Metabolic Routes in Inflammation: The Citrate Pathway and its Potential as Therapeutic Target-Reference-Cited by-同舟云学术

Metabolic Routes in Inflammation: The Citrate Pathway and its Potential as Therapeutic Target

Published:2020-01-03 Issue:40 Volume:26 Page:7104-7116
ISSN:0929-8673
Container-title:Current Medicinal Chemistry
language:en
Short-container-title:CMC

Author:

Infantino Vittoria¹,Pierri Ciro Leonardo²,Iacobazzi Vito²

Affiliation:

1. Department of Science, University of Basilicata, Potenza, Italy

2. Department of Biosciences, Biotechnology and Biopharmaceutics, University of Bari, Bari, Italy

Abstract

Significant metabolic changes occur in inflammation to respond to the new energetic needs of cells. Mitochondria are addressed not only to produce ATP, but also to supply substrates, such citrate, to produce pro-inflammatory molecules. In this context, most of the citrate is diverted from Krebs cycle and channeled into the “citrate pathway” leading to the increase in the export of citrate into cytosol by the Mitochondrial Citrate Carrier (CIC) followed by its cleavage into acetyl-CoA and oxaloacetate by ATP Citrate Lyase (ACLY). Acetyl- CoA is used to produce PGE2 and oxaloacetate to make NADPH needed for NO and ROS production. In addition, cytosolic citrate also provides precursors for itaconate synthesis. Citrate- derived itaconate acts as a negative regulator of inflammation by modulating the synthesis of the inflammatory mediators. Inhibition of CIC or ACLY by different synthetic and natural molecules results in the reduction of NO, ROS and PGE2 levels suggesting that the citrate pathway can be a new target to be addressed in inflammation. Beneficial effects can be obtained also in the oxidative stress and inflammatory conditions observed in Down syndrome.

Publisher

Bentham Science Publishers Ltd.

Subject

Pharmacology,Molecular Medicine,Drug Discovery,Biochemistry,Organic Chemistry

Reference63 articles.

1. Waguri-Nagaya Y.; Otsuka T.; Sugimura I.; Matsui N.; Asai K.; Nakajima K.; Tada T.; Akiyama S.; Kato T.; Synovial inflammation and hyperplasia induced by gliostatin/platelet-derived endothelial cell growth factor in rabbit knees. Rheumatol Int 2000,20(1),13-19

2. O’Neill L.A.; Hardie D.G.; Metabolism of inflammation limited by AMPK and pseudo-starvation. Nature 2013,493(7432),346-355

3. Akiyama H.; Barger S.; Barnum S.; Bradt B.; Bauer J.; Cole G.M.; Cooper N.R.; Eikelenboom P.; Emmerling M.; Fiebich B.L.; Finch C.E.; Frautschy S.; Griffin W.S.; Hampel H.; Hull M.; Landreth G.; Lue L.; Mrak R.; Mackenzie I.R.; McGeer P.L.; O’Banion M.K.; Pachter J.; Pasinetti G.; Plata-Salaman C.; Rogers J.; Rydel R.; Shen Y.; Streit W.; Strohmeyer R.; Tooyoma I.; Van Muiswinkel F.L.; Veerhuis R.; Walker D.; Webster S.; Wegrzyniak B.; Wenk G.; Wyss-Coray T.; Inflammation and Alzheimer’s disease. Neurobiol Aging 2000,21(3),383-421

4. Chandel N.S.; Mitochondria as signaling organelles. BMC Biol 2014,12,34

5. Murphy M.P.; How mitochondria produce reactive oxygen species. Biochem J 2009,417(1),1-13

Cited by 62 articles. 订阅此论文施引文献订阅此论文施引文献，注册后可以免费订阅5篇论文的施引文献，订阅后可以查看论文全部施引文献

1. Unveiling the toxicological effects and risks of prometryn on red swamp crayfish (Procambarus clarkii): Health assessments, ecological, and molecular insights;Science of The Total Environment;2024-11

2. Non-target metabolomics unravels the effect and mechanism of Lianpu Drink on spleen-stomach damp-heat syndrome;Journal of Chromatography B;2024-10

3. Transcriptional Regulation and Function of Malic Enzyme 1 in Human Macrophage Activation;Biomedicines;2024-09-13

4. Heterocyclic Nitrogen Compounds as Potential PDE4B Inhibitors in Activated Macrophages;Applied Sciences;2024-08-02

5. Metabolic Adaptations and Functional Activity of Macrophages in Homeostasis and Inflammation;Biochemistry (Moscow);2024-05