Your search keyword '"Princen, Hans M. G."' showing total 199 results

51. No Effect of Consumption of Green and Black Tea on Plasma Lipid and Antioxidant Levels and on LDL Oxidation in Smokers

Author

Princen, Hans M. G., primary, van Duyvenvoorde, Wim, additional, Buytenhek, Rien, additional, Blonk, Cor, additional, Tijburg, Lilian B. M., additional, Langius, Jacqueline A. E., additional, Meinders, A. Edo, additional, and Pijl, Hanno, additional

Published

1998

52. LDL Oxidation and Extent of Coronary Atherosclerosis

Author

van de Vijver, Lucy P. L., primary, Kardinaal, Alwine F. M., additional, van Duyvenvoorde, Wim, additional, Kruijssen, Dick A. C. M., additional, Grobbee, Diederick E., additional, van Poppel, Geert, additional, and Princen, Hans M. G., additional

Published

1998

53. Cafestol, the Cholesterol-Raising Factor in Boiled Coffee, Suppresses Bile Acid Synthesis by Downregulation of Cholesterol 7α-Hydroxylase and Sterol 27-Hydroxylase in Rat Hepatocytes

Author

Post, Sabine M., primary, de Wit, Elly C. M., additional, and Princen., Hans M. G., additional

Published

1997

54. Effects of Gemfibrozil and Ciprofibrate on Plasma Levels of Tissue-type Plasminogen Activator, Plasminogen Activator Inhibitor-1 and Fibrinogen in Hyperlipidaemic Patients

Author

Kockx, Maaike, additional, de Maat, Moniek P M, additional, Knipscheer, Haye C, additional, Kastelein, John J P, additional, Kluft, Cornelis, additional, Princen, Hans M G, additional, and Kooistra, Teake, additional

Published

1997

55. Structural Aspects of Bile Acids Involved in the Regulation of Cholesterol 7alpha-Hydroxylase and Sterol 27-Hydroxylase

Author

Twisk, Jaap, primary, Hoekman, Marco F. M., additional, Muller, Linda M., additional, Iida, Takashi, additional, Tamaru, Tamaaki, additional, Ijzerman, Ad, additional, Mager, Willem H., additional, and Princen, Hans M. G., additional

Published

1995

56. Bile acids exert negative feedback control on bile acid synthesis in cultured pig hepatocytes by suppression of cholesterol 7α-hydroxylase activity

Author

Kwekkeboom, Jaap, primary, Princen, Hans M. G., additional, van Voorthuizen, Eline M., additional, and Kempen, Herman Jan M., additional

Published

1990

57. CYP7A1 A-278C polymorphism affects the response of plasma lipids after dietary cholesterol or cafestol interventions in humans.

Author

Hofman, Maaike K., Weggemans, Rianne M., Zock, Peter L., Schouten, Evert G., Katan, Martijn B., and Princen, Hans M. G.

Subjects

BLOOD lipids, BLOOD cholesterol, GENETIC polymorphisms, NUTRITION, HIGH density lipoproteins, BLOOD lipoproteins, ALLELES, CHOLESTEROL, CLINICAL trials, COMPARATIVE studies, DOSE-effect relationship in pharmacology, CHOLESTEROL content of food, GENES, HETEROCYCLIC compounds, HYDROCARBONS, LIPIDS, RESEARCH methodology, MEDICAL cooperation, META-analysis, OXIDOREDUCTASES, PURINES, RESEARCH, EVALUATION research, GENOTYPES

Abstract

The response of plasma lipids to dietary cholesterol and fat varies among individuals. Variations in genes involved in cholesterol metabolism can be important in these interindividual differences. The rate-limiting enzyme in the conversion of cholesterol into bile acids is cholesterol 7alpha-hydroxylase (CYP7A1). We investigated the effect of the A278-C promoter polymorphism in the CYP7A1 gene on responses of plasma lipids to an increased intake in dietary cholesterol (742 +/- 114 mg/d), cafestol (57 +/- 6 mg/d), saturated fat [change of 8-9 energy percent/d (en%/d)] and trans fat (change of 10-11 en%/d) in 496 normolipidemic subjects. These responses were measured in 26 previously published dietary trials. After adjustment for the apolipoprotein E genotype effect, AA-subjects consuming a cholesterol-rich diet had a smaller increase in plasma HDL cholesterol than CC-subjects (0.00 +/- 0.02 vs. 0.17 +/- 0.04 mmol/L; P < 0.001). Upon intake of cafestol, AA-subjects had a smaller increase in plasma total cholesterol than CC-subjects (0.69 +/- 0.10 vs. 1.01 +/- 0.10 mmol/L; P = 0.028). No effects of the polymorphism were found in the saturated and trans fat interventions. In conclusion, the CYP7A1 polymorphism has a small but significant effect on the increase in plasma HDL cholesterol and plasma total cholesterol after an increased intake of dietary cholesterol and cafestol, respectively. [ABSTRACT FROM AUTHOR]

Published

2004

58. Acyl-coenzyme A: Cholesterol acyltransferase inhibitor, avasimibe, stimulates bile acid synthesis and cholesterol 7α-hydroxylase in cultured rat hepatocytes and in vivo in the rat.

Author

Post, Sabine M., Zoeteweij, J. Paul, Bos, Mettine H., de Wit, Elly C., Havinga, Rick, Kuipers, Folkert, and Princen, Hans M. G.

Published

1999

59. Insulin suppresses bile acid synthesis in cultured rat hepatocytes by down-regulation of cholesterol 7α-hydroxylase and sterol 27-hydroxylase gene transcription.

Author

Twisk, Jaap, Hoekman, Marco F. M., Lehmann, Eline M., Meijer, Piet, Mager, Willem H., and Princen, Hans M. G.

Published

1995

60. Regulation of low density lipoprotein receptor activity in primary cultures of human hepatocytes by serum lipoproteins.

Author

Havekes, Louis M., Verboom, Hans, de Wit, Elly, Yap, Sing Hiem, and Princen, Hans M. G.

Published

1986

61. CETP does not affect triglyceride production or clearance in APOE*3-Leiden mice

Author

Bijland, Silvia, van den Berg, Sjoerd A. A., Voshol, Peter J., van den Hoek, Anita M., Princen, Hans M. G., Havekes, Louis M., Rensen, Patrick C. N., and Willems van Dijk, Ko

Abstract

The cholesteryl ester transfer protein (CETP) facilitates the bidirectional transfer of cholesteryl esters and triglycerides (TG) between HDL and (V)LDL. By shifting cholesterol in plasma from HDL to (V)LDL in exchange for VLDL-TG, CETP aggravates atherosclerosis in hyperlipidemic APOE*3-Leiden (E3L) mice. The aim of this study was to investigate the role of CETP in TG metabolism and high-fat diet-induced obesity by using E3L mice with and without the expression of the human CETP gene. On chow, plasma lipid levels were comparable between both male and female E3L and E3L.CETP mice. Further mechanistic studies were performed using male mice. CETP expression increased the level of TG in HDL. CETP did not affect the postprandial plasma TG response or the hepatic VLDL-TG and VLDL-apolipoprotein B production rate. Moreover, CETP did not affect the plasma TG clearance rate or organ-specific TG uptake after infusion of VLDL-like emulsion particles. In line with the absence of an effect of CETP on tissue-specific TG uptake, CETP also did not affect weight gain in response to a high-fat diet. In conclusion, the CETP-induced increase of TG in the HDL fraction of E3L mice is not associated with changes in the production of TG or with tissue-specific clearance of TG from the plasma.

Published

2010

62. Fenofibrate increases HDL-cholesterol by reducing cholesteryl ester transfer protein expression

Author

van der Hoogt, Caroline C., de Haan, Willeke, Westerterp, Marit, Hoekstra, Menno, Dallinga-Thie, Geesje M., Romijn, Johannes A., Princen, Hans M. G., Jukema, J. Wouter, Havekes, Louis M., and Rensen, Patrick C. N.

Abstract

In addition to efficiently decreasing VLDL-triglycerides (TGs), fenofibrate increases HDL-cholesterol levels in humans. We investigated whether the fenofibrate-induced increase in HDL-cholesterol is dependent on the expression of the cholesteryl ester transfer protein (CETP). To this end, APOE*3-Leiden (E3L) transgenic mice without and with the human CETP transgene, under the control of its natural regulatory flanking regions, were fed a Western-type diet with or without fenofibrate. Fenofibrate (0.04% in the diet) decreased plasma TG in E3L and E3L.CETP mice (–59% and –60%; P < 0.001), caused by a strong reduction in VLDL. Whereas fenofibrate did not affect HDL-cholesterol in E3L mice, fenofibrate dose-dependently increased HDL-cholesterol in E3L.CETP mice (up to +91%). Fenofibrate did not affect the turnover of HDL-cholesteryl ester (CE), indicating that fenofibrate causes a higher steady-state HDL-cholesterol level without altering the HDL-cholesterol flux through plasma. Analysis of the hepatic gene expression profile showed that fenofibrate did not differentially affect the main players in HDL metabolism in E3L.CETP mice compared with E3L mice. However, in E3L.CETP mice, fenofibrate reduced hepatic CETP mRNA (–72%; P < 0.01) as well as the CE transfer activity in plasma (–73%; P < 0.01). We conclude that fenofibrate increases HDL-cholesterol by reducing the CETP-dependent transfer of cholesterol from HDL to (V)LDL, as related to lower hepatic CETP expression and a reduced plasma (V)LDL pool.

Published

2007

63. Differential Effects of Amlodipine and Atorvastatin Treatment and Their Combination on Atherosclerosis in ApoE3Leiden Transgenic Mice

Author

Delsing, Dianne J. M., Jukema, Wouter J., Wiel, Mark A. van de, Emeis, Jef J., van der Laarse, Arnoud, Havekes, Louis M., and Princen, Hans M. G.

