Hepatic Krüppel-like factor 16 (KLF16) targets PPARα to improve steatohepatitis and insulin resistance

Nannan Sun; Chuangpeng Shen; Lei Zhang; Xiaojie Wu; Yuanyuan Yu; Xiaoying Yang; Chen Yang; Chong Zhong; Zhao Gao; Wei Miao; Zehong Yang; Weihang Gao; Ling Hu; Kevin Williams; Changhui Liu; Yongsheng Chang; Yong Gao

doi:10.1136/gutjnl-2020-321774

Hepatic Krüppel-like factor 16 (KLF16) targets PPARα to improve steatohepatitis and insulin resistance

Nannan Sun, Chuangpeng Shen, Lei Zhang, Xiaojie Wu, Yuanyuan Yu, Xiaoying Yang, Chen Yang, Chong Zhong, Zhao Gao, Wei Miao, Zehong Yang, Weihang Gao, Ling Hu, Kevin Williams, Changhui Liu, Yongsheng Chang, Yong Gao

Research output: Contribution to journal › Article › peer-review

36 Scopus citations

Abstract

Objective Impaired hepatic fatty acids oxidation results in lipid accumulation and redox imbalance, promoting the development of fatty liver diseases and insulin resistance. However, the underlying pathogenic mechanism is poorly understood. Krüppel-like factor 16 (KLF16) is a transcription factor that abounds in liver. We explored whether and by what mechanisms KLF16 affects hepatic lipid catabolism to improve hepatosteatosis and insulin resistance. Design KLF16 expression was determined in patients with non-alcoholic fatty liver disease (NAFLD) and mice models. The role of KLF16 in the regulation of lipid metabolism was investigated using hepatocyte-specific KLF16-deficient mice fed a high-fat diet (HFD) or using an adenovirus/adeno-associated virus to alter KLF16 expression in mouse primary hepatocytes (MPHs) and in vivo livers. RNA-seq, luciferase reporter gene assay and ChIP analysis served to explore the molecular mechanisms involved. Results KLF16 expression was decreased in patients with NAFLD, mice models and oleic acid and palmitic acid (OA and PA) cochallenged hepatocytes. Hepatic KLF16 knockout impaired fatty acid oxidation, aggravated mitochondrial stress, ROS burden, advancing hepatic steatosis and insulin resistance. Conversely, KLF16 overexpression reduced lipid deposition and improved insulin resistance via directly binding the promoter of peroxisome proliferator-activated receptor α (PPARα) to accelerate fatty acids oxidation and attenuate mitochondrial stress, oxidative stress in db/db and HFD mice. PPARα deficiency diminished the KLF16-evoked protective effects against lipid deposition in MPHs. Hepatic-specific PPARα overexpression effectively rescued KLF16 deficiency-induced hepatic steatosis, altered redox balance and insulin resistance. Conclusions These findings prove that a direct KLF16-PPARα pathway closely links hepatic lipid homeostasis and redox balance, whose dysfunction promotes insulin resistance and hepatic steatosis.

Original language	English (US)
Pages (from-to)	2183-2195
Number of pages	13
Journal	Gut
Volume	70
Issue number	11
DOIs	https://doi.org/10.1136/gutjnl-2020-321774
State	Published - Nov 1 2021

Keywords

Fatty liver
Lipid metabolism
Nonalcoholic steatohepatitis

ASJC Scopus subject areas

Gastroenterology

Access to Document

10.1136/gutjnl-2020-321774

Cite this

@article{8d2fcef59d334e298798bb695c307e72,

title = "Hepatic Kr{\"u}ppel-like factor 16 (KLF16) targets PPARα to improve steatohepatitis and insulin resistance",

abstract = "Objective Impaired hepatic fatty acids oxidation results in lipid accumulation and redox imbalance, promoting the development of fatty liver diseases and insulin resistance. However, the underlying pathogenic mechanism is poorly understood. Kr{\"u}ppel-like factor 16 (KLF16) is a transcription factor that abounds in liver. We explored whether and by what mechanisms KLF16 affects hepatic lipid catabolism to improve hepatosteatosis and insulin resistance. Design KLF16 expression was determined in patients with non-alcoholic fatty liver disease (NAFLD) and mice models. The role of KLF16 in the regulation of lipid metabolism was investigated using hepatocyte-specific KLF16-deficient mice fed a high-fat diet (HFD) or using an adenovirus/adeno-associated virus to alter KLF16 expression in mouse primary hepatocytes (MPHs) and in vivo livers. RNA-seq, luciferase reporter gene assay and ChIP analysis served to explore the molecular mechanisms involved. Results KLF16 expression was decreased in patients with NAFLD, mice models and oleic acid and palmitic acid (OA and PA) cochallenged hepatocytes. Hepatic KLF16 knockout impaired fatty acid oxidation, aggravated mitochondrial stress, ROS burden, advancing hepatic steatosis and insulin resistance. Conversely, KLF16 overexpression reduced lipid deposition and improved insulin resistance via directly binding the promoter of peroxisome proliferator-activated receptor α (PPARα) to accelerate fatty acids oxidation and attenuate mitochondrial stress, oxidative stress in db/db and HFD mice. PPARα deficiency diminished the KLF16-evoked protective effects against lipid deposition in MPHs. Hepatic-specific PPARα overexpression effectively rescued KLF16 deficiency-induced hepatic steatosis, altered redox balance and insulin resistance. Conclusions These findings prove that a direct KLF16-PPARα pathway closely links hepatic lipid homeostasis and redox balance, whose dysfunction promotes insulin resistance and hepatic steatosis.",

