Your search keyword '"LIPID MEDIATORS"' showing total 1,863 results

51. Lipid mediators of cerebrospinal fluid in response to TBE and bacterial co-infections.

Author

Groth, Monika, Skrzydlewska, Elżbieta, Czupryna, Piotr, Biernacki, Michał, and Moniuszko-Malinowska, Anna

Subjects

*MIXED infections, *OXIDANT status, *LYME disease, *TICK-borne encephalitis, *TICK-borne diseases, *CEREBROSPINAL fluid examination, *RUMEN (Ruminants)

Abstract

T ick-borne diseases are caused by monoinfection or co-infection with different pathogens, including viruses, bacteria and protozoa. Tick-borne diseases are usually accompanied by oxidative stress which promotes the modifications of the host's lipid metabolism. The aim of the study was to compare total antioxidant status and the level of lipid mediators in the cerebrospinal fluid in response to tick-borne encephalitis (TBE) and bacterial co-infections that cause diseases such as that is Lyme borreliosis (LB) and human granulocytic anaplasmosis (HGA). In our study cerebrospinal fluid samples were obtained from 15 patients with TBE and 6 patients with TBE co-infection with LB and/or HGA at admission and after treatment. Control group consisted of 14 patients in whom meningitis was excluded. Total antioxidant status, levels of lipid peroxidation products, endocannabinoids and eicosanoids (determined by liquid and gas chromatography–mass spectrometry) were compared between the groups. It was found that in TBE patients, total antioxidant status was decreased and accompanied by increased levels of lipid peroxidation products (4-HNE, MDA, isoprostanes and neuroprostanes), major endocannabinoids (AEA and 2AG), and eicosanoids (both anti-inflammatory and pro-inflammatory), which generally declined after treatment. On the other hand, in co-infections, significant changes in the levels of some lipid mediators were observed even after the treatment. TBE alone or along with bacterial co-infections promote redox balance disturbances in the cerebrospinal fluid leading to oxidative stress and increased metabolism of phospholipids in the brain tissue reflected in the level of lipid peroxidation products and lipid mediators. Changes in the level of lipid mediators in patients with co-infections after treatment suggest further intensification of metabolic disturbances rather than their resolution. [Display omitted] • TBE as well as bacterial co-infections, promote redox balance disorders in the brain. • Endocannabinoids and eicosanoids increase in TBE and bacterial co-infections. • Endocannabinoids and eicosanoids levels do not change despite standard therapy. • Supplementation with antioxidants may be beneficial in TBE. [ABSTRACT FROM AUTHOR]

Published

2023

52. Ocular Treatments Targeting Separate Prostaglandin Receptors in Mice Exhibit Alterations in Intraocular Pressure and Optic Nerve Lipidome.

Author

Arcuri, Jennifer, Elbaz, Abdelrahman, Sharif, Najam A., and Bhattacharya, Sanjoy K.

Subjects

*PROSTAGLANDIN receptors, *OPTIC nerve, *INTRAOCULAR pressure, *LABORATORY mice, *RETINAL ganglion cells, *OPEN-angle glaucoma, *LIPIDOMICS

Abstract

Background: Prostaglandin (PG) receptor agonists are the first-line eyedrop medication treatment for glaucoma. The pathophysiology of this disease is not completely known, and elevated intraocular pressure (IOP) is the key risk factor. The membranes of the axons (of the retinal ganglion cells) passing through the optic nerve (ON) head experience significant damage. Lipids are an essential component of the cell's membranes, and their profile changes owing to neurodegeneration. In this investigation, three agonists for distinct PG receptors were used to lower IOP and to determine their effect on the ON lipids. We utilized DBA/2J mice as a model of progressive IOP increase and C57BL/6J mice as a model of ON crush. Methods: DBA/2J and C57BL/6J mice were treated daily for 2 weeks with Latanoprost, PF-04217329, or Rivenprost. The IOP was measured every 2 days and pattern electroretinogram was conducted for DBA/2J throughout the study. Lipidomics of ONs were performed for each model and treatment group. Results: Of the tested compounds, Latanoprost and Rivenprost were the most effective agents decreasing IOP in DBA/2J mice. Triglyceride levels increased in the ONs of DBA/2J mouse model, but phosphatidylethanolamine levels underwent highest level changes in the C57BL/6J mouse model when treated with Latanoprost. Conclusions: Topical ocular FP- and EP4-receptor agonists appreciably lowered IOP in the DBA/2J mice representing pigmentary glaucoma. The observed changes in ON lipidomics in the different models of neurodegeneration suggest possible use of such measures in the development of more effective medicines for both IOP reduction and ON protection. [ABSTRACT FROM AUTHOR]

Published

2023

53. First-Row Transition Metal Complexes Incorporating the 2-(2′-pyridyl)quinoxaline Ligand (pqx), as Potent Inflammatory Mediators: Cytotoxic Properties and Biological Activities against the Platelet-Activating Factor (PAF) and Thrombin.

Author

Margariti, Antigoni, Papakonstantinou, Vasiliki D., Stamatakis, George M., Demopoulos, Constantinos A., Machalia, Christina, Emmanouilidou, Evangelia, Schnakenburg, Gregor, Nika, Maria-Christina, Thomaidis, Nikolaos S., and Philippopoulos, Athanassios I.

Subjects

*INFLAMMATORY mediators, *THROMBIN, *MOLECULAR structure, *QUINOXALINES, *TRANSITION metal complexes, *DIMETHYL sulfoxide

Abstract

Inflammatory mediators constitute a recently coined term in the field of metal-based complexes with antiplatelet activities. Our strategy targets Platelet-Activating Factor (PAF) and its receptor, which is the most potent lipid mediator of inflammation. Thus, the antiplatelet (anti-PAF) potency of any substance could be exerted by inhibiting the PAF-induced aggregation in washed rabbit platelets (WRPs), which internationally is a well-accepted methodology. Herein, a series of mononuclear (mer-[Cr(pqx)Cl3(H2O]) (1), [Co(pqx)Cl2(DMF)] (2) (DMF = N,N′-dimethyl formamide), [Cu(pqx)Cl2(DMSO)] (3) (DMSO = dimethyl sulfoxide), [Zn(pqx)Cl2] (4)) and dinuclear complexes ([Mn(pqx)(H2O)2Cl2]2 (5), [Fe(pqx)Cl2]2 (6) and [Ni(pqx)Cl2]2 (7)) incorporating the 2-(2′-pyridyl)quinoxaline ligand (pqx), were biologically evaluated as inhibitors of the PAF- and thrombin-induced aggregation in washed rabbit platelets (WRPs). The molecular structure of the five-co-ordinate analog (3) has been elucidated by single-crystal X-ray diffraction revealing a trigonal bipyramidal geometry. All complexes are potent inhibitors of the PAF-induced aggregation in WRPs in the micromolar range. Complex (6) displayed a remarkable in vitro dual inhibition against PAF and thrombin, with IC50 values of 1.79 μM and 0.46 μM, respectively. Within the series, complex (5) was less effective (IC50 = 39 μM) while complex (1) was almost 12-fold more potent against PAF, as opposed to thrombin-induced aggregation. The biological behavior of complexes 1, 6 and 7 on PAF's basic metabolic enzymatic pathways reveals that they affect key biosynthetic and catabolic enzymes of PAF underlying the anti-inflammatory properties of the relevant complexes. The in vitro cytotoxic activities of all complexes in HEK293T (human embryonic kidney cells) and HeLa cells (cervical cancer cells) are described via the 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyl tetrazolium bromide (MTT) assay. The results reveal that complex 3 is the most potent within the series. [ABSTRACT FROM AUTHOR]

Published

2023

54. Differential impact of 5-lipoxygenase-activating protein antagonists on the biosynthesis of leukotrienes and of specialized pro-resolving mediators.

Author

Dahlke, Philipp, Peltner, Lukas K., Jordan, Paul M., and Werz, Oliver

Subjects

PROTEIN synthesis, LEUKOTRIENES, ARACHIDONIC acid, LIPOXINS, DOCOSAHEXAENOIC acid, MUSCARINIC receptors

Abstract

Lipoxygenases (LOX) transform arachidonic acid (AA, C20:4) and docosahexaenoic acid (DHA, C22:6) into bioactive lipid mediators (LMs) that comprise not only pro-inflammatory leukotrienes (LTs) but also the specialized pro-resolving mediators (SPMs) that promote inflammation resolution and tissue regeneration. The 5-LOX-activating protein (FLAP) is known to provide AA as a substrate to 5-LOX for generating LTs, such as LTB4, a potent chemoattractant and activator of phagocytes. Notably, 5-LOX is also involved in the biosynthesis of certain SPMs, namely, lipoxins and D-resolvins, implying a role of FLAP in SPM formation. FLAP antagonists have been intensively developed as LT biosynthesis inhibitors, but how they impact SPM formation is a matter of debate. Here, we show that FLAP antagonism suppresses the conversion of AA by 5-LOX to LT and lipoxins, while the conversion of DHA to SPM is unaffected. Screening of multiple prominent FLAP antagonists for their effects on LM formation in human M1- and M2-monocyte-derived macrophages by comprehensive LM profiling showed that all nine compounds reduced the production of 5-LOX-derived LTs but increased the formation of SPMs from DHA, e.g., resolvin D5. Some FLAP antagonists, especially those that contain an indole or benzimidazole moiety, even elicited SPM formation in resting M2-monocyte-derived macrophages. Intriguingly, in coincubations of human neutrophils and platelets that produce substantial AAderived lipoxin and DHA-derived RvD5, FLAP antagonism abolished lipoxin formation, but resolvin D5 levels remained unaffected. Conclusively, antagonism of FLAP suppresses the conversion of AA by 5-LOX to LTs and lipoxins but not the conversion of DHA by 5-LOX to SPM, which should be taken into account for the development of such compounds as antiinflammatory drugs. [ABSTRACT FROM AUTHOR]

Published

2023

55. n-3 Polyunsaturated Fatty Acids Modulate LPS-Induced ARDS and the Lung–Brain Axis of Communication in Wild-Type versus Fat-1 Mice Genetically Modified for Leukotriene B4 Receptor 1 or Chemerin Receptor 23 Knockout.

Author

Hernandez, Jessica, Schäffer, Julia, Herden, Christiane, Pflieger, Fabian Johannes, Reiche, Sylvia, Körber, Svenja, Kitagawa, Hiromu, Welter, Joelle, Michels, Susanne, Culmsee, Carsten, Bier, Jens, Sommer, Natascha, Kang, Jing X., Mayer, Konstantin, Hecker, Matthias, and Rummel, Christoph

Subjects

*CHEMERIN, *OMEGA-3 fatty acids, *ADULT respiratory distress syndrome, *OMEGA-6 fatty acids, *UNSATURATED fatty acids, *PNEUMONIA, *LUNG diseases, *IMMUNOSTAINING

Abstract

Specialized pro-resolving mediators (SPMs) and especially Resolvin E1 (RvE1) can actively terminate inflammation and promote healing during lung diseases such as acute respiratory distress syndrome (ARDS). Although ARDS primarily affects the lung, many ARDS patients also develop neurocognitive impairments. To investigate the connection between the lung and brain during ARDS and the therapeutic potential of SPMs and its derivatives, fat-1 mice were crossbred with RvE1 receptor knockout mice. ARDS was induced in these mice by intratracheal application of lipopolysaccharide (LPS, 10 µg). Mice were sacrificed at 0 h, 4 h, 24 h, 72 h, and 120 h post inflammation, and effects on the lung, liver, and brain were assessed by RT-PCR, multiplex, immunohistochemistry, Western blot, and LC-MS/MS. Protein and mRNA analyses of the lung, liver, and hypothalamus revealed LPS-induced lung inflammation increased inflammatory signaling in the hypothalamus despite low signaling in the periphery. Neutrophil recruitment in different brain structures was determined by immunohistochemical staining. Overall, we showed that immune cell trafficking to the brain contributed to immune-to-brain communication during ARDS rather than cytokines. Deficiency in RvE1 receptors and enhanced omega-3 polyunsaturated fatty acid levels (fat-1 mice) affect lung–brain interaction during ARDS by altering profiles of several inflammatory and lipid mediators and glial activity markers. [ABSTRACT FROM AUTHOR]

Published

2023

56. The oxylipin profile is associated with development of type 1 diabetes: the Diabetes Autoimmunity Study in the Young (DAISY)

Author

Buckner, Teresa, Vanderlinden, Lauren A, DeFelice, Brian C, Carry, Patrick M, Kechris, Katerina, Dong, Fran, Fiehn, Oliver, Frohnert, Brigitte I, Clare-Salzler, Michael, Rewers, Marian, and Norris, Jill M