Abstract

This study was designed to investigate the potential antiatherosclerotic effects of the calcium antagonist amlodipine as compared with the HMGCoA reductase inhibitor atorvastatin and the combination of both in ApoE3Leiden transgenic mice. Four groups of 15 ApoE3Leiden mice were put on a highcholesterol diet. One group received 0.002 wtwt amlodipine in the diet, which had no effect on plasma cholesterol levels. Another group received 0.01 wtwt atorvastatin, resulting in a decrease of plasma cholesterol by 50 by a reduction in very low density lipoprotein production. The combination group received both amlodipine and atorvastatin. After 28 weeks, atherosclerosis in the aortic root was quantified. Treatment with amlodipine had no significant effect on atherosclerotic lesion area, whereas atorvastatin markedly reduced atherosclerosis by 77 compared with the control group. Atorvastatin also reduced inflammation markers. The combination of amlodipine and atorvastatin tended to reduce lesion area by 61 compared with the atorvastatinonly group however, this effect did not reach statistical significance. Amlodipine treatment significantly reduced calcification in the lesions, whereas atorvastatin alone had no effect. The combination of amlodipine and atorvastatin resulted in a near absence of calcium deposits in the lesions. This study demonstrates that amlodipine treatment alone does not significantly reduce atherosclerotic lesion development. Atorvastatin was shown to have strong antiatherosclerotic effects, and cotreatment with amlodipine may potentiate the antiatherosclerotic effect of atorvastatin.

Published

2003

64. Regulation of cholesterol metabolism in the liver in vivo and in vitro

Author

COHEN, LOUIS H., primary, PRINCEN, HANS M. G., additional, KWEKKEBOOM, JAAP, additional, HAVEKES, LOUS M., additional, and KEMPEN, JAN HERMAN, additional

Published

1987

65. Fenofibrate Increases Very Low Density Lipoprotein Triglyceride Production Despite Reducing Plasma Triglyceride Levels in APOE*3-Leiden.CETP Mice.

Author

Bijland, Silvia, Pieterman, Elsbet J., Maas, Annemarie C. E., Van der Hoorn, José W. A., Van Erk, Marjan J., Van Klinken, Jan B., Havekes, Louis M., Van Dijk, Ko Willems, Princen, Hans M. G., and Rensen, Patrick C. N.

Subjects

*PEROXISOMES, *LOW density lipoproteins, *LABORATORY mice, *FENOFIBRATE, *TRIGLYCERIDES

Abstract

The peroxisome proliferator-activated receptor alpha (PPARα) activator fenofibrate efficiently decreases plasma triglycerides (TG), which is generally attributed to enhanced very low density lipoprotein (VLDL)-TG clearance and decreased VLDL-TG production. However, because data on the effect of fenofibrate on VLDL production are controversial, we aimed to investigate in (more) detail the mechanism underlying the TG-lowering effect by studying VLDL-TG production and clearance using APOE*3-Leiden.CETP mice, a unique mouse model for human-like lipoprotein metabolism. Male mice were fed a Western-type diet for 4 weeks, followed by the same diet without or with fenofibrate (30 mg/kg bodyweight/day) for 4 weeks. Fenofibrate strongly lowered plasma cholesterol (-38%) and TG (-60%) caused by reduction of VLDL. Fenofibrate markedly accelerated VLDL-TG clearance, as judged from a reduced plasma half-life of glycerol tri[³H]oleate-labeled VLDL-like emulsion particles (-68%). This was associated with an increased post-heparin lipoprotein lipase (LPL) activity (+110%) and an increased uptake of VLDL-derived fatty acids by skeletal muscle, white adipose tissue, and liver. Concomitantly, fenofibrate markedly increased the VLDL-TG production rate (+73%) but not the VLDL-apolipoprotein B (apoB) production rate. Kinetic studies using [³H] palmitic acid showed that fenofibrate increased VLDL-TG production by equally increasing incorporation of re-esterified plasma fatty acids and liver TG into VLDL, which was supported by hepatic gene expression profiling data. We conclude that fenofibrate decreases plasma TG by enhancing LPL-mediated VLDL-TG clearance, which results in a compensatory increase in VLDL-TG production by the liver. ] [ABSTRACT FROM AUTHOR]

Published

2010

66. Anacetrapib reduces progression of atherosclerosis, mainly by reducing non-HDL-cholesterol, improves lesion stability and adds to the beneficial effects of atorvastatin

Author

Elsbet J. Pieterman, Ko Willems van Dijk, Sam van der Tuin, Susan Kühnast, Jan B. van Klinken, Thomas F. Lüscher, Louis M. Havekes, Patrick C.N. Rensen, J. Wouter Jukema, Branko Simic, Ulf Landmesser, José W.A. van der Hoorn, Hans M.G. Princen, University of Zurich, and Princen, Hans M G

Subjects

Mouse, Atorvastatin, Apolipoprotein E3, Biomedical Innovation, Pharmacology, Efficacy, In vivo study, chemistry.chemical_compound, Basic Science, Life, Anacetrapib, Enzyme activity, High density lipoprotein cholesterol, Atherosclerotic plaque, biology, Anticholesteremic Agents, Cholesteryl ester transfer protein, HDL-cholesterol, Drug Combinations, Cholesterol blood level, Disease Progression, 10209 Clinic for Cardiology, Aorta atherosclerosis, Female, lipids (amino acids, peptides, and proteins), medicine.symptom, Animal cell, MHR - Metabolic Health Research, Cardiology and Cardiovascular Medicine, Healthy Living, medicine.drug, HDL function, Dose, Drug potentiation, Mice, Transgenic, 610 Medicine & health, Non-HDL-cholesterol, 2705 Cardiology and Cardiovascular Medicine, Treatment duration, Lesion, Cholesterylester transfer protein, medicine, Animals, Pyrroles, Animal model, Biology, Disease severity, CETP inhibitor, Oxazolidinones, Serum Amyloid A Protein, Cholesterol, business.industry, Cholesterol, HDL, nutritional and metabolic diseases, Nonhuman, Atherosclerosis, Cholesterol Ester Transfer Proteins, Diet, Drug efficacy, chemistry, Heptanoic Acids, Analysis of covariance, Risk reduction, biology.protein, ELSS - Earth, Life and Social Sciences, business, Controlled study, Aorta root

Abstract

The present study is the first intervention study in a well-established, translational mouse model for hyperlipidaemia and atherosclerosis showing that anacetrapib dose-dependently reduces atherosclerosis development and adds to the anti-atherogenic effects of atorvastatin. This effect is mainly ascribed to the reduction in non-HDL-C despite a remarkable increase in HDL-C and without affecting HDL functionality. In addition, anacetrapib improves lesion stability., Background The residual risk that remains after statin treatment supports the addition of other LDL-C-lowering agents and has stimulated the search for secondary treatment targets. Epidemiological studies propose HDL-C as a possible candidate. Cholesteryl ester transfer protein (CETP) transfers cholesteryl esters from atheroprotective HDL to atherogenic (V)LDL. The CETP inhibitor anacetrapib decreases (V)LDL-C by ∼15–40% and increases HDL-C by ∼40–140% in clinical trials. We evaluated the effects of a broad dose range of anacetrapib on atherosclerosis and HDL function, and examined possible additive/synergistic effects of anacetrapib on top of atorvastatin in APOE*3Leiden.CETP mice. Methods and results Mice were fed a diet without or with ascending dosages of anacetrapib (0.03; 0.3; 3; 30 mg/kg/day), atorvastatin (2.4 mg/kg/day) alone or in combination with anacetrapib (0.3 mg/kg/day) for 21 weeks. Anacetrapib dose-dependently reduced CETP activity (−59 to −100%, P < 0.001), thereby decreasing non-HDL-C (−24 to −45%, P < 0.001) and increasing HDL-C (+30 to +86%, P < 0.001). Anacetrapib dose-dependently reduced the atherosclerotic lesion area (−41 to −92%, P < 0.01) and severity, increased plaque stability index and added to the effects of atorvastatin by further decreasing lesion size (−95%, P < 0.001) and severity. Analysis of covariance showed that both anacetrapib (P < 0.05) and non-HDL-C (P < 0.001), but not HDL-C (P = 0.76), independently determined lesion size. Conclusion Anacetrapib dose-dependently reduces atherosclerosis, and adds to the anti-atherogenic effects of atorvastatin, which is mainly ascribed to a reduction in non-HDL-C. In addition, anacetrapib improves lesion stability.

Published

2015

67. A Novel, Orally Bioavailable, Small-Molecule Inhibitor of PCSK9 With Significant Cholesterol-Lowering Properties In Vivo.

Author

Suchowerska AK, Stokman G, Palmer JT, Coghlan PA, Pieterman EJ, Keijzer N, Lambert G, Chemello K, Jaafar AK, Parmar J, Yan L, Tong Y, Mu L, Princen HMG, Bonnar J, and Evison BJ

Subjects

Animals, Humans, Mice, Apolipoproteins E, Cholesterol, Cholesterol, LDL, Receptors, LDL genetics, Receptors, LDL metabolism, PCSK9 Inhibitors pharmacology, Hyperlipidemias drug therapy, Anticholesteremic Agents pharmacology

Abstract

Proprotein convertase subtilisin kexin type 9 (PCSK9) inhibits the clearance of low-density lipoprotein (LDL) cholesterol (LDL-C) from plasma by directly binding with the LDL receptor (LDLR) and sending the receptor for lysosomal degradation. As the interaction promotes elevated plasma LDL-C levels, and therefore a predisposition to cardiovascular disease, PCSK9 has attracted intense interest as a therapeutic target. Despite this interest, an orally bioavailable small-molecule inhibitor of PCSK9 with extensive lipid-lowering activity is yet to enter the clinic. We report herein the discovery of NYX-PCSK9i, an orally bioavailable small-molecule inhibitor of PCSK9 with significant cholesterol-lowering activity in hyperlipidemic APOE∗3-Leiden.CETP mice. NYX-PCSK9i emerged from a medicinal chemistry campaign demonstrating potent disruption of the PCSK9-LDLR interaction in vitro and functional protection of the LDLR of human lymphocytes from PCSK9-directed degradation ex vivo. APOE∗3-Leiden.CETP mice orally treated with NYX-PCSK9i demonstrated a dose-dependent decrease in plasma total cholesterol of up to 57%, while its combination with atorvastatin additively suppressed plasma total cholesterol levels. Importantly, the majority of cholesterol lowering by NYX-PCSK9i was in non-HDL fractions. A concomitant increase in total plasma PCSK9 levels and significant increase in hepatic LDLR protein expression strongly indicated on-target function by NYX-PCSK9i. Determinations of hepatic lipid and fecal cholesterol content demonstrated depletion of liver cholesteryl esters and promotion of fecal cholesterol elimination with NYX-PCSK9i treatment. All measured in vivo biomarkers of health indicate that NYX-PCSK9i has a good safety profile. NYX-PCSK9i is a potential new therapy for hypercholesterolemia with the capacity to further enhance the lipid-lowering activities of statins., Competing Interests: Conflict of Interest A. K. S., J. P., J. B., and B. J. E. are employees of Nyrada Inc. J. T. P. and G. L. are members of the Scientific Advisory Board of Nyrada Inc. J. T. P., G. L., J. B., and B. J. E. have share/stock options in Nyrada Inc. A. K. S., P. A. C., J. T. P., J. B., and B. J. E. are listed as inventors on the patent that discloses NYX-PCSK9i and related compounds. G. S., P. A. C., E. J. P., N. K., G. L., K. C., A. K. J., and H. M. G. P. are employees or members of their respective companies or laboratories who were contracted and/or consulted by Nyrada Inc. to perform specific research activities., (Copyright © 2022 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2022

68. Effects of mineral oil administration on the pharmacokinetics, metabolism and pharmacodynamics of atorvastatin and pravastatin in mice and dogs.

