Fibroblast growth factor signaling in non-alcoholic fatty liver disease and non-alcoholic steatohepatitis: Paving the way to hepatocellular carcinoma

被引:14
作者
Ocker, Matthias [1 ]
机构
[1] Charite Univ Med Berlin, Dept Gastroenterol CBF, D-10117 Berlin, Germany
来源
WORLD JOURNAL OF GASTROENTEROLOGY | 2020年 / 26卷 / 03期
关键词
Fibroblast growth factor; Fibroblast growth factor receptor; Non-alcoholic fatty liver disease; Non-alcoholic steatohepatitis; Fibrosis; Cirrhosis; Hepatocellular carcinoma; SERUM FGF21 LEVELS; FACTOR RECEPTOR 4; AMERICAN ASSOCIATION; INSULIN SENSITIVITY; HEPATIC STEATOSIS; UP-REGULATION; PROGRESSION; FGF19; EXPRESSION; INCREASES;
D O I
10.3748/wjg.v26.i3.279
中图分类号
R57 [消化系及腹部疾病];
学科分类号
摘要
Metabolic disorders are increasingly leading to non-alcoholic fatty liver disease, subsequent steatohepatitis, cirrhosis and hepatocellular carcinoma. Fibroblast growth factors and their receptors play an important role in maintaining metabolic homeostasis also in the liver and disorders in signaling have been identified to contribute to those pathophysiologic conditions leading to hepatic lipid accumulation and chronic inflammation. While specific and well tolerated inhibitors of fibroblast growth factor receptor activity are currently developed for (non-liver) cancer therapy, treatment of non-alcoholic fatty liver disease and non-alcoholic steatohepatitis is still limited. Fibroblast growth factor-mimicking or restoring approaches have recently evolved as a novel therapeutic option and the impact of such interactions with the fibroblast growth factor receptor signaling network during non-alcoholic fatty liver disease/non-alcoholic steatohepatitis development is reviewed here.
引用
收藏
页码:279 / 290
页数:12
相关论文
共 116 条
[1]   The breadth of FGF21's metabolic actions are governed by FGFR1 in adipose tissue [J].
Adams, Andrew C. ;
Yang, Chaofeng ;
Coskun, Tamer ;
Cheng, Christine C. ;
Gimeno, Ruth E. ;
Luo, Yongde ;
Kharitonenkov, Alexei .
MOLECULAR METABOLISM, 2013, 2 (01) :31-37
[2]   The Burden of Primary Liver Cancer and Underlying Etiologies From 1990 to 2015 at the Global, Regional, and National Level Results From the Global Burden of Disease Study 2015 [J].
Akinyemiju, Tomi ;
Abera, Semaw ;
Ahmed, Muktar ;
Alam, Noore ;
Alemayohu, Mulubirhan Assefa ;
Allen, Christine ;
Al-Raddadi, Rajaa ;
Alvis-Guzman, Nelson ;
Amoako, Yaw ;
Artaman, Al ;
Ayele, Tadesse Awoke ;
Barac, Aleksandra ;
Bensenor, Isabela ;
Berhane, Adugnaw ;
Bhutta, Zulfiqar ;
Castillo-Rivas, Jacqueline ;
Chitheer, Abdulaal ;
Choi, Jee-Young ;
Cowie, Benjamin ;
Dandona, Lalit ;
Dandona, Rakhi ;
Dey, Subhojit ;
Dicker, Daniel ;
Phuc, Huyen ;
Ekwueme, Donatus U. ;
Zaki, Maysaa El Sayed ;
Fischer, Florian ;
Furst, Thomas ;
Hancock, Jamie ;
Hay, Simon I. ;
Hotez, Peter ;
Jee, Sun Ha ;
Kasaeian, Amir ;
Khader, Yousef ;
Khang, Young-Ho ;
Kumar, G. Anil ;
Kutz, Michael ;
Larson, Heidi ;
Lopez, Alan ;
Lunevicius, Raimundas ;
Malekzadeh, Reza ;
McAlinden, Colm ;
Meier, Toni ;
Mendoza, Walter ;
Mokdad, Ali ;
Moradi-Lakeh, Maziar ;
Nagel, Gabriele ;
Nguyen, Quyen ;
Nguyen, Grant ;
Ogbo, Felix .