keywords = "Fatty liver, Lipid metabolism, Nonalcoholic steatohepatitis",

author = "Nannan Sun and Chuangpeng Shen and Lei Zhang and Xiaojie Wu and Yuanyuan Yu and Xiaoying Yang and Chen Yang and Chong Zhong and Zhao Gao and Wei Miao and Zehong Yang and Weihang Gao and Ling Hu and Kevin Williams and Changhui Liu and Yongsheng Chang and Yong Gao",

note = "Funding Information: This work was supported by the National Natural Science Foundation of China (grant nos. 81800738, 81773969, 81102883, 81800718 and 82070891), the first-class discipline construction major project of Guangzhou University of Chinese Medicine (Guangzhou University of Chinese Medicine Planning (2018, No. 6), Guangzhou University of Chinese Medicine Planning (2019, No. 5)), the Guangdong Science and Technology Collaborative Innovation Center for Sport Science (2019B110210004), the Natural Science Foundation of the Jiangsu Higher Education Institutions of China (No. 18KJB310015), the Jiangsu Shuangchuang Programme and the Starting Foundation for Talents of Xuzhou Medical University (No. D2018006). Shandong key research and development program (2019GSF108270) Funding Information: Funding This work was supported by the National Natural Science Foundation of China (grant nos. 81800738, 81773969, 81102883, 81800718 and 82070891), the first-class discipline construction major project of Guangzhou University of Chinese Medicine (Guangzhou University of Chinese Medicine Planning (2018, No. 6), Guangzhou University of Chinese Medicine Planning (2019, No. 5)), the Guangdong Science and Technology Collaborative Innovation Center for Sport Science (2019B110210004), the Natural Science Foundation of the Jiangsu Higher Education Institutions of China (No. 18KJB310015), the Jiangsu Shuangchuang Programme and the Starting Foundation for Talents of Xuzhou Medical University (No. D2018006). Shandong key research and development program (2019GSF108270). Publisher Copyright: {\textcopyright} Author(s) (or their employer(s)) 2021. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.",

year = "2021",

month = nov,

day = "1",

doi = "10.1136/gutjnl-2020-321774",

language = "English (US)",

volume = "70",

pages = "2183--2195",

journal = "Gut",

issn = "0017-5749",

publisher = "BMJ Publishing Group",

number = "11",

}

TY - JOUR

T1 - Hepatic Krüppel-like factor 16 (KLF16) targets PPARα to improve steatohepatitis and insulin resistance

AU - Sun, Nannan

AU - Shen, Chuangpeng

AU - Zhang, Lei

AU - Wu, Xiaojie

AU - Yu, Yuanyuan

AU - Yang, Xiaoying

AU - Yang, Chen

AU - Zhong, Chong

AU - Gao, Zhao

AU - Miao, Wei

AU - Yang, Zehong

AU - Gao, Weihang

AU - Hu, Ling

AU - Williams, Kevin

AU - Liu, Changhui

AU - Chang, Yongsheng

AU - Gao, Yong

N1 - Funding Information: This work was supported by the National Natural Science Foundation of China (grant nos. 81800738, 81773969, 81102883, 81800718 and 82070891), the first-class discipline construction major project of Guangzhou University of Chinese Medicine (Guangzhou University of Chinese Medicine Planning (2018, No. 6), Guangzhou University of Chinese Medicine Planning (2019, No. 5)), the Guangdong Science and Technology Collaborative Innovation Center for Sport Science (2019B110210004), the Natural Science Foundation of the Jiangsu Higher Education Institutions of China (No. 18KJB310015), the Jiangsu Shuangchuang Programme and the Starting Foundation for Talents of Xuzhou Medical University (No. D2018006). Shandong key research and development program (2019GSF108270) Funding Information: Funding This work was supported by the National Natural Science Foundation of China (grant nos. 81800738, 81773969, 81102883, 81800718 and 82070891), the first-class discipline construction major project of Guangzhou University of Chinese Medicine (Guangzhou University of Chinese Medicine Planning (2018, No. 6), Guangzhou University of Chinese Medicine Planning (2019, No. 5)), the Guangdong Science and Technology Collaborative Innovation Center for Sport Science (2019B110210004), the Natural Science Foundation of the Jiangsu Higher Education Institutions of China (No. 18KJB310015), the Jiangsu Shuangchuang Programme and the Starting Foundation for Talents of Xuzhou Medical University (No. D2018006). Shandong key research and development program (2019GSF108270). Publisher Copyright: © Author(s) (or their employer(s)) 2021. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.

