Your search keyword '"LIPOPROTEIN METABOLISM"' showing total 1,980 results

1. Replacing dietary carbohydrate with protein and fat improves lipoprotein subclass profile and liver fat in type 2 diabetes independent of body weight: evidence from 2 randomized controlled trials

Author

Thomsen, Mads N, Skytte, Mads J, Samkani, Amirsalar, Weber, Philip, Fenger, Mogens, Frystyk, Jan, Hansen, Elizaveta, Holst, Jens J, Madsbad, Sten, Magkos, Faidon, Thomsen, Henrik S, Walzem, Rosemary L, Haugaard, Steen B, and Krarup, Thure

Published

2025

2. Effects of age and diet on triglyceride metabolism in mice

Author

Spitler, Kathryn M., Shetty, Shwetha K., and Davies, Brandon S.J.

Published

2025

3. APOA2 increases cholesterol efflux capacity to plasma HDL by displacing the C-terminus of resident APOA1

Author

Sarkar, Snigdha, Morris, Jamie, You, Youngki, Sexmith, Hannah, Street, Scott E., Thibert, Stephanie M., Attah, Isaac K., Hutchinson Bunch, Chelsea M., Novikova, Irina V., Evans, James E., Shah, Amy S., Gordon, Scott M., Segrest, Jere P., Bornfeldt, Karin E., Vaisar, Tomas, Heinecke, Jay W., Davidson, W. Sean, and Melchior, John T.

Published

2024

4. Uncovering the health implications of abandoned mines through protein profiling of local residents

Author

Mun, Sora, Lee, You-Rim, Lee, Jiyeong, Lee, Seungyeon, Yun, Yeeun, Kim, Jeeyoung, Kwon, Jung-Yeon, Kim, Woo Jin, Cho, Yong Min, Hong, Young-Seoub, and Kang, Hee-Gyoo

Published

2024

5. Editorial: Women in lipids in cardiovascular disease

Author

Irena Levitan and Catherine Martel

Subjects

women in science, LDL, HDL, lipoprotein metabolism, lipophagy, Diseases of the circulatory (Cardiovascular) system, RC666-701

Published

2025

6. A suite of genome-engineered hepatic cells provides novel insights into the spatiotemporal metabolism of apolipoprotein B and apolipoprotein B–containing lipoprotein secretion.

Author

Meurs, Amber, Ndoj, Klevis, van den Berg, Marlene, Marinković, Goran, Tantucci, Matteo, Veenendaal, Tineke, Kuivenhoven, Jan Albert, Klumperman, Judith, and Zelcer, Noam

Subjects

*BLOOD lipids, *FLUORESCENT proteins, *APOLIPOPROTEIN B, *GENOME editing, *LOW density lipoprotein receptors

Abstract

Aims Apolipoprotein B (APOB)-containing very LDL (VLDL) production, secretion, and clearance by hepatocytes is a central determinant of hepatic and circulating lipid levels. Impairment of any of the aforementioned processes is associated with the development of multiple diseases. Despite the discovery of genes and processes that govern hepatic VLDL metabolism, our understanding of the different mechanistic steps involved is far from complete. An impediment to these studies is the lack of tractable hepatocyte-based systems to interrogate and follow APOB in cells, which the current study addresses. Methods and results To facilitate the cellular study of VLDL metabolism, we generated human hepatic HepG2 and Huh-7 cell lines in which CRISPR/Cas9-based genome engineering was used to introduce the fluorescent protein mNeonGreen into the APOB gene locus. This results in the production of APOB100-mNeon that localizes predominantly to the endoplasmic reticulum (ER) and Golgi by immunofluorescence and electron microscopy imaging. The production and secretion of APOB100-mNeon can be quantitatively followed in medium over time and results in the production of lipoproteins that are taken up via the LDL receptor pathway. Importantly, the production and secretion of APOB-mNeon is sensitive to established pharmacological and physiological treatments and to genetic modifiers known to influence VLDL production in humans. As a showcase, we used HepG2-APOBmNeon cells to interrogate ER-associated degradation of APOB. The use of a dedicated sgRNA library targeting all established membrane-associated ER-resident E3 ubiquitin ligases led to the identification of SYNV1 as the E3 responsible for the degradation of poorly lipidated APOB in HepG2 cells. Conclusions In summary, the engineered cells reported here allow the study of hepatic VLDL assembly and secretion and facilitate spatiotemporal interrogation induced by pharmacologic and genetic perturbations. [ABSTRACT FROM AUTHOR]

Published

2024

7. The role of genetically-influenced phospholipid transfer protein activity in lipoprotein metabolism and coronary artery disease.

Author

Ao, Linjun, Noordam, Raymond, Rensen, Patrick C.N., van Heemst, Diana, and Willems van Dijk, Ko

Subjects

PHOSPHOLIPIDS, CARRIER proteins, NUCLEAR magnetic resonance spectroscopy, LOGISTIC regression analysis, LIPOPROTEINS, CORONARY artery disease, METABOLOMICS, CONFIDENCE intervals, REGRESSION analysis

Abstract

• This study investigated the association of genetically-influenced PLTP activity with 168 metabolomic measures, quantified by 1-H nuclear magnetic resonance (1H-NMR) in over 58,000 individuals in the UK Biobank. • We show that high PLTP activity associates with lower TG concentration and larger HDL size, consistent with a role of PLTP in transfer of phospholipids from VLDL to HDL during LPL-mediated lipolytic conversion. • Despite small HDL has been reported to be negatively associated with CAD risk, lowering plasma PLTP activity does not significantly reduce CAD risk, which may be explained by pleiotropic effects of PLTP activity. Phospholipid transfer protein (PLTP) transfers surface phospholipids between lipoproteins and as such plays a role in lipoprotein metabolism, but with unclear effects on coronary artery disease (CAD) risk. We aimed to investigate the associations of genetically-influenced PLTP activity with 1-H nuclear magnetic resonance (1H-NMR) metabolomic measures and with CAD. Furthermore, using factorial Mendelian randomization (MR), we examined the potential additional effect of genetically-influenced PLTP activity on CAD risk on top of genetically-influenced low-density lipoprotein-cholesterol (LDL-C) lowering. Using data from UK Biobank, genetic scores for PLTP activity and LDL-C were calculated and dichotomised based on the median, generating four groups with combinations of high/low PLTP activity and high/low LDL-C levels for the factorial MR. Linear and logistic regressions were performed on 168 metabolomic measures (N = 58,514) and CAD (N = 318,734, N-cases=37,552), respectively, with results expressed as β coefficients (in standard deviation units) or odds ratios (ORs) and 95% confidence interval (CI). Irrespective of the genetically-influenced LDL-C, genetically-influenced low PLTP activity was associated with a higher high-density lipoprotein (HDL) particle concentration (β [95% CI]: 0.03 [0.01, 0.05]), smaller HDL size (-0.14 [-0.15, -0.12]) and higher triglyceride (TG) concentration (0.04 [0.02, 0.05]), but not with CAD (OR 0.99 [0.97, 1.02]). In factorial MR analyses, genetically-influenced low PLTP activity and genetically-influenced low LDL-C had independent associations with metabolomic measures, and genetically-influenced low PLTP activity did not show an additional effect on CAD risk. Low PLTP activity associates with higher HDL particle concentration, smaller HDL particle size and higher TG concentration, but no association with CAD risk was observed. [ABSTRACT FROM AUTHOR]

Published

2024

8. Brown adipose tissue facilitates the fever response following infection with Salmonella enterica serovar Typhimurium in mice

Author

Mohan Li, Marina Barros-Pinkelnig, Günter Weiss, Patrick C.N. Rensen, and Sander Kooijman

Subjects

brown fat, nonshivering thermogenesis, fever, lipoprotein metabolism, bacterial infection, Biochemistry, QD415-436

Abstract

Brown adipose tissue (BAT) combusts lipids and glucose to generate heat. Via this process of nonshivering thermogenesis, BAT plays a pivotal role in thermoregulation in cold environments, but its contribution to immune-induced fever is less clear. Male APOE∗3-Leiden.CETP mice, a well-established model for human-like lipoprotein metabolism, and wild-type mice were given an intraperitoneal injection of Salmonella enterica serovar Typhimurium (S.tm). Energy expenditure and substrate utilization, plasma lipid levels, fatty acid (FA) uptake by adipose tissues, and lipid content and thermogenic markers in adipose tissues were examined. S.tm infection led to a set of characteristic symptoms, including elevated body temperature and decreased body weight. Whole-body energy expenditure was significantly decreased 72 h postinfection, but fat oxidation was increased and accompanied by a substantial reduction in plasma triglyceride (TG) levels as demonstrated in APOE∗3-Leiden.CETP mice. S.tm infection strongly increased uptake of FAs from TG-rich lipoproteins by BAT, which showed a positive correlation with body temperature in infected mice. Upon histological examination of BAT from wild-type or APOE∗3-Leiden.CETP mice, elevated levels of tyrosine hydroxylase were observed, indicative of stimulated sympathetic activity. In addition, the gene expression profile was consistent with more adrenergic stimulation, while lipid content was reduced. Furthermore, browning of white adipose tissue was observed, evidenced by a modest increase in TG-derived FA uptake, the presence of multilocular cells, and induction of uncoupling protein 1 expression. We proposed that BAT, or thermogenic adipose tissue in general, is involved in the maintenance of elevated body temperature upon invasive bacterial infection.