JAMA ONCOLOGY, 2017, 3 (12) :1683-1691
[3]   Fibroblast growth factor 15/19 (FGF15/19) protects from diet-induced hepatic steatosis: development of an FGF19-based chimeric molecule to promote fatty liver regeneration [J].
Alvarez-Sola, Gloria ;
Uriarte, Iker ;
Ujue Latasa, M. ;
Fernandez-Barrena, Maite G. ;
Urtasun, Raquel ;
Elizalde, Maria ;
Barcena-Varela, Marina ;
Jimenez, Maddalen ;
Chang, Haisul C. ;
Barbero, Roberto ;
Catalan, Victoria ;
Rodriguez, Amaia ;
Fruhbeck, Gema ;
Gallego-Escuredo, Jose M. ;
Gavalda-Navarr, Aleix ;
Villarroya, Francesc ;
Rodriguez-Ortigosa, Carlos M. ;
Corrales, Fernando J. ;
Prieto, Jesus ;
Berraondo, Pedro ;
Berasain, Carmen ;
Avila, Matias A. .
GUT, 2017, 66 (10) :1818-1828
[4]   Dietary fructose as a risk factor for non-alcoholic fatty liver disease (NAFLD) [J].
Alwahsh, Salamah Mohammad ;
Gebhardt, Rolf .
ARCHIVES OF TOXICOLOGY, 2017, 91 (04) :1545-1563
[5]   Expression and function of fibroblast growth factor (FGF) 9 in hepatic stellate cells and its role in toxic liver injury [J].
Antoine, Marianne ;
Wirz, Werner ;
Tag, Carmen G. ;
Gressner, Axel M. ;
Marvituna, Meltem ;
Wycislo, Mathias ;
Hellerbrand, Claus ;
Kiefer, Paul .
BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 2007, 361 (02) :335-341
[6]   A long-acting FGF21 alleviates hepatic steatosis and inflammation in a mouse model of non-alcoholic steatohepatitis partly through an FGF21-adiponectin-IL17A pathway [J].
Bao, Lichen ;
Yin, Jun ;
Gao, Wen ;
Wang, Qun ;
Yao, Wenbing ;
Gao, Xiangdong .
BRITISH JOURNAL OF PHARMACOLOGY, 2018, 175 (16) :3379-3393
[7]   The FGF family: biology, pathophysiology and therapy [J].
Beenken, Andrew ;
Mohammadi, Moosa .
NATURE REVIEWS DRUG DISCOVERY, 2009, 8 (03) :235-253
[8]   Fibroblast growth factor 10 is critical for liver growth during embryogenesis and controls hepatoblast survival via β-catenin activation [J].
Berg, Tove ;
Rountree, C. Bart ;
Lee, Lily ;
Estrada, Joaquin ;
Sala, Frederic G. ;
Choe, Andrea ;
Veltmaat, Jacqueline M. ;
De langhe, Stijn ;
Lee, Rene ;
Tsukamoto, Hide ;
Crooks, Gay M. ;
Befusci, Saverio ;
Wang, Kasper S. .
HEPATOLOGY, 2007, 46 (04) :1187-1197
[9]   FGF21 regulates metabolism and circadian behavior by acting on the nervous system [J].
Bookout, Angie L. ;
de Groot, Marleen H. M. ;
Owen, Bryn M. ;
Lee, Syann ;
Gautron, Laurent ;
Lawrence, Heather L. ;
Ding, Xunshan ;
Elmquist, Joel K. ;
Takahashi, Joseph S. ;
Mangelsdorf, David J. ;
Kliewer, Steven A. .
NATURE MEDICINE, 2013, 19 (09) :1147-1152
[10]   An FGF response pathway that mediates hepatic gene induction in embryonic endoderm cells [J].
Calmont, Amelie ;
Wandzioch, Ewa ;
Tremblay, Kimberly D. ;
Minowada, George ;
Kaestner, Klaus H. ;
Martin, Gail R. ;
Zaret, Kenneth S. .
DEVELOPMENTAL CELL, 2006, 11 (03) :339-348
12345678910