Warning: Undefined array key "mm" in /www/wwwroot/www.ai-bt.com/si.php on line 10 Deprecated: trim(): Passing null to parameter #1 ($string) of type string is deprecated in /www/wwwroot/www.ai-bt.com/si.php on line 10 NAD+-boosting therapy alleviates nonalcoholic fatty liver disease via stimulating a novel exerkine Fndc5/irisin.

Literature DB >> 33754067

NAD⁺-boosting therapy alleviates nonalcoholic fatty liver disease via stimulating a novel exerkine Fndc5/irisin.

Dong-Jie Li^1,2,3, Si-Jia Sun^2,3, Jiang-Tao Fu¹, Shen-Xi Ouyang^2,3, Qin-Jie Zhao⁴, Li Su⁵, Qing-Xi Ji^2,3, Di-Ynag Sun¹, Jia-Hui Zhu^2,3, Guo-Yan Zhang^2,3, Jia-Wei Ma^2,3, Xiu-Ting Lan^2,3, Yi Zhao^2,3, Jie Tong^2,3, Guo-Qiang Li^1,6, Fu-Ming Shen^2,3, Pei Wang^1,2,3.

Abstract

Rationale: Nicotinamide adenine dinucleotide+ (NAD+)-boosting therapy has emerged as a promising strategy to treat various health disorders, while the underlying molecular mechanisms are not fully understood. Here, we investigated the involvement of fibronectin type III domain containing 5 (Fndc5) or irisin, which is a novel exercise-linked hormone, in the development and progression of nonalcoholic fatty liver disease (NAFLD).
Methods: NAD+-boosting therapy was achieved by administrating of nicotinamide riboside (NR) in human and mice. The Fndc5/irisin levels in tissues and blood were measured in NR-treated mice or human volunteers. The therapeutic action of NR against NAFLD pathologies induced by high-fat diet (HFD) or methionine/choline-deficient diet (MCD) were compared between wild-type (WT) and Fndc5-/- mice. Recombinant Fndc5/irisin was infused to NALFD mice via osmotic minipump to test the therapeutic action of Fndc5/irisin. Various biomedical experiments were conducted in vivo and in vitro to know the molecular mechanisms underlying the stimulation of Fndc5/irisin by NR treatment.
Results: NR treatment elevated plasma level of Fndc5/irisin in mice and human volunteers. NR treatment also increased Fndc5 expression in skeletal muscle, adipose and liver tissues in mice. In HFD-induced NAFLD mice model, NR displayed remarkable therapeutic effects on body weight gain, hepatic steatosis, steatohepatitis, insulin resistance, mitochondrial dysfunction, apoptosis and fibrosis; however, these actions of NR were compromised in Fndc5-/- mice. Chronic infusion of recombinant Fndc5/irisin alleviated the NAFLD pathological phenotypes in MCD-induced NAFLD mice model. Mechanistically, NR reduced the lipid stress-triggered ubiquitination of Fndc5, which increased Fndc5 protein stability and thus enhanced Fndc5 protein level. Using shRNA-mediated knockdown screening, we found that NAD+-dependent deacetylase SIRT2, rather than other sirtuins, interacts with Fndc5 to decrease Fndc5 acetylation, which reduces Fndc5 ubiquitination and stabilize it. Treatment of AGK2, a selective inhibitor of SIRT2, blocked the therapeutic action of NR against NAFLD pathologies and NR-induced Fndc5 deubiquitination/deacetylation. At last, we identified that the lysine sites K127/131 and K185/187/189 of Fndc5 may contribute to the SIRT2-dependent deacetylation and deubiquitination of Fndc5. Conclusions: The findings from this research for the first time demonstrate that NAD+-boosting therapy reverses NAFLD by regulating SIRT2-deppendent Fndc5 deacetylation and deubiquitination, which results in a stimulation of Fndc5/irisin, a novel exerkine. These results suggest that Fndc5/irisin may be a potential nexus between physical exercise and NAD+-boosting therapy in metabolic pathophysiology. © The author(s).

Entities: CellLine Chemical Disease Gene Mutation Species

Keywords: Fndc5; NAD+; SIRT2; irisin; nonalcoholic fatty liver disease; physical exercise

Mesh：

Substances：

Year: 2021 PMID： 33754067 PMCID： PMC7977447 DOI： 10.7150/thno.53652

Source DB: PubMed Journal: Theranostics ISSN： 1838-7640 Impact factor: 11.556

75 in total

1. A comprehensive immunohistochemical examination of the distribution of the fat-burning protein irisin in biological tissues.

Authors: Suleyman Aydin; Tuncay Kuloglu; Suna Aydin; Mehmet Kalayci; Musa Yilmaz; Tolga Cakmak; Serdal Albayrak; Sami Gungor; Neriman Colakoglu; Ibrahim Hanifi Ozercan
Journal: Peptides Date: 2014-09-27 Impact factor: 3.750

2. Mitochondrial dysfunction precedes insulin resistance and hepatic steatosis and contributes to the natural history of non-alcoholic fatty liver disease in an obese rodent model.