Subjects

Nutrition, Prevention, Autoimmune Disease, Clinical Research, Diabetes, Aetiology, 2.1 Biological and endogenous factors, Metabolic and endocrine, Adolescent, Arachidonic Acid, Autoantibodies, Autoimmunity, Case-Control Studies, Child, Child, Preschool, Chromatography, High Pressure Liquid, Diabetes Mellitus, Type 1, Docosahexaenoic Acids, Female, Follow-Up Studies, Glutamate Decarboxylase, HLA-DR3 Antigen, HLA-DR4 Antigen, Humans, Insulin, Linoleic Acid, Male, Oxylipins, Prospective Studies, Receptor-Like Protein Tyrosine Phosphatases, Class 8, Tandem Mass Spectrometry, Inflammation, Lipid mediators, Paediatric, Proinflammatory, Pro-resolving, Type 1 diabetes, Clinical Sciences, Paediatrics and Reproductive Medicine, Public Health and Health Services, Endocrinology & Metabolism

Abstract

Aims/hypothesisOxylipins are lipid mediators derived from polyunsaturated fatty acids. Some oxylipins are proinflammatory (e.g. those derived from arachidonic acid [ARA]), others are pro-resolving of inflammation (e.g. those derived from α-linolenic acid [ALA], docosahexaenoic acid [DHA] and eicosapentaenoic acid [EPA]) and others may be both (e.g. those derived from linoleic acid [LA]). The goal of this study was to examine whether oxylipins are associated with incident type 1 diabetes.MethodsWe conducted a nested case-control analysis in the Diabetes Autoimmunity Study in the Young (DAISY), a prospective cohort study of children at risk of type 1 diabetes. Plasma levels of 14 ARA-derived oxylipins, ten LA-derived oxylipins, six ALA-derived oxylipins, four DHA-derived oxylipins and two EPA-related oxylipins were measured by ultra-HPLC-MS/MS at multiple timepoints related to autoantibody seroconversion in 72 type 1 diabetes cases and 71 control participants, which were frequency matched on age at autoantibody seroconversion (of the case), ethnicity and sample availability. Linear mixed models were used to obtain an age-adjusted mean of each oxylipin prior to type 1 diabetes. Age-adjusted mean oxylipins were tested for association with type 1 diabetes using logistic regression, adjusting for the high risk HLA genotype HLA-DR3/4,DQB1*0302. We also performed principal component analysis of the oxylipins and tested principal components (PCs) for association with type 1 diabetes. Finally, to investigate potential critical timepoints, we examined the association of oxylipins measured before and after autoantibody seroconversion (of the cases) using PCs of the oxylipins at those visits.ResultsThe ARA-related oxylipin 5-HETE was associated with increased type 1 diabetes risk. Five LA-related oxylipins, two ALA-related oxylipins and one DHA-related oxylipin were associated with decreased type 1 diabetes risk. A profile of elevated LA- and ALA-related oxylipins (PC1) was associated with decreased type 1 diabetes risk (OR 0.61; 95% CI 0.40, 0.94). A profile of elevated ARA-related oxylipins (PC2) was associated with increased diabetes risk (OR 1.53; 95% CI 1.03, 2.29). A critical timepoint analysis showed type 1 diabetes was associated with a high ARA-related oxylipin profile at post-autoantibody-seroconversion but not pre-seroconversion.Conclusions/interpretationThe protective association of higher LA- and ALA-related oxylipins demonstrates the importance of both inflammation promotion and resolution in type 1 diabetes. Proinflammatory ARA-related oxylipins may play an important role once the autoimmune process has begun.

Published

2021

57. Lipid droplets in pathogen infection and host immunity

Author

Tan, Yan-jie, Jin, Yi, Zhou, Jun, and Yang, Yun-fan

Published

2024

58. Plasma and serum oxylipin, endocannabinoid, bile acid, steroid, fatty acid and nonsteroidal anti-inflammatory drug quantification in a 96-well plate format

Author

Pedersen, Theresa L, Gray, Ira J, and Newman, John W

Subjects

Analytical Chemistry, Chemical Sciences, Nutrition, Aged, Anti-Inflammatory Agents, Anti-Inflammatory Agents, Non-Steroidal, Bile Acids and Salts, Chromatography, Liquid, Endocannabinoids, Fatty Acids, Female, Humans, Male, Oxylipins, Pharmaceutical Preparations, Steroids, Tandem Mass Spectrometry, Lipid mediators, High-throughput, Metabolic profiling, NIST SRM 1950, Other Chemical Sciences, Analytical chemistry, Chemical engineering, Nanotechnology

Abstract

The goal of this research was to develop a high-throughput, cost-effective method for metabolic profiling of lipid mediators and hormones involved in the regulation of inflammation and energy metabolism, along with polyunsaturated fatty acids and common over-the-counter non-steroidal anti-inflammatory drugs (NSAIDs). We describe a 96-well plate protein precipitation and filtration procedure for 50 μL of plasma or serum in the presence of 37 deuterated analogs and 2 instrument internal standards. Data is acquired in two back-to-back UPLC-MS/MS analyses using electrospray ionization with positive/negative switching and scheduled multiple reaction monitoring for the determination of 145 compounds, including oxylipins, endocannabinoids and like compounds, bile acids, glucocorticoids, sex steroids, polyunsaturated fatty acids, and 3 NSAIDs. Intra- and inter-batch variability was 70% of metabolites above the LOQ in both matrices, but higher inter-batch variability was observed for serum oxylipins and some bile acids. Results for NIST Standard Reference Material 1950, compared favorably with the 20 certified metabolite values covered by this assay, and we provide new data for oxylipins, N-acylethanolamides, glucocorticoids, and 17-hydroxy-progesterone in this material. Application to two independent cohorts of elderly men and women showed the routine detection of 86 metabolites, identified fasting state influences on essential fatty acid-derived oxylipins, N-acylethanolamides and conjugated bile acids, identified rare presence of high and low testosterone levels and the presence of NSAIDs in ∼10% of these populations. The described method appears valuable for investigations in large cohort studies to provide insight into metabolic cross-talk between the array of mediators assessed here.

Published

2021

59. Plasma Linoleate Diols Are Potential Biomarkers for Severe COVID-19 Infections

Author

McReynolds, Cindy B, Cortes-Puch, Irene, Ravindran, Resmi, Khan, Imran H, Hammock, Bruce G, Shih, Pei-an Betty, Hammock, Bruce D, and Yang, Jun

Subjects

Medical Biochemistry and Metabolomics, Biomedical and Clinical Sciences, Lung, Emerging Infectious Diseases, Infectious Diseases, Coronaviruses, 2.1 Biological and endogenous factors, Cardiovascular, Inflammatory and immune system, linoleate diol, lipid mediators, COVID-19, inflammation, leukotoxin, EpOME, DiHOME, ARDS, Physiology, Medical Physiology, Psychology, Biochemistry and cell biology, Medical physiology

Abstract

Polyunsaturated fatty acids are metabolized into regulatory lipids important for initiating inflammatory responses in the event of disease or injury and for signaling the resolution of inflammation and return to homeostasis. The epoxides of linoleic acid (leukotoxins) regulate skin barrier function, perivascular and alveolar permeability and have been associated with poor outcomes in burn patients and in sepsis. It was later reported that blocking metabolism of leukotoxins into the vicinal diols ameliorated the deleterious effects of leukotoxins, suggesting that the leukotoxin diols are contributing to the toxicity. During quantitative profiling of fatty acid chemical mediators (eicosanoids) in COVID-19 patients, we found increases in the regioisomeric leukotoxin diols in plasma samples of hospitalized patients suffering from severe pulmonary involvement. In rodents these leukotoxin diols cause dramatic vascular permeability and are associated with acute adult respiratory like symptoms. Thus, pathways involved in the biosynthesis and degradation of these regulatory lipids should be investigated in larger biomarker studies to determine their significance in COVID-19 disease. In addition, incorporating diols in plasma multi-omics of patients could illuminate the COVID-19 pathological signature along with other lipid mediators and blood chemistry.

Published

2021

60. Combined Therapy With Avastin, a PAF Receptor Antagonist and a Lipid Mediator Inhibited Glioblastoma Tumor Growth

Author

Flores, Valerie A Cruz, Menghani, Hemant, Mukherjee, Pranab K, Marrero, Luis, Obenaus, Andre, Dang, Quan, Khoutorova, Larissa, Reid, Madigan M, Belayev, Ludmila, and Bazan, Nicolas G

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Brain Disorders, Rare Diseases, Brain Cancer, Neurosciences, Cancer, glioma, platelet-activating factor, lipid mediators, oncology, stroke, Pharmacology and Pharmaceutical Sciences, Pharmacology and pharmaceutical sciences

Abstract

Glioblastoma multiforme (GBM) is an aggressive, highly proliferative, invasive brain tumor with a poor prognosis and low survival rate. The current standard of care for GBM is chemotherapy combined with radiation following surgical intervention, altogether with limited efficacy, since survival averages 18 months. Improvement in treatment outcomes for patients with GBM requires a multifaceted approach due to the dysregulation of numerous signaling pathways. Recently emerging therapies to precisely modulate tumor angiogenesis, inflammation, and oxidative stress are gaining attention as potential options to combat GBM. Using a mouse model of GBM, this study aims to investigate Avastin (suppressor of vascular endothelial growth factor and anti-angiogenetic treatment), LAU-0901 (a platelet-activating factor receptor antagonist that blocks pro-inflammatory signaling), Elovanoid; ELV, a novel pro-homeostatic lipid mediator that protects neural cell integrity and their combination as an alternative treatment for GBM. Female athymic nude mice were anesthetized with ketamine/xylazine, and luciferase-modified U87MG tumor cells were stereotactically injected into the right striatum. On post-implantation day 13, mice received one of the following: LAU-0901, ELV, Avastin, and all three compounds in combination. Bioluminescent imaging (BLI) was performed on days 13, 20, and 30 post-implantation. Mice were perfused for ex vivo MRI on day 30. Bioluminescent intracranial tumor growth percentage was reduced by treatments with LAU-0901 (43%), Avastin (77%), or ELV (86%), individually, by day 30 compared to saline treatment. In combination, LAU-0901/Avastin, ELV/LAU-0901, or ELV/Avastin had a synergistic effect in decreasing tumor growth by 72, 92, and 96%, respectively. Additionally, tumor reduction was confirmed by MRI on day 30, which shows a decrease in tumor volume by treatments with LAU-0901 (37%), Avastin (67%), or ELV (81.5%), individually, by day 30 compared to saline treatment. In combination, LAU-0901/Avastin, ELV/LAU-0901, or ELV/Avastin had a synergistic effect in decreasing tumor growth by 69, 78.7, and 88.6%, respectively. We concluded that LAU-0901 and ELV combined with Avastin exert a better inhibitive effect in GBM progression than monotherapy. To our knowledge, this is the first study that demonstrates the efficacy of these novel therapeutic regimens in a model of GBM and may provide the basis for future therapeutics in GBM patients.

Published

2021

61. Combined Therapy With Avastin, a PAF Receptor Antagonist and a Lipid Mediator Inhibited Glioblastoma Tumor Growth.

Author

Cruz Flores, Valerie A, Menghani, Hemant, Mukherjee, Pranab K, Marrero, Luis, Obenaus, Andre, Dang, Quan, Khoutorova, Larissa, Reid, Madigan M, Belayev, Ludmila, and Bazan, Nicolas G

Subjects

glioma, lipid mediators, oncology, platelet-activating factor, stroke, Brain Disorders, Neurosciences, Cancer, Rare Diseases, Brain Cancer, Pharmacology and Pharmaceutical Sciences

Abstract

Glioblastoma multiforme (GBM) is an aggressive, highly proliferative, invasive brain tumor with a poor prognosis and low survival rate. The current standard of care for GBM is chemotherapy combined with radiation following surgical intervention, altogether with limited efficacy, since survival averages 18 months. Improvement in treatment outcomes for patients with GBM requires a multifaceted approach due to the dysregulation of numerous signaling pathways. Recently emerging therapies to precisely modulate tumor angiogenesis, inflammation, and oxidative stress are gaining attention as potential options to combat GBM. Using a mouse model of GBM, this study aims to investigate Avastin (suppressor of vascular endothelial growth factor and anti-angiogenetic treatment), LAU-0901 (a platelet-activating factor receptor antagonist that blocks pro-inflammatory signaling), Elovanoid; ELV, a novel pro-homeostatic lipid mediator that protects neural cell integrity and their combination as an alternative treatment for GBM. Female athymic nude mice were anesthetized with ketamine/xylazine, and luciferase-modified U87MG tumor cells were stereotactically injected into the right striatum. On post-implantation day 13, mice received one of the following: LAU-0901, ELV, Avastin, and all three compounds in combination. Bioluminescent imaging (BLI) was performed on days 13, 20, and 30 post-implantation. Mice were perfused for ex vivo MRI on day 30. Bioluminescent intracranial tumor growth percentage was reduced by treatments with LAU-0901 (43%), Avastin (77%), or ELV (86%), individually, by day 30 compared to saline treatment. In combination, LAU-0901/Avastin, ELV/LAU-0901, or ELV/Avastin had a synergistic effect in decreasing tumor growth by 72, 92, and 96%, respectively. Additionally, tumor reduction was confirmed by MRI on day 30, which shows a decrease in tumor volume by treatments with LAU-0901 (37%), Avastin (67%), or ELV (81.5%), individually, by day 30 compared to saline treatment. In combination, LAU-0901/Avastin, ELV/LAU-0901, or ELV/Avastin had a synergistic effect in decreasing tumor growth by 69, 78.7, and 88.6%, respectively. We concluded that LAU-0901 and ELV combined with Avastin exert a better inhibitive effect in GBM progression than monotherapy. To our knowledge, this is the first study that demonstrates the efficacy of these novel therapeutic regimens in a model of GBM and may provide the basis for future therapeutics in GBM patients.

