Lactate at the crossroads of metabolism, inflammation, and autoimmunity

Pucino, Valentina; Bombardieri, Michèle; Pitzalis, Costantino; Mauro, Claudio

doi:10.1002/eji.201646477

Cited by 158 publications

(149 citation statements)

References 75 publications

(147 reference statements)

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“…Furthermore, expression of the lactate transporter SLC5a12 in synovial tissue was shown to correlate with the clinical T cell score, and in-vivo blockade of lactate transporters resulted in the release of T cells from the inflammatory site [28]. These findings provide a rationale for the therapeutic targeting of specific lactate transporters on T cells in autoimmune diseases such as RA (reviewed in [38]). These findings provide a rationale for the therapeutic targeting of specific lactate transporters on T cells in autoimmune diseases such as RA (reviewed in [38]).…”

Section: The Role Of T Cell Metabolism In Ramentioning

confidence: 97%

“…These data suggest that the elevated lactate concentrations observed in the RA joint inhibit the glycolysis and migration of effector T cells, resulting in their retention at the site of inflammation and also increasing their production of IL-17. These findings provide a rationale for the therapeutic targeting of specific lactate transporters on T cells in autoimmune diseases such as RA (reviewed in [38]). Consistent with this, expression levels of the lactate transporter MCT4 and glycolytic enzymes HK2, GPI, triosephosphate isomerase (TPI), enolase 1 (Eno 1), PKM2 and LDH are significantly reduced in Th17 cells obtained from HIF1α -/compared to wild-type (WT) mice [31], demonstrating the dependence of increased glycolytic enzymatic REVIEW SERIES: TRANSLATING IMMUNOMETABOLISM activity on the oxygen sensing pathway.…”

Section: The Role Of T Cell Metabolism In Ramentioning

confidence: 98%

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Altered metabolic pathways regulate synovial inflammation in rheumatoid arthritis

Fearon

Hanlon

Wade

et al. 2018

Clinical and Experimental Immunology

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Rheumatoid arthritis is characterized by synovial proliferation, neovascularization and leucocyte extravasation leading to joint destruction and functional disability. The blood vessels in the inflamed synovium are highly dysregulated, resulting in poor delivery of oxygen; this, along with the increased metabolic demand of infiltrating immune cells and inflamed resident cells, results in the lack of key nutrients at the site of inflammation. In these adverse conditions synovial cells must adapt to generate sufficient energy to support their proliferation and activation status, and thus switch their cell metabolism from a resting regulatory state to a highly metabolically active state. This alters redox-sensitive signalling pathways and also results in the accumulation of metabolic intermediates which, in turn, can act as signalling molecules that further exacerbate the inflammatory response. The RA synovium is a multi-cellular tissue, and while many cell types interact to promote the inflammatory response, their metabolic requirements differ. Thus, understanding the complex interplay between hypoxia-induced signalling pathways, metabolic pathways and the inflammatory response will provide better insight into the underlying mechanisms of disease pathogenesis. OTHER ARTICLES PUBLISHED IN THIS REVIEW SERIESTranslating immunometabolism: towards curing human diseases by targeting metabolic processes underpinning the immune response. Clinical and Experimental Immunology 2019, 197: 141-142. T cell metabolism in chronic viral infection. Clinical and Experimental Immunology 2019, 197: 143-152. Sculpting tumor microenvironment with immune system: from immunometabolism to immunoediting. Clinical and Experimental Immunology 2019, 197: 153-160. Sensing between reactions -how the metabolic microenvironment shapes immunity.

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Section: The Role Of T Cell Metabolism In Ramentioning

confidence: 97%

Section: The Role Of T Cell Metabolism In Ramentioning

confidence: 98%

Altered metabolic pathways regulate synovial inflammation in rheumatoid arthritis

Fearon

Hanlon

Wade

et al. 2018

Clinical and Experimental Immunology

View full text Add to dashboard Cite

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“…Low glucose and high lacate has long been recognized as typical for the rheumatoid joint [58]. Extracellular pH sustains an important cell-cell communication network, as acid-sensing ion channels sense the metabolic activity of cellular partners in their direct surroundings [59]. Lactate has immediate impact on the functional behavior of T-cells [45], modifying their polarization, mobility and cytotoxic capacity.…”