Author

Gopaul VS, Pieterman EJ, Princen HMG, Bergenholm L, Lundborg E, Cavallin A, Johansson MJ, Hawthorne G, Björkbom A, Hammarberg M, Li X, Jarke A, Bright J, Svensson L, Jansson-Löfmark R, Abrahamsson B, Agrawal R, and Hurt-Camejo E

Subjects

Animals, Atorvastatin, Dogs, Mice, Mice, Inbred C57BL, Mineral Oil, Pravastatin, Pyrroles, Heptanoic Acids, Hydroxymethylglutaryl-CoA Reductase Inhibitors

Abstract

We investigated the effects of mineral oil on statin pharmacokinetics and inflammatory markers in animal models. A new synthesis strategy produced regioisomers that facilitated the characterization of the main metabolite (M1) of atorvastatin, a lipophilic statin, in C57BL/6NCrl mice. The chemical structure of M1 in mice was confirmed as ortho-hydroxy β-oxidized atorvastatin. Atorvastatin and M1 pharmacokinetics and inflammatory markers were assessed in C57BL6/J mice given atorvastatin 5 mg/kg/day or 10 mg/kg/day, as a single dose or for 21 days, with or without 10 µL or 30 µL mineral oil. No consistent differences in plasma exposure of atorvastatin or M1 were observed in mice after single or repeat dosing of atorvastatin with or without mineral oil. However, mice administered atorvastatin 10 mg/kg with 30 µL mineral oil for 21 days had significantly increased plasma levels of serum amyloid A (mean 9.6 µg/mL vs 7.9 µg/mL without mineral oil; p < 0.01) and significantly increased proportions of C62L high B cells (mean 18% vs 12% without mineral oil; p = 0.04). There were no statistically significant differences for other inflammatory markers assessed. In dogs, pharmacokinetics of atorvastatin, its two hydroxy metabolites and pravastatin (a hydrophilic statin) were evaluated after single administration of atorvastatin 10 mg plus pravastatin 40 mg with or without 2 g mineral oil. Pharmacokinetics of atorvastatin, hydroxylated atorvastatin metabolites or pravastatin were not significantly different after single dosing with or without mineral oil in dogs. Collectively, the results in mice and dogs indicate that mineral oil does not affect atorvastatin or pravastatin pharmacokinetics, but could cause low-grade inflammation with chronic oral administration, which warrants further investigation., (Copyright © 2021. Published by Elsevier B.V.)

Published

2021

69. No effects of PCSK9-inhibitor treatment on spatial learning, locomotor activity, and novel object recognition in mice.

Author

Schlunk F, Fischer P, Princen HMG, Rex A, Prinz V, Foddis M, Lütjohann D, Laufs U, and Endres M

Subjects

Animals, Antibodies, Mice, Proprotein Convertase 9 immunology, Behavior, Animal drug effects, Locomotion drug effects, PCSK9 Inhibitors, Protease Inhibitors pharmacology, Recognition, Psychology drug effects, Spatial Learning drug effects

Abstract

Monoclonal anti-proprotein convertase subtilisin/kexin type 9 (PSCK9) neutralizing antibodies effectively lower plasma cholesterol levels and decrease cardiovascular events but also raised some concern that cognitive function could worsen as a side effect. Here, we performed experiments in mice to characterize the effect of anti-PCSK9 antibodies on behavior and cognitive function in detail. APOE*3Leiden.CETP mice and B6129SF1/J wildtype mice were fed a Western type diet and treated with the fully human anti-PCSK9 antibody CmAb1 (PL-45134; 10mg*kg -1 s.c.) or vehicle for 6 weeks. Locomotor activity, anxiety levels, recognition memory, and spatial learning were investigated using the open field, novel object recognition test, and Morris water maze, respectively. Serum cholesterol levels in APOE*3Leiden.CETP mice after treatment with anti-PCSK9 antibody were significantly lower compared to controls whereas cholesterol levels in B6129SF1/J wildtype mice remained unchanged at low levels. No apparent differences were found regarding locomotor activity, anxiety, recognition memory, and spatial learning between animals treated with anti-PCSK9 antibody or vehicle in APOE*3Leiden.CETP and B6129SF1/J wildtype mice. In this study, we found no evidence that treatment with anti-PCSK9 antibodies lead to differences in behavior or changes of cognition in mice., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2021

70. Effects of Inhibition or Deletion of PCSK9 (Proprotein Convertase Subtilisin/Kexin Type 9) on Intracerebral Hemorrhage Volumes in Mice.

Author

Schlunk F, Fischer P, Princen HMG, Rex A, Prinz V, Foddis M, Lütjohann D, Laufs U, and Endres M

Subjects

Animals, Apolipoprotein E3 genetics, Cerebral Hemorrhage pathology, Cholesterol Ester Transfer Proteins genetics, Diet, Western, Mice, Mice, Knockout, PCSK9 Inhibitors, Cerebral Hemorrhage genetics, Hypercholesterolemia genetics, Proprotein Convertase 9 genetics

Published

2020

71. Alirocumab, evinacumab, and atorvastatin triple therapy regresses plaque lesions and improves lesion composition in mice.

Author

Pouwer MG, Pieterman EJ, Worms N, Keijzer N, Jukema JW, Gromada J, Gusarova V, and Princen HMG

Subjects

Administration, Oral, Animals, Antibodies, Monoclonal administration & dosage, Antibodies, Monoclonal, Humanized administration & dosage, Anticholesteremic Agents administration & dosage, Atorvastatin administration & dosage, Drug Therapy, Combination, Female, Mice, Mice, Inbred C57BL, Mice, Transgenic, Plaque, Atherosclerotic chemically induced, Plaque, Atherosclerotic pathology, Antibodies, Monoclonal therapeutic use, Antibodies, Monoclonal, Humanized therapeutic use, Anticholesteremic Agents therapeutic use, Atorvastatin therapeutic use, Plaque, Atherosclerotic drug therapy

Abstract

Atherosclerosis-related CVD causes nearly 20 million deaths annually. Most patients are treated after plaques develop, so therapies must regress existing lesions. Current therapies reduce plaque volume, but targeting all apoB-containing lipoproteins with intensive combinations that include alirocumab or evinacumab, monoclonal antibodies against cholesterol-regulating proprotein convertase subtilisin/kexin type 9 and angiopoietin-like protein 3, may provide more benefit. We investigated the effect of such lipid-lowering interventions on atherosclerosis in APOE*3-Leiden.CETP mice, a well-established model for hyperlipidemia. Mice were fed a Western-type diet for 13 weeks and thereafter matched into a baseline group (euthanized at 13 weeks) and five groups that received diet alone (control) or with treatment [atorvastatin; atorvastatin and alirocumab; atorvastatin and evinacumab; or atorvastatin, alirocumab, and evinacumab (triple therapy)] for 25 weeks. We measured effects on cholesterol levels, plaque composition and morphology, monocyte adherence, and macrophage proliferation. All interventions reduced plasma total cholesterol (37% with atorvastatin to 80% with triple treatment; all P < 0.001). Triple treatment decreased non-HDL-C to 1.0 mmol/l (91% difference from control; P < 0.001). Atorvastatin reduced atherosclerosis progression by 28% versus control ( P < 0.001); double treatment completely blocked progression and diminished lesion severity. Triple treatment regressed lesion size versus baseline in the thoracic aorta by 50% and the aortic root by 36% (both P < 0.05 vs. baseline), decreased macrophage accumulation through reduced proliferation, and abated lesion severity. Thus, high-intensive cholesterol-lowering triple treatment targeting all apoB-containing lipoproteins regresses atherosclerotic lesion area and improves lesion composition in mice, making it a promising potential approach for treating atherosclerosis., (Copyright © 2020 Pouwer et al.)

Published

2020

72. Icosabutate Exerts Beneficial Effects Upon Insulin Sensitivity, Hepatic Inflammation, Lipotoxicity, and Fibrosis in Mice.

Author

van den Hoek AM, Pieterman EJ, van der Hoorn JW, Iruarrizaga-Lejarreta M, Alonso C, Verschuren L, Skjæret T, Princen HMG, and Fraser DA

Abstract

Icosabutate is a structurally engineered eicosapentaenoic acid derivative under development for nonalcoholic steatohepatitis (NASH). In this study, we investigated the absorption and distribution properties of icosabutate in relation to liver targeting and used rodents to evaluate the effects of icosabutate on glucose metabolism, insulin resistance, as well as hepatic steatosis, inflammation, lipotoxicity, and fibrosis. The absorption, tissue distribution, and excretion of icosabutate was investigated in rats along with its effects in mouse models of insulin resistance ( ob/ob ) and metabolic inflammation/NASH (high-fat/cholesterol-fed APOE*3Leiden.CETP mice) and efficacy was compared with synthetic peroxisome proliferator-activated receptor α (PPAR-α) (fenofibrate) and/or PPAR-γ/(α) (pioglitazone and rosiglitazone) agonists. Icosabutate was absorbed almost entirely through the portal vein, resulting in rapid hepatic accumulation. Icosabutate demonstrated potent insulin-sensitizing effects in ob/ob mice, and unlike fenofibrate or pioglitazone, it significantly reduced plasma alanine aminotransferase. In high-fat/cholesterol-fed APOE*3Leiden.CETP mice, icosabutate, but not rosiglitazone, reduced microvesicular steatosis and hepatocellular hypertrophy. Although both rosiglitazone and icosabutate reduced hepatic inflammation, only icosabutate elicited antifibrotic effects in association with decreased hepatic concentrations of multiple lipotoxic lipid species and an oxidative stress marker. Hepatic gene-expression analysis confirmed the changes in lipid metabolism, inflammatory and fibrogenic response, and energy metabolism, and revealed the involved upstream regulators. In conclusion, icosabutate selectively targets the liver through the portal vein and demonstrates broad beneficial effects following insulin sensitivity, hepatic microvesicular steatosis, inflammation, lipotoxicity, oxidative stress, and fibrosis. Icosabutate therefore offers a promising approach to the treatment of both dysregulated glucose/lipid metabolism and inflammatory disorders of the liver, including NASH., (© 2019 The Authors. Hepatology Communications published by Wiley Periodicals, Inc., on behalf of the American Association for the Study of Liver Diseases.)