Published

2021

62. Assessment of novel drugs for treating preterm labour using a translational model

Author

Mohammed, Ammar, Harris, Lynda, Marshall, Kay, and Fischer, Deborah

Subjects

618.3, COX, Placenta, SE175, Liposomes, LOX, lipid mediators, Targeted Drug Delivery, Uterine stimulants, Rock inhibitors, Ripasudil, Mouse oestrous cycle, Nitric oxide, Pregnancy complications, Preterm Labour

Abstract

The uterus and placenta are essential organs playing key roles in reproductive processes. Labour is modulated by several factors such as sex hormones, nitric oxide, prostaglandins and the ROCK pathway, which stimulate the uterus via the phosphorylation of myosin-light chain (MLC). Abnormal function of these factors may lead to preterm labour (PTL) which still has no effective management strategies. The aims of this project were to: (i) examine the regulation of myometrial contractility in non-pregnant and pregnant mice, (ii) assess the ability of ripasudil (a ROCK inhibitor) to diminish uterine contractions, (iii) evaluate the effect of NO on myometrial contractility, and (iv) investigate the influence of administrating empty and NO-loaded liposomes on the level of lipid mediators in the uterus and placenta from C57 and eNOS KO pregnant mice at term. Results showed a significant higher contractility of the upper segment of uterus as compared to the lower segment (p < 0.05). During pregnancy, stimulation of the uterus by oxytocin, U46619 and 5-HT upregulates the production of the di-phosphorylated MLC by 378.1%, 379.6% and 271%, respectively. Ripasudil was able to inhibit spontaneous and drug-induced myometrial contractility in non-pregnant and pregnant mice. Ripasudil inhibited the mono- and di-phosphorylation of MLC in the myometrium from both mice; it was more effective on ppMLC formation (88.61% and 86.76%). The lack of NO caused a significant increase in myometrial (by 132.5%) and amplitude of contractions (by 132.1%) in eNOS KOs. Vehicle- and SE175-Liposome treatments led to a significant reduction in the level of Cyclooxygenase (COX) and Lipoxygenase (LOX) derived lipid mediators in the myometrium and placentas from pregnant C57 WT and eNOS KO mice. Exposure to the SE175-Liposome significantly increased the level of myometrial DHETs (by 199.1%, 153% and 450.6%) and placental DiHDPA (by >4×108 ) compared with the Free SE175. SE175 significantly increased the concetration of the 15 HETrE. The majority of lipid mediators detected were the LOXderived (myometrium) and COX-derived (placenta). In conclusion, the data support the higher myogenic activity of uterus in pregnant mice. It demonstrated for the first time that ppMLC is expressed in mouse myometrium and that ROCK inhibition is a promising tocolytic candidate for the treatment of PTL. Targeted liposomes were effective in modulating the level of certain lipid mediators. Administration of NOdonors at late pregnancy can regulate uterine activity and control placental blood flow.

Published

2020

63. Is Lipid Metabolism of Value in Cancer Research and Treatment? Part II: Role of Specialized Pro-Resolving Mediators in Inflammation, Infections, and Cancer

Author

Muhammad Usman Babar, Ala F. Nassar, Xinxin Nie, Tianxiang Zhang, Jianwei He, Jacky Yeung, Paul Norris, Hideki Ogura, Anne Muldoon, Lieping Chen, and Stephania Libreros

Subjects

lipid mediators, resolution, docosahexaenoic acid, efferocytosis, cancer, respiratory inflammation, Microbiology, QR1-502

Abstract

Acute inflammation is the body’s first defense in response to pathogens or injury that is partially governed by a novel genus of endogenous lipid mediators that orchestrate the resolution of inflammation, coined specialized pro-resolving mediators (SPMs). SPMs, derived from omega-3-polyunstaturated fatty acids (PUFAs), include the eicosapentaenoic acid-derived and docosahexaenoic acid-derived Resolvins, Protectins, and Maresins. Herein, we review their biosynthesis, structural characteristics, and therapeutic effectiveness in various diseases such as ischemia, viral infections, periodontitis, neuroinflammatory diseases, cystic fibrosis, lung inflammation, herpes virus, and cancer, especially focusing on therapeutic effectiveness in respiratory inflammation and ischemia-related injuries. Resolvins are sub-nanomolar potent agonists that accelerate the resolution of inflammation by reducing excessive neutrophil infiltration, stimulating macrophage functions including phagocytosis, efferocytosis, and tissue repair. In addition to regulating neutrophils and macrophages, Resolvins control dendritic cell migration and T cell responses, and they also reduce the pro-inflammatory cytokines, proliferation, and metastasis of cancer cells. Importantly, several lines of evidence have demonstrated that Resolvins reduce tumor progression in melanoma, oral squamous cell carcinoma, lung cancer, and liver cancer. In addition, Resolvins enhance tumor cell debris clearance by macrophages in the tumor’s microenvironment. Resolvins, with their unique stereochemical structure, receptors, and biosynthetic pathways, provide a novel therapeutical approach to activating resolution mechanisms during cancer progression.

Published

2024

64. Characterization of Lysophospholipase D Activity in Mammalian Cell Membranes

Author

Yuhuan Xie, Krishna M. Ella, Terra C. Gibbs, Marianne E. Yohannan, Stewart M. Knoepp, Pravita Balijepalli, G. Patrick Meier, and Kathryn E. Meier

Subjects

lipid mediators, phospholipases, signal transduction, Cytology, QH573-671

Abstract

Lysophosphatidic acid (LPA) is a lipid mediator that binds to G-protein-coupled receptors, eliciting a wide variety of responses in mammalian cells. Lyso-phospholipids generated via phospholipase A2 (PLA2) can be converted to LPA by a lysophospholipase D (lyso-PLD). Secreted lyso-PLDs have been studied in more detail than membrane-localized lyso-PLDs. This study utilized in vitro enzyme assays with fluorescent substrates to examine LPA generation in membranes from multiple mammalian cell lines (PC12, rat pheochromocytoma; A7r5, rat vascular smooth muscle; Rat-1, rat fibroblast; PC-3, human prostate carcinoma; and SKOV-3 and OVCAR-3, human ovarian carcinoma). The results show that membranes contain a lyso-PLD activity that generates LPA from a fluorescent alkyl-lyso-phosphatidylcholine, as well as from naturally occurring acyl-linked lysophospholipids. Membrane lyso-PLD and PLD activities were distinguished by multiple criteria, including lack of effect of PLD2 over-expression on lyso-PLD activity and differential sensitivities to vanadate (PLD inhibitor) and iodate (lyso-PLD inhibitor). Based on several lines of evidence, including siRNA knockdown, membrane lyso-PLD is distinct from autotaxin, a secreted lyso-PLD. PC-3 cells express GDE4 and GDE7, recently described lyso-PLDs that localize to membranes. These findings demonstrate that membrane-associated lyso-D activity, expressed by multiple mammalian cell lines, can contribute to LPA production.

Published

2024

65. Editorial: Lipidomics of oxylipins in biological systems.

Author

Patrignani, Paola, Schebb, Nils Helge, Werz, Oliver, and Steinhilber, Dieter

Subjects

LIPIDOMICS, OXYLIPINS, BIOLOGICAL systems

Published

2023

66. Lipid droplets control mitogenic lipid mediator production in human cancer cells

Author

Eva Jarc Jovičić, Anja Pucer Janež, Thomas O. Eichmann, Špela Koren, Vesna Brglez, Paul M. Jordan, Jana Gerstmeier, Duško Lainšček, Anja Golob-Urbanc, Roman Jerala, Gérard Lambeau, Oliver Werz, Robert Zimmermann, and Toni Petan

Subjects

Lipid droplets, Diacylglycerol acyltransferase, Adipose triglyceride lipase, Phospholipase A2, Lipid mediators, Cancer, Internal medicine, RC31-1245

Abstract

Objectives: Polyunsaturated fatty acids (PUFAs) are structural components of membrane phospholipids and precursors of oxygenated lipid mediators with diverse functions, including the control of cell growth, inflammation and tumourigenesis. However, the molecular pathways that control the availability of PUFAs for lipid mediator production are not well understood. Here, we investigated the crosstalk of three pathways in the provision of PUFAs for lipid mediator production: (i) secreted group X phospholipase A2 (GX sPLA2) and (ii) cytosolic group IVA PLA2 (cPLA2α), both mobilizing PUFAs from membrane phospholipids, and (iii) adipose triglyceride lipase (ATGL), which mediates the degradation of triacylglycerols (TAGs) stored in cytosolic lipid droplets (LDs). Methods: We combined lipidomic and functional analyses in cancer cell line models to dissect the trafficking of PUFAs between membrane phospholipids and LDs and determine the role of these pathways in lipid mediator production, cancer cell proliferation and tumour growth in vivo. Results: We demonstrate that lipid mediator production strongly depends on TAG turnover. GX sPLA2 directs ω-3 and ω-6 PUFAs from membrane phospholipids into TAG stores, whereas ATGL is required for their entry into lipid mediator biosynthetic pathways. ATGL controls the release of PUFAs from LD stores and their conversion into cyclooxygenase- and lipoxygenase-derived lipid mediators under conditions of nutrient sufficiency and during serum starvation. In starving cells, ATGL also promotes the incorporation of LD-derived PUFAs into phospholipids, representing substrates for cPLA2α. Furthermore, we demonstrate that the built-up of TAG stores by acyl-CoA:diacylglycerol acyltransferase 1 (DGAT1) is required for the production of mitogenic lipid signals that promote cancer cell proliferation and tumour growth. Conclusion: This study shifts the paradigm of PLA2-driven lipid mediator signalling and identifies LDs as central lipid mediator production hubs. Targeting DGAT1-mediated LD biogenesis is a promising strategy to restrict lipid mediator production and tumour growth.

Published

2023

67. Genetic deletion of 12/15 lipoxygenase delays vascular remodeling and limits cardiorenal dysfunction after pressure overload

Author

Dae Hyun Lee, Vasundhara Kain, Da-Zhi Wang, Donald G. Rokosh, Sumanth D. Prabhu, and Ganesh V. Halade

Subjects

Heart failure, Inflammation-resolution signaling, Lipid mediators, Lipoxygenase, Pressure overload, Transverse aortic constriction, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

The lipid metabolizing enzyme 12/15 lipoxygenase (12/15LOX) induces proinflammatory responses that may increase cardiovascular and renal complications after cardiac insult. To define the role of 12/15LOX, 8–12-week-old male C57BL/6J wild-type (WT; n = 49) and 12/15LOX−/− mice (n = 50) were subject to transverse aortic constriction (TAC) and monitored for 7, 28, and 56 days (d) post-TAC. Compared with WT, 12/15LOX−/− mice experienced less left ventricle (LV) dysfunction with limited LV hypertrophy and lung edema post-TAC. 12/15LOX deletion decreased TAC-induced proinflammatory mediators 12-HETE and prostaglandins with modulation in mir-7a-5p, mir 26a-5p, miR-21e-5p, and miR-107-3p during chronic remodeling period (after d28). At d7 post-TAC, 12/15LOX−/− mice showed increased cardiac gene expression of Arg-1 and the prostanoid receptors EP2 and EP4. The EP4 receptor expression was consistently elevated from d7 till d56 in 12/15LOX−/− mice post-TAC compared with WT controls. Post-TAC, wheat germ agglutinin staining revealed less cardiomyocyte hypertrophy at d28 and d56 in 12/15LOX−/− mice compared with WT. TAC-induced vascular remodeling was marked by disruption in the endothelium, evident by irregular CD31 staining and increased alpha-smooth muscle actin (α-SMA) in WT mice at d28 and d56. Compared to WT, 12/15LOX−/− mice exhibited a diminished expression of NGAL in the kidney, suggesting that 12/15LOX−/− reduced cardiorenal dysfunction post-TAC. In WT-TAC mice, structural analyses of the kidney revealed glomerular swelling during the maladaptive phase of heart failure, with decreases in the capsula glomeruli space and glomerular sclerosis compared to 12/15LOX−/− mice. Overall, vascular and kidney inflammation markers were higher in WT than in 12/15LOX−/− post-TAC. Thus, deletion of 12/15LOX limits LV hypertrophy associated with perivascular inflammation and cardiorenal remodeling after pressure overload. Deficiency of 12/15 LOX serves a dual role in delaying an early adaptive interstitial remodeling with long-term protective effects on cardiac hypertrophy and cardiac fibrosis and detrimental adverse vascular remodeling during later maladaptive remodeling after pressure overload.

