High-density lipoprotein mediates anti-inflammatory reprogramming of macrophages via the transcriptional regulator ATF3

Nardo, Dominic De; Labzin, Larisa I.; Kono, Hajime; Seki, Reiko; Schmidt, Susanne V.; Beyer, Marc; Xu, Dakang; Zimmer, Sebastian; Lahrmann, Catharina; Schildberg, Frank A.; Vogelhuber, Johanna; Kraut, Michael; Ulas, Thomas; Kerksiek, Anja; Krebs, Wolfgang; Bode, Niklas; Grebe, Alena; Fitzgerald, Michael L.; Hernandez, Nicholas; Williams, Bryan R.G.; Knolle, Percy A.; Kneilling, Manfred; Röcken, Martin; Lütjohann, Dieter; Wright, Samuel D.; Schultze, Joachim L.; Latz, Eicke

doi:10.1038/ni.2784

Cited by 363 publications

(302 citation statements)

References 49 publications

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“…B, for microscale thermophoresis analysis FH5-7 was incubated with labeled apoE2. The concentration of labeled ligand was 0.0013 M, and the starting concentration for the unlabeled FH5-7 was 5 M. The average of two experiments suggested a K d value of 0.202 M. vitro and in vivo studies, it is evident that HDL has an important role in reducing inflammation (28). This is possibly at least partially due to binding of complement regulators FH and clusterin to HDL particles.…”

Section: Discussionmentioning

confidence: 97%

Complement Factor H Binds to Human Serum Apolipoprotein E and Mediates Complement Regulation on High Density Lipoprotein Particles

Haapasalo

Kessel

Nissilä

et al. 2015

Journal of Biological Chemistry

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Background: Factor H is the main complement alternative pathway regulator in plasma. Results: Factor H binds to apoE leading to reduced complement activity against HDL particles. Conclusion: Interaction of factor H with HDL particles is involved in complement regulation in plasma. Significance: Complement regulation on HDL particles by factor H could be involved in disease processes caused by alternative pathway dysregulation.

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Section: Discussionmentioning

confidence: 97%

Complement Factor H Binds to Human Serum Apolipoprotein E and Mediates Complement Regulation on High Density Lipoprotein Particles

Haapasalo

Kessel

Nissilä

et al. 2015

Journal of Biological Chemistry

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“…ATF3 functions as a negative regulator of the inflammatory responses in macrophages by antagonizing TLR-induced NF-B signaling (35), and ATF3 deletion increases lipid accumulation and foam cell formation through epigenetic repression of the cholesterol 25-hydroxylase gene Ch25h (36). ATF3 has been demonstrated to mediate the anti-inflammatory and metabolic activities of high density lipoprotein (HDL) by down-regulating TLR-induced proinflammatory cytokines (37). Here, we provide novel evidence that ATF3 plays an important role in linking lipid metabolism and immunity through regulation of MDSC development and activation.…”

Section: Discussionmentioning

confidence: 99%

Glucocorticoid Induces Hepatic Steatosis by Inhibiting Activating Transcription Factor 3 (ATF3)/S100A9 Protein Signaling in Granulocytic Myeloid-derived Suppressor Cells

Liu

Wei

Shi

et al. 2016

Journal of Biological Chemistry

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Glucocorticoids (GCs) used as inflammation suppressors have harmful side effects, including induction of hepatic steatosis. The underlying mechanisms of GC-promoted dysregulation of lipid metabolism, however, are not fully understood. GCs could facilitate the accumulation of myeloid-derived suppressor cells (MDSC) in the liver of animals, and the potential role of MDSCs in GC-induced hepatic steatosis was therefore investigated in this study. We demonstrated that granulocytic (G)-MDSC accumulation mediated the effects of GCs on the fatty liver, in which activating transcription factor 3 (ATF3)/S100A9 signaling plays an important role. ATF3-deficient mice developed hepatic steatosis and displayed expansion of G-MDSCs in the liver and multiple immune organs, which shared high similarity with the phenotype observed in GC-treated wild-type littermates. Adoptive transfer of GC-induced or ATF3-deficient G-MDSCs promoted lipid accumulation in the liver, whereas depletion of G-MDSCs alleviated these effects. Mechanistic studies showed that in MDSCs, ATF3 was transrepressed by the GC receptor GR through direct binding to the negative GR-response element. S100A9 is the major transcriptional target of ATF3 in G-MDSCs. Silencing S100A9 clearly alleviated G-MDSCs expansion and hepatic steatosis caused by ATF3 deficiency or GC treatment. Our study uncovers an important role of G-MDSCs in GC-induced hepatic steatosis, in which ATF3 may have potential therapeutic implications.

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“…Thus, Atf3 −/− mice are more susceptible to endotoxic shock due to excessive cytokine production (Hoetzenecker et al 2012). ATF3 also mediates high-density lipoprotein (HDL)-induced anti-inflammatory reprogramming of macrophages by transcriptional repression of inflammatory genes (De Nardo et al 2014). In neutrophils, ATF3 restricts neutrophil recruitment by reducing neutrophil chemokine production that promotes neutrophil chemotaxis (Boespflug et al 2014).…”

Section: Atf3mentioning

confidence: 99%

Physiological/pathological ramifications of transcription factors in the unfolded protein response

2017

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Numerous environmental, physiological, and pathological insults disrupt protein-folding homeostasis in the endoplasmic reticulum (ER), referred to as ER stress. Eukaryotic cells evolved a set of intracellular signaling pathways, collectively termed the unfolded protein response (UPR), to maintain a productive ER protein-folding environment through reprogramming gene transcription and mRNA translation. The UPR is largely dependent on transcription factors (TFs) that modulate expression of genes involved in many physiological and pathological conditions, including development, metabolism, inflammation, neurodegenerative diseases, and cancer. Here we summarize the current knowledge about these mechanisms, their impact on physiological/pathological processes, and potential therapeutic applications.

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High-density lipoprotein mediates anti-inflammatory reprogramming of macrophages via the transcriptional regulator ATF3

Cited by 363 publications

References 49 publications

Complement Factor H Binds to Human Serum Apolipoprotein E and Mediates Complement Regulation on High Density Lipoprotein Particles

Complement Factor H Binds to Human Serum Apolipoprotein E and Mediates Complement Regulation on High Density Lipoprotein Particles

Glucocorticoid Induces Hepatic Steatosis by Inhibiting Activating Transcription Factor 3 (ATF3)/S100A9 Protein Signaling in Granulocytic Myeloid-derived Suppressor Cells

Physiological/pathological ramifications of transcription factors in the unfolded protein response

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