Authors: R Scott Rector; John P Thyfault; Grace M Uptergrove; E Matthew Morris; Scott P Naples; Sarah J Borengasser; Catherine R Mikus; Matthew J Laye; M Harold Laughlin; Frank W Booth; Jamal A Ibdah
Journal: J Hepatol Date: 2010-03-04 Impact factor: 25.083

3. CD38 Dictates Age-Related NAD Decline and Mitochondrial Dysfunction through an SIRT3-Dependent Mechanism.

Authors: Juliana Camacho-Pereira; Mariana G Tarragó; Claudia C S Chini; Veronica Nin; Carlos Escande; Gina M Warner; Amrutesh S Puranik; Renee A Schoon; Joel M Reid; Antonio Galina; Eduardo N Chini
Journal: Cell Metab Date: 2016-06-14 Impact factor: 27.287

4. Hepatic NAD(+) deficiency as a therapeutic target for non-alcoholic fatty liver disease in ageing.

Authors: Can-Can Zhou; Xi Yang; Xia Hua; Jian Liu; Mao-Bing Fan; Guo-Qiang Li; Jie Song; Tian-Ying Xu; Zhi-Yong Li; Yun-Feng Guan; Pei Wang; Chao-Yu Miao
Journal: Br J Pharmacol Date: 2016-06-27 Impact factor: 8.739

5. A spontaneous mutation in the nicotinamide nucleotide transhydrogenase gene of C57BL/6J mice results in mitochondrial redox abnormalities.

Authors: Juliana A Ronchi; Tiago R Figueira; Felipe G Ravagnani; Helena C F Oliveira; Anibal E Vercesi; Roger F Castilho
Journal: Free Radic Biol Med Date: 2013-06-07 Impact factor: 7.376

6. Irisin inhibits hepatic gluconeogenesis and increases glycogen synthesis via the PI3K/Akt pathway in type 2 diabetic mice and hepatocytes.

Authors: Tong-Yan Liu; Chang-Xiang Shi; Run Gao; Hai-Jian Sun; Xiao-Qing Xiong; Lei Ding; Qi Chen; Yue-Hua Li; Jue-Jin Wang; Yu-Ming Kang; Guo-Qing Zhu
Journal: Clin Sci (Lond) Date: 2015-07-13 Impact factor: 6.124

7. Nicotinic ACh receptor α7 inhibits PDGF-induced migration of vascular smooth muscle cells by activating mitochondrial deacetylase sirtuin 3.

Authors: Dong-Jie Li; Jie Tong; Fei-Yan Zeng; Mengqi Guo; Yong-Hua Li; Hongbo Wang; Pei Wang
Journal: Br J Pharmacol Date: 2018-11-04 Impact factor: 8.739

8. A polymorphism in the Irisin-encoding gene (FNDC5) associates with hepatic steatosis by differential miRNA binding to the 3'UTR.

Authors: Mayada Metwally; Ali Bayoumi; Manuel Romero-Gomez; Khaled Thabet; Miya John; Leon A Adams; Xiaoqi Huo; Rocio Aller; Carmelo García-Monzón; María Teresa Arias-Loste; Elisabetta Bugianesi; Luca Miele; Rocio Gallego-Durán; Janett Fischer; Thomas Berg; Christopher Liddle; Liang Qiao; Jacob George; Mohammed Eslam
Journal: J Hepatol Date: 2018-10-31 Impact factor: 25.083

9. SRT1720 improves survival and healthspan of obese mice.

Authors: Robin K Minor; Joseph A Baur; Ana P Gomes; Theresa M Ward; Anna Csiszar; Evi M Mercken; Kotb Abdelmohsen; Yu-Kyong Shin; Carles Canto; Morten Scheibye-Knudsen; Melissa Krawczyk; Pablo M Irusta; Alejandro Martín-Montalvo; Basil P Hubbard; Yongqing Zhang; Elin Lehrmann; Alexa A White; Nathan L Price; William R Swindell; Kevin J Pearson; Kevin G Becker; Vilhelm A Bohr; Myriam Gorospe; Josephine M Egan; Mark I Talan; Johan Auwerx; Christoph H Westphal; James L Ellis; Zoltan Ungvari; George P Vlasuk; Peter J Elliott; David A Sinclair; Rafael de Cabo
Journal: Sci Rep Date: 2011-08-18 Impact factor: 4.379

10. Irisin alleviates liver ischemia-reperfusion injury by inhibiting excessive mitochondrial fission, promoting mitochondrial biogenesis and decreasing oxidative stress.

Authors: Jianbin Bi; Jia Zhang; Yifan Ren; Zhaoqing Du; Qingshan Li; Yue Wang; Shasha Wei; Lifei Yang; Jingyao Zhang; Chang Liu; Yi Lv; Rongqian Wu
Journal: Redox Biol Date: 2018-10-24 Impact factor: 11.799

12 in total

Review 1. Antioxidant Effects of Irisin in Liver Diseases: Mechanistic Insights.