Published

2023

68. Glucocorticoids regulate lipid mediator networks by reciprocal modulation of 15-lipoxygenase isoforms affecting inflammation resolution.

Author

Zhigang Rao, Brunner, Elena, Giszas, Benjamin, Iyer-Bierhoff, Aishwarya, Gerstmeier, Jana, Börner, Friedemann, Jordan, Paul M., Pace, Simona, Meyer, Katharina P. L., Hofstetter, Robert K., Merk, Daniel, Paulenz, Christian, Heinzel, Thorsten, Grunert, Philip C., Stallmach, Andreas, Serhan, Charles N., Werner, Markus, and Werz, Oliver

Subjects

*CRITICALLY ill, *INFLAMMATORY bowel diseases, *GLUCOCORTICOIDS, *COVID-19, *ANTI-inflammatory agents, *INFLAMMATION

Abstract

Glucocorticoids (GC) are potent anti-inflammatory agents, broadly used to treat acute and chronic inflammatory diseases, e.g., critically ill COVID-19 patients or patients with chronic inflammatory bowel diseases. GC not only limit inflammation but also promote its resolution although the underlying mechanisms are obscure. Here, we reveal reciprocal regulation of 15-lipoxygenase (LOX) isoform expression in human monocyte/macrophage lineages by GC with respective consequences for the biosynthesis of specialized proresolving mediators (SPM) and their 15-LOX-derived monohydroxylated precursors (mono-15-OH). Dexamethasone robustly up-regulated pre-mRNA, mRNA, and protein levels of ALOX15B/15-LOX-2 in blood monocyte--derived macrophage (MDM) phenotypes, causing elevated SPM and mono-15-OH production in inflammatory cell types. In sharp contrast, dexamethasone blocked ALOX15/15-LOX-1 expression and impaired SPM formation in proresolving M2-MDM. These dexamethasone actions were mimicked by prednisolone and hydrocortisone but not by progesterone, and they were counteracted by the GC receptor (GR) antagonist RU486. Chromatin immunoprecipitation (ChIP) assays revealed robust GR recruitment to a putative enhancer region within intron 3 of the ALOX15B gene but not to the transcription start site. Knockdown of 15-LOX-2 in M1-MDM abolished GC-induced SPM formation and mono-15-OH production. Finally, ALOX15B/15-LOX-2 upregulation was evident in human monocytes from patients with GC-treated COVID-19 or patients with IBD. Our findings may explain the proresolving GC actions and offer opportunities for optimizing GC pharmacotherapy and proresolving mediator production. [ABSTRACT FROM AUTHOR]

Published

2023

69. Short-Term Caloric Restriction and Subsequent Re-Feeding Compromise Liver Health and Associated Lipid Mediator Signaling in Aged Mice.

Author

Schädel, Patrick, Wichmann-Costaganna, Mareike, Czapka, Anna, Gebert, Nadja, Ori, Alessandro, and Werz, Oliver

Abstract

Aging is characterized by alterations in the inflammatory microenvironment, which is tightly regulated by a complex network of inflammatory mediators. Excessive calorie consumption contributes to age- and lifestyle-associated diseases like obesity, type 2 diabetes, cardiovascular disorders, and cancer, while limited nutrient availability may lead to systemic health-promoting adaptations. Geroprotective effects of short-term caloric restriction (CR) can beneficially regulate innate immune receptors and interferon signaling in the liver of aged mice, but how CR impacts the hepatic release of immunomodulatory mediators like cytokines and lipid mediators (LM) is elusive. Here, we investigated the impact of aging on the inflammatory microenvironment in the liver and its linkage to calorie consumption. The livers of female young and aged C57BL/6JRj mice, as well as of aged mice after caloric restriction (CR) up to 28 days, with and without subsequent re-feeding (2 days), were evaluated. Surprisingly, despite differences in the hepatic proteome of young and old mice, aging did not promote a pro-inflammatory environment in the liver, but it reduced lipoxygenase-mediated formation of LM from polyunsaturated fatty acids without affecting the expression of the involved lipoxygenases and related oxygenases. Moreover, CR failed to ameliorate the secretion of pro-inflammatory cytokines but shifted the LM production to the formation of monohydroxylated LM with inflammation-resolving features. Unexpectedly, re-feeding after CR even further decreased the inflammatory response as LM species were markedly downregulated. Our findings raise the question of how short-term CR is indeed beneficial as a nutritional intervention for healthy elderly subjects and further stress the necessity to address tissue-specific inflammatory states. [ABSTRACT FROM AUTHOR]

Published

2023

70. Get me out of here: Sphingosine 1‐phosphate signaling and T cell exit from tissues during an immune response.

Author

Hallisey, Victoria M. and Schwab, Susan R.

Subjects

*T cells, *IMMUNE response, *SPHINGOSINE, *CELL communication, *LYMPHOID tissue

Abstract

Summary: During an immune response, the duration of T cell residence in lymphoid and non‐lymphoid tissues likely affects T cell activation, differentiation, and memory development. The factors that govern T cell transit through inflamed tissues remain incompletely understood, but one important determinant of T cell exit from tissues is sphingosine 1‐phosphate (S1P) signaling. In homeostasis, S1P levels are high in blood and lymph compared to lymphoid organs, and lymphocytes follow S1P gradients out of tissues into circulation using varying combinations of five G‐protein coupled S1P receptors. During an immune response, both the shape of S1P gradients and the expression of S1P receptors are dynamically regulated. Here we review what is known, and key questions that remain unanswered, about how S1P signaling is regulated in inflammation and in turn how S1P shapes immune responses. [ABSTRACT FROM AUTHOR]

Published

2023

71. Regulation of CD8 T‐cell signaling, metabolism, and cytotoxic activity by extracellular lysophosphatidic acid.

Author

Torres, Raul M., Turner, Jacqueline A., D'Antonio, Marc, Pelanda, Roberta, and Kremer, Kimberly N.

Subjects

*LYSOPHOSPHOLIPIDS, *CYTOTOXIC T cells, *T cells, *CD8 antigen, *G protein coupled receptors, *TUBULINS

Abstract

Summary: Lysophosphatidic acid (LPA) is an endogenous bioactive lipid that is produced extracellularly and signals to cells via cognate LPA receptors, which are G‐protein coupled receptors (GPCRs). Mature lymphocytes in mice and humans express three LPA receptors, LPA2, LPA5, and LPA6, and work from our group has determined that LPA5 signaling by T lymphocytes inhibits specific antigen‐receptor signaling pathways that ultimately impair lymphocyte activation, proliferation, and function. In this review, we discuss previous and ongoing work characterizing the ability of an LPA‐LPA5 axis to serve as a peripheral immunological tolerance mechanism that restrains adaptive immunity but is subverted during settings of chronic inflammation. Specifically, LPA‐LPA5 signaling is found to regulate effector cytotoxic CD8 T cells by (at least) two mechanisms: (i) regulating the actin‐microtubule cytoskeleton in a manner that impairs immunological synapse formation between an effector CD8 T cell and antigen‐specific target cell, thus directly impairing cytotoxic activity, and (ii) shifting T‐cell metabolism to depend on fatty‐acid oxidation for mitochondrial respiration and reducing metabolic efficiency. The in vivo outcome of LPA5 inhibitory activity impairs CD8 T‐cell killing and tumor immunity in mouse models providing impetus to consider LPA5 antagonism for the treatment of malignancies and chronic infections. [ABSTRACT FROM AUTHOR]

Published

2023

72. The leukotriene B4 receptors BLT1 and BLT2 as potential therapeutic targets.

Author

Yokomizo, Takehiko and Shimizu, Takao

Subjects

*MACULAR degeneration, *IMMUNOLOGIC diseases, *THERAPEUTICS, *DRUG target, *CHEMOTACTIC factors, *ALLERGIC conjunctivitis, *ECZEMA

Abstract

Summary: Leukotriene B4 (LTB4) was recognized as an arachidonate‐derived chemotactic factor for inflammatory cells and an important drug target even before the molecular identification of its receptors. We cloned the high‐ and low‐affinity LTB4 receptors, BLT1 and BLT2, respectively, and examined their functions by generating and studying gene‐targeted mice. BLT1 is involved in the pathogenesis of various inflammatory and immune diseases, including asthma, psoriasis, contact dermatitis, allergic conjunctivitis, age‐related macular degeneration, and immune complex‐mediated glomerulonephritis. Meanwhile, BLT2 is a high‐affinity receptor for 12‐hydroxyheptadecatrienoic acid, which is involved in the maintenance of dermal and intestinal barrier function, and the acceleration of skin and corneal wound healing. Thus, BLT1 antagonists and BLT2 agonists are promising candidates in the treatment of inflammatory diseases. [ABSTRACT FROM AUTHOR]

Published

2023

73. GPR35 and mediators from platelets and mast cells in neutrophil migration and inflammation.

Author

De Giovanni, Marco, Chen, Hongwen, Li, Xiaochun, and Cyster, Jason G.

Subjects

*CELL migration, *MAST cells, *TISSUE physiology, *BLOOD platelets, *G protein coupled receptors

Abstract

Summary: Neutrophil recruitment from circulation to sites of inflammation is guided by multiple chemoattractant cues emanating from tissue cells, immune cells, and platelets. Here, we focus on the function of one G‐protein coupled receptor, GPR35, in neutrophil recruitment. GPR35 has been challenging to study due the description of multiple ligands and G‐protein couplings. Recently, we found that GPR35‐expressing hematopoietic cells respond to the serotonin metabolite 5‐hydroxyindoleacetic acid (5‐HIAA). We discuss distinct response profiles of GPR35 to 5‐HIAA compared to other ligands. To place the functions of 5‐HIAA in context, we summarize the actions of serotonin in vascular biology and leukocyte recruitment. Important sources of serotonin and 5‐HIAA are platelets and mast cells. We discuss the dynamics of cell migration into inflamed tissues and how multiple platelet and mast cell‐derived mediators, including 5‐HIAA, cooperate to promote neutrophil recruitment. Additional actions of GPR35 in tissue physiology are reviewed. Finally, we discuss how clinically approved drugs that modulate serotonin uptake and metabolism may influence 5‐HIAA‐GPR35 function, and we speculate about broader influences of the GPR35 ligand‐receptor system in immunity and disease. [ABSTRACT FROM AUTHOR]

Published

2023

74. Resolvin D1 prevents injurious neutrophil swarming in transplanted lungs.

Author

Wenjun Li, Shepherd, Hailey M., Yuriko Terada, Shay, Ashley E., Bery, Amit I., Gelman, Andrew E., Lavine, Kory J., Serhan, Charles N., and Kreisel, Daniel

Subjects

*NEUTROPHILS, *LUNGS, *REPERFUSION injury, *TRANSPLANTATION of organs, tissues, etc., *SOFT tissue injuries

Abstract

Neutrophils are the primary cell type involved in lung ischemia-reperfusion injury (IRI), which remains a frequent and morbid complication after organ transplantation. Endogenous lipid mediators that become activated during acute inflammation-resolution have gained increasing recognition for their protective role(s) in promoting the restoration of homeostasis, but their influence on early immune responses following transplantation remains to be uncovered. Resolvin D1, 7S,8R,17S-trihydroxy-4Z, 9E,11E,13Z,15E,19Z-docosahexaenoic acid (RvD1), is a potent stereoselective mediator that exhibits proresolving and anti-inflammatory actions in the setting of tissue injury. Here, using metabololipidomics, we demonstrate that endogenous proresolving mediators including RvD1 are increased in human and murine lung grafts immediately following transplantation. In mouse grafts, we observe lipid mediator class switching early after reperfusion. We use intravital two-photon microscopy to reveal that RvD1 treatment significantly limits early neutrophil infiltration and swarming, thereby ameliorating early graft dysfunction in transplanted syngeneic lungs subjected to severe IRI. Through integrated analysis of single-cell RNA sequencing data of donor and recipient immune cells from lung grafts, we identify transcriptomic changes induced by RvD1. These results support a role for RvD1 as a potent modality for preventing early neutrophil-mediated tissue damage after lung IRI that may be therapeutic in the clinics. [ABSTRACT FROM AUTHOR]

Published

2023

75. Resolvin D1 Inhibits Corneal Inflammation in Staphylococcus Aureus Keratitis.

Author

Kim, Sang Yoon and Lee, Ji Eun

Subjects

*STAPHYLOCOCCUS aureus, *CORNEA, *KERATITIS, *OPTICAL coherence tomography, *LIPOXINS, *CORNEAL opacity, *ORTHOKERATOLOGY

Abstract

To investigate the role of lipid mediator, resolvin D1 (RvD1), in corneal inflammation. The anti-inflammatory effect of RvD1 on stimulated human corneal epithelial cells (HCECs) was assessed. C57BL/6 mice corneas were abraded and treated with RvD1 after stimulation with Staphylococcus aureus. Cytokine levels in the corneas, cervical drainage lymph nodes (DLNs), and spleens were measured. Anterior segment photography and optical coherence tomography quantified the changes in corneal thickness and haziness. Neutrophil infiltration in the cornea was examined by haematoxylin and eosin (H&E) staining and immunohistochemistry. RvD1 significantly inhibited cytokine production in HCECs and mouse corneas, cervical DLNs, and spleens while stimulating interleukin-10 (IL-10) production. Corneal opacity development, thickening, and neutrophil infiltration significantly reduced in response to RvD1 stimulation in the S. aureus-infected mice corneas. RvD1 inhibited S. aureus-induced corneal inflammation. These results potentiate RvD1 as an anti-inflammatory therapy for patients with corneal inflammation induced by bacterial keratitis. [ABSTRACT FROM AUTHOR]

Published

2023

76. Omega-3 to omega-6 fatty acid oxidation ratio as a novel inflammation resolution marker for metabolic complications in obesity.