Published

2019

73. The APOE ∗ 3-Leiden Heterozygous Glucokinase Knockout Mouse as Novel Translational Disease Model for Type 2 Diabetes, Dyslipidemia, and Diabetic Atherosclerosis.

Author

Pouwer MG, Heinonen SE, Behrendt M, Andréasson AC, van Koppen A, Menke AL, Pieterman EJ, van den Hoek AM, Jukema JW, Leighton B, Jönsson-Rylander AC, and Princen HMG

Subjects

Animals, Atherosclerosis blood, Blood Glucose metabolism, Cholesterol blood, Diabetes Complications blood, Diabetes Mellitus, Type 2 blood, Dyslipidemias blood, Female, Heterozygote, Inflammation, Lipids blood, Mice, Mice, Knockout, Phenotype, Risk, Translational Research, Biomedical, Triglycerides metabolism, Apolipoprotein E3 genetics, Atherosclerosis genetics, Diabetes Complications genetics, Diabetes Mellitus, Type 2 genetics, Disease Models, Animal, Dyslipidemias genetics

Abstract

Background: There is a lack of predictive preclinical animal models combining atherosclerosis and type 2 diabetes. APOE∗3-Leiden (E3L) mice are a well-established model for diet-induced hyperlipidemia and atherosclerosis, and glucokinase +/- (GK +/- ) mice are a translatable disease model for glucose control in type 2 diabetes. The respective mice respond similarly to lipid-lowering and antidiabetic drugs as humans. The objective of this study was to evaluate/characterize the APOE ∗ 3-Leiden.glucokinase +/- (E3L.GK +/- ) mouse as a novel disease model to study the metabolic syndrome and diabetic complications., Methods: Female E3L.GK +/- , E3L, and GK +/- mice were fed fat- and cholesterol-containing diets for 37 weeks, and plasma parameters were measured throughout. Development of diabetic macro- and microvascular complications was evaluated., Results: Cholesterol and triglyceride levels were significantly elevated in E3L and E3L.GK +/- mice compared to GK +/- mice, whereas fasting glucose was significantly increased in E3L.GK +/- and GK +/- mice compared to E3L. Atherosclerotic lesion size was increased 2.2-fold in E3L.GK +/- mice as compared to E3L ( p = 0.037), which was predicted by glucose exposure ( R 2 = 0.636, p = 0.001). E3L and E3L.GK +/- mice developed NASH with severe inflammation and fibrosis which, however, was not altered by introduction of the defective GK phenotype, whereas mild kidney pathology with tubular vacuolization was present in all three phenotypes., Conclusions: We conclude that the E3L.GK +/- mouse is a promising novel diet-inducible disease model for investigation of the etiology and evaluation of drug treatment on diabetic atherosclerosis.

Published

2019

74. Atorvastatin accelerates clearance of lipoprotein remnants generated by activated brown fat to further reduce hypercholesterolemia and atherosclerosis.

Author

Hoeke G, Wang Y, van Dam AD, Mol IM, Gart E, Klop HG, van den Berg SM, Pieterman EH, Princen HMG, Groen AK, Rensen PCN, Berbée JFP, and Boon MR

Subjects

Adipose Tissue metabolism, Animals, Atherosclerosis metabolism, Calorimetry, Indirect, Cholesterol Ester Transfer Proteins blood, Cholesterol Ester Transfer Proteins genetics, Female, Gene Expression Profiling, Humans, Hydroxymethylglutaryl-CoA Reductase Inhibitors pharmacology, Hypercholesterolemia metabolism, Hyperlipidemias metabolism, Lipids blood, Liver metabolism, Mice, Mice, Knockout, ApoE, Proprotein Convertase 9 blood, Proprotein Convertase 9 genetics, Receptors, Adrenergic, beta-3 metabolism, Triglycerides metabolism, Adipose Tissue, Brown metabolism, Atherosclerosis drug therapy, Atorvastatin pharmacology, Hypercholesterolemia drug therapy, Lipoproteins metabolism

Abstract

Background and Aims: Activation of brown adipose tissue (BAT) reduces both hyperlipidemia and atherosclerosis by increasing the uptake of triglyceride-derived fatty acids by BAT, accompanied by formation and clearance of lipoprotein remnants. We tested the hypothesis that the hepatic uptake of lipoprotein remnants generated by BAT activation would be accelerated by concomitant statin treatment, thereby further reducing hypercholesterolemia and atherosclerosis., Methods: APOE*3-Leiden.CETP mice were fed a Western-type diet and treated without or with the selective β3-adrenergic receptor (AR) agonist CL316,243 that activates BAT, atorvastatin (statin) or both., Results: β3-AR agonism increased energy expenditure as a result of an increased fat oxidation by activated BAT, which was not further enhanced by statin addition. Accordingly, statin treatment neither influenced the increased uptake of triglyceride-derived fatty acids from triglyceride-rich lipoprotein-like particles by BAT nor further lowered plasma triglyceride levels induced by β3-AR agonism. Statin treatment increased the hepatic uptake of the formed cholesterol-enriched remnants generated by β3-AR agonism. Consequently, statin treatment further lowered plasma cholesterol levels. Importantly, statin, in addition to β3-AR agonism, also further reduced the atherosclerotic lesion size as compared to β3-AR agonism alone, without altering lesion severity and composition., Conclusions: Statin treatment accelerates the hepatic uptake of remnants generated by BAT activation, thereby increasing the lipid-lowering and anti-atherogenic effects of BAT activation in an additive fashion. We postulate that, in clinical practice, combining statin treatment with BAT activation is a promising new avenue to combat hyperlipidemia and cardiovascular disease., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

75. Genetic and Pharmacologic Inactivation of ANGPTL3 and Cardiovascular Disease.

Author

Dewey FE, Gusarova V, Dunbar RL, O'Dushlaine C, Schurmann C, Gottesman O, McCarthy S, Van Hout CV, Bruse S, Dansky HM, Leader JB, Murray MF, Ritchie MD, Kirchner HL, Habegger L, Lopez A, Penn J, Zhao A, Shao W, Stahl N, Murphy AJ, Hamon S, Bouzelmat A, Zhang R, Shumel B, Pordy R, Gipe D, Herman GA, Sheu WHH, Lee IT, Liang KW, Guo X, Rotter JI, Chen YI, Kraus WE, Shah SH, Damrauer S, Small A, Rader DJ, Wulff AB, Nordestgaard BG, Tybjærg-Hansen A, van den Hoek AM, Princen HMG, Ledbetter DH, Carey DJ, Overton JD, Reid JG, Sasiela WJ, Banerjee P, Shuldiner AR, Borecki IB, Teslovich TM, Yancopoulos GD, Mellis SJ, Gromada J, and Baras A

Subjects

Aged, Angiopoietin-Like Protein 3, Angiopoietin-like Proteins, Angiopoietins genetics, Animals, Antibodies, Monoclonal adverse effects, Antibodies, Monoclonal pharmacology, Atherosclerosis metabolism, Cardiovascular Diseases prevention & control, Coronary Artery Disease metabolism, Disease Models, Animal, Dose-Response Relationship, Drug, Double-Blind Method, Dyslipidemias blood, Female, Humans, Lipid Metabolism drug effects, Male, Mice, Mice, Inbred Strains, Middle Aged, Angiopoietins antagonists & inhibitors, Antibodies, Monoclonal administration & dosage, Atherosclerosis drug therapy, Coronary Artery Disease genetics, Dyslipidemias drug therapy, Lipids blood, Mutation

Abstract

Background: Loss-of-function variants in the angiopoietin-like 3 gene (ANGPTL3) have been associated with decreased plasma levels of triglycerides, low-density lipoprotein (LDL) cholesterol, and high-density lipoprotein (HDL) cholesterol. It is not known whether such variants or therapeutic antagonism of ANGPTL3 are associated with a reduced risk of atherosclerotic cardiovascular disease., Methods: We sequenced the exons of ANGPTL3 in 58,335 participants in the DiscovEHR human genetics study. We performed tests of association for loss-of-function variants in ANGPTL3 with lipid levels and with coronary artery disease in 13,102 case patients and 40,430 controls from the DiscovEHR study, with follow-up studies involving 23,317 case patients and 107,166 controls from four population studies. We also tested the effects of a human monoclonal antibody, evinacumab, against Angptl3 in dyslipidemic mice and against ANGPTL3 in healthy human volunteers with elevated levels of triglycerides or LDL cholesterol., Results: In the DiscovEHR study, participants with heterozygous loss-of-function variants in ANGPTL3 had significantly lower serum levels of triglycerides, HDL cholesterol, and LDL cholesterol than participants without these variants. Loss-of-function variants were found in 0.33% of case patients with coronary artery disease and in 0.45% of controls (adjusted odds ratio, 0.59; 95% confidence interval, 0.41 to 0.85; P=0.004). These results were confirmed in the follow-up studies. In dyslipidemic mice, inhibition of Angptl3 with evinacumab resulted in a greater decrease in atherosclerotic lesion area and necrotic content than a control antibody. In humans, evinacumab caused a dose-dependent placebo-adjusted reduction in fasting triglyceride levels of up to 76% and LDL cholesterol levels of up to 23%., Conclusions: Genetic and therapeutic antagonism of ANGPTL3 in humans and of Angptl3 in mice was associated with decreased levels of all three major lipid fractions and decreased odds of atherosclerotic cardiovascular disease. (Funded by Regeneron Pharmaceuticals and others; ClinicalTrials.gov number, NCT01749878 .).

Published

2017

76. Comment on "Hypercholesterolemia with consumption of PFOA-laced Western diets is dependent on strain and sex of mice" by Rebholz S.L. et al. Toxicol. Rep. 2016 (3) 46-54.

Author

Princen HMG, Pouwer MG, and Pieterman EJ

Published

2016

77. Salsalate attenuates diet induced non-alcoholic steatohepatitis in mice by decreasing lipogenic and inflammatory processes.