Authors: Junzhou Zhao; Linlan Qiao; Jian Dong; Rongqian Wu
Journal: Oxid Med Cell Longev Date: 2022-01-07 Impact factor: 6.543

2. SIRT2-mediated deacetylation and deubiquitination of C/EBPβ prevents ethanol-induced liver injury.

Authors: Yingting Zhang; Xidai Long; Xin Ruan; Qian Wei; Lin Zhang; Lulu Wo; Dongdong Huang; Longshuai Lin; Difei Wang; Li Xia; Qinghua Zhao; Junling Liu; Qian Zhao; Ming He
Journal: Cell Discov Date: 2021-10-12 Impact factor: 10.849

3. BMPER alleviates ischemic brain injury by protecting neurons and inhibiting neuroinflammation via Smad3-Akt-Nrf2 pathway.

Authors: Peng Ding; Wei Chen; Xiaodi Yan; Jinxiang Zhang; Cheng Li; Guangming Zhang; Yongqiang Wang; Yonghua Li
Journal: CNS Neurosci Ther Date: 2021-12-14 Impact factor: 5.243

4. Postconditioning with Irisin Attenuates Lung Ischemia/Reperfusion Injury by Suppressing Ferroptosis via Induction of the Nrf2/HO-1 Signal Axis.

Authors: Yun Wang; Zhe Dong; Zongze Zhang; Yanlin Wang; Kun Yang; Xinyi Li
Journal: Oxid Med Cell Longev Date: 2022-03-02 Impact factor: 6.543

NAD⁺-boosting therapy alleviates nonalcoholic fatty liver disease via stimulating a novel exerkine Fndc5/irisin.

1. A comprehensive immunohistochemical examination of the distribution of the fat-burning protein irisin in biological tissues.

2. Mitochondrial dysfunction precedes insulin resistance and hepatic steatosis and contributes to the natural history of non-alcoholic fatty liver disease in an obese rodent model.

3. CD38 Dictates Age-Related NAD Decline and Mitochondrial Dysfunction through an SIRT3-Dependent Mechanism.

4. Hepatic NAD(+) deficiency as a therapeutic target for non-alcoholic fatty liver disease in ageing.

5. A spontaneous mutation in the nicotinamide nucleotide transhydrogenase gene of C57BL/6J mice results in mitochondrial redox abnormalities.

6. Irisin inhibits hepatic gluconeogenesis and increases glycogen synthesis via the PI3K/Akt pathway in type 2 diabetic mice and hepatocytes.

7. Nicotinic ACh receptor α7 inhibits PDGF-induced migration of vascular smooth muscle cells by activating mitochondrial deacetylase sirtuin 3.

8. A polymorphism in the Irisin-encoding gene (FNDC5) associates with hepatic steatosis by differential miRNA binding to the 3'UTR.

9. SRT1720 improves survival and healthspan of obese mice.

10. Irisin alleviates liver ischemia-reperfusion injury by inhibiting excessive mitochondrial fission, promoting mitochondrial biogenesis and decreasing oxidative stress.

Review 1. Antioxidant Effects of Irisin in Liver Diseases: Mechanistic Insights.

2. SIRT2-mediated deacetylation and deubiquitination of C/EBPβ prevents ethanol-induced liver injury.

3. BMPER alleviates ischemic brain injury by protecting neurons and inhibiting neuroinflammation via Smad3-Akt-Nrf2 pathway.

4. Postconditioning with Irisin Attenuates Lung Ischemia/Reperfusion Injury by Suppressing Ferroptosis via Induction of the Nrf2/HO-1 Signal Axis.

5. MicroRNA-665-3p exacerbates nonalcoholic fatty liver disease in mice.

6. Selective targeting of CD38 hydrolase and cyclase activity as an approach to immunostimulation.

Review 7. Balancing NAD⁺ deficits with nicotinamide riboside: therapeutic possibilities and limitations.

Review 8. Multiple Roles of SIRT2 in Regulating Physiological and Pathological Signal Transduction.

Review 9. Irisin-Associated Neuroprotective and Rehabilitative Strategies for Stroke.

Review 10. The Potential Role of Cellular Senescence in Non-Alcoholic Fatty Liver Disease.

Review 1. Antioxidant Effects of Irisin in Liver Diseases: Mechanistic Insights.

Review 7. Balancing NAD+ deficits with nicotinamide riboside: therapeutic possibilities and limitations.

Review 8. Multiple Roles of SIRT2 in Regulating Physiological and Pathological Signal Transduction.

Review 9. Irisin-Associated Neuroprotective and Rehabilitative Strategies for Stroke.

Review 10. The Potential Role of Cellular Senescence in Non-Alcoholic Fatty Liver Disease.

Review 7. Balancing NAD⁺ deficits with nicotinamide riboside: therapeutic possibilities and limitations.