Author

Sarajlic, Philip, Vigor, Claire, Avignon, Antoine, Zhou, Bingqing, Oger, Camille, Galano, Jean-Marie, Durand, Thierry, Sultan, Ariane, and Bäck, Magnus

Abstract

The oxidative metabolism of polyunsaturated fatty acids (PUFAs) leads to bioactive isoprostanoids. The aim was to establish the associations of a complete urinary isoprostanoid profiling in a cohort study of carefully phenotyped obese subjects to determine possible potential differential implications for omega-6 PUFA- and omega-3 PUFA-derived isoprostanoids for obesity, metabolic indicators, and inflammation. PUFA peroxidation compounds were determined in urine samples from obese human subjects (n = 46) by liquid chromatography coupled to tandem mass spectrometry. Increased omega-6 arachidonic acid (AA) oxidation, mainly represented by 5-F 2c isoprostane (5-F 2c -IsoP) and metabolites of 15-F 2t -IsoP, was associated with body mass index, glycated hemoglobin (HbA1c) and mean arterial blood pressure. In addition, we identified the omega-3 PUFA-derived urinary metabolites 14-F 4t -NeuroP from docosahexaenoic acid (DHA) and 5-F 3t -IsoP from eicosapentaenoic acid (EPA), which declined with age. The omega-3 to omega-6 oxidation ratio was a significant predictor of inflammation in obesity. The findings point to full urinary isoprostanoid profiling as a more sensitive measure of PUFA oxidative stress in obesity-induced metabolic complications compared with individual isoprostanoid measures. Furthermore, the results suggest the balance between the omega-3 and omega-6 PUFA oxidation as determinative for the consequences of oxidative stress on inflammation in obesity. What is already known about this subject? • Oxidative stress is increased and associated with low-grade chronic inflammation in obesity. • Oxidative non-enzymatic metabolism of polyunsaturated fatty acids yields bioactive isoprostanoids What are the new findings in this study? • Urinary isoprostanoid profiling associate with obesity-induced metabolic complications • Omega-3 to omega-6 fatty acid oxidation ratio emerged as a novel determinative for the consequences of oxidative stress on inflammation in obesity. How might your results change the direction of research or the focus of clinical practice • Dietary implications for the control of oxidative stress-associated inflammation in obesity. • Mechanistic studies may elucidate the mechanistic implications of omega-3 PUFA-derived oxidative products as pro-resolving mediators of obesity-induced inflammation. [ABSTRACT FROM AUTHOR]

Published

2023

77. Harmonized procedures lead to comparable quantification of total oxylipins across laboratories

Author

Mainka, Malwina, Dalle, Céline, Pétéra, Mélanie, Dalloux-Chioccioli, Jessica, Kampschulte, Nadja, Ostermann, Annika I, Rothe, Michael, Bertrand-Michel, Justine, Newman, John W, Gladine, Cécile, and Schebb, Nils Helge

Subjects

Medical Biochemistry and Metabolomics, Biomedical and Clinical Sciences, Clinical Research, Calibration, Chromatography, Liquid, Humans, Oxylipins, Quality Control, Tandem Mass Spectrometry, eicosanoids, lipidomics, liquid chromatography, mass spectrometry, quantitation, harmonization, plasma lipids, interlaboratory comparison, oxidized fatty acids, lipid mediators, Biochemistry and Cell Biology, Biochemistry & Molecular Biology, Biochemistry and cell biology, Medical biochemistry and metabolomics

Abstract

Oxylipins are potent lipid mediators involved in a variety of physiological processes. Their profiling has the potential to provide a wealth of information regarding human health and disease and is a promising technology for translation into clinical applications. However, results generated by independent groups are rarely comparable, which increases the need for the implementation of internationally agreed upon protocols. We performed an interlaboratory comparison for the MS-based quantitative analysis of total oxylipins. Five independent laboratories assessed the technical variability and comparability of 133 oxylipins using a harmonized and standardized protocol, common biological materials (i.e., seven quality control plasmas), standard calibration series, and analytical methods. The quantitative analysis was based on a standard calibration series with isotopically labeled internal standards. Using the standardized protocol, the technical variance was within ±15% for 73% of oxylipins; however, most epoxy fatty acids were identified as critical analytes due to high variabilities in concentrations. The comparability of concentrations determined by the laboratories was examined using consensus value estimates and unsupervised/supervised multivariate analysis (i.e., principal component analysis and partial least squares discriminant analysis). Interlaboratory variability was limited and did not interfere with our ability to distinguish the different plasmas. Moreover, all laboratories were able to identify similar differences between plasmas. In summary, we show that by using a standardized protocol for sample preparation, low technical variability can be achieved. Harmonization of all oxylipin extraction and analysis steps led to reliable, reproducible, and comparable oxylipin concentrations in independent laboratories, allowing the generation of biologically meaningful oxylipin patterns.

Published

2020

78. Distribution of Free and Esterified Oxylipins in Cream, Cell, and Skim Fractions of Human Milk

Author

Gan, Junai, Zhang, Zhichao, Kurudimov, Karina, German, J Bruce, and Taha, Ameer Y

Subjects

Medical Biochemistry and Metabolomics, Biomedical and Clinical Sciences, Nutrition, Pediatric, Chromatography, High Pressure Liquid, Esterification, Female, Humans, Linoleic Acid, Milk, Human, Oxylipins, Tandem Mass Spectrometry, Fractions, Human milk, LC-MS, MS, Lipid mediators, Lipidomics, LC-MS/MS, Agricultural and Veterinary Sciences, Engineering, Medical and Health Sciences, Nutrition & Dietetics, Medical biochemistry and metabolomics

Abstract

Human milk contains oxylipins involved in infant development. Although oxylipins have been identified in whole or skim milk, their localization within human milk cream, cell, and skim fractions is not known. This study determined the distribution of free and esterified oxylipins in cream, cell, and skim fractions of human milk. Out of 72 oxylipins probed by mass-spectrometry, 42, 29, and 41 oxylipins (free or bound) were detected in cream, cell, and skim fractions, respectively. Over 90% of free and bound oxylipins were derived from linoleic acid in all milk fractions. Other oxylipins were derived from n-6 arachidonic acid and dihomo-gamma-linolenic acid, and n-3 alpha-linolenic acid, eicosapentaenoic acid, and docosahexaenoic acid. Free oxylipins were more abundant in skim milk (59.9% of total oxylipins) compared to cream and cell pellet, whereas esterified oxylipins were most abundant in milk cream and cell pellets (74.9-76.9%). The heterogenous distribution of oxylipins in different fractions of human milk may regulate the guided release of these bioactive signaling molecules within infants.

Published

2020

79. Specialized pro-resolving lipid mediators in cardiovascular disease, diagnosis, and therapy

Author

Kim, Alexander S and Conte, Michael S

Subjects

Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Atherosclerosis, Cardiovascular, Heart Disease, 2.1 Biological and endogenous factors, 5.1 Pharmaceuticals, Good Health and Well Being, Animals, Cardiovascular Diseases, Humans, Lipid Metabolism, Lipids, Cardiovascular disease, Inflammation, Resolution, Lipid mediators, Resolvins, Intimal hyperplasia, Drug delivery, Pharmacology & Pharmacy, Pharmacology and pharmaceutical sciences

Abstract

Persistent inflammation is the key aggravator in many cardiovascular diseases, including atherosclerosis, aneurysm, injury/reperfusion, thrombosis, and neointimal hyperplasia following surgical or percutaneous interventions. Resolution is an active process orchestrated by specialized pro-resolving lipid mediators (SPMs) which tamp down acute inflammatory signals, promote healing and facilitate a return to homeostasis. SPMs are endogenously derived from poly-unsaturated fatty acids, and their biologic activity is mediated via specific G-protein coupled receptor binding. The potency of SPM in regulating the inflammatory response has encouraged investigation into their therapeutic and diagnostic use in cardiovascular pathologies. Herein we describe the translational groundwork which has established the synthesis and interactions of SPM in cardiovascular and hematologic cells, the therapeutic effects of SPM in animal models of cardiovascular disease, and some early technologies that harness and attempt to optimize SPM delivery and "resolution pharmacology". Further studies are required to precisely determine the mechanisms of resolution in the cardiovascular system and to determine the clinical settings in which SPM can be utilized to optimize patient outcomes.

Published

2020

80. Metabolic biological markers for diagnosing and monitoring the course of tuberculosis

Author

M. V. Korotetskaya and E. I. Rubakova

Subjects

tuberculosis, immune response, metabolism, enzymes, lipid mediators, eicosanoids, Infectious and parasitic diseases, RC109-216

Abstract

The international biomedical community has been currently facing a need to find a simple and most accessible type of analysis that helps to diagnose tuberculosis (TB) with the maximum reliability even before the onset of clinical manifestations. Tuberculosis results in more deaths than any other pathogen, second only to pneumonia caused by the SARS-CoV-2 virus, but the majority of infected people remain asymptomatic. In addition, it is important to develop methods to distinguish various forms of tuberculosis infection course at early stages and to reliably stratify patients into appropriate groups (persons with a rapidly progressing infection, chronic course, latent infection carriers). Immunometabolism investigates a relationship between bioenergetic pathways and specific functions of immune cells that has recently become increasingly important in scientific research. The host anti-mycobacteria immune response in tuberculosis is regulated by a number of metabolic networks that can interact both cooperatively and antagonistically, influencing an outcome of the disease. The balance between inflammatory and immune reactions limits the spread of mycobacteria in vivo and protects from developing tuberculosis. Cytokines are essential for host defense, but if uncontrolled, some mediators may contribute to developing disease and pathology. Differences in plasma levels of metabolites between individuals with advanced infection, LTBI and healthy individuals can be detected long before the onset of the major related clinical signs. Changes in amino acid and cortisol level may be detected as early as 12 months before the onset of the disease and become more prominent at verifying clinical diagnosis. Assessing serum level of certain amino acids and their ratios may be used as additional diagnostic markers of active pulmonary TB. Metabolites, including serum fatty acids, amino acids and lipids may contribute to detecting active TB. Metabolic profiles indicate about increased indolamine 2.3-dioxygenase 1 (IDO1) activity, decreased phospholipase activity, increased adenosine metabolite level, and fibrous lesions in active vs. latent infection. TB treatment can be adjusted based on individual patient metabolism and biomarker profiles. Thus, exploring immunometabolism in tuberculosis is necessary for development of new therapeutic strategies.

Published

2022

81. Polyunsaturated Fatty Acids: Conversion to Lipid Mediators, Roles in Inflammatory Diseases and Dietary Sources.

Author

Harwood, John L.

Subjects

*UNSATURATED fatty acids, *ESSENTIAL fatty acids, *FREE radical reactions, *LINOLEIC acid, *FISH oils, *INFLAMMATORY mediators, *CARBON compounds, *LIPIDS

Abstract

Polyunsaturated fatty acids (PUFAs) are important components of the diet of mammals. Their role was first established when the essential fatty acids (EFAs) linoleic acid and α-linolenic acid were discovered nearly a century ago. However, most of the biochemical and physiological actions of PUFAs rely on their conversion to 20C or 22C acids and subsequent metabolism to lipid mediators. As a generalisation, lipid mediators formed from n-6 PUFAs are pro-inflammatory while those from n-3 PUFAs are anti-inflammatory or neutral. Apart from the actions of the classic eicosanoids or docosanoids, many newly discovered compounds are described as Specialised Pro-resolving Mediators (SPMs) which have been proposed to have a role in resolving inflammatory conditions such as infections and preventing them from becoming chronic. In addition, a large group of molecules, termed isoprostanes, can be generated by free radical reactions and these too have powerful properties towards inflammation. The ultimate source of n-3 and n-6 PUFAs are photosynthetic organisms which contain Δ-12 and Δ-15 desaturases, which are almost exclusively absent from animals. Moreover, the EFAs consumed from plant food are in competition with each other for conversion to lipid mediators. Thus, the relative amounts of n-3 and n-6 PUFAs in the diet are important. Furthermore, the conversion of the EFAs to 20C and 22C PUFAs in mammals is rather poor. Thus, there has been much interest recently in the use of algae, many of which make substantial quantities of long-chain PUFAs or in manipulating oil crops to make such acids. This is especially important because fish oils, which are their main source in human diets, are becoming limited. In this review, the metabolic conversion of PUFAs into different lipid mediators is described. Then, the biological roles and molecular mechanisms of such mediators in inflammatory diseases are outlined. Finally, natural sources of PUFAs (including 20 or 22 carbon compounds) are detailed, as well as recent efforts to increase their production. [ABSTRACT FROM AUTHOR]

Published

2023

82. Sleep deprivation in obesogenic setting alters lipidome and microbiome toward suboptimal inflammation in acute heart failure.