Author

Liang W, Verschuren L, Mulder P, van der Hoorn JW, Verheij J, van Dam AD, Boon MR, Princen HM, Havekes LM, Kleemann R, and van den Hoek AM

Subjects

Alanine Transaminase blood, Animals, Apolipoproteins E genetics, Aspartate Aminotransferases blood, Blood Glucose analysis, Body Weight drug effects, Cholesterol Ester Transfer Proteins genetics, Cholesterol, Dietary adverse effects, Diet, High-Fat adverse effects, Gene Expression Regulation drug effects, Insulin blood, Lipid Metabolism drug effects, Lipid Metabolism genetics, Lipogenesis drug effects, Liver drug effects, Liver metabolism, Liver pathology, Male, Mice, Transgenic, Non-alcoholic Fatty Liver Disease blood, Non-alcoholic Fatty Liver Disease metabolism, Non-alcoholic Fatty Liver Disease pathology, Salicylates pharmacology, Non-alcoholic Fatty Liver Disease drug therapy, Salicylates therapeutic use

Abstract

Background and Purpose: Salsalate (salicylsalicylic acid) is an anti-inflammatory drug that was recently found to exert beneficial metabolic effects on glucose and lipid metabolism. Although its utility in the prevention and management of a wide range of vascular disorders, including type 2 diabetes and metabolic syndrome has been suggested before, the potential of salsalate to protect against non-alcoholic steatohepatitis (NASH) remains unclear. The aim of the present study was therefore to ascertain the effects of salsalate on the development of NASH., Experimental Approach: Transgenic APOE*3Leiden.CETP mice were fed a high-fat and high-cholesterol diet with or without salsalate for 12 and 20 weeks. The effects on body weight, plasma biochemical variables, liver histology and hepatic gene expression were assessed., Key Results: Salsalate prevented weight gain, improved dyslipidemia and insulin resistance and ameliorated diet-induced NASH, as shown by decreased hepatic microvesicular and macrovesicular steatosis, reduced hepatic inflammation and reduced development of fibrosis. Salsalate affected lipid metabolism by increasing β-oxidation and decreasing lipogenesis, as shown by the activation of PPAR-α, PPAR-γ co-activator 1β, RXR-α and inhibition of genes controlled by the transcription factor MLXIPL/ChREBP. Inflammation was reduced by down-regulation of the NF-κB pathway, and fibrosis development was prevented by down-regulation of TGF-β signalling., Conclusions and Implications: Salsalate exerted a preventive effect on the development of NASH and progression to fibrosis. These data suggest a clinical application of salsalate in preventing NASH., (© 2015 The British Pharmacological Society.)

Published

2015

78. Anacetrapib reduces (V)LDL cholesterol by inhibition of CETP activity and reduction of plasma PCSK9.

Author

van der Tuin SJ, Kühnast S, Berbée JF, Verschuren L, Pieterman EJ, Havekes LM, van der Hoorn JW, Rensen PC, Jukema JW, Princen HM, Willems van Dijk K, and Wang Y

Subjects

Animals, Cardiovascular Diseases prevention & control, Cholesterol Ester Transfer Proteins antagonists & inhibitors, Cholesterol Ester Transfer Proteins metabolism, Down-Regulation, Drug Evaluation, Preclinical, Dyslipidemias drug therapy, Dyslipidemias enzymology, Female, Gene Expression drug effects, Gene Regulatory Networks, Hypolipidemic Agents therapeutic use, Lipid Metabolism drug effects, Metabolic Networks and Pathways, Mice, Transgenic, Oxazolidinones therapeutic use, Proprotein Convertase 9, Cholesterol, VLDL blood, Dyslipidemias blood, Hypolipidemic Agents pharmacology, Oxazolidinones pharmacology, Proprotein Convertases blood, Serine Endopeptidases blood

Abstract

Recently, we showed in APOE*3-Leiden cholesteryl ester transfer protein (E3L.CETP) mice that anacetrapib attenuated atherosclerosis development by reducing (V)LDL cholesterol [(V)LDL-C] rather than by raising HDL cholesterol. Here, we investigated the mechanism by which anacetrapib reduces (V)LDL-C and whether this effect was dependent on the inhibition of CETP. E3L.CETP mice were fed a Western-type diet alone or supplemented with anacetrapib (30 mg/kg body weight per day). Microarray analyses of livers revealed downregulation of the cholesterol biosynthesis pathway (P < 0.001) and predicted downregulation of pathways controlled by sterol regulatory element-binding proteins 1 and 2 (z-scores -2.56 and -2.90, respectively; both P < 0.001). These data suggest increased supply of cholesterol to the liver. We found that hepatic proprotein convertase subtilisin/kexin type 9 (Pcsk9) expression was decreased (-28%, P < 0.01), accompanied by decreased plasma PCSK9 levels (-47%, P < 0.001) and increased hepatic LDL receptor (LDLr) content (+64%, P < 0.01). Consistent with this, anacetrapib increased the clearance and hepatic uptake (+25%, P < 0.001) of [(14)C]cholesteryl oleate-labeled VLDL-mimicking particles. In E3L mice that do not express CETP, anacetrapib still decreased (V)LDL-C and plasma PCSK9 levels, indicating that these effects were independent of CETP inhibition. We conclude that anacetrapib reduces (V)LDL-C by two mechanisms: 1) inhibition of CETP activity, resulting in remodeled VLDL particles that are more susceptible to hepatic uptake; and 2) a CETP-independent reduction of plasma PCSK9 levels that has the potential to increase LDLr-mediated hepatic remnant clearance., (Copyright © 2015 by the American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

79. Innovative pharmaceutical interventions in cardiovascular disease: Focusing on the contribution of non-HDL-C/LDL-C-lowering versus HDL-C-raising: A systematic review and meta-analysis of relevant preclinical studies and clinical trials.

Author

Kühnast S, Fiocco M, van der Hoorn JW, Princen HM, and Jukema JW

Subjects

Animals, Humans, Cardiovascular Diseases drug therapy, Cardiovascular Diseases metabolism, Cholesterol, HDL metabolism, Cholesterol, LDL metabolism, Drug Evaluation, Preclinical, Randomized Controlled Trials as Topic

Abstract

Non-HDL-cholesterol is well recognised as a primary causal risk factor in cardiovascular disease. However, despite consistent epidemiological evidence for an inverse association between HDL-C and coronary heart disease, clinical trials aimed at raising HDL-C (AIM-HIGH, HPS2-THRIVE, dal-OUTCOMES) failed to meet their primary goals. This systematic review and meta-analysis investigated the effects of established and novel treatment strategies, specifically targeting HDL, on inhibition of atherosclerosis in cholesteryl ester transfer protein-expressing animals, and the prevention of clinical events in randomised controlled trials. Linear regression analyses using data from preclinical studies revealed associations for TC and non-HDL-C and lesion area (R(2)=0.258, P=0.045; R(2)=0.760, P<0.001), but not for HDL-C (R(2)=0.030, P=0.556). In clinical trials, non-fatal myocardial infarction risk was significantly less in the treatment group with pooled odd ratios of 0.87 [0.81; 0.94] for all trials and 0.85 [0.78; 0.93] after excluding some trials due to off-target adverse events, whereas all-cause mortality was not affected (OR 1.05 [0.99-1.10]). Meta-regression analyses revealed a trend towards an association between between-group differences in absolute change from baseline in LDL-C and non-fatal myocardial infarction (P=0.066), whereas no correlation was found for HDL-C (P=0.955). We conclude that the protective role of lowering LDL-C and non-HDL-C is well-established. The contribution of raising HDL-C on inhibition of atherosclerosis and the prevention of cardiovascular disease remains undefined and may be dependent on the mode of action of HDL-C-modification. Nonetheless, treatment strategies aimed at improving HDL function and raising apolipoprotein A-I may be worth exploring., (Copyright © 2015 Elsevier B.V. All rights reserved.)

Published

2015

80. No effects of atorvastatin (10 mg/d or 80 mg/d) on nitric oxide, prostacyclin, thromboxane and oxidative stress in type 2 diabetes mellitus patients of the DALI study.

Author

Tsikas D, Pham VV, Suchy MT, van de Ree MA, Huisman MV, Frölich JC, and Princen HM

Subjects

6-Ketoprostaglandin F1 alpha metabolism, Aged, Creatinine metabolism, Dinoprost analogs & derivatives, Dinoprost urine, Dose-Response Relationship, Drug, Double-Blind Method, Female, Humans, Male, Middle Aged, Atorvastatin pharmacology, Diabetes Mellitus, Type 2 metabolism, Hydroxymethylglutaryl-CoA Reductase Inhibitors pharmacology, Nitric Oxide biosynthesis, Oxidative Stress drug effects, Prostaglandins I biosynthesis, Thromboxanes biosynthesis

Abstract

The present study describes the effects of atorvastatin on whole body synthesis of nitric oxide (NO), prostacyclin (PGI2), and thromboxane A2 (TxA2), on oxidative stress and nitrite/nitrate-related renal carbonic anhydrase (CA) activity in patients with type 2 diabetes mellitus (T2DM). A double-blind, randomized, placebo-controlled parallel-group trial (the DALI study group) on 217 patients with T2DM and dyslipidemia was performed. Urinary samples were collected before and after administration of a standard dose (10 mg/d, n=73), a maximal dose atorvastatin (80 mg/d, n=72) or placebo (n=72) for 30 weeks. Urinary nitrite and nitrate were measured to assess whole body NO synthesis. The urinary molar ratio of nitrate to nitrite (UNOxR) served as a measure of renal CA activity. Free radical- and cyclooxygenase (COX)-catalyzed lipid peroxidation was estimated by measuring urinary 8-iso-prostaglandin F2α (8-iso-PGF2α). In subgroups, systemic PGI2 and TxA2 synthesis was assessed by measuring their major urinary metabolites 2,3-dinor-6-keto-prostaglandin F1α and 2,3-dinor-thromboxane B2, respectively. All biochemical parameters were measured by GC-MS and GC-MS/MS methods. T2DM patients had elevated levels of nitrate, nitrite, UNOxR, and 8-iso-PGF2α compared to healthy non-diabetic and normolipidemic subjects. Thirty-week treatment with atorvastatin (10 or 80 mg/d) did not significantly alter NO, PGI2, TxA2 and 8-iso-PGF2α synthesis and did not improve the renal reabsorption of nitrite which is considered an important reservoir of NO. Our study suggests that atorvastatin (10 or 80 mg/d) does not provide cardiovascular benefit beyond its cholesterol lowering effect in patients with T2DM., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

81. Anacetrapib reduces progression of atherosclerosis, mainly by reducing non-HDL-cholesterol, improves lesion stability and adds to the beneficial effects of atorvastatin.