Published

2024

9. Interindividual differences in aronia juice tolerability linked to gut microbiome and metabolome changes—secondary analysis of a randomized placebo-controlled parallel intervention trial

Author

Lackner, Sonja, Mahnert, Alexander, Moissl-Eichinger, Christine, Madl, Tobias, Habisch, Hansjörg, Meier-Allard, Nathalie, Kumpitsch, Christina, Lahousen, Theresa, Kohlhammer-Dohr, Alexandra, Mörkl, Sabrina, Strobl, Herbert, and Holasek, Sandra

Published

2024

10. ASGR1 deficiency diverts lipids toward adipose tissue but results in liver damage during obesity

Author

Svecla, Monika, Da Dalt, Lorenzo, Moregola, Annalisa, Nour, Jasmine, Baragetti, Andrea, Uboldi, Patrizia, Donetti, Elena, Arnaboldi, Lorenzo, Beretta, Giangiacomo, Bonacina, Fabrizia, and Norata, Giuseppe Danilo

Published

2024

11. Pharmacological treatment with FGF21 strongly improves plasma cholesterol metabolism to reduce atherosclerosis.

Author

Liu, Cong, Schönke, Milena, Zhou, Enchen, Li, Zhuang, Kooijman, Sander, Boon, Mariëtte, Larsson, Mikael, Wallenius, Kristina, Dekker, Niek, Barlind, Louise, Peng, Xiao-Rong, Wang, Yanan, and Rensen, Patrick

Subjects

Adipose-liver axis, Atherosclerotic cardiovascular disease, Brown adipose tissue, Dyslipidaemia, Lipoprotein metabolism, Adipose Tissue, Brown, Adipose Tissue, White, Adiposity, Animals, Anticholesteremic Agents, Apolipoprotein E3, Atherosclerosis, Biomarkers, Cholesterol, Disease Models, Animal, Energy Metabolism, Fibroblast Growth Factors, Hypercholesterolemia, Lipid Metabolism, Lipoproteins, VLDL, Liver, Mice, Transgenic, Plaque, Atherosclerotic, Recombinant Proteins, Triglycerides

Abstract

AIMS: Fibroblast growth factor (FGF) 21, a key regulator of energy metabolism, is currently evaluated in humans for treatment of type 2 diabetes and non-alcoholic steatohepatitis. However, the effects of FGF21 on cardiovascular benefit, particularly on lipoprotein metabolism in relation to atherogenesis, remain elusive. METHODS AND RESULTS: Here, the role of FGF21 in lipoprotein metabolism in relation to atherosclerosis development was investigated by pharmacological administration of a half-life extended recombinant FGF21 protein to hypercholesterolaemic APOE*3-Leiden.CETP mice, a well-established model mimicking atherosclerosis initiation and development in humans. FGF21 reduced plasma total cholesterol, explained by a reduction in non-HDL-cholesterol. Mechanistically, FGF21 promoted brown adipose tissue (BAT) activation and white adipose tissue (WAT) browning, thereby enhancing the selective uptake of fatty acids from triglyceride-rich lipoproteins into BAT and into browned WAT, consequently accelerating the clearance of the cholesterol-enriched remnants by the liver. In addition, FGF21 reduced body fat, ameliorated glucose tolerance and markedly reduced hepatic steatosis, related to up-regulated hepatic expression of genes involved in fatty acid oxidation and increased hepatic VLDL-triglyceride secretion. Ultimately, FGF21 largely decreased atherosclerotic lesion area, which was mainly explained by the reduction in non-HDL-cholesterol as shown by linear regression analysis, decreased lesion severity, and increased atherosclerotic plaque stability index. CONCLUSION: FGF21 improves hypercholesterolaemia by accelerating triglyceride-rich lipoprotein turnover as a result of activating BAT and browning of WAT, thereby reducing atherosclerotic lesion severity and increasing atherosclerotic lesion stability index. We have thus provided additional support for the clinical use of FGF21 in the treatment of atherosclerotic cardiovascular disease.

Published

2022

12. High-density lipoproteins and non-alcoholic fatty liver disease

Author

Menno Hoekstra and Miranda Van Eck

Subjects

High-density lipoprotein, Fatty liver disease, Steatohepatitis, Hepatocytes, Steatosis, Lipoprotein metabolism, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Background and aims: Non-alcoholic fatty liver disease (NAFLD), a high incidence liver pathology, is associated with a ∼1.5-fold higher cardiovascular disease risk. This phenomenon is generally attributed to the NAFLD-associated increase in circulating levels of pro-atherogenic apolipoprotein B100-containing small dense low-density lipoprotein and plasma hypertriglyceridemia. However, also a significant reduction in cholesterol transported by anti-atherogenic high-density lipoproteins (HDL) is frequently observed in subjects suffering from NAFLD as compared to unaffected people. In this review, we summarize data regarding the relationship between NAFLD and plasma HDL-cholesterol levels, with a special focus on highlighting potential causality between the NAFLD pathology and changes in HDL metabolism. Methods and results: Publications in PUBMED describing the relationship between HDL levels and NAFLD susceptibility and/or disease severity, either in human clinical settings or genetically-modified mouse models, were critically reviewed for subsequent inclusion in this manuscript. Furthermore, relevant literature describing effects on lipid loading in cultured hepatocytes of models with genetic alterations related to HDL metabolism have been summarized. Conclusions: Although in vitro observations suggest causality between HDL formation by hepatocytes and protection against NAFLD-like lipid accumulation, current literature remains inconclusive on whether relative HDL deficiency is actually driving the development of fatty liver disease in humans. In light of the current obesity pandemic and the associated marked rise in NAFLD incidence, it is of clear scientific and societal interest to gain further insight into the relationship between HDL-cholesterol levels and fatty liver development to potentially uncover the therapeutic potential of pharmacological HDL level and/or function modulation.

Published

2023

13. Total Outflow of High-Density Lipoprotein–Cholesteryl Esters from Plasma Is Decreased in a Model of 3/4 Renal Mass Reduction.

Author

Luna-Luna, María, Franco, Martha, Carreón-Torres, Elizabeth, Pérez-Hernández, Nonanzit, Fragoso, José Manuel, Bautista-Pérez, Rocío, and Pérez-Méndez, Óscar

Subjects

*CHOLESTERYL ester transfer protein, *ESTERS, *HIGH density lipoproteins, *LIPOPROTEINS, *LOW density lipoproteins, *TRITIUM

Abstract

(1) Background: Previous studies have enriched high-density lipoproteins (HDL) using cholesteryl esters in rabbits with a three-quarter reduction in functional renal mass, suggesting that the kidneys participate in the cholesterol homeostasis of these lipoproteins. However, the possible role of the kidneys in lipoprotein metabolism is still controversial. To understand the role of the kidneys in regulating the HDL lipid content, we determined the turnover of HDL-cholesteryl esters in rabbits with a three-quarter renal mass reduction. (2) Methods: HDL subclass characterization was conducted, and the kinetics of plasma HDL-cholesteryl esters, labeled with tritium, were studied in rabbits with a 75% reduction in functional renal mass (Ntx). (3) Results: The reduced renal mass triggered the enrichment of cholesterol, specifically cholesteryl esters, in HDL subclasses. The exchange of cholesteryl esters between HDL and apo B-containing lipoproteins (VLDL/LDL) was not significantly modified in Ntx rabbits. Moreover, the cholesteryl esters of HDL and VLDL/LDL fluxes from the plasmatic compartment tended to decrease, but they only reached statistical significance when both fluxes were added to the Nxt group. Accordingly, the fractional catabolic rate (FCR) of the HDL-cholesteryl esters was lower in Ntx rabbits, concomitantly with its accumulation in HDL subclasses, probably because of the reduced mass of renal cells requiring this lipid from lipoproteins. [ABSTRACT FROM AUTHOR]

Published

2023

14. Endocrine Function and Metabolic Outcomes After Pancreas and Islet Transplantation

Author

Robertson, R. Paul, Gruessner, Rainer W. G., editor, and Gruessner, Angelika C., editor

Published

2023

15. Lipoprotein Metabolism and Alterations Induced by Insulin Resistance and Diabetes

Author

Tomkin, Gerald H., Owens, Daphne, Veves, Aristidis, Series Editor, Jenkins, Alicia J., editor, and Toth, Peter P., editor

Published

2023

16. Lipoprotein (a) [Lp(a)]

Author

Salama, Mostafa, Kumar, Seema, Ashraf, Ambika, editor, and Sunil, Bhuvana, editor

Published

2023

17. Obicetrapib Alone and in Combination with Ezetimibe Reduces Non-HDL-Cholesterol by Enhanced LDL-Receptor-Mediated VLDL Clearance and Increased Net Fecal Sterol Excretion in ApoE*3-Leiden.CETP Mice.

Author

Inia, José A., Keijzer, Nanda, Worms, Nicole, van Nieuwkoop, Anita, Ditmarsch, Marc, Jukema, J. Wouter, Groen, Albert K., Kastelein, John, Pieterman, Elsbet J., and Princen, Hans M.G.

Abstract

Background and Aims: Obicetrapib is a selective cholesteryl ester transfer protein (CETP) inhibitor in clinical development for the treatment of hypercholesterolemia and cardiovascular risk. It reduces apolipoprotein B (ApoB) and low-density lipoprotein cholesterol (LDL-C) and increases high-density lipoprotein cholesterol (HDL-C). Ezetimibe reduces absorption of biliary and dietary cholesterol from the small intestine, also reducing LDL-C levels. The current study elucidates the mechanism for decreases in non-HDL-C by obicetrapib alone and with ezetimibe in a mouse model for hyperlipidemia and atherosclerosis. Methods: Female ApoE*3-Leiden.CETP transgenic mice were fed a Western diet with 0.05% w/w cholesterol (equivalent to daily human intake) or this diet containing obicetrapib (2 mg/kg/day), ezetimibe (1 mg/kg/day), or obicetrapib with ezetimibe. Results: Obicetrapib, ezetimibe, and the combination reduced total plasma cholesterol levels (-42%, -23% and -62%).Obicetrapib alone and in combination with ezetimibe nearly completely blocked CETP activity (-99% and -100%) resulting in increased HDL-C (+260% and +245%) and ApoA1 (98% and 81%). Obicetrapib, ezetimibe, and the combination enhanced clearance of VLDL-like particles (half-life: -44%, -23% and -57%) and enhanced hepatic LDL receptor expression (+63% and +74%). Increased bile acid excretion in obicetrapib-treated mice (+41%) and increased neutral sterol excretion in ezetimibe-treated mice was observed, and was more pronounced in combination with obicetrapib (+68% and +100%), resulting in a net fecal sterol loss. Conclusions: Obicetrapib alone and with ezetimibe reduced non-HDL-C levels by increased VLDL lipolysis, increased VLDL clearance and elevated LDL receptor levels, and enhanced fecal bile acid and neutral sterol excretion. [ABSTRACT FROM AUTHOR]