Author

Halade, Ganesh V., Mat, Yusuf, Gowda, Siddabasave Gowda B., Jain, Shalini, Hui, Shu‐Ping, Yadav, Hariom, and Kain, Vasundhara

Abstract

Sleep is a fundamental medicine for cardiac homeostasis, and sleep‐deprived individuals are prone to higher incidences of heart attack. The lipid‐dense diet (obesogenic diet‐OBD) is a cumulative risk factor for chronic inflammation in cardiovascular disease; thus, understanding how sleep fragmentation (SF) in an obesity setting impacts immune and cardiac health is an unmet medical need. We hypothesized whether the co‐existence of SF with OBD dysregulates gut homeostasis and leukocyte‐derived reparative/resolution mediators, thereby impairing cardiac repair. Two‐month‐old male C57BL/6J mice were randomized first into two groups, then four groups; Control, control + SF, OBD, and OBD + SF mice subjected to myocardial infarction (MI). OBD mice had higher levels of plasma linolenic acid with a decrease in eicosapentaenoic and docosahexaenoic acid. The OBD mice had lower Lactobacillus johnsonii indicating a loss of probiotic microbiota. SF in OBD mice increased Firmicutes/Bacteroidetes ratio indicative of a detrimental change in SF‐directed microbiome. OBD + SF group increased in the neutrophil: lymphocyte ratio suggestive of suboptimal inflammation. As a result of SF, resolution mediators (RvD2, RvD3, RvD5, LXA4, PD1, and MaR1) decreased and inflammatory mediators (PGD2, PGE2, PGF2a, 6k‐PGF1a) were increased in OBD mice post‐MI. At the site of infarction, the proinflammatory cytokines Ccl2, IL1β, and IL‐6 were amplified in OBD + SF indicating a robust proinflammatory milieu post‐MI. Also, brain circadian genes (Bmal1, Clock) were downregulated in SF‐subjected control mice, but remained elevated in OBD mice post‐MI. SF superimposed on obesity dysregulated physiological inflammation and disrupted resolving response thereby impaired cardiac repair and signs of pathological inflammation. [ABSTRACT FROM AUTHOR]

Published

2023

83. Accumulation of polyunsaturated fatty acid‐derived metabolites in the sarcopenic muscle of aging mice.

Author

Kadoguchi, Tomoyasu, Shimada, Kazunori, Fukui, Naoshi, Tanaka, Nobuho, Tsuno, Hirotaka, Shiozawa, Tomoyuki, Fukao, Kosuke, Nishitani‐Yokoyama, Miho, Isoda, Kikuo, Matsushita, Satoshi, Yokoyama, Norihiko, and Daida, Hiroyuki

Subjects

*UNSATURATED fatty acids, *BIOLOGICAL models, *PROSTAGLANDINS, *SKELETAL muscle, *ANIMAL experimentation, *LIQUID chromatography, *SARCOPENIA, *EICOSANOIDS, *AGING, *MASS spectrometry, *RESEARCH funding, *THROMBOXANES, *ARACHIDONIC acid, *METABOLITES, *MICE, *METABOLISM

Abstract

Aim: Although it is known that advanced age alters skeletal muscle lipid metabolism, the role(s) of polyunsaturated fatty acid‐derived metabolites (mostly eicosanoids and docosanoids) in sarcopenia are not clear. We therefore examined the changes in the metabolites of arachidonic acid, eicosapentaenoic acid and docosahexaenoic acid in the sarcopenic muscle of aged mice. Methods: We used 6‐ and 24‐month‐old male C57BL/6J mice as healthy and sarcopenic muscle models, respectively. Skeletal muscles were removed from the lower limb and subjected to a liquid chromatography–tandem mass spectrometry analysis. Results: The liquid chromatography–tandem mass spectrometry analysis detected distinct changes of metabolites in the muscles of the aged mice. Of the 63 metabolites identified, nine were significantly higher in the sarcopenic muscle of aged mice compared with the healthy muscle of young mice. In particular, prostaglandin E2, prostaglandin F2a, thromboxane B2, 5‐hydroxyeicosatetraenoic acid, and 15‐oxo‐eicosatetraenoic acid (arachidonic acid‐derived metabolites), 12‐hydroxy‐eicosapentaenoic acid and 14,15‐epoxy‐eicosatetraenoic acid (eicosapentaenoic acid‐derived metabolites) and 10‐hydroxydocosa‐hexaenoic acid and 14‐hydroxyoctadeca‐pentaenoic acid (docosahexaenoic acid‐derived metabolites) were significantly higher in aged tissue compared with young tissue (all P < 0.05). Conclusions: We observed the accumulation of metabolites in the sarcopenic muscle of aged mice. Our results may provide new insights into the pathogenesis and progression of aging‐ or disease‐related sarcopenia. Geriatr Gerontol Int 2023; 23: 297–303. [ABSTRACT FROM AUTHOR]

Published

2023

84. The Role of α-Linolenic Acid and Its Oxylipins in Human Cardiovascular Diseases.

Author

Cambiaggi, Lucia, Chakravarty, Akash, Noureddine, Nazek, and Hersberger, Martin

Subjects

*OXYLIPINS, *OMEGA-3 fatty acids, *CARDIOVASCULAR diseases, *CYTOCHROME P-450, *C-reactive protein

Abstract

α-linolenic acid (ALA) is an essential C-18 n-3 polyunsaturated fatty acid (PUFA), which can be elongated to longer n-3 PUFAs, such as eicosapentaenoic acid (EPA). These long-chain n-3 PUFAs have anti-inflammatory and pro-resolution effects either directly or through their oxylipin metabolites. However, there is evidence that the conversion of ALA to the long-chain PUFAs is limited. On the other hand, there is evidence in humans that supplementation of ALA in the diet is associated with an improved lipid profile, a reduction in the inflammatory biomarker C-reactive protein (CRP) and a reduction in cardiovascular diseases (CVDs) and all-cause mortality. Studies investigating the cellular mechanism for these beneficial effects showed that ALA is metabolized to oxylipins through the Lipoxygenase (LOX), the Cyclooxygenase (COX) and the Cytochrome P450 (CYP450) pathways, leading to hydroperoxy-, epoxy-, mono- and dihydroxylated oxylipins. In several mouse and cell models, it has been shown that ALA and some of its oxylipins, including 9- and 13-hydroxy-octadecatrienoic acids (9-HOTrE and 13-HOTrE), have immunomodulating effects. Taken together, the current literature suggests a beneficial role for diets rich in ALA in human CVDs, however, it is not always clear whether the described effects are attributable to ALA, its oxylipins or other substances present in the supplemented diets. [ABSTRACT FROM AUTHOR]

Published

2023

85. Fatty Acid Composition and Metabolism in Leishmania Parasite Species: Potential Biomarkers or Drug Targets for Leishmaniasis?

Author

Leroux, Marine, Luquain-Costaz, Céline, Lawton, Philippe, Azzouz-Maache, Samira, and Delton, Isabelle

Subjects

*FATTY acids, *LEISHMANIASIS, *FATTY acid analysis, *DRUG target, *UNSATURATED fatty acids, *OILSEEDS

Abstract

Fatty acids have received growing interest in Leishmania biology with the characterization of the enzymes allowing the complete fatty acid synthesis of this trypanosomatid parasite. This review presents a comparative analysis of the fatty acid profiles of the major classes of lipids and phospholipids in different species of Leishmania with cutaneous or visceral tropism. Specificities relating to the parasite forms, resistance to antileishmanial drugs, and host/parasite interactions are described as well as comparisons with other trypanosomatids. Emphasis is placed on polyunsaturated fatty acids and their metabolic and functional specificities, in particular, their conversion into oxygenated metabolites that are inflammatory mediators able to modulate metacyclogenesis and parasite infectivity. The impact of lipid status on the development of leishmaniasis and the potential of fatty acids as therapeutic targets or candidates for nutritional interventions are discussed. [ABSTRACT FROM AUTHOR]

Published

2023

86. Cell-Type-Specific Gene Regulatory Networks of Pro-Inflammatory and Pro-Resolving Lipid Mediator Biosynthesis in the Immune System.

Author

Hoch, Matti, Rauthe, Jannik, Cesnulevicius, Konstantin, Schultz, Myron, Lescheid, David, Wolkenhauer, Olaf, Chiurchiù, Valerio, and Gupta, Shailendra

Subjects

*GENE regulatory networks, *BIOSYNTHESIS, *GENETIC regulation, *IMMUNE system, *GENETIC transcription regulation, *LIPIDS, *MACHINE learning

Abstract

Lipid mediators are important regulators in inflammatory responses, and their biosynthetic pathways are targeted by commonly used anti-inflammatory drugs. Switching from pro-inflammatory lipid mediators (PIMs) to specialized pro-resolving (SPMs) is a critical step toward acute inflammation resolution and preventing chronic inflammation. Although the biosynthetic pathways and enzymes for PIMs and SPMs have now been largely identified, the actual transcriptional profiles underlying the immune cell type-specific transcriptional profiles of these mediators are still unknown. Using the Atlas of Inflammation Resolution, we created a large network of gene regulatory interactions linked to the biosynthesis of SPMs and PIMs. By mapping single-cell sequencing data, we identified cell type-specific gene regulatory networks of the lipid mediator biosynthesis. Using machine learning approaches combined with network features, we identified cell clusters of similar transcriptional regulation and demonstrated how specific immune cell activation affects PIM and SPM profiles. We found substantial differences in regulatory networks in related cells, accounting for network-based preprocessing in functional single-cell analyses. Our results not only provide further insight into the gene regulation of lipid mediators in the immune response but also shed light on the contribution of selected cell types in their biosynthesis. [ABSTRACT FROM AUTHOR]

Published

2023

87. Mediterranean diet component oleic acid increases protective lipid mediators and improves trabecular bone in a Porphyromonas gingivalis inoculation model.

Author

Döding, Annika, Hüfner, Mira, Nachtsheim, Franziska, Iffarth, Viktoria, Bölter, Anna, Bastian, Asisa, Symmank, Judit, Andreas, Nico, Schädel, Patrick, Thürmer, Maria, Becker, Kathrin, Wolf, Michael, Jacobs, Collin, Kamradt, Thomas, Koeberle, Andreas, Werz, Oliver, Sigusch, Bernd, and Schulze‐Späte, Ulrike

Subjects

*MEDITERRANEAN diet, *WESTERN diet, *BIOLOGICAL models, *LIPOPOLYSACCHARIDES, *IN vitro studies, *MONOUNSATURATED fatty acids, *BODY weight, *FIBROBLASTS, *INFLAMMATION, *FOOD consumption, *ANIMAL experimentation, *NUTRITION, *GRAM-negative anaerobic bacteria, *PERIODONTAL disease, *ALVEOLAR process, *PLACEBOS, *TREATMENT effectiveness, *LINOLEIC acid, *GINGIVAL hyperplasia, *DESCRIPTIVE statistics, *TUMOR necrosis factors, *RESEARCH funding, *LIPIDS, *CANCELLOUS bone, *MICE

Abstract

Aim: Therapeutic modulation of bacterial‐induced inflammatory host response is being investigated in gingival inflammation and periodontal disease pathology. Therefore, dietary intake of the monounsaturated fatty acid (FA) oleic acid (OA (C18:1)), which is the main component of Mediterranean‐style diets, and saturated FA palmitic acid (PA (C16:0)), which is a component of Western‐style diets, was investigated for their modifying potential in an oral inoculation model of Porphyromonas gingivalis. Materials and Methods: Normal‐weight C57BL/6‐mice received OA‐ or PA‐enriched diets (PA‐ED, OA‐ED, PA/OA‐ED) or normal standard diet for 16 weeks and were inoculated with P. gingivalis/placebo (n = 12/group). Gingival inflammation, alveolar bone structure, circulating lipid mediators, and in vitro cellular response were determined. Results: FA treatment of P. gingivalis‐lipopolysaccharide‐incubated gingival fibroblasts (GFbs) modified inflammatory activation, which only PA exacerbated with concomitant TNF‐α stimulation. Mice exhibited no signs of acute inflammation in gingiva or serum and no inoculation‐ or nutrition‐associated changes of the crestal alveolar bone. However, following P. gingivalis inoculation, OA‐ED improved oral trabecular bone micro‐architecture and enhanced circulating pro‐resolving mediators resolvin D4 (RvD4) and 4‐hydroxydocosahexaenoic acid (4‐HDHA), whereas PA‐ED did not. In vitro experiments demonstrated significantly improved differentiation in RvD4‐ and 4‐HDHA‐treated primary osteoblast cultures and reduced the expression of osteoclastogenic factors in GF. Further, P. gingivalis infection of OA‐ED animals led to a serum composition that suppressed osteoclastic differentiation in vitro. Conclusions: Our results underline the preventive impact of Mediterranean‐style OA‐EDs by indicating their pro‐resolving nature beyond anti‐inflammatory properties. [ABSTRACT FROM AUTHOR]

Published

2023

88. Enriched PUFA environment of Leishmania infantum promastigotes promotes the accumulation of lipid mediators and favors parasite infectivity towards J774 murine macrophages.