PY - 2021/11/1

Y1 - 2021/11/1

N2 - Objective Impaired hepatic fatty acids oxidation results in lipid accumulation and redox imbalance, promoting the development of fatty liver diseases and insulin resistance. However, the underlying pathogenic mechanism is poorly understood. Krüppel-like factor 16 (KLF16) is a transcription factor that abounds in liver. We explored whether and by what mechanisms KLF16 affects hepatic lipid catabolism to improve hepatosteatosis and insulin resistance. Design KLF16 expression was determined in patients with non-alcoholic fatty liver disease (NAFLD) and mice models. The role of KLF16 in the regulation of lipid metabolism was investigated using hepatocyte-specific KLF16-deficient mice fed a high-fat diet (HFD) or using an adenovirus/adeno-associated virus to alter KLF16 expression in mouse primary hepatocytes (MPHs) and in vivo livers. RNA-seq, luciferase reporter gene assay and ChIP analysis served to explore the molecular mechanisms involved. Results KLF16 expression was decreased in patients with NAFLD, mice models and oleic acid and palmitic acid (OA and PA) cochallenged hepatocytes. Hepatic KLF16 knockout impaired fatty acid oxidation, aggravated mitochondrial stress, ROS burden, advancing hepatic steatosis and insulin resistance. Conversely, KLF16 overexpression reduced lipid deposition and improved insulin resistance via directly binding the promoter of peroxisome proliferator-activated receptor α (PPARα) to accelerate fatty acids oxidation and attenuate mitochondrial stress, oxidative stress in db/db and HFD mice. PPARα deficiency diminished the KLF16-evoked protective effects against lipid deposition in MPHs. Hepatic-specific PPARα overexpression effectively rescued KLF16 deficiency-induced hepatic steatosis, altered redox balance and insulin resistance. Conclusions These findings prove that a direct KLF16-PPARα pathway closely links hepatic lipid homeostasis and redox balance, whose dysfunction promotes insulin resistance and hepatic steatosis.

AB - Objective Impaired hepatic fatty acids oxidation results in lipid accumulation and redox imbalance, promoting the development of fatty liver diseases and insulin resistance. However, the underlying pathogenic mechanism is poorly understood. Krüppel-like factor 16 (KLF16) is a transcription factor that abounds in liver. We explored whether and by what mechanisms KLF16 affects hepatic lipid catabolism to improve hepatosteatosis and insulin resistance. Design KLF16 expression was determined in patients with non-alcoholic fatty liver disease (NAFLD) and mice models. The role of KLF16 in the regulation of lipid metabolism was investigated using hepatocyte-specific KLF16-deficient mice fed a high-fat diet (HFD) or using an adenovirus/adeno-associated virus to alter KLF16 expression in mouse primary hepatocytes (MPHs) and in vivo livers. RNA-seq, luciferase reporter gene assay and ChIP analysis served to explore the molecular mechanisms involved. Results KLF16 expression was decreased in patients with NAFLD, mice models and oleic acid and palmitic acid (OA and PA) cochallenged hepatocytes. Hepatic KLF16 knockout impaired fatty acid oxidation, aggravated mitochondrial stress, ROS burden, advancing hepatic steatosis and insulin resistance. Conversely, KLF16 overexpression reduced lipid deposition and improved insulin resistance via directly binding the promoter of peroxisome proliferator-activated receptor α (PPARα) to accelerate fatty acids oxidation and attenuate mitochondrial stress, oxidative stress in db/db and HFD mice. PPARα deficiency diminished the KLF16-evoked protective effects against lipid deposition in MPHs. Hepatic-specific PPARα overexpression effectively rescued KLF16 deficiency-induced hepatic steatosis, altered redox balance and insulin resistance. Conclusions These findings prove that a direct KLF16-PPARα pathway closely links hepatic lipid homeostasis and redox balance, whose dysfunction promotes insulin resistance and hepatic steatosis.

KW - Fatty liver

KW - Lipid metabolism

KW - Nonalcoholic steatohepatitis

UR - http://www.scopus.com/inward/record.url?scp=85097842469&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85097842469&partnerID=8YFLogxK

U2 - 10.1136/gutjnl-2020-321774

DO - 10.1136/gutjnl-2020-321774

M3 - Article

C2 - 33257471

AN - SCOPUS:85097842469

SN - 0017-5749

VL - 70

SP - 2183

EP - 2195

JO - Gut

JF - Gut

IS - 11

ER -

Hepatic Krüppel-like factor 16 (KLF16) targets PPARα to improve steatohepatitis and insulin resistance

Abstract

Keywords

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this