Published

2024

18. Lipoprotein lipidomics in obesity-associated metabolic and hepatic disorders

Author

Mocciaro, Gabriele, Griffin, Julian, and Vacca, Michele

Subjects

Obesity, lipoprotein metabolism, LC-MS, lipidomics

Abstract

Over the last few decades, obesity has reached epidemic proportions. Obesity is strongly associated with insulin resistance (IR), hyperglycaemia, mixed dyslipidaemia, and hypertension. These metabolic risk factors, grouped under the definition of the Metabolic Syndrome (MetS), increase the risk of cardiovascular disease (CVD). Non-alcoholic fatty liver disease (NAFLD) is one of the most common co-morbidities of MetS. NAFLD ranges from simple steatosis to more aggressive forms, with the potential to evolve to hepatocellular carcinoma and CVD. Lipoprotein dysmetabolism is crucial to both MetS and NAFLD and few studies have investigated the circulating lipidome, defined as the complete lipid profile in a specific tissue/biofluid, in these conditions. The work contained in this thesis studied the lipoprotein remodelling occurring in two cohorts; MetS cohort including 11 healthy people and 14 MetS subjects and BioNASH cohort including 20 healthy people and 89 biopsy-proven patients across the entire spectrum of NAFLD. To this end, we employed state-of-the-art analytical techniques (mass spectrometry-based) along with molecular biology assays to study the serum and lipoprotein lipidome of these patients. In the MetS study, we found that the circulating lipidome of MetS was characterised by a phospholipid (PL) dysmetabolism. The latter was driven, at least in part, by a reduced activity of the enzyme lecithin-cholesterol acyltransferase (LCAT). Dysfunctional LCAT could partly mediate the elevated CVD risk in MetS patients. Our study demonstrated, for the first time, the link between reduced LCAT activity and plasma lipidome in MetS. In the BioNASH cohort, we observed a generalised PL and polyunsaturated fatty acids (PUFA) depletion in NAFLD compared to the control group. By using fast protein liquid chromatography, we isolated HDL and VLDL fractions where we performed lipidomic analyses. As opposed to VLDL, the HDL lipidome was characterised by PL and PUFA depletion. These changes have been reported in hepatic lipidomic studies of NAFLD patients, thus suggesting a close link between peripheral tissues and the liver via HDL. These results provide the basis for the study of HDL composition as a novel player in the pathogenesis of NAFLD. In conclusion, these data demonstrate how the study of lipoprotein metabolism in obesity-related metabolic disorders can shed light on novel pathophysiological mechanisms. Further efforts along these lines will clarify the role of LCAT in MetS and CVD alongside establishing the contribution of the HDL lipidome to the liver composition of NAFLD patients.

Published

2021

19. Pharmacological activation of constitutive androstane receptor induces female-specific modulation of hepatic metabolism

Author

Marine Huillet, Frédéric Lasserre, Marie-Pierre Gratacap, Beatrice Engelmann, Justine Bruse, Arnaud Polizzi, Tiffany Fougeray, Céline Marie Pauline Martin, Clémence Rives, Anne Fougerat, Claire Naylies, Yannick Lippi, Géraldine Garcia, Elodie Rousseau-Bacquie, Cécile Canlet, Laurent Debrauwer, Ulrike Rolle-Kampczyk, Martin von Bergen, Bernard Payrastre, Elisa Boutet-Robinet, Laurence Gamet-Payrastre, Hervé Guillou, Nicolas Loiseau, and Sandrine Ellero-Simatos

Subjects

Sexual dimorphism, Hepatic xenobiotic metabolism, Lipoprotein metabolism, Platelet aggregation, Trimethylamine-N-oxide, Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

Background & Aims: The constitutive androstane receptor (CAR) is a nuclear receptor that binds diverse xenobiotics and whose activation leads to the modulation of the expression of target genes involved in xenobiotic detoxification and energy metabolism. Although CAR hepatic activity is considered to be higher in women than in men, its sex-dependent response to an acute pharmacological activation has seldom been investigated. Methods: The hepatic transcriptome, plasma markers, and hepatic metabolome, were analysed in Car+/+ and Car-/- male and female mice treated either with the CAR-specific agonist 1,4-bis[2-(3,5-dichloropyridyloxy)]benzene (TCPOBOP) or with vehicle. Results: Although 90% of TCPOBOP-sensitive genes were modulated in a sex-independent manner, the remaining 10% showed almost exclusive female liver specificity. These female-specific CAR-sensitive genes were mainly involved in xenobiotic metabolism, inflammation, and extracellular matrix organisation. CAR activation also induced higher hepatic oxidative stress and hepatocyte cytolysis in females than in males. Hepatic expression of flavin monooxygenase 3 (Fmo3) was almost abolished and was associated with a decrease in hepatic trimethylamine-N-oxide (TMAO) concentration in TCPOBOP-treated females. In line with a potential role in the control of TMAO homeostasis, CAR activation decreased platelet hyper-responsiveness in female mice supplemented with dietary choline. Conclusions: More than 10% of CAR-sensitive genes are sex-specific and influence hepatic and systemic responses such as platelet aggregation. CAR activation may be an important mechanism of sexually-dimorphic drug-induced liver injury. Impact and implications: CAR is activated by many drugs and pollutants. Its pharmacological activation had a stronger impact on hepatic gene expression and metabolism in females than in males, and had a specific impact on liver toxicity and trimethylamine metabolism. Sexual dimorphism should be considered when testing and/or prescribing xenobiotics known to activate CAR.

Published

2024

20. Anti-Hyperlipidemic Effect of Fucoidan Fractions Prepared from Iceland Brown Algae Ascophyllum nodosum in an Hyperlipidemic Mice Model.

Author

He, Yunhai, Li, Yutong, Shen, Peili, Li, Shangkun, Zhang, Linsong, Wang, Qiukuan, Ren, Dandan, Liu, Shu, Zhang, Demeng, and Zhou, Hui

Abstract

Ascophyllum nodosum, a brown algae abundantly found along the North Atlantic coast, is recognized for its high polysaccharide content. In this study, we investigated the anti-hyperlipidemic effect of fucoidans derived from A. nodosum, aiming to provide information for their potential application in anti-hyperlipidemic therapies and to explore comprehensive utilization of this Iceland brown seaweed. The crude fucoidan prepared from A. nodosum was separated using a diethylethanolamine column, resulting in two fucoidan fractions, AFC-1 and AFC-2. Both fractions were predominantly composed of fucose and xylose. AFC-1 exhibited a higher sulfate content of 27.8% compared to AFC-2 with 17.0%. AFC-2 was primarily sulfated at the hydroxy group of C2, whereas AFC-1 was sulfated at both the hydroxy groups of C2 and C4. To evaluate the anti-hyperlipidemic effect, a hyperlipidemia mouse model was established by feeding mice a high-fat diet. The effects of AFC-1, AFC-2, and the crude extract were investigated, with the drug atorvastatin used as a positive comparison. Among the different fucoidan fractions and doses, the high dose of AFC-2 administration demonstrated the most significant anti-hyperlipidemic effect across various aspects, including physiological parameters, blood glucose levels, lipid profile, histological analysis, and the activities of oxidative stress-related enzymes and lipoprotein-metabolism-related enzymes (p < 0.05 for the final body weight and p < 0.01 for the rest indicators, compared with the model group), and its effect is comparable to the atorvastatin administration. Furthermore, fucoidan administration resulted in a lower degree of loss in gut flora diversity compared to atorvastatin administration. These findings highlight the significant biomedical potential of fucoidans derived from A. nodosum as a promising therapeutic solution for hypolipidemia. [ABSTRACT FROM AUTHOR]

Published

2023

21. Hepatitis B Virus Targets Lipid Transport Pathways to Infect HepatocytesSummary

Author

Knud Esser, Xiaoming Cheng, Jochen M. Wettengel, Julie Lucifora, Lea Hansen-Palmus, Katharina Austen, Armando A. Roca Suarez, Sarah Heintz, Barbara Testoni, Firat Nebioglu, Minh Tu Pham, Shangqing Yang, Alma Zernecke, Dirk Wohlleber, Marc Ringelhan, Mathias Broxtermann, Daniel Hartmann, Norbert Hüser, Julia Mergner, Andreas Pichlmair, Wolfgang E. Thasler, Mathias Heikenwalder, Georg Gasteiger, Andreas Blutke, Axel Walch, Percy A. Knolle, Ralf Bartenschlager, and Ulrike Protzer

Subjects

Transcytosis, Transinfection, Liver Targeting, Lipoprotein Metabolism, Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

Background & Aims: A single hepatitis B virus (HBV) particle is sufficient to establish chronic infection of the liver after intravenous injection, suggesting that the virus targets hepatocytes via a highly efficient transport pathway. We therefore investigated whether HBV uses a physiological liver-directed pathway that supports specific host-cell targeting in vivo. Methods: We established the ex vivo perfusion of intact human liver tissue that recapitulates the liver physiology to investigate HBV liver targeting. This model allowed us to investigate virus-host cell interactions in a cellular microenvironment mimicking the in vivo situation. Results: HBV was rapidly sequestered by liver macrophages within 1 hour after a virus pulse perfusion but was detected in hepatocytes only after 16 hours. We found that HBV associates with lipoproteins in serum and within machrophages. Electron and immunofluorescence microscopy corroborated a co-localization in recycling endosomes within peripheral and liver macrophages. Recycling endosomes accumulated HBV and cholesterol, followed by transport of HBV back to the cell surface along the cholesterol efflux pathway. To reach hepatocytes as final target cells, HBV was able to utilize the hepatocyte-directed cholesterol transport machinery of macrophages. Conclusions: Our results propose that by binding to liver targeted lipoproteins and using the reverse cholesterol transport pathway of macrophages, HBV hijacks the physiological lipid transport pathways to the liver to most efficiently reach its target organ. This may involve transinfection of liver macrophages and result in deposition of HBV in the perisinusoidal space from where HBV can bind its receptor on hepatocytes.