Author

Leroux, Marine, Bouazizi‐Ben Messaoud, Hana, Luquain‐Costaz, Céline, Jordheim, Lars P., Le Faouder, Pauline, Gustin, Marie‐Paule, Aoun, Karim, Lawton, Philippe, Azzouz‐Maache, Samira, and Delton, Isabelle

Abstract

Leishmania parasites are the causative agents of visceral or cutaneous leishmaniasis in humans and of canine leishmaniosis. The macrophage is the predilected host cell of Leishmania in which the promastigote stage is transformed into amastigote. We previously showed changes in the fatty acid composition (FA) of lipids in two strains of Leishmania donovani upon differentiation of promastigote to amastigote, including increased proportions of arachidonic acid (AA) and to a less extent of docosahexaenoic acid (DHA). Here, we carried out supplementation with AA or DHA on two Leishmania infantum strains, a visceral (MON‐1) and a cutaneous (MON‐24), to evaluate the role of these FA in parasite/macrophage interactions. The proportions of AA or DHA in total lipids were significantly increased in promastigotes cultured in AA‐ or DHA‐supplemented media compared to controls. The content of FA‐derived oxygenated metabolites was enhanced in supplemented strains, generating especially epoxyeicosatrienoic acids (11,12‐ and 14,15‐EET) and hydroxyeicosatetraenoic acids (5‐ and 8‐ HETE) from AA, and hydroxydocosahexaenoic acids (14‐ and 17‐HDoHE) from DHA. For both MON‐1 and MON‐24, AA‐supplemented promastigotes showed higher infectivity towards J774 macrophages as evidenced by higher intracellular amastigote numbers. Higher infectivity was observed after DHA supplementation for MON‐24 but not MON‐1 strain. ROS production by macrophages increased upon parasite infection, but only minor change was observed between control and supplemented parasites. We propose that under high AA or DHA environment that is associated with AA or DHA enrichment of promastigote lipids, FA derivatives can accumulate in the parasite, thereby modulating parasite infectivity towards host macrophages. [ABSTRACT FROM AUTHOR]

Published

2023

89. Differential impact of 5-lipoxygenase-activating protein antagonists on the biosynthesis of leukotrienes and of specialized pro-resolving mediators

Author

Philipp Dahlke, Lukas K. Peltner, Paul M. Jordan, and Oliver Werz

Subjects

5-lipoxygenase-activating protein, 15-lipoxygenase, lipid mediators, leukotrienes, specialized pro-resolving mediators, lipoxins, Therapeutics. Pharmacology, RM1-950

Abstract

Lipoxygenases (LOX) transform arachidonic acid (AA, C20:4) and docosahexaenoic acid (DHA, C22:6) into bioactive lipid mediators (LMs) that comprise not only pro-inflammatory leukotrienes (LTs) but also the specialized pro-resolving mediators (SPMs) that promote inflammation resolution and tissue regeneration. The 5-LOX-activating protein (FLAP) is known to provide AA as a substrate to 5-LOX for generating LTs, such as LTB4, a potent chemoattractant and activator of phagocytes. Notably, 5-LOX is also involved in the biosynthesis of certain SPMs, namely, lipoxins and D-resolvins, implying a role of FLAP in SPM formation. FLAP antagonists have been intensively developed as LT biosynthesis inhibitors, but how they impact SPM formation is a matter of debate. Here, we show that FLAP antagonism suppresses the conversion of AA by 5-LOX to LT and lipoxins, while the conversion of DHA to SPM is unaffected. Screening of multiple prominent FLAP antagonists for their effects on LM formation in human M1- and M2-monocyte-derived macrophages by comprehensive LM profiling showed that all nine compounds reduced the production of 5-LOX-derived LTs but increased the formation of SPMs from DHA, e.g., resolvin D5. Some FLAP antagonists, especially those that contain an indole or benzimidazole moiety, even elicited SPM formation in resting M2-monocyte-derived macrophages. Intriguingly, in coincubations of human neutrophils and platelets that produce substantial AA-derived lipoxin and DHA-derived RvD5, FLAP antagonism abolished lipoxin formation, but resolvin D5 levels remained unaffected. Conclusively, antagonism of FLAP suppresses the conversion of AA by 5-LOX to LTs and lipoxins but not the conversion of DHA by 5-LOX to SPM, which should be taken into account for the development of such compounds as anti-inflammatory drugs.

Published

2023

90. Production profile of lipid mediators in conjunctival lavage fluid in allergic and infectious conjunctivitis in guinea pigs

Author

Akane Hayashi, Koji Kobayashi, Tatsuro Nakamura, Nanae Nagata, and Takahisa Murata

Subjects

conjunctivitis, lipid mediators, tear, biomarker, eosinophils, neutrophils, Immunologic diseases. Allergy, RC581-607

Abstract

IntroductionConjunctivitis is a major ocular disease classified into allergic or infectious. The pathological features of conjunctivitis are not fully understood despite its high morbidity rate; thus, its differentiation can be difficult.Materials and methodsWe used ovalbumin-induced allergic conjunctivitis and lipopolysaccharide-induced infectious conjunctivitis models of guinea pigs. Both models showed conjunctival swelling. Histological studies revealed that numerous eosinophils infiltrated the conjunctiva in the allergic model, whereas neutrophils infiltrated the conjunctiva in the infectious model. We collected conjunctival lavage fluid (COLF) and comprehensively analyzed lipid production using liquid chromatography-tandem mass spectrometry.ResultsCOLF showed increase of 20 and 12 lipid species levels in the allergic and infectious models, respectively. Specifically, the levels of a major allergic mediator, prostaglandin D2 and its three metabolites and several cytochrome P450-catalyzed lipids increased in the allergic model. In the infectious model, the levels of prostaglandin E2 and 8-iso-prostaglandin E2 increased, indicating tissue inflammation. Moreover, the level of 12-oxo-eicosatetraenoic acid, a lipoxygenase metabolite, increased in the infectious model.ConclusionThese differences in lipid production in the COLF reflected the pathological features of allergic and infectious conjunctivitis.

Published

2023

91. Global Proteomics Analysis of Lysophosphatidic Acid Signaling in PC-3 Human Prostate Cancer Cells: Role of CCN1

Author

Pravita Balijepalli, Guihua Yue, Bhagwat Prasad, and Kathryn E. Meier

Subjects

lipid mediators, prostate cancer, matricellular proteins, extracellular matrix, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Cysteine-rich angiogenic factor 61 (CCN1/Cyr61) is a matricellular protein that is induced and secreted in response to growth factors. Our previous work showed that 18:1-lysophosphatidic acid (LPA), which activates the G protein-coupled receptor LPAR1, induces CCN1 between 2–4 h in PC-3 human prostate cancer cells in a manner than enhances cell-substrate adhesion. While the time course of induction suggests that CCN1 contributes to intermediate events in LPA action, the roles of CCN1 in LPA-mediated signal transduction have not been fully elucidated. This study utilized a comprehensive global proteomics approach to identify proteins up- or down-regulated in response to treatment of PC-3 cells with LPA for three hours, during the time of peak CCN1 levels. In addition, the effects of siRNA-mediated CCN1 knockdown on LPA responses were analyzed. The results show that, in addition to CCN1, LPA increased the levels of multiple proteins. Proteins up-regulated by LPA included metastasis-associated in colon cancer protein 1 (MACC1) and thrombospondin-1 (TSP1/THBS1); both MACC1 and TSP1 regulated cancer cell adhesion and motility. LPA down-regulated thioredoxin interacting protein (TXNIP). CCN1 knockdown suppressed the LPA-induced up-regulation of 30 proteins; these included MACC1 and TSP1, as confirmed by immunoblotting. Gene ontology and STRING analyses revealed multiple pathways impacted by LPA and CCN1. These results indicate that CCN1 contributes to LPA signaling cascades that occur during the intermediate phase after the initial stimulus. The study provides a rationale for the development of interventions to disrupt the LPA-CCN1 axis.

Published

2024

92. Mechanisms of 3-Hydroxyl 3-Methylglutaryl CoA Reductase in Alzheimer’s Disease

Author

Xun Zhou, Xiaolang Wu, Rui Wang, Lu Han, Huilin Li, and Wei Zhao

Subjects

Alzheimer’s disease, HMGCR, lipid mediators, lipid metabolism, neuroinflammation, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Alzheimer’s disease (AD) is the most common neurodegenerative disease worldwide and has a high incidence in the elderly. Unfortunately, there is no effective therapy for AD owing to its complicated pathogenesis. However, the development of lipid-lowering anti-inflammatory drugs has heralded a new era in the treatment of Alzheimer’s disease. Several studies in recent years have shown that lipid metabolic dysregulation and neuroinflammation are associated with the pathogenesis of AD. 3-Hydroxyl 3-methylglutaryl CoA reductase (HMGCR) is a rate-limiting enzyme in cholesterol synthesis that plays a key role in cholesterol metabolism. HMGCR inhibitors, known as statins, have changed from being solely lipid-lowering agents to neuroprotective compounds because of their effects on lipid levels and inflammation. In this review, we first summarize the main regulatory mechanism of HMGCR affecting cholesterol biosynthesis. We also discuss the pathogenesis of AD induced by HMGCR, including disordered lipid metabolism, oxidative stress, inflammation, microglial proliferation, and amyloid-β (Aβ) deposition. Subsequently, we explain the possibility of HMGCR as a potential target for AD treatment. Statins-based AD treatment is an ascent field and currently quite controversial; therefore, we also elaborate on the current application prospects and limitations of statins in AD treatment.

Published

2023

93. Walnuts change lipoprotein composition suppressing TNFα-stimulated cytokine production by diabetic adipocyte.

Author

Borkowski, Kamil, Yim, Sun J, Holt, Roberta R, Hackman, Robert M, Keen, Carl L, Newman, John W, and Shearer, Gregory C

Subjects

Cells, Cultured, Adipocytes, Humans, Juglans, Nuts, Diabetes Mellitus, Hypercholesterolemia, Fatty Acids, Lipoproteins, Tumor Necrosis Factor-alpha, Cytokines, Middle Aged, Female, Adipokines, Oxylipins, Diet, Dietary lipids, LDL, Lipid mediators, Lipoprotein metabolism, Diabetes, 2.1 Biological and endogenous factors, Aetiology, Metabolic and endocrine, Biochemistry and Cell Biology, Food Sciences, Nutrition and Dietetics, Nutrition & Dietetics

Abstract

Walnut consumption can provide both vascular and metabolic health benefits, and walnut-induced changes in lipoprotein particle chemical payloads may be responsible for these health benefits. To explore this possibility with a focus on metabolic health, this study investigated the impact of walnut consumption on lipoprotein lipid composition and changes in LDL anti-inflammatory properties, as reported by inflamed adipocyte. Hypercholesterolemic, postmenopausal females were treated with 40 g/day (i.e., 1.6 servings/day; n=15) of walnuts for 4 weeks. Fatty acids and their oxygenated metabolites, i.e., oxylipins, were quantified in isolated lipoproteins. Human primary adipocytes were exposed to LDL and TNFα-stimulated adipokine production was measured. Walnut treatment elevated α-linolenic acid and its epoxides in all lipoproteins and depleted mid-chain alcohols in VLDL and LDL, but not HDL. Walnuts also reduced TNFα-induced diabetic adipocyte production of IL-6 (-48%, P=.0006) and IL-8 (-30%, P=.01), changes inversely correlated with levels of α-linolenic acid-derived epoxides but not α-linolenic acid itself. In conclusion, modest walnut consumption can alter lipoprotein lipid profiles and enhance their ability to inhibit TNFα-dependent pro-inflammatory responses in human diabetic primary adipocytes. Moreover, this study suggests the oxylipins, rather than the parent fatty acids, mediate LDL action of adipocytes.

