Glycolysis in Innate Immune Cells Contributes to Autoimmunity

Xu, Yue; Chen, Yongkang; Zhang, Xuan; Ma, Jie; Liu, Yudong; Cui, Liyan; Wang, Fang

doi:10.3389/fimmu.2022.920029

Cited by 13 publications

(11 citation statements)

References 187 publications

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“…Since activated host cells consume more glucose than resting cells, glycolysis is activated during training/stimulation of the innate immune cells to meet the energy demand to serve a proinflammatory role ( 93 ). Although glycolysis is not an efficient way for the cell to generate ATP, this process can rapidly be induced upon stimulation of the innate immune cells ( 94 ). The primary function of the glycolysis cycle is to break glucose molecules to produce ATP and release pyruvate, which is further transformed into acetyl CoA and participates either in the TCA or fatty acid oxidation (FAO) cycle.…”

Section: Main Textmentioning

confidence: 99%

“…The persistent activation of glycolysis is regulated by a key transcriptional regulator, namely the hypoxia-inducible factor-1 alpha (HIF1α), which is stabilized by succinate, an intermediate metabolite of glycolysis. Furthermore, succinate and fumarate can act as epigenetic modulators for antagonizing histone or DNA methylation and facilitating long-lasting expression of genes involved in the glycolysis pathway ( 94 , 95 ). The increased glycolysis impacts the mammalian target of rapamycin (mTOR) and HIF-1α pathway representing the metabolic basis of trained immunity ( 96 ).…”

Section: Main Textmentioning

confidence: 99%

“…It has been reported that β-glucan can induce OXPHOS shift, resulting in a higher intracellular ratio of NAD + to its reduced form NADH, thus producing more ATP ( 97 , 101 , 102 ). However, recent findings suggest that trained innate immune cells can activate both glycolysis and OXPHOS pathways at the same time ( 94 ) to serve as cellular energy sources to meet the demands of activated/trained cells ( 103 ). In a study by Arts et al., the stimulation of macrophages with β-glucan and BCG upregulated the expression of glycolytic enzymes with an increase in NAD + and NADH ratio ( 104 ).…”

Section: Main Textmentioning

confidence: 99%

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The causes and consequences of trained immunity in myeloid cells

Bhargavi,

Subbian

2024

Front. Immunol.

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Conventionally, immunity in humans has been classified as innate and adaptive, with the concept that only the latter type has an immunological memory/recall response against specific antigens or pathogens. Recently, a new concept of trained immunity (a.k.a. innate memory response) has emerged. According to this concept, innate immune cells can exhibit enhanced responsiveness to subsequent challenges, after initial stimulation with antigen/pathogen. Thus, trained immunity enables the innate immune cells to respond robustly and non-specifically through exposure or re-exposure to antigens/infections or vaccines, providing enhanced resistance to unrelated pathogens or reduced infection severity. For example, individuals vaccinated with BCG to protect against tuberculosis were also protected from malaria and SARS-CoV-2 infections. Epigenetic modifications such as histone acetylation and metabolic reprogramming (e.g. shift towards glycolysis) and their inter-linked regulations are the key factors underpinning the immune activation of trained cells. The integrated metabolic and epigenetic rewiring generates sufficient metabolic intermediates, which is crucial to meet the energy demand required to produce proinflammatory and antimicrobial responses by the trained cells. These factors also determine the efficacy and durability of trained immunity. Importantly, the signaling pathways and regulatory molecules of trained immunity can be harnessed as potential targets for developing novel intervention strategies, such as better vaccines and immunotherapies against infectious (e.g., sepsis) and non-infectious (e.g., cancer) diseases. However, aberrant inflammation caused by inappropriate onset of trained immunity can lead to severe autoimmune pathological consequences, (e.g., systemic sclerosis and granulomatosis). In this review, we provide an overview of conventional innate and adaptive immunity and summarize various mechanistic factors associated with the onset and regulation of trained immunity, focusing on immunologic, metabolic, and epigenetic changes in myeloid cells. This review underscores the transformative potential of trained immunity in immunology, paving the way for developing novel therapeutic strategies for various infectious and non-infectious diseases that leverage innate immune memory.

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Section: Main Textmentioning

confidence: 99%

Section: Main Textmentioning

confidence: 99%

Section: Main Textmentioning

confidence: 99%

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The causes and consequences of trained immunity in myeloid cells

Bhargavi,

Subbian

2024

Front. Immunol.