Published

2023

22. Role of apolipoprotein C1 in lipoprotein metabolism, atherosclerosis and diabetes: a systematic review

Author

Alexia Rouland, David Masson, Laurent Lagrost, Bruno Vergès, Thomas Gautier, and Benjamin Bouillet

Subjects

Apolipoprotein C1, Diabetes, Atherosclerosis, Lipoprotein metabolism, Triglyceride-rich lipoproteins, High density lipoproteins, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Abstract Apolipoprotein C1 (apoC1) is a small size apolipoprotein whose exact role is not totally clarified but which seems to modulate significantly the metabolism of lipoproteins. ApoC1 is involved in the metabolism of triglyceride-rich lipoproteins by inhibiting the binding of very low density lipoproteins (VLDL) to VLDL-receptor (VLDL-R), to low density lipoprotein receptor (LDL-R) and to LDL receptor related protein (LRP), by reducing the activity of lipoprotein lipase (LPL) and by stimulating VLDL production, all these effects leading to increase plasma triglycerides. ApoC1 takes also part in the metabolism of high density lipoproteins (HDL) by inhibiting Cholesterol Ester Transfer Protein (CETP). The functionality of apoC1 on CETP activity is impaired in diabetes that might account, at least in part, for the increased plasma CETP activity observed in patients with diabetes. Its different effects on lipoprotein metabolism with a possible role in the modulation of inflammation makes the net impact of apoC1 on cardiometabolic risk difficult to figure out and apoC1 might be considered as pro-atherogenic or anti-atherogenic depending on the overall metabolic context. Making the link between total plasma apoC1 levels and the risk of cardio-metabolic diseases is difficult due to the high exchangeability of this small protein whose biological effects might depend essentially on its association with VLDL or HDL. The role of apoC1 in humans is not entirely elucidated and further studies are needed to determine its precise role in lipid metabolism and its possible pleiotropic effects on inflammation and vascular wall biology. In this review, we will present data on apoC1 structure and distribution among lipoproteins, on the effects of apoC1 on VLDL metabolism and HDL metabolism and we will discuss the possible links between apoC1, atherosclerosis and diabetes.

Published

2022

23. Atherosclerosis, Diabetes Mellitus, and Cancer: Common Epidemiology, Shared Mechanisms, and Future Management.

Author

Katsi, Vasiliki, Papakonstantinou, Ilias, and Tsioufis, Konstantinos

Subjects

*EPIDEMIOLOGY of cancer, *LIPID metabolism, *ENDOTHELIUM diseases, *DIABETES, *ATHEROSCLEROSIS, *HOMEOSTASIS

Abstract

The involvement of cardiovascular disease in cancer onset and development represents a contemporary interest in basic science. It has been recognized, from the most recent research, that metabolic syndrome-related conditions, ranging from atherosclerosis to diabetes, elicit many pathways regulating lipid metabolism and lipid signaling that are also linked to the same framework of multiple potential mechanisms for inducing cancer. Otherwise, dyslipidemia and endothelial cell dysfunction in atherosclerosis may present common or even interdependent changes, similar to oncogenic molecules elevated in many forms of cancer. However, whether endothelial cell dysfunction in atherosclerotic disease provides signals that promote the pre-clinical onset and proliferation of malignant cells is an issue that requires further understanding, even though more questions are presented with every answer. Here, we highlight the molecular mechanisms that point to a causal link between lipid metabolism and glucose homeostasis in metabolic syndrome-related atherosclerotic disease with the development of cancer. The knowledge of these breakthrough mechanisms may pave the way for the application of new therapeutic targets and for implementing interventions in clinical practice. [ABSTRACT FROM AUTHOR]

Published

2023

24. Hyperbaric Oxygen Therapy Ameliorates Sperm Parameters in Apolipoprotein E Knockout Mice Testes by Attenuating Oxidative Stress and Inflammation.

Author

Liu, Huijun, Wang, Danni, Ma, Yang, Sun, Huiting, Wang, Linxiao, Shi, Yichao, Wang, Jiaping, and Chen, Xia

Abstract

Apolipoprotein E (ApoE) is a member of apolipoprotein (apo) family and plays critical role in lipid metabolism. In this study, the relationship between abnormal lipid metabolism caused by ApoE-deficient and male reproduction was investigated. The effect of hyperbaric oxygen (HBO) therapy on 7-month-old ApoE-knockout male mice was assessed subsequently. Mice were randomly divided into 3 groups: control group (WT), ApoE (− / −) group (AP-CON), and ApoE (− / −) plus HBO group (AP-HBO), which received HBO treatment. We found that ApoE knockout caused a decrease in male reproductive capacity due to the reduced total sperm motility, progressive motility (PR), and lower blastocyst formation rate. HBO treatment could accelerate serum lipoprotein metabolism including LDL, T-CHO, and TG and semen quality. As a result, fertilization and blastocyst formation of AP-HBO group were higher than that of AP-CON, proving positive therapeutic effect. Mechanism exploration found that HBO treatment ameliorated the testicular microenvironment by attenuating inflammatory factor production and oxidative stress, eventually improved the sperm motility. Collectively, our study provided more evidences of HBO treatment for improving the semen quality of patients with abnormal lipid metabolism caused by ApoE-deficient. [ABSTRACT FROM AUTHOR]

Published

2023

25. 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

26. Non-alcoholic fatty liver disease is characterised by a reduced polyunsaturated fatty acid transport via free fatty acids and high-density lipoproteins (HDL)

Author

Gabriele Mocciaro, Michael Allison, Benjamin Jenkins, Vian Azzu, Isabel Huang-Doran, Luis Vicente Herrera-Marcos, Zoe Hall, Antonio Murgia, Davies Susan, Mattia Frontini, Antonio Vidal-Puig, Albert Koulman, Julian L. Griffin, and Michele Vacca

Subjects

Non-alcoholic fatty liver disease (NAFLD), Obesity, Lipoprotein metabolism, Lipidomics, LC-MS, Internal medicine, RC31-1245

Abstract

Background and objectives: Non-alcoholic fatty liver disease (NAFLD) develops due to impaired hepatic lipid fluxes and is a risk factor for chronic liver disease and atherosclerosis. Lipidomic studies consistently reported characteristic hepatic/VLDL “lipid signatures” in NAFLD; whole plasma traits are more debated. Surprisingly, the HDL lipid composition by mass spectrometry has not been characterised across the NAFLD spectrum, despite HDL being a possible source of hepatic lipids delivered from peripheral tissues alongside free fatty acids (FFA). This study characterises the HDL lipidomic signature in NAFLD, and its correlation with metabolic and liver disease markers. Methods: We used liquid chromatography-mass spectrometry to determine the whole serum and HDL lipidomic profile in 89 biopsy-proven NAFLD patients and 20 sex and age-matched controls. Results: In the whole serum of NAFLD versus controls, we report a depletion in polyunsaturated (PUFA) phospholipids (PL) and FFA; with PUFA PL being also lower in HDL, and negatively correlated with BMI, insulin resistance, triglycerides, and hepatocyte ballooning. In the HDL of the NAFLD group we also describe higher saturated ceramides, which positively correlate with insulin resistance and transaminases. Conclusion: NAFLD features lower serum lipid species containing polyunsaturated fatty acids; the most affected lipid fractions are FFA and (HDL) phospholipids; our data suggest a possible defect in the transfer of PUFA from peripheral tissues to the liver in NAFLD. Mechanistic studies are required to explore the biological implications of our findings addressing if HDL composition can influence liver metabolism and damage, thus contributing to NAFLD pathophysiology.

Published

2023

27. Time-restricted feeding attenuates hypercholesterolaemia and atherosclerosis development during circadian disturbance in APOE∗3-Leiden.CETP miceResearch in context

Author

Wietse In Het Panhuis, Milena Schönke, Melanie Modder, Hannah E. Tom, Reshma A. Lalai, Amanda C.M. Pronk, Trea C.M. Streefland, Linda W.M. van Kerkhof, Martijn E.T. Dollé, Marie A.C. Depuydt, Ilze Bot, Winnie G. Vos, Laura A. Bosmans, Bram W. van Os, Esther Lutgens, Patrick C.N. Rensen, and Sander Kooijman

Subjects

Circadian disturbance, Time-restricted feeding, Lipoprotein metabolism, Inflammation, Atherosclerotic cardiovascular disease, Medicine, Medicine (General), R5-920

Abstract

Summary: Background: Circadian disturbance (CD) is the consequence of a mismatch between endogenous circadian rhythms, behaviour, and/or environmental cycles, and frequently occurs during shift work. Shift work has been associated with elevated risk for atherosclerotic cardiovascular disease (asCVD) in humans, but evidence for the effectiveness of prevention strategies is lacking. Methods: Here, we applied time-restricted feeding (TRF) as a strategy to counteract atherosclerosis development during CD in female APOE∗3-Leiden.CETP mice, a well-established model for humanized lipoprotein metabolism. Control groups were subjected to a fixed 12:12 h light–dark cycle, while CD groups were subjected to 6-h phase advancement every 3 days. Groups had either ad libitum (AL) access to food or were subjected to TRF with restricted food access to the dark phase. Findings: TRF did not prevent the increase in the relative abundance of circulating inflammatory monocytes and elevation of (postprandial) plasma triglycerides during CD. Nonetheless, TRF reduced atherosclerotic lesion size and prevented an elevation in macrophage content of atherosclerotic lesions during CD, while it increased the relative abundance of anti-inflammatory monocytes, prevented activation of T cells, and lowered plasma total cholesterol levels and markers of hepatic cholesterol synthesis. These effects were independent of total food intake. Interpretation: We propose that time restricted eating could be a promising strategy for the primary prevention of asCVD risk in shift workers, which warrants future study in humans. Funding: This work was funded by the Novo Nordisk Foundation, the Netherlands Ministry of Social Affairs and Employment, Amsterdam Cardiovascular Sciences, and the Dutch Heart Foundation.

Published

2023

28. Combined glucose-dependent insulinotropic polypeptide receptor and glucagon-like peptide-1 receptor agonism attenuates atherosclerosis severity in APOE*3-Leiden.CETP mice.