Author

Kühnast S, van der Tuin SJ, van der Hoorn JW, van Klinken JB, Simic B, Pieterman E, Havekes LM, Landmesser U, Lüscher TF, Willems van Dijk K, Rensen PC, Jukema JW, and Princen HM

Subjects

Animals, Atorvastatin, Cholesterol Ester Transfer Proteins metabolism, Cholesterol, HDL drug effects, Cholesterol, HDL physiology, Disease Progression, Drug Combinations, Female, Heptanoic Acids administration & dosage, Mice, Transgenic, Oxazolidinones administration & dosage, Pyrroles administration & dosage, Serum Amyloid A Protein metabolism, Anticholesteremic Agents pharmacology, Atherosclerosis prevention & control, Heptanoic Acids pharmacology, Oxazolidinones pharmacology, Pyrroles pharmacology

Abstract

Background: The residual risk that remains after statin treatment supports the addition of other LDL-C-lowering agents and has stimulated the search for secondary treatment targets. Epidemiological studies propose HDL-C as a possible candidate. Cholesteryl ester transfer protein (CETP) transfers cholesteryl esters from atheroprotective HDL to atherogenic (V)LDL. The CETP inhibitor anacetrapib decreases (V)LDL-C by ∼15-40% and increases HDL-C by ∼40-140% in clinical trials. We evaluated the effects of a broad dose range of anacetrapib on atherosclerosis and HDL function, and examined possible additive/synergistic effects of anacetrapib on top of atorvastatin in APOE*3Leiden.CETP mice., Methods and Results: Mice were fed a diet without or with ascending dosages of anacetrapib (0.03; 0.3; 3; 30 mg/kg/day), atorvastatin (2.4 mg/kg/day) alone or in combination with anacetrapib (0.3 mg/kg/day) for 21 weeks. Anacetrapib dose-dependently reduced CETP activity (-59 to -100%, P < 0.001), thereby decreasing non-HDL-C (-24 to -45%, P < 0.001) and increasing HDL-C (+30 to +86%, P < 0.001). Anacetrapib dose-dependently reduced the atherosclerotic lesion area (-41 to -92%, P < 0.01) and severity, increased plaque stability index and added to the effects of atorvastatin by further decreasing lesion size (-95%, P < 0.001) and severity. Analysis of covariance showed that both anacetrapib (P < 0.05) and non-HDL-C (P < 0.001), but not HDL-C (P = 0.76), independently determined lesion size., Conclusion: Anacetrapib dose-dependently reduces atherosclerosis, and adds to the anti-atherogenic effects of atorvastatin, which is mainly ascribed to a reduction in non-HDL-C. In addition, anacetrapib improves lesion stability., (© The Author 2014. Published by Oxford University Press on behalf of the European Society of Cardiology.)

Published

2015

82. PCSK9 inhibition fails to alter hepatic LDLR, circulating cholesterol, and atherosclerosis in the absence of ApoE.

Author

Ason B, van der Hoorn JW, Chan J, Lee E, Pieterman EJ, Nguyen KK, Di M, Shetterly S, Tang J, Yeh WC, Schwarz M, Jukema JW, Scott R, Wasserman SM, Princen HM, and Jackson S

Subjects

Animals, Antibodies immunology, Atherosclerosis blood, Atherosclerosis enzymology, Atherosclerosis genetics, Cholesterol Ester Transfer Proteins metabolism, Female, Gene Knockout Techniques, Humans, Liver drug effects, Mice, Proprotein Convertase 9, Proprotein Convertases deficiency, Proprotein Convertases genetics, Proprotein Convertases immunology, Serine Endopeptidases deficiency, Serine Endopeptidases genetics, Serine Endopeptidases immunology, Apolipoproteins E deficiency, Atherosclerosis metabolism, Cholesterol blood, Liver metabolism, Proprotein Convertases metabolism, Receptors, LDL metabolism, Serine Endopeptidases metabolism

Abstract

LDL cholesterol (LDL-C) contributes to coronary heart disease. Proprotein convertase subtilisin/kexin type 9 (PCSK9) increases LDL-C by inhibiting LDL-C clearance. The therapeutic potential for PCSK9 inhibitors is highlighted by the fact that PCSK9 loss-of-function carriers exhibit 15-30% lower circulating LDL-C and a disproportionately lower risk (47-88%) of experiencing a cardiovascular event. Here, we utilized pcsk9(-/-) mice and an anti-PCSK9 antibody to study the role of the LDL receptor (LDLR) and ApoE in PCSK9-mediated regulation of plasma cholesterol and atherosclerotic lesion development. We found that circulating cholesterol and atherosclerotic lesions were minimally modified in pcsk9(-/-) mice on either an LDLR- or ApoE-deficient background. Acute administration of an anti-PCSK9 antibody did not reduce circulating cholesterol in an ApoE-deficient background, but did reduce circulating cholesterol (-45%) and TGs (-36%) in APOE*3Leiden.cholesteryl ester transfer protein (CETP) mice, which contain mouse ApoE, human mutant APOE3*Leiden, and a functional LDLR. Chronic anti-PCSK9 antibody treatment in APOE*3Leiden.CETP mice resulted in a significant reduction in atherosclerotic lesion area (-91%) and reduced lesion complexity. Taken together, these results indicate that both LDLR and ApoE are required for PCSK9 inhibitor-mediated reductions in atherosclerosis, as both are needed to increase hepatic LDLR expression., (Copyright © 2014 by the American Society for Biochemistry and Molecular Biology, Inc.)

Published

2014

83. Alirocumab inhibits atherosclerosis, improves the plaque morphology, and enhances the effects of a statin.

Author

Kühnast S, van der Hoorn JW, Pieterman EJ, van den Hoek AM, Sasiela WJ, Gusarova V, Peyman A, Schäfer HL, Schwahn U, Jukema JW, and Princen HM

Subjects

Animals, Antibodies, Monoclonal, Humanized, Atherosclerosis genetics, Atherosclerosis metabolism, Atherosclerosis pathology, Cholesterol genetics, Dose-Response Relationship, Drug, Drug Synergism, Female, Humans, Macrophages pathology, Mice, Mice, Transgenic, Monocytes pathology, Antibodies, Monoclonal pharmacology, Atherosclerosis drug therapy, Cholesterol metabolism, Hydroxymethylglutaryl-CoA Reductase Inhibitors pharmacology, Macrophages metabolism, Monocytes metabolism

Abstract

Proprotein convertase subtilisin/kexin type 9 (PCSK9) inhibition is a potential novel strategy for treatment of CVD. Alirocumab is a fully human PCSK9 monoclonal antibody in phase 3 clinical development. We evaluated the antiatherogenic potential of alirocumab in APOE*3Leiden.CETP mice. Mice received a Western-type diet and were treated with alirocumab (3 or 10 mg/kg, weekly subcutaneous dosing) alone and in combination with atorvastatin (3.6 mg/kg/d) for 18 weeks. Alirocumab alone dose-dependently decreased total cholesterol (-37%; -46%, P < 0.001) and TGs (-36%; -39%, P < 0.001) and further decreased cholesterol in combination with atorvastatin (-48%; -58%, P < 0.001). Alirocumab increased hepatic LDL receptor protein levels but did not affect hepatic cholesterol and TG content. Fecal output of bile acids and neutral sterols was not changed. Alirocumab dose-dependently decreased atherosclerotic lesion size (-71%; -88%, P < 0.001) and severity and enhanced these effects when added to atorvastatin (-89%; -98%, P < 0.001). Alirocumab reduced monocyte recruitment and improved the lesion composition by increasing the smooth muscle cell and collagen content and decreasing the macrophage and necrotic core content. Alirocumab dose-dependently decreases plasma lipids and, as a result, atherosclerosis development, and it enhances the beneficial effects of atorvastatin in APOE*3Leiden.CETP mice. In addition, alirocumab improves plaque morphology., (Copyright © 2014 by the American Society for Biochemistry and Molecular Biology, Inc.)

Published

2014

84. Resveratrol protects against atherosclerosis, but does not add to the antiatherogenic effect of atorvastatin, in APOE*3-Leiden.CETP mice.

Author

Berbée JF, Wong MC, Wang Y, van der Hoorn JW, Khedoe PP, van Klinken JB, Mol IM, Hiemstra PS, Tsikas D, Romijn JA, Havekes LM, Princen HM, and Rensen PC

Subjects

Animals, Atherosclerosis pathology, Atorvastatin, Biomarkers blood, Cholesterol, Dietary administration & dosage, Cholesterol, LDL blood, Drug Synergism, Female, Hydroxymethylglutaryl-CoA Reductase Inhibitors pharmacology, Inflammation drug therapy, Mice, Mice, Transgenic, Oxidative Stress drug effects, Resveratrol, Atherosclerosis drug therapy, Heptanoic Acids pharmacology, Pyrroles pharmacology, Stilbenes pharmacology

Abstract

Resveratrol is a major constituent of traditional Asian medicinal herbs and red wine and is suggested to be a potential antiatherosclerotic drug due to its proposed hypolipidemic, anti-inflammatory and antioxidative properties. The aim of this study was to evaluate whether resveratrol protects against atherosclerosis development in APOE*3-Leiden.CETP (E3L.CETP) mice and adds to the antiatherogenic effect of mild statin treatment, currently the most widely used antiatherogenic therapy. E3L.CETP mice were fed a cholesterol-rich diet without (control) or with resveratrol (0.01% w/w), atorvastatin (0.0027% w/w) or both for 14 weeks. During the study plasma lipid, inflammatory and oxidative stress parameters were determined. Resveratrol reduced atherosclerotic lesion area (-52%) in the aortic root, comparable to atorvastatin (-40%) and the combination of both drugs (-47%). The collagen/macrophage ratio in the atherosclerotic lesion, a marker of plaque stability, was increased by resveratrol (+108%), atorvastatin (+124%) and the combination (+154%). Resveratrol decreased plasma cholesterol levels (-19%) comparable to atorvastatin (-19%) and the combination (-22%), which was completely confined to (very)low-density lipoprotein cholesterol levels in all groups. Post hoc analyses showed that the antiatherogenic effect of atorvastatin could be explained by cholesterol lowering, while the antiatherosclerotic effect of resveratrol could be attributed to factors additional to cholesterol lowering. Markers of inflammation and oxidative stress were not different, but resveratrol improved macrophage function. We conclude that resveratrol potently reduces atherosclerosis development and induces a more stable lesion phenotype in E3L.CETP mice. However, under the experimental conditions tested, resveratrol does not add to the antiatherogenic effect of atorvastatin., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

