcoholic fatty liver disease
stroke‐prone spontaneously hypertensive 5/Dmcr
url https://doi.org/10.1002/fsn3.2439
work_keys_str_mv AT mayakudo lcitrullineinhibitsbodyweightgainandhepaticfataccumulationbyimprovinglipidmetabolisminaratnonalcoholicfattyliverdiseasemodel
AT yoshieyamagishi lcitrullineinhibitsbodyweightgainandhepaticfataccumulationbyimprovinglipidmetabolisminaratnonalcoholicfattyliverdiseasemodel
AT shiorisuguro lcitrullineinhibitsbodyweightgainandhepaticfataccumulationbyimprovinglipidmetabolisminaratnonalcoholicfattyliverdiseasemodel
AT masaakinishihara lcitrullineinhibitsbodyweightgainandhepaticfataccumulationbyimprovinglipidmetabolisminaratnonalcoholicfattyliverdiseasemodel
AT hisaeyoshitomi lcitrullineinhibitsbodyweightgainandhepaticfataccumulationbyimprovinglipidmetabolisminaratnonalcoholicfattyliverdiseasemodel
AT misahayashi lcitrullineinhibitsbodyweightgainandhepaticfataccumulationbyimprovinglipidmetabolisminaratnonalcoholicfattyliverdiseasemodel
AT minggao lcitrullineinhibitsbodyweightgainandhepaticfataccumulationbyimprovinglipidmetabolisminaratnonalcoholicfattyliverdiseasemodel
_version_ 1717379239259406336

Similar Items