Author

van Eenige, Robin, Ying, Zhixiong, Tramper, Naomi, Wiebing, Vera, Siraj, Zohor, de Boer, Jan Freark, Lambooij, Joost M., Guigas, Bruno, Qu, Hongchang, Coskun, Tamer, Boon, Mariëtte R., Rensen, Patrick C.N., and Kooijman, Sander

Subjects

*GLUCAGON-like peptide-1 receptor, *ADIPOSE tissue diseases, *ATHEROSCLEROSIS, *WHITE adipose tissue, *BROWN adipose tissue, *WESTERN diet, *REGULATION of body weight

Abstract

Combined agonism of the glucose-dependent insulinotropic polypeptide receptor (GIPR) and the glucagon-like peptide-1 receptor (GLP1R) is superior to single GLP1R agonism in terms of glycemic control and lowering body weight in individuals with obesity and with or without type 2 diabetes mellitus. As both GIPR and GLP1R signaling have also been implicated in improving inflammatory responses and lipid handling, two crucial players in atherosclerosis development, here we aimed to investigate the effects of combined GIPR/GLP1R agonism in APOE*3-Leiden.CETP mice, a well-established mouse model for human-like lipoprotein metabolism and atherosclerosis development. Female APOE*3-Leiden.CETP mice were fed a Western-type diet (containing 16% fat and 0.15% cholesterol) to induce dyslipidemia, and received subcutaneous injections with either vehicle, a GIPR agonist (GIPFA-085), a GLP1R agonist (GLP-140) or both agonists. In the aortic root area, atherosclerosis development was assessed. Combined GIPR/GLP1R agonism attenuated the development of severe atherosclerotic lesions, while single treatments only showed non-significant improvements. Mechanistically, combined GIPR/GLP1R agonism decreased markers of systemic low-grade inflammation. In addition, combined GIPR/GLP1R agonism markedly lowered plasma triglyceride (TG) levels as explained by reduced hepatic very-low-density lipoprotein (VLDL)-TG production as well as increased TG-derived fatty acid uptake by brown and white adipose tissue which was coupled to enhanced hepatic uptake of core VLDL remnants. Combined GIPR/GLP1R agonism attenuates atherosclerosis severity by diminishing inflammation and increasing VLDL turnover. We anticipate that combined GIPR/GLP1R agonism is a promising strategy to lower cardiometabolic risk in humans. [Display omitted] • Combined GIPR/GLP1R agonism attenuates atherosclerosis severity. • Less systemic low-grade inflammation and lower plasma triglyceride levels underly the reduced atherosclerosis severity. • The lowered plasma triglyceride levels upon combined GIPR/GLP1R agonism are the result of higher VLDL turnover. [ABSTRACT FROM AUTHOR]

Published

2023

29. Exercise increases myocardial free fatty acid oxidation in subjects with metabolic dysfunction-associated fatty liver disease.

Author

Risikesan, Jeyanthini, Heebøll, Sara, Kumarathas, Indumathi, Funck, Kristian L., Søndergaard, Esben, Johansen, Rakel F., Ringgaard, Steffen, Tolbod, Lars P., Johannsen, Mogens, Kanstrup, Helle L., Grønbæk, Henning, Frystyk, Jan, Gormsen, Lars C., and Nielsen, Søren

Subjects

*FATTY liver, *FATTY acid oxidation, *FREE fatty acids, *BLOOD lactate, *SUPPLY & demand

Abstract

Metabolic dysfunction-associated fatty liver disease (MAFLD) is associated with dyslipidemia and may promote cardiac lipotoxicity. Myocardial free fatty acids (FFA) oxidation (MO FFA) is normal in pre-diabetes, but reduced in heart failure. We hypothesized that during exercise MO FFA , very low-density lipoprotein triglycerides (VLDL-TG) secretion, hepatic FFA utilization, and lactate production differ among obese subjects with and without MAFLD. Nine obese subjects with MAFLD and 8 matched subjects without MAFLD (Control) without a history of heart failure and cardiovascular disease were compared before and after 90-min exercise at 50% Peak oxygen consumption. Basal and exercise induced cardiac and hepatic FFA oxidation, uptake and re-esterification and VLDL-TG secretion were measured using [11C]palmitate positron-emission tomography and [1–14C]VLDL-TG. In the heart, increased MO FFA was observed after exercise in MAFLD, whereas MO FFA decreased in Control (basal vs exercise, MAFLD: 4.1 (0.8) vs 4.8 (0.8) μmol·100 ml−1 min−1; Control: 4.9 (1.8) vs 4.0 (1.1); μmol·100 ml−1 min−1, mean (SD), p < 0.048). Hepatic FFA fluxes were significantly lower in MAFLD than Control and increased ≈ two-fold in both groups. VLDL-TG secretion was 50% greater in MAFLD at rest and similarly suppressed during exercise. Plasma lactate increased significantly less in MAFLD than Control during exercise. Using robust tracer-techniques we found that obese subjects with MAFLD do not downregulate MO FFA during exercise compared to Control, possibly due to diminished lactate supply. Hepatic FFA fluxes are significantly lower in MAFLD than Control, but increase similarly with exercise. VLDL-TG export remains greater in MAFLD compared to Control. Basal and post-exercise myocardial and hepatic FFA, VLDL-TG and lactate metabolism is abnormal in subjects with MAFLD compared to Control. [Display omitted] • Exercise has opposite effects on heart FFA use in subjects with and without MAFLD. • Hepatic FFA utilization increases similarly after exercise. • VLDL-TG secretion and oxidation rates are greater in subjects with MAFLD. • Lactate increase during exercise is significantly impaired in MAFLD. [ABSTRACT FROM AUTHOR]

Published

2023

30. Obicetrapib Alone and in Combination with Ezetimibe Reduces Atherosclerotic Lesion Prevalence, Size and Severity in ApoE*3-Leiden.CETP Mice.

Author

Inia, José A., Keijzer, Nanda, Worms, Nicole, van Nieuwkoop, Anita, Ditmarsch, Marc, Jukema, J. Wouter, Kastelein, John, Pieterman, Elsbet J., and Princen, Hans M.G.

Abstract

Background and Aims: Obicetrapib is a selective, potent, cholesteryl ester transfer protein (CETP) inhibitor in clinical development for the treatment of hypercholesterolemia and reduction of cardiovascular risk. It strongly reduces apolipoprotein B (ApoB) and low-density lipoprotein cholesterol (LDL-C) and increases plasma high-density lipoprotein cholesterol (HDL-C). Ezetimibe is a potent, selective inhibitor of biliary and dietary cholesterol absorption from the small intestine, also reducing LDL-C levels. The current study evaluated the effect of obicetrapib monotherapy and in combination with ezetimibe on atherosclerosis development in a mouse model for hyperlipidemia and atherosclerosis. Methods: Female ApoE*3-Leiden.CETP transgenic mice were fed a Western diet with 0.05% w/w cholesterol (equivalent to daily human intake) or this diet containing obicetrapib alone (2 mg/kg/day), ezetimibe alone (on average 0.6 mg/kg/day), or the combination of obicetrapib and ezetimibe. After 28 weeks of treatment, atherosclerosis development was measured in the aortic roots. Results: Obicetrapib, ezetimibe, and the combination reduced total plasma cholesterol levels (-31%, -19% and -53%), mainly attributed to a decrease in non-HDL-C levels (-53%, -19% and -75%). Obicetrapib and combination treatment nearly completely blocked CETP activity (-98% and -98%). Obicetrapib, ezetimibe, and the combination reduced atherosclerotic lesion size (-90%, -50% and -98%) and reduced severe lesions (-82%, -31% and -98%). The percentage of unaffected segments was increased by obicetrapib and the combination treatment (+347%, +442%). Conclusions: Obicetrapib alone and the combination with ezetimibe robustly lowers non-HDL-C levels and impedes atherosclerosis development through a large decrease in atherosclerotic lesion size and severity. [ABSTRACT FROM AUTHOR]

Published

2024

31. Cell-associated heparin-like molecules modulate the ability of LDL to regulate PCSK9 uptake.

Author

Galvan, Adri and Chorba, John

Subjects

atherosclerosis, cholesterol, coreceptor, dyslipidemias, familial hypercholesterolemia, lipoprotein metabolism, low density lipoprotein, low density lipoprotein receptor, mechanism, proprotein convertase subtilisin/kexin type 9, receptors/lipoprotein, single nucleotide polymorphism, Gene Expression Regulation, HEK293 Cells, Hep G2 Cells, Heparin, Heparin Lyase, Humans, Lipoproteins, LDL, Proprotein Convertase 9, Protein Transport, Receptors, LDL

Abstract

Proprotein convertase subtilisin/kexin type 9 (PCSK9) targets the LDL receptor (LDLR) for degradation, increasing plasma LDL and, consequently, cardiovascular risk. Uptake of secreted PCSK9 is required for its effect on the LDLR, and LDL itself inhibits this uptake, though how it does so remains unclear. In this study, we investigated the relationship between LDL, the PCSK9:LDLR interaction, and PCSK9 uptake. We show that LDL inhibits binding of PCSK9 to the LDLR in vitro more impressively than it inhibits PCSK9 uptake in cells. Furthermore, cell-surface heparin-like molecules (HLMs) can partly explain this difference, consistent with heparan sulfate proteoglycans (HSPGs) acting as coreceptors for PCSK9. We also show that HLMs can interact with either PCSK9 or LDL to modulate the inhibitory activity of LDL on PCSK9 uptake, with such inhibition rescued by competition with the entire PCSK9 prodomain, but not its truncated variants. Additionally, we show that the gain-of-function PCSK9 variant, S127R, located in the prodomain near the HSPG binding site, exhibits increased affinity for HLMs, potentially explaining its phenotype. Overall, our findings suggest a model where LDL acts as a negative regulator of PCSK9 function by decreasing its uptake via direct interactions with either the LDLR or HLMs.

Published

2019

32. Editorial: The role of dietary fatty acids in metabolic health

Author

Laura Bordoni, Manja Zec, Nenad Naumovski, and Domenico Sergi

Subjects

fatty acids, cardiometabolic health, lipid metabolism, lipotoxicity and nutrition, lipoprotein metabolism, Physiology, QP1-981

Published

2023

33. Glycoprotein and Lipoprotein Profiles Assessed by 1H-NMR and Its Relation to Ascending Aortic Dilatation in Bicuspid Aortic Valve Disease.

Author

Antequera-González, Borja, Faiges, Marta, Martínez-Micaelo, Neus, Galian-Gay, Laura, Ligero, Carmen, Ferré-Vallverdú, María, Masana, Lluís, Amigó, Núria, Evangelista, Arturo, and Alegret, Josep M.

