The metabolic ER stress sensor IRE1α suppresses alternative activation of macrophages and impairs energy expenditure in obesity

Shan, Bo; Wang, Xiaoxia; Wu, Ying; Xu, Chi; Xia, Zhongfang; Dai, Jianli; Shao, Mengle; Zhao, Feng; He, Shengqi; Liu, Yang; Zhang, Mingliang; Nan, Fa‐Jun; Li, Jia; Liu, Jian‐Miao; Liu, Jianfeng; Jia, Weiping; Qiu, Yifu; Song, Bei; Han, Jing; Rui, Liangyou; Duan, Si‐Bo; Liu, Yong

doi:10.1038/ni.3709

Cited by 283 publications

(255 citation statements)

References 51 publications

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“…P-S52-eIF2α was detected to a low extent in resting DCs and did not increase upon 2-DG treatment and PAMPs stimulation (Figure 7A), in agreement with a recent report showing that LPS did not affect eIF2α phosphorylation (44). The mRNA expression of DDIT3 /CHOP was enhanced by 2-DG and blunted by mannose in the presence of PAMPs (Figure 7B), thus suggesting that mannose may counter some of the mechanisms triggered by the stimuli by acting as a substrate for the formation of dolichol-linked oligosaccharide.…”

Section: Resultssupporting

confidence: 93%

“…The interplay between the PERK and IRE1α routes through STAT3 (Figure 10) is supported by recent data showing that STAT3 plays a critical role in the activation of a non-canonical UPR cascade involving Ire1α and Xbp1 under combined cytokine stimulation (58). Our finding of a stable phosphorylation of eIF2α (Figure 7A) agrees with a recent report showing similar results in M2-polarized macrophages stimulated with LPS, thus suggesting that some stimuli activate the UPR in the absence of a stimulatory effect on eIF2α phosphorylation (44). …”

Section: Discussionsupporting

confidence: 92%

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Endoplasmic Reticulum Stress Sensor IRE1α Enhances IL-23 Expression by Human Dendritic Cells

et al. 2017

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Human monocyte-derived dendritic cells (DCs) exposed to pathogen-associated molecular patterns (PAMPs) undergo bioenergetic changes that influence the immune response. We found that stimulation with PAMPs enhanced glycolysis in DCs, whereas oxidative phosphorylation remained unaltered. Glucose starvation and the hexokinase inhibitor 2-deoxy-d-glucose (2-DG) modulated cytokine expression in stimulated DCs. Strikingly, IL23A was markedly induced upon 2-DG treatment, but not during glucose deprivation. Since 2-DG can also rapidly inhibit protein N-glycosylation, we postulated that this compound could induce IL-23 in DCs via activation of the endoplasmic reticulum (ER) stress response. Indeed, stimulation of DCs with PAMPs in the presence of 2-DG robustly activated inositol-requiring protein 1α (IRE1α) signaling and to a lesser extent the PERK arm of the unfolded protein response. Additional ER stressors such as tunicamycin and thapsigargin also promoted IL-23 expression by PAMP-stimulated DCs. Pharmacological, biochemical, and genetic analyses using conditional knockout mice revealed that IL-23 induction in ER stressed DCs stimulated with PAMPs was IRE1α/X-box binding protein 1-dependent upon zymosan stimulation. Interestingly, we further evidenced PERK-mediated and CAAT/enhancer-binding protein β-dependent trans-activation of IL23A upon lipopolysaccharide treatment. Our findings uncover that the ER stress response can potently modulate cytokine expression in PAMP-stimulated human DCs.