85. Niacin reduces plasma CETP levels by diminishing liver macrophage content in CETP transgenic mice.

Author

Li Z, Wang Y, van der Sluis RJ, van der Hoorn JW, Princen HM, Van Eck M, Van Berkel TJ, Rensen PC, and Hoekstra M

Subjects

Adipose Tissue, White drug effects, Adipose Tissue, White metabolism, Animals, Apolipoprotein E3 genetics, Cholesterol Ester Transfer Proteins blood, Cholesterol Ester Transfer Proteins genetics, Female, Gene Expression, Humans, Hypolipidemic Agents toxicity, Lipoproteins, LDL blood, Lipoproteins, VLDL blood, Liver cytology, Liver metabolism, Liver X Receptors, Macrophages cytology, Macrophages metabolism, Mice, Mice, Transgenic, Niacin toxicity, Orphan Nuclear Receptors metabolism, Cholesterol Ester Transfer Proteins metabolism, Hypolipidemic Agents pharmacology, Liver drug effects, Macrophages drug effects, Niacin pharmacology

Abstract

The anti-dyslipidemic drug niacin has recently been shown to reduce the hepatic expression and plasma levels of CETP. Since liver macrophages contribute to hepatic CETP expression, we investigated the role of macrophages in the CETP-lowering effect of niacin in mice. In vitro studies showed that niacin does not directly attenuate CETP expression in macrophages. Treatment of normolipidemic human CETP transgenic mice, fed a Western-type diet with niacin for 4 weeks, significantly reduced the hepatic cholesterol concentration (-20%), hepatic CETP gene expression (-20%), and plasma CETP mass (-30%). Concomitantly, niacin decreased the hepatic expression of CD68 (-44%) and ABCG1 (-32%), both of which are specific markers for the hepatic macrophage content. The decrease in hepatic CETP expression was significantly correlated with the reduction of hepatic macrophage markers. Furthermore, niacin attenuated atherogenic diet-induced inflammation in liver, as evident from decreased expression of TNF-alpha (-43%). Niacin similarly decreased the macrophage markers and absolute macrophage content in hyperlipidemic APOE*3-Leiden.CETP transgenic mice on a Western-type diet. In conclusion, niacin decreases hepatic CETP expression and plasma CETP mass by attenuating liver inflammation and macrophage content in response to its primary lipid-lowering effect, rather than by attenuating the macrophage CETP expression level., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

86. Distribution of perfluorooctanesulfonate and perfluorooctanoate into human plasma lipoprotein fractions.

Author

Butenhoff JL, Pieterman E, Ehresman DJ, Gorman GS, Olsen GW, Chang SC, and Princen HM

Subjects

Centrifugation, Density Gradient, Cross-Sectional Studies, Dose-Response Relationship, Drug, Humans, Protein Binding, Alkanesulfonic Acids blood, Caprylates blood, Fluorocarbons blood, Lipoproteins blood

Abstract

Some cross-sectional epidemiological studies have reported positive associations of serum concentrations of non-high density lipoprotein cholesterol with serum perfluorooctanesulfonate (PFOS) and perfluorooctanoate (PFOA). However, the strength of the reported associations is inconsistent for exposure-response across three orders of magnitude of serum PFOS and/or PFOA concentrations. These positive associations are unexpected based on toxicological/mechanistic studies, suggesting that the associations may have a biological, rather than a causal, basis. This study tested the hypothesis that PFOS and PFOA distribute into serum lipoprotein fractions such that increases in serum lipoproteins would result in corresponding increases in serum concentrations of PFOS and PFOA. Based on observed binding of PFOS and PFOA to isolated β-lipoproteins in physiological saline (96% and 40% bound, respectively) in preliminary experiments using ultrafiltration and LC-MS/MS methods, binding to human donor plasma lipoprotein fractions was investigated by two density gradient methods. The majority of PFOS and PFOA recovered masses were found in lipoprotein-depleted plasma. Plasma density gradient fractionation data suggested that maximally 9% of PFOS distributes to lipoprotein-containing fractions, yet only 1% or less of PFOA is so distributed. These data do not support a strong role for plasma lipoprotein fractions in explaining the inconsistent dose-response associations reported in cross-sectional epidemiological studies., (Copyright © 2012 Elsevier Ireland Ltd. All rights reserved.)

Published

2012

87. Aliskiren inhibits atherosclerosis development and improves plaque stability in APOE*3Leiden.CETP transgenic mice with or without treatment with atorvastatin.

Author

Kühnast S, van der Hoorn JW, van den Hoek AM, Havekes LM, Liau G, Jukema JW, and Princen HM

Subjects

Animals, Atherosclerosis genetics, Atorvastatin, Female, Mice, Mice, Transgenic, Amides pharmacology, Apolipoproteins E genetics, Atherosclerosis prevention & control, Fumarates pharmacology, Heptanoic Acids pharmacology, Hydroxymethylglutaryl-CoA Reductase Inhibitors pharmacology, Pyrroles pharmacology

Abstract

Objective: Aliskiren is the first commercially available, orally active, direct renin inhibitor approved to treat hypertension. The renin-angiotensin system has been shown to be a significant contributor to the development of hypercholesterolemia-induced atherosclerosis. The aim of this study was to evaluate the antiatherosclerotic and plaque stabilization effects of aliskiren alone and in combination with atorvastatin., Methods: APOE*3Leiden.CETP mice (n = 14-17/group) were fed a western-type diet (containing 0.25% cholesterol) alone or were treated with either aliskiren (15 mg/kg per day), atorvastatin (3.6 mg/kg per day) or a combination of aliskiren and atorvastatin. Effects on SBP, total cholesterol, inflammation markers and atherosclerotic size and composition were assessed., Results: Aliskiren reduced SBP (-19%, P < 0.001) and atorvastatin reduced total cholesterol (-24%, P < 0.001). Atherosclerotic lesion area was reduced by aliskiren (-40%, P < 0.01), atorvastatin (-61%, P < 0.001) and the combination treatment (-69%, P < 0.001). Aliskiren alone and together with atorvastatin decreased the number of T cells in the aortic root area (-60%, P < 0.01; -41%, P < 0.05), as well as macrophage (-64%, P < 0.001; -72%, P < 0.001) and necrotic area (-52%, P = 0.071; -84%, P < 0.001) in the lesion. Atorvastatin alone and together with aliskiren decreased monocyte adherence (-43%, P < 0.05 and -51%, P < 0.01) and monocyte chemoattractant protein-1 (both -36%, P < 0.01). The combination treatment decreased the number of lesions (-17%, P < 0.05) and E-selectin (-17%, P < 0.05)., Conclusion: Aliskiren inhibited atherosclerosis development and improved plaque stability alone and in combination with atorvastatin, possibly via a mechanism involving T cells. These results suggest a potential benefit of using aliskiren in a clinical setting, particularly in combination with statin treatment.

Published

2012

88. Perfluoroalkyl sulfonates cause alkyl chain length-dependent hepatic steatosis and hypolipidemia mainly by impairing lipoprotein production in APOE*3-Leiden CETP mice.

Author

Bijland S, Rensen PC, Pieterman EJ, Maas AC, van der Hoorn JW, van Erk MJ, Havekes LM, Willems van Dijk K, Chang SC, Ehresman DJ, Butenhoff JL, and Princen HM

Subjects

Alkanesulfonic Acids chemistry, Alkanesulfonic Acids toxicity, Animals, Fatty Liver metabolism, Fluorocarbons chemistry, Humans, Liver drug effects, Liver metabolism, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, Quantitative Structure-Activity Relationship, Sulfonic Acids chemistry, Sulfonic Acids toxicity, Surface-Active Agents chemistry, Cholesterol Ester Transfer Proteins genetics, Fatty Liver chemically induced, Fluorocarbons toxicity, Lipid Metabolism drug effects, Surface-Active Agents toxicity

Abstract

Perfluorobutane sulfonate (PFBS), perfluorohexane sulfonate (PFHxS), and perfluorooctane sulfonate (PFOS) are stable perfluoroalkyl sulfonate (PFAS) surfactants, and PFHxS and PFOS are frequently detected in human biomonitoring studies. Some epidemiological studies have shown modest positive correlations of serum PFOS with non-high-density lipoprotein (HDL)-cholesterol (C). This study investigated the mechanism underlying the effect of PFAS surfactants on lipoprotein metabolism. APOE*3-Leiden.CETP mice were fed a Western-type diet with PFBS, PFHxS, or PFOS (30, 6, and 3 mg/kg/day, respectively) for 4-6 weeks. Whereas PFBS modestly reduced only plasma triglycerides (TG), PFHxS and PFOS markedly reduced TG, non-HDL-C, and HDL-C. The decrease in very low-density lipoprotein (VLDL) was caused by enhanced lipoprotein lipase-mediated VLDL-TG clearance and by decreased production of VLDL-TG and VLDL-apolipoprotein B. Reduced HDL production, related to decreased apolipoprotein AI synthesis, resulted in decreased HDL. PFHxS and PFOS increased liver weight and hepatic TG content. Hepatic gene expression profiling data indicated that these effects were the combined result of peroxisome proliferator-activated receptor alpha and pregnane X receptor activation. In conclusion, the potency of PFAS to affect lipoprotein metabolism increased with increasing alkyl chain length. PFHxS and PFOS reduce plasma TG and total cholesterol mainly by impairing lipoprotein production, implying that the reported positive correlations of serum PFOS and non-HDL-C are associative rather than causal.