Subjects

*AORTIC valve diseases, *MITRAL valve, *AORTA, *AORTIC valve, *MAGNETIC resonance

Abstract

Introduction: The bicuspid aortic valve (BAV) confers a high risk of ascending aorta dilatation (AAoD), although its progression seems highly variable. Furthermore, the implication of lipoprotein metabolism and inflammation in the mechanisms that underlie AAoD is not fully established. The aim of this study consisted of evaluating the impact of the lipoprotein and glycoprotein profiles in AAOD as well as its progression in BAV aortopathy. Methods: Using 1H-nuclear magnetic resonance (1H-NMR), we analyzed and compared the lipoprotein and glycoprotein profiles of plasma samples from 152 BAV patients with dilated and nondilated ascending aorta. Additionally, these profiles were also compared for 119 of these patients who were prospectively followed-up clinically and by echocardiography in the long-term (5 years). Ascending aorta dilation velocity (mm/year) was calculated for this analysis. Results: Several parameters related to the lipoprotein profile including remnant cholesterol, small LDL and IDL-cholesterol were found to be significantly increased in the dilated group compared to those in the nondilated group. The glycoprotein A-nuclear magnetic resonance (NMR) signal, a novel inflammation biomarker, was also observed to be increased in the dilated group. After performing multivariate analysis, remnant cholesterol remained an independent variable related to AAoD. In the long-term follow-up, proatherogenic lipoprotein parameters were related to ascending aorta dilatation velocity ascending. After a lineal regression analysis, non-HDL particles remained as an independent predictor of ascending aorta dilation velocity. Conclusions: Patients with BAV and AAoD presented a more pro-atherogenic profile assessed by 1H-NMR, especially related to triglyceride-rich lipoproteins. This pro-atherogenic profile seems to contribute to the higher growth rate of ascending aorta diameter. [ABSTRACT FROM AUTHOR]

Published

2023

34. ASGR1 Deficiency Inhibits Atherosclerosis in Western Diet-Fed ApoE -/- Mice by Regulating Lipoprotein Metabolism and Promoting Cholesterol Efflux.

Author

Zhang Y, Jiang X, Wang W, Lei L, Sheng R, Li S, Luo J, Liu H, Zhang J, Han X, Li Y, Zhang Y, Wang C, Si S, Jin ZG, and Xu Y

Subjects

Animals, Mice, Male, Mice, Knockout, Aortic Diseases pathology, Aortic Diseases prevention & control, Aortic Diseases genetics, Aortic Diseases metabolism, Plaque, Atherosclerotic, Aorta pathology, Aorta metabolism, ATP Binding Cassette Transporter, Subfamily G, Member 5 genetics, ATP Binding Cassette Transporter, Subfamily G, Member 5 metabolism, Macrophages metabolism, Signal Transduction, Apolipoproteins E genetics, Apolipoproteins E deficiency, Atherosclerosis genetics, Atherosclerosis metabolism, Atherosclerosis pathology, Atherosclerosis prevention & control, Diet, Western, Disease Models, Animal, Liver metabolism, Liver pathology, Cholesterol blood, Cholesterol metabolism, Mice, Inbred C57BL, Mice, Knockout, ApoE, Asialoglycoprotein Receptor metabolism, Asialoglycoprotein Receptor genetics

Abstract

Background: Atherosclerosis is the most common cause of cardiovascular diseases. Clinical studies indicate that loss-of-function ASGR1 (asialoglycoprotein receptor 1) is significantly associated with lower plasma cholesterol levels and reduces cardiovascular disease risk. However, the effect of ASGR1 on atherosclerosis remains incompletely understood; whether inhibition of ASGR1 causes liver injury remains controversial. Here, we comprehensively investigated the effects and the underlying molecular mechanisms of ASGR1 deficiency and overexpression on atherosclerosis and liver injury in mice., Methods: We engineered Asgr1 knockout mice ( Asgr1 -/- ), Asgr1 and ApoE double-knockout mice ( Asgr1 -/- ApoE -/- ), and ASGR1-overexpressing mice on an ApoE -/- background and then fed them different diets to assess the role of ASGR1 in atherosclerosis and liver injury., Results: After being fed a Western diet for 12 weeks, Asgr1 -/- ApoE -/- mice exhibited significantly decreased atherosclerotic lesion areas in the aorta and aortic root sections, reduced plasma VLDL (very-low-density lipoprotein) cholesterol and LDL (low-density lipoprotein) cholesterol levels, decreased VLDL production, and increased fecal cholesterol contents. Conversely, ASGR1 overexpression in ApoE -/- mice increased atherosclerotic lesions in the aorta and aortic root sections, augmented plasma VLDL cholesterol and LDL cholesterol levels and VLDL production, and decreased fecal cholesterol contents. Mechanistically, ASGR1 deficiency reduced VLDL production by inhibiting the expression of MTTP (microsomal triglyceride transfer protein) and ANGPTL3 (angiopoietin-like protein 3)/ANGPTL8 (angiopoietin-like protein 8) but increasing LPL (lipoprotein lipase) activity, increased LDL uptake by increasing LDLR (LDL receptor) expression, and promoted cholesterol efflux through increasing expression of LXRα (liver X receptor-α), ABCA1 (ATP-binding cassette subfamily A member 1), ABCG5 (ATP-binding cassette subfamily G member 5), and CYP7A1 (cytochrome P450 family 7 subfamily A member 1). These underlying alterations were confirmed in ASGR1-overexpressing ApoE -/- mice. In addition, ASGR1 deficiency exacerbates liver injury in Western diet-induced Asgr1 -/- ApoE -/- mice and high-fat diet-induced but not normal laboratory diet-induced and high-fat and high-cholesterol diet-induced Asgr1 -/- mice, while its overexpression mitigates liver injury in Western diet-induced ASGR1-overexpressing ApoE -/- mice., Conclusions: Inhibition of ASGR1 inhibits atherosclerosis in Western diet-fed ApoE -/- mice, suggesting that inhibiting ASGR1 may serve as a novel therapeutic strategy to treat atherosclerosis and cardiovascular diseases., Competing Interests: None.

Published

2024

35. Editorial: The role of dietary fatty acids in metabolic health.

Author

Bordoni, Laura, Zec, Manja, Naumovski, Nenad, and Sergi, Domenico

Subjects

FATTY acids, OMEGA-6 fatty acids, MOLECULAR biology, APOLIPOPROTEIN E, SATURATED fatty acids, FREE fatty acids, UNSATURATED fatty acids, ATHEROSCLEROSIS

Published

2023

36. Long-term fasting: Multi-system adaptations in humans (GENESIS) study–A single-arm interventional trial

Author

Franziska Grundler, Magalie Viallon, Robin Mesnage, Massimiliano Ruscica, Clemens von Schacky, Frank Madeo, Sebastian J. Hofer, Sarah J. Mitchell, Pierre Croisille, and Françoise Wilhelmi de Toledo

Subjects

organ size, lipoprotein metabolism, metabolomics, microbiome, long-term fasting, magnetic resonance imaging (MRI), Nutrition. Foods and food supply, TX341-641

Abstract

Fasting provokes fundamental changes in the activation of metabolic and signaling pathways leading to longer and healthier lifespans in animal models. Although the involvement of different metabolites in fueling human fasting metabolism is well known, the contribution of tissues and organs to their supply remains partly unclear. Also, changes in organ volume and composition remain relatively unexplored. Thus, processes involved in remodeling tissues during fasting and food reintroduction need to be better understood. Therefore, this study will apply state-of-the-art techniques to investigate the effects of long-term fasting (LF) and food reintroduction in humans by a multi-systemic approach focusing on changes in body composition, organ and tissue volume, lipid transport and storage, sources of protein utilization, blood metabolites, and gut microbiome profiles in a single cohort. This is a prospective, single-arm, monocentric trial. One hundred subjects will be recruited and undergo 9 ± 3 day-long fasting periods (250 kcal/day). We will assess changes in the composition of organs, bones and blood lipid profiles before and after fasting, as well as high-density lipoprotein (HDL) transport and storage, untargeted metabolomics of peripheral blood mononuclear cells (PBMCs), protein persulfidation and shotgun metagenomics of the gut microbiome. The first 32 subjects, fasting for 12 days, will be examined in more detail by magnetic resonance imaging (MRI) and spectroscopy to provide quantitative information on changes in organ volume and function, followed by an additional follow-up examination after 1 and 4 months. The study protocol was approved by the ethics board of the State Medical Chamber of Baden-Württemberg on 26.07.2021 and registered at ClinicalTrials.gov (NCT05031598). The results will be disseminated through peer-reviewed publications, international conferences and social media.Clinical trial registration[ClinicalTrials.gov], identifier [NCT05031598].

Published

2022

37. Anti-Hyperlipidemic Effect of Fucoidan Fractions Prepared from Iceland Brown Algae Ascophyllum nodosum in an Hyperlipidemic Mice Model

Author

Yunhai He, Yutong Li, Peili Shen, Shangkun Li, Linsong Zhang, Qiukuan Wang, Dandan Ren, Shu Liu, Demeng Zhang, and Hui Zhou

Subjects

Ascophyllum nodosum, fucoidan, anti-hyperlipidemic, antioxidant enzyme, lipoprotein metabolism, gut flora, Biology (General), QH301-705.5

Abstract

Ascophyllum nodosum, a brown algae abundantly found along the North Atlantic coast, is recognized for its high polysaccharide content. In this study, we investigated the anti-hyperlipidemic effect of fucoidans derived from A. nodosum, aiming to provide information for their potential application in anti-hyperlipidemic therapies and to explore comprehensive utilization of this Iceland brown seaweed. The crude fucoidan prepared from A. nodosum was separated using a diethylethanolamine column, resulting in two fucoidan fractions, AFC-1 and AFC-2. Both fractions were predominantly composed of fucose and xylose. AFC-1 exhibited a higher sulfate content of 27.8% compared to AFC-2 with 17.0%. AFC-2 was primarily sulfated at the hydroxy group of C2, whereas AFC-1 was sulfated at both the hydroxy groups of C2 and C4. To evaluate the anti-hyperlipidemic effect, a hyperlipidemia mouse model was established by feeding mice a high-fat diet. The effects of AFC-1, AFC-2, and the crude extract were investigated, with the drug atorvastatin used as a positive comparison. Among the different fucoidan fractions and doses, the high dose of AFC-2 administration demonstrated the most significant anti-hyperlipidemic effect across various aspects, including physiological parameters, blood glucose levels, lipid profile, histological analysis, and the activities of oxidative stress-related enzymes and lipoprotein-metabolism-related enzymes (p < 0.05 for the final body weight and p < 0.01 for the rest indicators, compared with the model group), and its effect is comparable to the atorvastatin administration. Furthermore, fucoidan administration resulted in a lower degree of loss in gut flora diversity compared to atorvastatin administration. These findings highlight the significant biomedical potential of fucoidans derived from A. nodosum as a promising therapeutic solution for hypolipidemia.