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Section: Resultssupporting

confidence: 93%

Section: Discussionsupporting

confidence: 92%

Endoplasmic Reticulum Stress Sensor IRE1α Enhances IL-23 Expression by Human Dendritic Cells

et al. 2017

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“…While cause and effect between macrophage reactivity and adipose pathology are not well established, data in this manuscript suggests that macrophage reactivity is a cause rather than a consequence of adiposopathy and mediates, at least in part, the pathologic processes of metabolic and neurologic dysfunction. This scenario is supported by other studies demonstrating that prevention of inflammatory signaling in myeloid cells not only prevents high-fat diet-induced obesity and metabolic dysfunction, but also increases brown adipose tissue activity, white adipose browning, and energy expenditure [64], [65]. While energy expenditure was not measured in the present study, the decreased expression of markers of ER stress in visceral adipose suggests improved adipose physiology.…”

Section: Discussionsupporting

confidence: 88%

Myeloid-specific deletion of NOX2 prevents the metabolic and neurologic consequences of high fat diet

Pepping¹,

Vandanmagsar²,

Fernandez-Kim³

et al. 2017

PLoS ONE

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High fat diet-induced obesity is associated with inflammatory and oxidative signaling in macrophages that likely participates in metabolic and physiologic impairment. One key factor that could drive pathologic changes in macrophages is the pro-inflammatory, pro-oxidant enzyme NADPH oxidase. However, NADPH oxidase is a pleiotropic enzyme with both pathologic and physiologic functions, ruling out indiscriminant NADPH oxidase inhibition as a viable therapy. To determine if targeted inhibition of monocyte/macrophage NADPH oxidase could mitigate obesity pathology, we generated mice that lack the NADPH oxidase catalytic subunit NOX2 in myeloid lineage cells. C57Bl/6 control (NOX2-FL) and myeloid-deficient NOX2 (mNOX2-KO) mice were given high fat diet for 16 weeks, and subject to comprehensive metabolic, behavioral, and biochemical analyses. Data show that mNOX2-KO mice had lower body weight, delayed adiposity, attenuated visceral inflammation, and decreased macrophage infiltration and cell injury in visceral adipose relative to control NOX2-FL mice. Moreover, the effects of high fat diet on glucose regulation and circulating lipids were attenuated in mNOX2-KO mice. Finally, memory was impaired and markers of brain injury increased in NOX2-FL, but not mNOX2-KO mice. Collectively, these data indicate that NOX2 signaling in macrophages participates in the pathogenesis of obesity, and reinforce a key role for macrophage inflammation in diet-induced metabolic and neurologic decline. Development of macrophage/immune-specific NOX-based therapies could thus potentially be used to preserve metabolic and neurologic function in the context of obesity.

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“…showed that classical macrophage markers of inflammation such as CD38 and CD274 are not induced in response to metabolic stimuli, which indicates that alternative activation pathways, including fatty acid-driven PPARγ signaling, may underlie metaflammatory phenotypes (Kratz et al, 2014). Interestingly, recent studies also support the concept that chronic ER stress in obesity may lead to inflammatory polarization in adipose tissue macrophages (Shan et al, 2017). It was also demonstrated that GPS2, a component of the co-repressor complex, restrains expression of pro-inflammatory mediators in ATMs.…”

Section: Innate Immune Cellular Mediators Of Inflammationmentioning

confidence: 82%

Foundations of Immunometabolism and Implications for Metabolic Health and Disease

2017

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Highly ordered interactions between immune and metabolic responses are evolutionarily conserved and paramount for tissue and organismal health. Disruption of these interactions underlies the emergence of many pathologies, particularly chronic non-communicable diseases such as obesity and diabetes. Here, we examine decades of research identifying the complex immunometabolic signaling networks and the cellular and molecular events that occur in the setting of altered nutrient and energy exposures and offer a historical perspective. Furthermore, we describe recent advances such as the discovery that a broad complement of immune cells play a role in immunometabolism and the emerging evidence that nutrients and metabolites modulate inflammatory pathways. Lastly, we discuss how this work may eventually lead to tangible therapeutic advancements to promote health.

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The metabolic ER stress sensor IRE1α suppresses alternative activation of macrophages and impairs energy expenditure in obesity

Cited by 283 publications

References 51 publications

Endoplasmic Reticulum Stress Sensor IRE1α Enhances IL-23 Expression by Human Dendritic Cells

Endoplasmic Reticulum Stress Sensor IRE1α Enhances IL-23 Expression by Human Dendritic Cells

Myeloid-specific deletion of NOX2 prevents the metabolic and neurologic consequences of high fat diet

Foundations of Immunometabolism and Implications for Metabolic Health and Disease

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