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“…As elevated autoantibodies and deposition of immune complexes are the main characteristics of SLE patients, most pathological studies conducted on SLE so far have focused on abnormalities of the adaptive immune response [6 ▪ ]. However, the immune response mediated by innate immune cells, which acts early and upstream of adaptive immune response [7], has recently drawn significant attention in SLE pathogenesis [8,9 ▪ ]. The present review explores the complex associations between innate immune cells and SLE pathogenesis, with focus on neutrophils as these cells are found in large numbers and play critical immune functions [10 ▪ ]…”

Section: Introductionmentioning

confidence: 99%

Insights into the pathogenic role of neutrophils in systemic lupus erythematosus

Jiang

Zhang

et al. 2022

Current Opinion in Rheumatology

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Purpose of reviewAlthough dysregulated adaptive immune response has been considered as the main culprit for systemic lupus erythematosus (SLE), emerging studies have indicated that innate immunity, functioning upstream of adaptive immunity, acts as an important trigger of autoimmune diseases and promotes SLE development. Here, we have reviewed the most recent findings to highlight the influence of neutrophils on SLE pathogenesis.Recent findingsNeutrophils participate in SLE development mainly via promoting self-antigen exposure and autoantibody production, advocating the release of type I interferons (IFNs) and other pro-inflammatory cytokines, and mediating systemic tissue injury. A recent study revealed that neutrophil ferroptosis exerts a strong pathogenic effect in SLE, and that dysregulated innate immunity is adequate to disrupt the homeostasis of immune tolerance.SummaryInsights into the pathogenic role of neutrophils in SLE will contribute to a more comprehensive understanding of this disease and may propose novel clinical targets for accurate diagnosis and precision medicine.

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“…The effect of acute ethanol-exposure on glycolysis and glycolysis-regulating enzymes in immunosuppressed macrophages is not fully understood ( 9 , 33 , 38 ). Glycolytic enzymes are known to regulate basic cellular functions and immune response, in addition to the regulation of glycolysis ( 39 – 41 ). Specifically, the platelet isoform of phosphofructokinase (PFKP), a key glycolysis-regulating enzyme, serves as a protein kinase that regulates autophagy.…”

Section: Introductionmentioning

confidence: 99%

SIRT2-PFKP interaction dysregulates phagocytosis in macrophages with acute ethanol-exposure

et al. 2023

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Alcohol abuse, reported by 1/8th critically ill patients, is an independent risk factor for death in sepsis. Sepsis kills over 270,000 patients/year in the US. We reported that the ethanol-exposure suppresses innate-immune response, pathogen clearance, and decreases survival in sepsis-mice via sirtuin 2 (SIRT2). SIRT2 is an NAD+-dependent histone-deacetylase with anti-inflammatory properties. We hypothesized that in ethanol-exposed macrophages, SIRT2 suppresses phagocytosis and pathogen clearance by regulating glycolysis. Immune cells use glycolysis to fuel increased metabolic and energy demand of phagocytosis. Using ethanol-exposed mouse bone marrow- and human blood monocyte-derived macrophages, we found that SIRT2 mutes glycolysis via deacetylating key glycolysis regulating enzyme phosphofructokinase-platelet isoform (PFKP), at mouse lysine 394 (mK394, human: hK395). Acetylation of PFKP at mK394 (hK395) is crucial for PFKP function as a glycolysis regulating enzyme. The PFKP also facilitates phosphorylation and activation of autophagy related protein 4B (Atg4B). Atg4B activates microtubule associated protein 1 light chain-3B (LC3). LC3 is a driver of a subset of phagocytosis, the LC3-associated phagocytosis (LAP), which is crucial for segregation and enhanced clearance of pathogens, in sepsis. We found that in ethanol-exposed cells, the SIRT2-PFKP interaction leads to decreased Atg4B-phosphorylation, decreased LC3 activation, repressed phagocytosis and LAP. Genetic deficiency or pharmacological inhibition of SIRT2 reverse PFKP-deacetylation, suppressed LC3-activation and phagocytosis including LAP, in ethanol-exposed macrophages to improve bacterial clearance and survival in ethanol with sepsis mice.

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Glycolysis in Innate Immune Cells Contributes to Autoimmunity

Cited by 13 publications

References 187 publications

The causes and consequences of trained immunity in myeloid cells

The causes and consequences of trained immunity in myeloid cells

Insights into the pathogenic role of neutrophils in systemic lupus erythematosus

SIRT2-PFKP interaction dysregulates phagocytosis in macrophages with acute ethanol-exposure

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