Published

2023

38. Cholesteryl Ester Transfer Protein and Lipid Metabolism and Cardiovascular Diseases

Author

Oliveira, Helena C. F., Raposo, Helena F., Crusio, Wim E., Series Editor, Dong, Haidong, Series Editor, Radeke, Heinfried H., Series Editor, Rezaei, Nima, Series Editor, and Jiang, Xian-Cheng, editor

Published

2020

39. Signs in Disorders of Lipid Metabolism and Obesity

Author

Manni, Andrea, Quarde, Akuffo, Manni, Andrea, and Quarde, Akuffo

Published

2020

40. Lipidomic Approaches to Study HDL Metabolism in Patients with Central Obesity Diagnosed with Metabolic Syndrome.

Author

Mocciaro, Gabriele, D'Amore, Simona, Jenkins, Benjamin, Kay, Richard, Murgia, Antonio, Herrera-Marcos, Luis Vicente, Neun, Stefanie, Sowton, Alice P., Hall, Zoe, Palma-Duran, Susana Alejandra, Palasciano, Giuseppe, Reimann, Frank, Murray, Andrew, Suppressa, Patrizia, Sabbà, Carlo, Moschetta, Antonio, Koulman, Albert, Griffin, Julian L., and Vacca, Michele

Subjects

*METABOLIC syndrome, *HDL cholesterol, *CHOLESTERYL ester transfer protein, *METABOLISM, *OBESITY, *FREE fatty acids, *LIPID metabolism

Abstract

The metabolic syndrome (MetS) is a cluster of cardiovascular risk factors characterised by central obesity, atherogenic dyslipidaemia, and changes in the circulating lipidome; the underlying mechanisms that lead to this lipid remodelling have only been partially elucidated. This study used an integrated "omics" approach (untargeted whole serum lipidomics, targeted proteomics, and lipoprotein lipidomics) to study lipoprotein remodelling and HDL composition in subjects with central obesity diagnosed with MetS (vs. controls). Compared with healthy subjects, MetS patients showed higher free fatty acids, diglycerides, phosphatidylcholines, and triglycerides, particularly those enriched in products of de novo lipogenesis. On the other hand, the "lysophosphatidylcholines to phosphatidylcholines" and "cholesteryl ester to free cholesterol" ratios were reduced, pointing to a lower activity of lecithin cholesterol acyltransferase (LCAT) in MetS; LCAT activity (directly measured and predicted by lipidomic ratios) was positively correlated with high-density lipoprotein cholesterol (HDL-C) and negatively correlated with body mass index (BMI) and insulin resistance. Moreover, many phosphatidylcholines and sphingomyelins were significantly lower in the HDL of MetS patients and strongly correlated with BMI and clinical metabolic parameters. These results suggest that MetS is associated with an impairment of phospholipid metabolism in HDL, partially led by LCAT, and associated with obesity and underlying insulin resistance. This study proposes a candidate strategy to use integrated "omics" approaches to gain mechanistic insights into lipoprotein remodelling, thus deepening the knowledge regarding the molecular basis of the association between MetS and atherosclerosis. [ABSTRACT FROM AUTHOR]

Published

2022

41. Fasting and postprandial plasma metabolite responses to a 12-wk dietary intervention in tissue-specific insulin resistance : a secondary analysis of the PERSonalized glucose Optimization through Nutritional intervention (PERSON) randomized trial

Author

Gijbels, Anouk, Jardon, Kelly M., Trouwborst, Inez, Manusama, Koen C.M., Goossens, Gijs H., Blaak, Ellen E., Feskens, Edith J.M., Afman, Lydia A., Gijbels, Anouk, Jardon, Kelly M., Trouwborst, Inez, Manusama, Koen C.M., Goossens, Gijs H., Blaak, Ellen E., Feskens, Edith J.M., and Afman, Lydia A.

Abstract

Background: We previously showed that dietary intervention effects on cardiometabolic health were driven by tissue-specific insulin resistance (IR) phenotype: individuals with predominant muscle IR (MIR) benefited more from a low-fat, high-protein, and high-fiber (LFHP) diet, whereas individuals with predominant liver insulin resistance (LIR) benefited more from a high-monounsaturated fatty acid (HMUFA) diet. Objectives: To further characterize the effects of LFHP and HMUFA diets and their interaction with tissue-specific IR, we investigated dietary intervention effects on fasting and postprandial plasma metabolite profile. Methods: Adults with MIR or LIR (40–75 y, BMI 25–40 kg/m2) were randomly assigned to a 12-wk HMUFA or LFHP diet (n = 242). After the exclusion of statin use, 214 participants were included in this prespecified secondary analysis. Plasma samples were collected before (T = 0) and after (T = 30, 60, 120, and 240 min) a high-fat mixed meal for quantification of 247 metabolite measures using nuclear magnetic resonance spectroscopy. Results: A larger reduction in fasting VLDL-triacylglycerol (TAG) and VLDL particle size was observed in individuals with MIR following the LFHP diet and those with LIR following the HMUFA diet, although no longer statistically significant after false discovery rate (FDR) adjustment. No IR phenotype-by-diet interactions were found for postprandial plasma metabolites assessed as total area under the curve (tAUC). Irrespective of IR phenotype, the LFHP diet induced greater reductions in postprandial plasma tAUC of the larger VLDL particles and small HDL particles, and TAG content in most VLDL subclasses and the smaller LDL and HDL subclasses (for example, VLDL-TAG tAUC standardized mean change [95% CI] LFHP = −0.29 [−0.43, −0.16] compared with HMUFA = −0.04 [−0.16, 0.09]; FDR-adjusted P for diet × time = 0.041). Conclusions: Diet effects on plasma metabolite profiles were more pronounced than phenotype-by-diet interactions. A

Published

2024

42. Applications and Limitations of Mouse Models for Understanding Human Atherosclerosis

Author

von Scheidt, Moritz, Zhao, Yuqi, Kurt, Zeyneb, Pan, Calvin, Zeng, Lingyao, Yang, Xia, Schunkert, Heribert, and Lusis, Aldons J

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Genetics, Aging, Heart Disease - Coronary Heart Disease, Prevention, Heart Disease, Atherosclerosis, Cardiovascular, Human Genome, 2.1 Biological and endogenous factors, Animals, Disease Models, Animal, Genetic Variation, Genome-Wide Association Study, Humans, Mice, Risk Factors, Signal Transduction, CAD risk factors, common and complex disease, diabetes, engineered mouse models, genome-wide association studies, lesions analysis, lipoprotein metabolism, mouse atherosclerosis genes, passenger genes, pathway modeling, Biochemistry and Cell Biology, Medical Biochemistry and Metabolomics, Endocrinology & Metabolism, Biochemistry and cell biology, Medical biochemistry and metabolomics

Abstract

Most of the biological understanding of mechanisms underlying coronary artery disease (CAD) derives from studies of mouse models. The identification of multiple CAD loci and strong candidate genes in large human genome-wide association studies (GWASs) presented an opportunity to examine the relevance of mouse models for the human disease. We comprehensively reviewed the mouse literature, including 827 literature-derived genes, and compared it to human data. First, we observed striking concordance of risk factors for atherosclerosis in mice and humans. Second, there was highly significant overlap of mouse genes with human genes identified by GWASs. In particular, of the 46 genes with strong association signals in CAD GWASs that were studied in mouse models, all but one exhibited consistent effects on atherosclerosis-related phenotypes. Third, we compared 178 CAD-associated pathways derived from human GWASs with 263 from mouse studies and observed that the majority were consistent between the species.

Published

2017

43. Insights into the Tunnel Mechanism of Cholesteryl Ester Transfer Protein through All-atom Molecular Dynamics Simulations*

Author

Lei, Dongsheng, Rames, Matthew, Zhang, Xing, Zhang, Lei, Zhang, Shengli, and Ren, Gang

Subjects

Chemical Sciences, Theoretical and Computational Chemistry, Atherosclerosis, Bioengineering, Cardiovascular, Cholesterol Ester Transfer Proteins, Cholesterol Esters, Humans, Microscopy, Electron, Molecular Dynamics Simulation, Protein Conformation, cholesterol, cholesterol metabolism, cholesterol regulation, cholesterol-binding protein, lipid metabolism, lipid transport, lipid-protein interaction, lipoprotein metabolism, molecular dynamics, Biological Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology, Biological sciences, Biomedical and clinical sciences, Chemical sciences

Abstract

Cholesteryl ester transfer protein (CETP) mediates cholesteryl ester (CE) transfer from the atheroprotective high density lipoprotein (HDL) cholesterol to the atherogenic low density lipoprotein cholesterol. In the past decade, this property has driven the development of CETP inhibitors, which have been evaluated in large scale clinical trials for treating cardiovascular diseases. Despite the pharmacological interest, little is known about the fundamental mechanism of CETP in CE transfer. Recent electron microscopy (EM) experiments have suggested a tunnel mechanism, and molecular dynamics simulations have shown that the flexible N-terminal distal end of CETP penetrates into the HDL surface and takes up a CE molecule through an open pore. However, it is not known whether a CE molecule can completely transfer through an entire CETP molecule. Here, we used all-atom molecular dynamics simulations to evaluate this possibility. The results showed that a hydrophobic tunnel inside CETP is sufficient to allow a CE molecule to completely transfer through the entire CETP within a predicted transfer time and at a rate comparable with those obtained through physiological measurements. Analyses of the detailed interactions revealed several residues that might be critical for CETP function, which may provide important clues for the effective development of CETP inhibitors and treatment of cardiovascular diseases.