Published

2019

94. Brain oxylipin concentrations following hypercapnia/ischemia: effects of brain dissection and dissection time[S]

Author

Hennebelle, Marie, Metherel, Adam H, Kitson, Alex P, Otoki, Yurika, Yang, Jun, Lee, Kin Sing Stephen, Hammock, Bruce D, Bazinet, Richard P, and Taha, Ameer Y

Subjects

Medical Biochemistry and Metabolomics, Biomedical and Clinical Sciences, Neurosciences, Animals, Brain, Brain Ischemia, Cluster Analysis, Hypercapnia, Male, Oxylipins, Rats, brain lipids, polyunsaturated fatty acid metabolites, lipid mediators, Biochemistry and Cell Biology, Biochemistry & Molecular Biology, Biochemistry and cell biology, Medical biochemistry and metabolomics

Abstract

PUFAs are precursors to bioactive oxylipin metabolites that increase in the brain following CO2-induced hypercapnia/ischemia. It is not known whether the brain-dissection process and its duration also alter these metabolites. We applied CO2 with or without head-focused microwave fixation for 2 min to evaluate the effects of CO2-induced asphyxiation, dissection, and dissection time on brain oxylipin concentrations. Compared with head-focused microwave fixation (control), CO2 followed by microwave fixation prior to dissection increased oxylipins derived from lipoxygenase (LOX), 15-hydroxyprostaglandin dehydrogenase (PGDH), cytochrome P450 (CYP), and soluble epoxide hydrolase (sEH) enzymatic pathways. This effect was enhanced when the duration of postmortem ischemia was prolonged by 6.4 min prior to microwave fixation. Brains dissected from rats subjected to CO2 without microwave fixation showed greater increases in LOX, PGDH, CYP and sEH metabolites compared with all other groups, as well as increased cyclooxygenase metabolites. In nonmicrowave-irradiated brains, sEH metabolites and one CYP metabolite correlated positively and negatively with dissection time, respectively. This study presents new evidence that the dissection process and its duration increase brain oxylipin concentrations, and that this is preventable by microwave fixation. When microwave fixation is not available, lipidomic studies should account for dissection time to reduce these artifacts.

Published

2019

95. Modulation of Inflammation-Related Lipid Mediator Pathways by Celastrol During Human Macrophage Polarization

Author

Zhang K, Jordan PM, Pace S, Hofstetter RK, Werner M, Chen X, and Werz O

Subjects

inflammation, macrophages, lipoxygenase, cyclooxygenase, lipid mediators, specialized pro-resolving mediators, celastrol., Pathology, RB1-214, Therapeutics. Pharmacology, RM1-950

Abstract

Kehong Zhang,1,2 Paul Mike Jordan,1 Simona Pace,1 Robert K Hofstetter,1 Markus Werner,1 Xinchun Chen,2 Oliver Werz1 1Department of Pharmaceutical/Medicinal Chemistry, Institute of Pharmacy, Friedrich Schiller University Jena, Jena, D-07743, Germany; 2Guangdong Provincial Key Laboratory of Regional Immunity and Diseases, Department of Pathogen Biology, Shenzhen University School of Medicine, Shenzhen, 518000, People’s Republic of ChinaCorrespondence: Oliver Werz, Email oliver.werz@uni-jena.deBackground and Purpose: Celastrol (CS) is a major active ingredient of the Chinese/Asian herb Tripterygium wilfordii that is frequently used as phytomedicine to treat inflammation and autoimmune diseases. We showed before that short-term exposure to CS (1 μM) favorably impacts the biosynthesis of inflammation-related lipid mediators (LM) in human polarized macrophages by modulating the activities of different lipoxygenases (LOXs). However, whether CS regulates the expression of LOXs and other related LM-biosynthetic enzymes during macrophage polarization is unknown. Here, we investigated how CS affects LM-biosynthetic enzyme expression on the protein level and studied concomitant LM signature profiles during polarization of human monocyte-derived macrophages (MDM) towards M1- and M2-like phenotypes.Methods and Results: We used LM metabololipidomics to study the long-term effects of CS on LM profile signatures after manipulation of human monocyte-derived macrophages (MDM) during polarization. Exposure of MDM to low concentrations of CS (ie, 0.2 μM) during polarization to an inflammatory M1 phenotype potently suppressed the formation of pro-inflammatory cyclooxygenase (COX)- and 5-LOX-derived LM, especially prostaglandin (PG)E2. Notably, gene and enzyme expression of COX-2 and microsomal PGE2 synthase (mPGES)-1 as well as M1 markers were strongly decreased by CS during M1-MDM polarization, along with impaired activation of nuclear factor-κB and p38 mitogen-activated protein kinase. During IL-4-induced M2 polarization, CS decreased the capacity of the resulting M2-MDM to generate pro-inflammatory COX and 5-LOX products as well but it also reduced the formation of 12/15-LOX products and specialized pro-resolving mediators, without affecting the levels of liberated fatty acid substrates.Conclusion: Depending on the timing and concentration, CS not only favorably affects LOX activities in macrophages but also the expression of LM-biosynthetic enzymes during macrophage polarization connected to changes of inflammation-related LM which might be of relevance for potential application of CS to treat inflammatory disorders.Graphical Abstract: Keywords: inflammation, macrophages, lipoxygenase, cyclooxygenase, lipid mediators, specialized pro-resolving mediators, celastrol

Published

2022

96. Genome-wide analysis of oxylipins and oxylipin profiles in a pediatric population

Author

Teresa Buckner, Randi K. Johnson, Lauren A. Vanderlinden, Patrick M. Carry, Alex Romero, Suna Onengut-Gumuscu, Wei-Min Chen, Soojeong Kim, Oliver Fiehn, Brigitte I. Frohnert, Tessa Crume, Wei Perng, Katerina Kechris, Marian Rewers, and Jill M. Norris

Subjects

oxylipin, inflammation, pediatric, genome-wide association study, polyunsaturated fatty acids, lipid mediators, Nutrition. Foods and food supply, TX341-641

Abstract

BackgroundOxylipins are inflammatory biomarkers derived from omega-3 and-6 fatty acids implicated in inflammatory diseases but have not been studied in a genome-wide association study (GWAS). The aim of this study was to identify genetic loci associated with oxylipins and oxylipin profiles to identify biologic pathways and therapeutic targets for oxylipins.MethodsWe conducted a GWAS of plasma oxylipins in 316 participants in the Diabetes Autoimmunity Study in the Young (DAISY). DNA samples were genotyped using the TEDDY-T1D Exome array, and additional variants were imputed using the Trans-Omics for Precision Medicine (TOPMed) multi-ancestry reference panel. Principal components analysis of 36 plasma oxylipins was used to capture oxylipin profiles. PC1 represented linoleic acid (LA)- and alpha-linolenic acid (ALA)-related oxylipins, and PC2 represented arachidonic acid (ARA)-related oxylipins. Oxylipin PC1, PC2, and the top five loading oxylipins from each PC were used as outcomes in the GWAS (genome-wide significance: p

Published

2023

97. Editorial: Streaming inflammation: From damage to healing and resilience–Volume II

Author

Pallavi R. Devchand, Eric E. Schadt, and Garret A. FitzGerald

Subjects

resilience, disease states, drug target, healing, identity, lipid mediators, Therapeutics. Pharmacology, RM1-950

Published

2023

98. Allosteric Activation of 15‐Lipoxygenase‐1 by Boswellic Acid Induces the Lipid Mediator Class Switch to Promote Resolution of Inflammation.

Author

Börner, Friedemann, Pace, Simona, Jordan, Paul M., Gerstmeier, Jana, Gomez, Mario, Rossi, Antonietta, Gilbert, Nathaniel C., Newcomer, Marcia E., and Werz, Oliver

Subjects

*CATALYTIC domains, *LIPOXYGENASES, *LIPIDS, *INFLAMMATION, *PERITONITIS

Abstract

Specialized pro‐resolving mediators (SPM), primarily produced in innate immune cells, exert crucial bioactions for resolving inflammation. Among various lipoxygenases (LOX), 15‐LOX‐1 is key for SPM biosynthesis, but cellular activation principles of 15‐LOX‐1 are unexplored. It was shown that 3‐O‐acetyl‐11‐keto‐β‐boswellic acid (AKBA) shifts 5‐LOX regiospecificity from 5‐ to 12‐lipoxygenation products. Here, it is demonstrated that AKBA additionally activates cellular 15‐LOX‐1 via an allosteric site accomplishing robust SPM formation in innate immune cells, particularly in M2 macrophages. Compared to ionophore, AKBA‐induced LOX activation is Ca2+‐ and phosphorylation‐independent, with modest induction of 5‐LOX products. AKBA docks into a groove between the catalytic and regulatory domains of 15‐LOX‐1 interacting with R98; replacement of R98 by alanine abolishes AKBA‐induced 15‐LOX product formation in HEK293 cells. In zymosan‐induced murine peritonitis, AKBA strikingly elevates SPM levels and promotes inflammation resolution. Together, targeted allosteric modulation of LOX activities governs SPM formation and offers new concepts for inflammation resolution pharmacotherapy. [ABSTRACT FROM AUTHOR]

Published

2023

99. Remodeling of Adipose Tissues by Fatty Acids: Mechanistic Update on Browning and Thermogenesis by n-3 Polyunsaturated Fatty Acids.

Author

Raj, Radha Raman, Lofquist, Sydney, and Lee, Mi-Jeong

Subjects

*OMEGA-3 fatty acids, *UNSATURATED fatty acids, *TISSUE remodeling, *BODY temperature regulation, *FATTY acids, *FAT cells, *ADIPOSE tissues

Abstract

Enhancing thermogenesis by increasing the amount and activity of brown and brite adipocytes is a potential therapeutic target for obesity and its associated diseases. Diet plays important roles in energy metabolism and a myriad of dietary components including lipids are known to regulate thermogenesis through recruitment and activation of brown and brite adipocytes. Depending on types of fatty acids (FAs), the major constituent in lipids, their health benefits differ. Long-chain polyunsaturated FAs (PUFAs), especially n-3 PUFAs remodel adipose tissues in a healthier manner with reduced inflammation and enhanced thermogenesis, while saturated FAs exhibit contrasting effects. Lipid mediators derived from FAs act as autocrine/paracrine as well as endocrine factors to regulate thermogenesis. We discuss lipid mediators that may contribute to the differential effects of FAs on adipose tissue remodeling and hence, cardiometabolic diseases. We also discuss current understanding of molecular and cellular mechanisms through which n-3 PUFAs enhance thermogenesis. Elucidating molecular details of beneficial effects of n-3 PUFAs on thermogenesis is expected to provide information that can be used for development of novel therapeutics for obesity and its associated diseases. [ABSTRACT FROM AUTHOR]

Published

2023

100. Follicular Fluid Components in Reduced Ovarian Reserve, Endometriosis, and Idiopathic Infertility.

Author

Collodel, Giulia, Gambera, Laura, Stendardi, Anita, Nerucci, Fabiola, Signorini, Cinzia, Pisani, Caterina, Marcheselli, Marzia, Vellucci, Francesca Letizia, Pizzasegale, Silvana Enrica, Micheli, Lucia, and Moretti, Elena

Subjects

*ENDOMETRIOSIS, *OVARIAN reserve, *REPRODUCTIVE technology, *FEMALE infertility, *INFERTILITY, *OLDER women, *ANTI-Mullerian hormone

Abstract

Follicular fluid (FF) molecules, and their increase or decrease, can contribute to appropriate follicular growth and oocyte maturation, thus being related to female infertility conditions. In this paper, we studied the changes and the relationships of some biochemical components, hormones, antioxidant enzymes, F2-Isoprostanes (F2-IsoPs), and resolvin (Rv) D1 in the FF of infertile women with different reproductive conditions such as endometriosis, reduced ovarian reserve, and idiopathic infertility during assisted reproductive techniques (ART). In the whole population, positive correlations between albumin (ALB)/iron (Fe), ALB/beta-2-microglobulin (B2MG), and F2-IsoPs/RvD1 were detected in the FF. In FF from aged women, increased levels of follicle stimulating hormone (FSH) and reduced anti-Müllerian hormone (AMH) levels were associated with a worse oocyte quality. The negative ART outcome was influenced by patient age and AMH, B2MG, and FSH levels. Moreover, the reduced ovarian reserve condition was characterised by a significant decrease in oocyte number and quality, AMH amount, and lactate dehydrogenase (LDH) activity, as well as by an increase in age and FSH levels. In the presence of endometriosis, high levels of MDA and RvD1 were detected in FF, with a decrease in luteinising hormone (LH). Finally, among the molecules examined, none characterised the condition of idiopathic infertility. These data could support the identification of new FF markers in different reproductive disorders, suggesting the need for personalised therapeutic approaches and optimised ART outcomes. In particular, the evaluation of resolvins and lipid mediators in FF could be a promising field of investigation with which to understand the entity of oxidative stress and inflammation in some female infertility conditions. [ABSTRACT FROM AUTHOR]

Published

2023