Metabolic and Innate Immune Cues Merge into a Specific Inflammatory Response via the UPR

Mogilenko Denis A.; Haas Joel T.; Lhomme Laurent; Fleury Sebastien; Quemener Sandrine; Levavasseur Matthieu; Becquart Coralie; Wartelle Julien; Bogomolova Alexandra; Pineau Laurent; Molendi-Coste Olivier; Lancel Steve; Dehondt Helene; Gheeraert Celine; Melchior Aurelie; Dewas Cedric; Nikitin Artemii; Pic Samuel; Rabhi Nabil; Annicotte Jean-Sebastien; Oyadomari Seiichi; Velasco-Hernandez Talia; Cammenga Jorg; Foretz Marc; Viollet Benoit; Vukovic Milica; Villacreces Arnaud; Kranc Kamil; Carmeliet Peter; Marot Guillemette; Boulter Alexis; Tavernier Simon; Berod Luciana; Longhi Maria P.; Paget Christophe; Janssens Sophie; Staumont-Salle Delphine; Aksoy Ezra; Staels Bart; Dombrowicz David

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Metabolic and Innate Immune Cues Merge into a Specific Inflammatory Response via the UPR

机译：代谢和先天免疫提示通过UPR合并成特定的炎症反应

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Innate immune responses are intricately linked with intracellular metabolism of myeloid cells. Toll-like receptor (TLR) stimulation shifts intracellular metabolism toward glycolysis, while anti-inflammatory signals depend on enhanced mitochondrial respiration. How exogenous metabolic signals affect the immune response is unknown. We demonstrate that TLR-dependent responses of dendritic cells (DCs) are exacerbated by a high-fatty-acid (FA) metabolic environment. FAs suppress the TLR-induced hexokinase activity and perturb tricarboxylic acid cycle metabolism. These metabolic changes enhance mitochondria! reactive oxygen species (mtROS) production and, in turn, the unfolded protein response (UPR), leading to a distinct transcriptomic signature with IL-23 as hallmark. Interestingly, chemical or genetic suppression of glycolysis was sufficient to induce this specific immune response. Conversely, reducing mtROS production or DC-specific deficiency in XBP1 attenuated IL-23 expression and skin inflammation in an IL-23-dependent model of psoriasis. Thus, fine-tuning of innate immunity depends on optimization of metabolic demands and minimization of mtROS-induced UPR.

机译：先天免疫反应与骨髓细胞的细胞内代谢复杂相关。 Toll样受体（TLR）刺激将细胞内代谢移向糖酵解，而抗炎信号取决于增强的线粒体呼吸。外源性代谢信号如何影响免疫应答是未知的。我们证明树枝状细胞（DCS）的TLR依赖性反应被高脂肪酸（FA）代谢环境恶化。 Fas抑制TLR诱导的六酮酶活性和扰动三羧酸循环代谢。这些代谢变化增强了线粒体！反应性氧物种（MTROS）生产，又展开蛋白反应（UPR），导致IL-23作为标志的不同转录组签名。有趣的是，化学或遗传抑制的糖酵解足以诱导这种特定的免疫应答。相反，降低XBP1中的MTROS生产或直流特异性缺乏，在牛皮癣的IL-23依赖性模型中衰减IL-23表达和皮肤炎症。因此，先天免疫的微调取决于优化代谢需求和MTROS诱导的UPR的最小化。

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《Cell》 |2019年第5期|共35页
作者
Mogilenko Denis A.; Haas Joel T.; Lhomme Laurent; Fleury Sebastien; Quemener Sandrine; Levavasseur Matthieu; Becquart Coralie; Wartelle Julien; Bogomolova Alexandra; Pineau Laurent; Molendi-Coste Olivier; Lancel Steve; Dehondt Helene; Gheeraert Celine; Melchior Aurelie; Dewas Cedric; Nikitin Artemii; Pic Samuel; Rabhi Nabil; Annicotte Jean-Sebastien; Oyadomari Seiichi; Velasco-Hernandez Talia; Cammenga Jorg; Foretz Marc; Viollet Benoit; Vukovic Milica; Villacreces Arnaud; Kranc Kamil; Carmeliet Peter; Marot Guillemette; Boulter Alexis; Tavernier Simon; Berod Luciana; Longhi Maria P.; Paget Christophe; Janssens Sophie; Staumont-Salle Delphine; Aksoy Ezra; Staels Bart; Dombrowicz David;
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Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille CHU Lille EGID CNRS UMR 8199 F-59019 Lille France;