Published

2016

44. Insights into the Tunnel Mechanism of Cholesteryl Ester Transfer Protein through All-atom Molecular Dynamics Simulations

Author

Ren, Gang [Lawrence Berkeley National Lab. (LBNL), Berkeley, CA (United States)]

Published

2016

45. Esterification of 4β-hydroxycholesterol and other oxysterols in human plasma occurs independently of LCAT

Author

Daisuke Yamamuro, Hisataka Yamazaki, Jun-ichi Osuga, Kenta Okada, Tetsuji Wakabayashi, Akihito Takei, Shoko Takei, Manabu Takahashi, Shuichi Nagashima, Adriaan G. Holleboom, Masayuki Kuroda, Hideaki Bujo, and Shun Ishibashi

Subjects

cholesterol/acyltransferase, inborn error of metabolism, lipoprotein metabolism, oxidized lipids, enzyme, liquid chromatography, Biochemistry, QD415-436

Abstract

The acyltransferase LCAT mediates FA esterification of plasma cholesterol. In vitro studies have shown that LCAT also FA-esterifies several oxysterols, but in vivo evidence is lacking. Here, we measured both free and FA-esterified forms of sterols in 206 healthy volunteers and 8 individuals with genetic LCAT deficiency, including familial LCAT deficiency (FLD) and fish-eye disease (FED). In the healthy volunteers, the mean values of the ester-to-total molar ratios of the following sterols varied: 4β-hydroxycholesterol (4βHC), 0.38; 5,6α-epoxycholesterol (5,6αEC), 0.46; 5,6β-epoxycholesterol (5,6βEC), 0.51; cholesterol, 0.70; cholestane-3β,5α,6β-triol (CT), 0.70; 7-ketocholesterol (7KC), 0.75; 24S-hydroxycholesterol (24SHC), 0.80; 25-hydroxycholesterol (25HC), 0.81; 27-hydroxycholesterol (27HC), 0.86; and 7α-hydroxycholesterol (7αHC), 0.89. In the individuals with LCAT deficiency, the plasma levels of the FA-esterified forms of cholesterol, 5,6αEC, 5,6βEC, CT, 7αHC, 7KC, 24SHC, 25HC, and 27HC, were significantly lower than those in the healthy volunteers. The individuals with FLD had significantly lower FA-esterified forms of 7αHC, 24SHC, and 27HC than those with FED. It is of note that, even in the three FLD individuals with negligible plasma cholesteryl ester, substantial amounts of the FA-esterified forms of 4βHC, 5,6αEC, 7αHC, 7KC, and 27HC were present. We conclude that LCAT has a major role in the FA esterification of many plasma oxysterols but contributes little to the FA esterification of 4βHC. Substantial FA esterification of 4βHC, 5,6αEC, 7αHC, 7KC, and 27HC is independent of LCAT.

Published

2020

46. Aging and plasma triglyceride metabolism

Author

Kathryn M. Spitler and Brandon S.J. Davies

Subjects

lipolysis, lipoprotein metabolism, lipoprotein lipase, adipose tissue, chylomicrons, inflammation, Biochemistry, QD415-436

Abstract

The risk for metabolic disease, including metabolic syndrome, insulin resistance, and diabetes, increases with age. Altered plasma TG metabolism and changes in fatty acid partitioning are also major contributors to metabolic disease. Plasma TG metabolism itself is altered by age in humans and rodents. As discussed in this review, the age-induced changes in human TG metabolism include increased plasma TG levels, reduced postprandial plasma TG clearance rates, reduced postheparin LPL activity, decreased adipose tissue lipolysis, and elevated ectopic fat deposition, all of which could potentially contribute to age-associated metabolic diseases. Similar observations have been made in aged rats. We highlight the limitations of currently available data and propose that mechanistic studies are needed to understand the extent to which age-induced alterations in TG metabolism contribute to metabolic disease. Such mechanistic insights could aid in therapeutic strategies for preventing or managing metabolic disease in older individuals.

Published

2020

47. A high-throughput mass spectrometry-based assay for large-scale profiling of circulating human apolipoproteins[S]

Author

Valentin Blanchard, Damien Garçon, Catherine Jaunet, Kevin Chemello, Stéphanie Billon-Crossouard, Audrey Aguesse, Aya Garfa, Gilles Famchon, Amada Torres, Cédric Le May, Matthieu Pichelin, Edith Bigot-Corbel, Gilles Lambert, Bertrand Cariou, Samy Hadjadj, Michel Krempf, Kalyane Bach-Ngohou, and Mikaël Croyal

Subjects

proteomics, lipoprotein metabolism, metabolic disease, assay development, isotopic labeling, lipid metabolism, Biochemistry, QD415-436

Abstract

Apolipoproteins govern lipoprotein metabolism and are promising biomarkers of metabolic and cardiovascular diseases. Unlike immunoassays, MS enables the quantification and phenotyping of multiple apolipoproteins. Hence, here, we aimed to develop a LC-MS/MS assay that can simultaneously quantitate 18 human apolipoproteins [A-I, A-II, A-IV, A-V, B48, B100, C-I, C-II, C-III, C-IV, D, E, F, H, J, L1, M, and (a)] and determined apoE, apoL1, and apo(a) phenotypes in human plasma and serum samples. The plasma and serum apolipoproteins were trypsin digested through an optimized procedure and peptides were extracted and analyzed by LC-MS/MS. The method was validated according to standard guidelines in samples spiked with known peptide amounts. The LC-MS/MS results were compared with those obtained with other techniques, and reproducibility, dilution effects, and stabilities were also assessed. Peptide markers were successfully selected for targeted apolipoprotein quantification and phenotyping. After optimization, the assay was validated for linearity, lower limits of quantification, accuracy (biases: –14.8% to 12.1%), intra-assay variability [coefficients of variation (CVs): 1.5–14.2%], and inter-assay repeatability (CVs: 4.1–14.3%). Bland-Altman plots indicated no major statistically significant differences between LC-MS/MS and other techniques. The LC-MS/MS results were reproducible over five repeated experiments (CVs: 1.8–13.7%), and we identified marked differences among the plasma and serum samples. The LC-MS/MS assay developed here is rapid, requires only small sampling volumes, and incurs reasonable costs, thus making it amenable for a wide range of studies of apolipoprotein metabolism. We also highlight how this assay can be implemented in laboratories.

Published

2020

48. A novel NanoBiT-based assay monitors the interaction between lipoprotein lipase and GPIHBP1 in real time[S]

Author

Shwetha K. Shetty, Rosemary L. Walzem, and Brandon S.J. Davies

Subjects

triglyceride, lipolysis, lipoprotein metabolism, chylomicrons, endothelial cell, glycosylphosphatidylinositol-anchored high density lipoprotein binding protein 1, Biochemistry, QD415-436

Abstract

The hydrolysis of triglycerides in triglyceride-rich lipoproteins by LPL is critical for the delivery of triglyceride-derived fatty acids to tissues, including heart, skeletal muscle, and adipose tissues. Physiologically active LPL is normally bound to the endothelial cell protein glycosylphosphatidylinositol-anchored high-density lipoprotein binding protein 1 (GPIHBP1), which transports LPL across endothelial cells, anchors LPL to the vascular wall, and stabilizes LPL activity. Disruption of LPL-GPIHBP1 binding significantly alters triglyceride metabolism and lipid partitioning. In this study, we modified the NanoLuc® Binary Technology split-luciferase system to develop a novel assay that monitors the binding of LPL to GPIHBP1 on endothelial cells in real time. We validated the specificity and sensitivity of the assay using endothelial lipase and a mutant version of LPL and found that this assay reliably and specifically detected the interaction between LPL and GPIHBP1. We then interrogated various endogenous and exogenous inhibitors of LPL-mediated lipolysis for their ability to disrupt the binding of LPL to GPIHBP1. We found that angiopoietin-like (ANGPTL)4 and ANGPTL3-ANGPTL8 complexes disrupted the interactions of LPL and GPIHBP1, whereas the exogenous LPL blockers we tested (tyloxapol, poloxamer-407, and tetrahydrolipstatin) did not. We also found that chylomicrons could dissociate LPL from GPIHBP1 and found evidence that this dissociation was mediated in part by the fatty acids produced by lipolysis. These results demonstrate the ability of this assay to monitor LPL-GPIHBP1 binding and to probe how various agents influence this important complex.

Published

2020

49. Lipoprotein(a) and cardiovascular disease.

Author

Boffa MB and Koschinsky ML

Subjects

Humans, Animals, Atherosclerosis metabolism, Atherosclerosis blood, Lipoprotein(a) blood, Lipoprotein(a) metabolism, Cardiovascular Diseases metabolism, Cardiovascular Diseases blood

Abstract

Elevated plasma levels of lipoprotein(a) (Lp(a)) are a prevalent, independent, and causal risk factor for atherosclerotic cardiovascular disease and calcific aortic valve disease. Lp(a) consists of a lipoprotein particle resembling low density lipoprotein and the covalently-attached glycoprotein apolipoprotein(a) (apo(a)). Novel therapeutics that specifically and potently lower Lp(a) levels are currently in advanced stages of clinical development, including in large, phase 3 cardiovascular outcomes trials. However, fundamental unanswered questions remain concerning some key aspects of Lp(a) biosynthesis and catabolism as well as the true pathogenic mechanisms of the particle. In this review, we describe the salient biochemical features of Lp(a) and apo(a) and how they underlie the disease-causing potential of Lp(a), the factors that determine plasma Lp(a) concentrations, and the mechanism of action of Lp(a)-lowering drugs., (© 2024 The Author(s).)

Published

2024

50. Functioning of Organosulfur Compounds from Garlic (Allium sativum Linn) in Targeting Risk Factor-Mediated Atherosclerosis: A Cross Talk Between Alternative and Modern Medicine

Author

Ahmad, Parvej, Alvi, Sahir Sultan, Khan, M. Salman, Akhtar, Mohd Sayeed, editor, Swamy, Mallappa Kumara, editor, and Sinniah, Uma Rani, editor

Published

2019