Section: Ra Macrophages – Glucose-intoxicated Hyperinflammatory Effementioning

confidence: 99%

Metabolic signatures of T-cells and macrophages in rheumatoid arthritis

Weyand

Zeisbrich

Goronzy

2017

Current Opinion in Immunology

113

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In most autoimmune diseases, a decade-long defect in self-tolerance eventually leads to clinically relevant, tissue-destructive inflammatory disease. The pathogenic potential of chronic persistent immune responses during the pre-clinical and clinical phase is ultimately linked to the bioenergetic fitness of innate and adaptive immune cells. Chronic immune cell stimulation, high cellular turn-over, structural damage to the host tissue and maladaptive wound healing, all require a reliable supply of nutrients, oxygen, and biosynthetic precursors. Here, we use the model system of rheumatoid arthritis (RA) to discuss immunometabolism from the vantage point of T-cells and macrophages that encounter fundamentally different metabolic stress scenarios in the RA host. We outline the general principle that both insufficient nutrient supply, as well as nutrient excess generate cellular stress responses and guide immune function. ATPlow, NADPHhigh, ROSlow T-cells hyperproliferate and are forced into premature senescence. ATPhigh, ROShigh macrophages dimerize the glycolytic enzyme pyruvate kinase to amplify STAT3-dependent inflammatory effector functions. A corollary of this model is that simple nutraceutical interventions will be insufficient to re-educate the immune system in RA. Instead, interference with cell-type-exclusive and differentiation-stage-dependent metabolic setpoints will be needed to reprogram arthritogenic pathways.

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“…RA is traditionally associated with the presence of rheumatoid factors and anticyclic citrullinated peptide autoantibodies . Interestingly, Th17 cells have been identified in germinal centres of ectopic lymphoid structures (ELS) in joints of RA patients . In mice, Th17 cells induce ELS in joints while germinal centre‐resident Th17 cells reduce sialylation of IgG, thus promoting pathogenic autoantibody production .…”

Section: Th17 Cells and Rheumatoid Arthritis (Ra) Pathogenesismentioning

confidence: 99%

“…47 Interestingly, Th17 cells have been identified in germinal centres of ectopic lymphoid structures (ELS) in joints of RA patients. 58 In mice, Th17 cells induce ELS in joints while germinal centre-resident Th17 cells reduce sialylation of IgG, thus promoting pathogenic autoantibody production. 46 Relevant to the link between Th17 cells and autoantibody production is that BAFF activates both plasma cells and Th17 cells and exacerbates joint pathology.…”

Section: Arthritis (Ra) Pathogenesismentioning

confidence: 99%

Functional and phenotypic heterogeneity of Th17 cells in health and disease

Byström

Clanchy

Taher

et al. 2018

Eur J Clin Investigation

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Background Th17 cells have nonredundant roles in maintaining immunity, particularly at mucosal surfaces. These roles are achieved principally through the production of cytokines and the recruitment of other immune cells to maintain the integrity of mucosal barriers and prevent the dissemination of microorganisms. Th17 cells are heterogeneous and exhibit a considerable degree of plasticity. This allows these cells to respond to changing environmental challenges. However, Th17 cells also play pro‐inflammatory roles in chronic autoimmune diseases. The trigger(s) that initiate these Th17 responses in chronic autoimmune diseases remain unclear. Design In this report, we provide an overview of studies involving animal models, patient data, genome wide association studies and clinical trials targeting IL‐17 for treatment of patients to gain a better understanding of the pathogenic roles of Th17 cells play in a range of autoimmune diseases. Results The report sheds light on likely triggers that initiate or perpetuate Th17 responses that promote chronic inflammation and autoimmunity. The divergent effects of tumour necrosis factor alpha blockade on Th17 cells in patients, is explored. Furthermore, we highlight the role of Th17 cells in inducing autoreactive B cells, leading to autoantibody production. Pathogenic bacterial species can change Th17 cell phenotype and responses. These findings provide insights into how Th17 cells could be induced to promoting autoimmune disease pathogenesis. Conclusion This article provides an overview of the distinct roles Th17 cells play in maintaining immunity at mucosal surfaces and in skin mucosa and how their functional flexibility could be linked with chronic inflammation in autoimmune rheumatic diseases.

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Lactate at the crossroads of metabolism, inflammation, and autoimmunity

Cited by 158 publications

References 75 publications

Altered metabolic pathways regulate synovial inflammation in rheumatoid arthritis

Altered metabolic pathways regulate synovial inflammation in rheumatoid arthritis

Metabolic signatures of T-cells and macrophages in rheumatoid arthritis

Functional and phenotypic heterogeneity of Th17 cells in health and disease

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