SRY-Box Containing Gene 4 Promotes Liver Steatosis by Upregulation of SREBP-1c

Jiao, Yang; Zhao, Jiejie; Zhang, Zhijian; Li, Min; Xi, Yu; Yz, Yang; Liu, Jie; Liao, Shengjie; Li, Duanzhuo; Wang, Yuxing; Zhang, Die; Chen, Yulu; Shi, Guojun; Liu, Bin; Lu, Yan; Li, Xiaoying

doi:10.2337/db18-0184

Cited by 17 publications

(10 citation statements)

References 53 publications

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“…Among the SREBP isoforms, SREBP-1c predominantly regulates the transcription of genes participating in FFA synthesis, whereas SREBP-1a and SREBP-2 are associated with cholesterol synthesis [23]. Recently, SOX4, another member of the SOX family, has been shown to promote liver steatosis by directly regulating the transcription of SREBP-1c [24]. In the present study, the expression of SREBP-1a and SREBP-1c could not be observed, limiting our possible conclusions.…”

Section: Discussioncontrasting

confidence: 71%

Transcription factor SOX2 contributes to nonalcoholic fatty liver disease development by regulating the expression of the fatty acid transporter CD36

Shen

Chen

et al. 2021

FEBS Letters

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Section: Discussioncontrasting

confidence: 71%

Transcription factor SOX2 contributes to nonalcoholic fatty liver disease development by regulating the expression of the fatty acid transporter CD36

Shen

Chen

et al. 2021

FEBS Letters

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“…Those mRNAs revealed a trend towards the inverse patterns in A1cf -/liver (Supplemental Figure 7D). SOX4 overexpression in liver was shown to stabilize b-CATENIN, increase cell proliferation, promoting steatosis and HCC progression (29)(30)(31)(32), while SPARCL1 overexpression was correlated with tumor angiogenesis in HCC (33,34). Since SMAD9 inhibits Bone Morphogenetic Protein (BMP) signaling (34) we asked if the decreased expression of Smad9 in A1cf +/Tg liver was accompanied by changes in Bmp7 mRNA.…”

Section: Transcriptome-wide Analysis Of A1cf +/Tg Liver and Isolated mentioning

confidence: 99%

Apobec1 complementation factor overexpression promotes hepatic steatosis, fibrosis, and hepatocellular cancer

Blanc¹,

Riordan²,

Soleyman-Jahi³

et al. 2021

Journal of Clinical Investigation

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RNA binding protein Apobec1 Complementation Factor (A1CF) regulates posttranscriptional ApoB mRNA editing but the range of RNA targets and long-term impact of altered A1CF expression on liver function are unknown. Here we studied hepatocyte-specific A1cf transgenic (A1cf +/Tg), A1cf +/Tg Apobec1-/and A1cf-/mice fed chow or high fat/high fructose diets using RNA-Seq, RNA-CLIP Seq and tissue microarrays from human hepatocellular cancer (HCC). A1cf +/Tg mice exhibited increased hepatic proliferation and steatosis, with increased lipogenic gene expression (Mogat1, Mogat2, Cidea, Cd36) associated with shifts in polysomal RNA distribution. Aged A1cf +/Tg mice developed spontaneous fibrosis, dysplasia and HCC, which was accelerated on a high fat/fructose diet and independent of Apobec1. RNA-Seq revealed increased expression of mRNAs involved in oxidative stress (Gstm3, Gpx3, Cbr3), inflammatory response (Il19, Cxcl14, Tnfa, Ly6c), extracellular matrix organization (Mmp2, Col1a1, Col4a1), proliferation (Kif20a, Mcm2, Mcm4, Mcm6) with a subset of mRNAs (including Sox4, Sox9, Cdh1) identified in RNA CLIP-Seq. Increased A1CF expression in human HCC correlated with advanced fibrosis and with reduced survival in a subset with nonalcoholic fatty liver disease. In conclusion, we show that hepatic A1CF overexpression selectively alters polysomal distribution and mRNA expression, promoting lipogenic, proliferative and inflammatory pathways leading to HCC.

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“…Li et al showed that inhibiting SREBP-1c activity can exert an anti-hepatic steatosis effect in diet-induced obese mice [3]. The correlation between inhibition of the SREBP-1c/FAS pathway and decreased liver lipid synthesis has been well established [16–18]. Therefore, the activation of the AMPK/ACC/CPT-1A pathway and inhibition of the SREBP-1c/FAS pathways may be potential targets for screening drugs to prevent hepatic lipid accumulation.…”

Section: Introductionmentioning

confidence: 99%

Diosgenin ameliorates palmitic acid-induced lipid accumulation via AMPK/ACC/CPT-1A and SREBP-1c/FAS signaling pathways in LO2 cells

Fang

Chen

et al. 2019

BMC Complement Altern Med

121

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Background Non-alcoholic fatty liver disease (NAFLD) is the most common chronic liver disease and is characterized by excessive hepatic lipid accumulation. Many studies have suggested that lipid overload is the key initial factor that contributes to hepatic steatosis. Our previous study indicated that diosgenin (DSG) has a beneficial effect on energy metabolism, but the underlying mechanism remains unclear. Methods Human normal hepatocytes (LO2 cells) were incubated with palmitic acid to establish the cell model of nonalcoholic fatty liver. The effects of DSG on lipid metabolism, glucose uptake and mitochondrial function were evaluated. Furthermore, the mechanism of DSG on oxidative stress, lipid consumption and lipid synthesis in LO2 cells was investigated. Results The results indicated that palmitic acid induced obvious lipid accumulation in LO2 cells and that DSG treatment significantly reduced the intracellular lipid content. DSG treatment upregulated expression of lipolysis proteins, including phospho-AMP activated protein kinase (p-AMPK), phospho-acetyl-coA carboxylase (p-ACC) and carnitine acyl transferase 1A (CPT-1A), and inhibited expression of lipid synthesis-related proteins, including sterol regulatory element-binding protein 1c (SREBP-1c) and fatty acid synthase (FAS). Additionally, DSG-treated cells displayed a marked improvement in mitochondrial function, with less production of reactive oxygen species and a higher mitochondrial membrane potential compared with the model group. Conclusion This study suggests that DSG can reduce intracellular lipid accumulation in LO2 cells and that the underlying mechanism may be related to the improving oxidative stress, increasing fatty acid β-oxidation and decreasing lipid synthesis. The above changes might be mediated by the activation of the AMPK/ACC/CPT-1A pathway and inhibition of the SREBP-1c/FAS pathway.

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SRY-Box Containing Gene 4 Promotes Liver Steatosis by Upregulation of SREBP-1c

Cited by 17 publications

References 53 publications

Transcription factor SOX2 contributes to nonalcoholic fatty liver disease development by regulating the expression of the fatty acid transporter CD36

Transcription factor SOX2 contributes to nonalcoholic fatty liver disease development by regulating the expression of the fatty acid transporter CD36

Apobec1 complementation factor overexpression promotes hepatic steatosis, fibrosis, and hepatocellular cancer

Diosgenin ameliorates palmitic acid-induced lipid accumulation via AMPK/ACC/CPT-1A and SREBP-1c/FAS signaling pathways in LO2 cells

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