Univ Lille Inst Pasteur Lille CHU Lille EGID CNRS UMR 8199 F-59019 Lille France;

Tokushima Univ Fujii Mem Inst Med Sci Inst Adv Med Sci Tokushima 7708503 Japan;

Linkoping Univ Inst Clin &

Expt Med Dept Hematol S-58185 Linkoping Sweden;

Linkoping Univ Inst Clin &

Expt Med Dept Hematol S-58185 Linkoping Sweden;

Univ Paris 05 Sorbonne Paris Cite F-75006 Paris France;

Univ Paris 05 Sorbonne Paris Cite F-75006 Paris France;

Queen Mary Univ London Barts &

London Sch Med &

Dent Ctr Haematooncol London EC1M 6BQ England;

Queen Mary Univ London Barts &

London Sch Med &

Dent Ctr Haematooncol London EC1M 6BQ England;

Queen Mary Univ London Barts &

London Sch Med &

Dent Ctr Haematooncol London EC1M 6BQ England;

VIB Lab Angiogenesis &

Vasc Metab Ctr Canc Biol B-3000 Leuven Belgium;

Univ Lille MODAL Team Inria Lille Nord Europe F-59650 Villeneuve Dascq France;

Univ Florida Coll Med Gainesville FL 32610 USA;

Univ Ghent Lab Immunoregulat &

Mucosal Immunol VIB Ctr Inflammat Res B-9052 Ghent Belgium;

TWINCORE Inst Infect Immunol Ctr Expt &

Clin Infect Res D-30625 Hannover Niedersachsen Germany;

Queen Mary Univ London Barts &

London Sch Med &

Dent William Harvey Res Inst London EC1M 6BQ England;

Univ Tours INSERM CEPR UMR 1100 F-37041 Tours France;

Univ Ghent Dept Internal Med &

Pediat B-9052 Ghent Belgium;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Queen Mary Univ London Ctr Biochem Pharmacol William Harvey Res Inst London EC1M 6BQ England;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

Univ Lille Inst Pasteur Lille EGID INSERM CHU Lille U1011 F-59019 Lille France;

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中图分类细胞生物学;
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1. Metabolic and Innate Immune Cues Merge into a Specific Inflammatory Response via the UPR [J] . Mogilenko Denis A., Haas Joel T., Lhomme Laurent, Cell . 2019,第5期

机译：代谢和先天免疫提示通过UPR合并成特定的炎症反应
2. Similar Metabolic, Innate Immunity, and Adipokine Profiles in Adult and Pediatric Sepsis Versus Systemic Inflammatory Response Syndrome-A Pilot Study [J] . Tavladaki Theonymfi, Spanaki Anna Maria, Dimitriou Helen, Pediatric critical care medicine: a journal of the Society of Critical Care Medicine and the World Federation of Pediatric Intensive and Critical Care Societies . 2017,第11期

机译：在成人和儿科脓毒症中类似的代谢，先天免疫和己平曲线与全身炎症反应综合征 - 一项试验研究
3. Unfolded protein response (UPR) signaling regulates arsenic trioxide-mediated macrophage innate immune function disruption [J] . SrivastavaR.K., LiC., ChaudharyS.C., Toxicology and Applied Pharmacology . 2013,第3期

机译：折叠蛋白反应（UPR）信号调节三氧化二砷介导的巨噬细胞先天免疫功能破坏
4. Innate immune responses in inflammatory bowel disease [C] . E. CARIO, D. K. PODOLSK Falk Symposium . 2007

机译：炎症性肠病中的先天免疫反应
5. Host response in cutaneous inflammatory disorders: Mechanisms of innate and adaptive immunity. [D] . Kim, Jenny Jiyon. 2001

机译：皮肤炎性疾病中的宿主反应：先天和适应性免疫的机制。
6. Innate immune response to pulmonary contusion: Identification of cell-type specific inflammatory responses [O] . J. Jason Hoth, Jonathan D. Wells, Barbara K. Yoza, -1

机译：肺挫伤的先天免疫反应：鉴定细胞型特异性炎症反应
7. Metabolic and Innate Immune Cues Merge into a Specific Inflammatory Response via the UPR [O] . Denis A. Mogilenko, Joel T. Haas, Laurent L’homme, 2019

机译：代谢和先天免疫提示通过UPR合并成特定的炎症反应

Metabolic and Innate Immune Cues Merge into a Specific Inflammatory Response via the UPR

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