Published

2011

89. PXR agonism decreases plasma HDL levels in ApoE3-Leiden.CETP mice.

Author

de Haan W, de Vries-van der Weij J, Mol IM, Hoekstra M, Romijn JA, Jukema JW, Havekes LM, Princen HM, and Rensen PC

Subjects

ATP Binding Cassette Transporter 1, ATP-Binding Cassette Transporters metabolism, Animals, Cholesterol Ester Transfer Proteins blood, Female, Immunoblotting, Lipids analysis, Lipids blood, Lipoproteins analysis, Lipoproteins blood, Liver metabolism, Mice, Mice, Transgenic, Pregnane X Receptor, RNA, Messenger metabolism, Receptors, Steroid metabolism, Scavenger Receptors, Class B metabolism, Apolipoprotein E3 genetics, Cholesterol Ester Transfer Proteins genetics, Cholesterol, HDL blood, Pregnenolone Carbonitrile pharmacology, Receptors, Steroid agonists

Abstract

Pregnane X receptor (PXR) agonism has been shown to affect multiple steps in both the synthesis and catabolism of HDL, but its integrated effect on HDL metabolism in vivo remains unclear. The aim of this study was to evaluate the net effect of PXR agonism on HDL metabolism in ApoE3-Leiden (E3L) and E3L.CETP mice, well-established models for human-like lipoprotein metabolism. Female mice were fed a diet with increasing amounts of the potent PXR agonist 5-pregnen-3beta-ol-20-one-16alpha-carbonitrile (PCN). In E3L and E3L.CETP mice, PCN increased liver lipids as well as plasma cholesterol and triglycerides. However, whereas PCN increased cholesterol contained in large HDL-1 particles in E3L mice, it dose-dependently decreased HDL-cholesterol in E3L.CETP mice, indicating that CETP expression dominates the effect of PCN on HDL metabolism. Analysis of the hepatic expression of genes involved in HDL metabolism showed that PCN decreased expression of genes involved in HDL synthesis (Abca1, Apoa1), maturation (Lcat, Pltp) and clearance (Sr-b1). The HDL-increasing effect of PCN, observed in E3L mice, is likely caused by a marked decrease in hepatic SR-BI protein expression, and completely reversed by CETP expression. We conclude that chronic PXR agonism dose-dependently reduces plasma HDL-cholesterol in the presence of CETP.

Published

2009

90. Niacin increases HDL by reducing hepatic expression and plasma levels of cholesteryl ester transfer protein in APOE*3Leiden.CETP mice.

Author

van der Hoorn JW, de Haan W, Berbée JF, Havekes LM, Jukema JW, Rensen PC, and Princen HM

Subjects

Animals, Apolipoprotein A-I metabolism, Apolipoprotein E3 genetics, Atherosclerosis genetics, Atherosclerosis metabolism, Bile metabolism, Cholesterol Ester Transfer Proteins blood, Cholesterol Ester Transfer Proteins genetics, Dietary Fats metabolism, Disease Models, Animal, Dose-Response Relationship, Drug, Feces chemistry, Female, Humans, Liver metabolism, Mice, Mice, Transgenic, RNA, Messenger metabolism, Time Factors, Triglycerides blood, Up-Regulation, Apolipoprotein E3 metabolism, Atherosclerosis drug therapy, Cholesterol Ester Transfer Proteins metabolism, Cholesterol, HDL metabolism, Hypolipidemic Agents pharmacology, Liver drug effects, Niacin pharmacology

Abstract

Objective: Niacin potently decreases plasma triglycerides and LDL-cholesterol. In addition, niacin is the most potent HDL-cholesterol-increasing drug used in the clinic. In the present study, we aimed at elucidation of the mechanism underlying its HDL-raising effect., Methods and Results: In APOE*3Leiden transgenic mice expressing the human CETP transgene, niacin dose-dependently decreased plasma triglycerides (up to -77%, P<0.001) and total cholesterol (up to -66%, P<0.001). Concomitantly, niacin dose-dependently increased HDL-cholesterol (up to +87%, P<0.001), plasma apoAI (up to +72%, P<0.001), as well as the HDL particle size. In contrast, in APOE*3Leiden mice, not expressing CETP, niacin also decreased total cholesterol and triglycerides but did not increase HDL-cholesterol. In fact, in APOE*3Leiden.CETP mice, niacin dose-dependently decreased the hepatic expression of CETP (up to -88%; P<0.01) as well as plasma CETP mass (up to -45%, P<0.001) and CETP activity (up to -52%, P<0.001). Additionally, niacin dose-dependently decreased the clearance of apoAI from plasma and reduced the uptake of apoAI by the kidneys (up to -90%, P<0.01)., Conclusions: Niacin markedly increases HDL-cholesterol in APOE*3Leiden.CETP mice by reducing CETP activity, as related to lower hepatic CETP expression and a reduced plasma (V)LDL pool, and increases HDL-apoAI by decreasing the clearance of apoAI from plasma.

Published

2008

91. Preferential campesterol incorporation into various tissues in apolipoprotein E*3-Leiden mice consuming plant sterols or stanols.

Author

Plat J, de Jong A, Volger OL, Princen HM, and Mensink RP

Subjects

Animals, Apolipoprotein E3 genetics, Cholesterol blood, Cholesterol metabolism, Female, Mice, Mice, Transgenic, Osmolar Concentration, Phytosterols blood, Phytosterols metabolism, Phytosterols pharmacology, Sitosterols blood, Sitosterols metabolism, Sitosterols pharmacology, Tissue Distribution, Apolipoprotein E3 metabolism, Cholesterol analogs & derivatives, Diet, Phytosterols administration & dosage, Sitosterols administration & dosage

Abstract

Intestinal absorption of plant sterols and stanols is much lower as compared with that of cholesterol; and therefore, serum concentrations are low. Circulating plant sterols and stanols are incorporated into tissues. However, hardly any data are available about tissue distributions of individual plant sterols and stanols, particularly in relation to their serum concentrations. We therefore fed female apolipoprotein E*3-Leiden mice a control diet, a plant sterol-enriched diet (1g/100 g diet), or a plant stanol-enriched diet (1g/100 g diet) for 8 weeks. In the sterol group, serum cholesterol-standardized campesterol and sitosterol concentrations were, respectively, 8 and 7 times higher as compared with those in the control group. Consequently, the serum campesterol-sitosterol ratio remained essentially unchanged. Cholesterol-standardized plant sterol concentrations increased significantly in all analyzed tissues, except brain. However, the campesterol-sitosterol ratio also increased in all tissues (except in liver and spleen), suggesting that campesterol is preferentially incorporated over sitosterol in those tissues. For the stanol group, serum plant stanol concentrations also increased; but the increase was but less pronounced. We conclude that, in apolipoprotein E*3-Leiden mice, campesterol is preferentially incorporated into most tissues over sitosterol, which cannot be deduced from changes in serum concentrations.

Published

2008

92. Torcetrapib does not reduce atherosclerosis beyond atorvastatin and induces more proinflammatory lesions than atorvastatin.

Author

de Haan W, de Vries-van der Weij J, van der Hoorn JW, Gautier T, van der Hoogt CC, Westerterp M, Romijn JA, Jukema JW, Havekes LM, Princen HM, and Rensen PC

Subjects

Animals, Atherosclerosis pathology, Atorvastatin, Cholesterol Ester Transfer Proteins antagonists & inhibitors, Drug Synergism, Heptanoic Acids therapeutic use, Mice, Mice, Inbred Strains, Pyrroles therapeutic use, Quinolines therapeutic use, Atherosclerosis drug therapy, Heptanoic Acids pharmacology, Inflammation chemically induced, Pyrroles pharmacology, Quinolines pharmacology

Abstract

Background: Although cholesteryl ester transfer protein (CETP) inhibition is regarded as a promising strategy to reduce atherosclerosis by increasing high-density lipoprotein cholesterol, the CETP inhibitor torcetrapib given in addition to atorvastatin had no effect on atherosclerosis and even increased cardiovascular death in the recent Investigation of Lipid Level Management to Understand its Impact in Atherosclerotic Events trial. Therefore, we evaluated the antiatherogenic potential and adverse effects of torcetrapib in humanized APOE*3-Leiden.CETP (E3L.CETP) mice., Methods and Results: E3L.CETP mice were fed a cholesterol-rich diet without drugs or with torcetrapib (12 mg x kg(-1) x d(-1)), atorvastatin (2.8 mg x kg(-1) x d(-1)), or both for 14 weeks. Torcetrapib decreased CETP activity in both the absence and presence of atorvastatin (-74% and -73%, respectively; P<0.001). Torcetrapib decreased plasma cholesterol (-20%; P<0.01), albeit to a lesser extent than atorvastatin (-42%; P<0.001) or the combination of torcetrapib and atorvastatin (-40%; P<0.001). Torcetrapib increased high-density lipoprotein cholesterol in the absence (30%) and presence (34%) of atorvastatin. Torcetrapib and atorvastatin alone reduced atherosclerotic lesion size (-43% and -46%; P<0.05), but combination therapy did not reduce atherosclerosis compared with atorvastatin alone. Remarkably, compared with atorvastatin, torcetrapib enhanced monocyte recruitment and expression of monocyte chemoattractant protein-1 and resulted in lesions of a more inflammatory phenotype, as reflected by an increased macrophage content and reduced collagen content., Conclusions: CETP inhibition by torcetrapib per se reduces atherosclerotic lesion size but does not enhance the antiatherogenic potential of atorvastatin. However, compared with atorvastatin, torcetrapib introduces lesions of a less stable phenotype.

Published

2008

93. The impact of metabolic syndrome and CRP on vascular phenotype in type 2 diabetes mellitus.

Author

Alizadeh Dehnavi R, Beishuizen ED, van de Ree MA, Le Cessie S, Huisman MV, Kluft C, Princen HM, and Tamsma JT

Subjects

Aged, Biomarkers blood, E-Selectin blood, Female, Fibrinogen analysis, Humans, Inflammation, Male, Middle Aged, Phenotype, Plasminogen Activator Inhibitor 1 blood, Thrombomodulin blood, Tissue Plasminogen Activator, Tunica Intima pathology, Tunica Media pathology, Vascular Cell Adhesion Molecule-1 blood, von Willebrand Factor analysis, C-Reactive Protein analysis, Diabetes Mellitus, Type 2 physiopathology, Metabolic Syndrome physiopathology

Abstract

Background: The burden of cardiovascular disease in diabetes mellitus type 2 (DM2) patients is variable. We hypothesize that metabolic syndrome (MS) and low-grade systemic inflammation modify the extent of atherosclerosis in DM2., Methods: Vascular phenotype was determined using the following endothelium-related, hemostatic, and sonographic endpoints in 62 DM2 patients with mild dyslipidemia: sVCAM, sE-selectin, von Willebrand factor (VWF), fibrinogen, s-thrombomodulin (sTM), tPA, PAI-1, flow-mediated dilation (FMD), and intima media thickness (IMT). The impact of MS load (number of criteria present), MS components, and CRP on these parameters was assessed., Results: Serum sVCAM, sTM, and tPA levels significantly increased with increasing MS load. IMT also significantly increased from 0.602+/-0.034 (one MS criterion) to 0.843+/-0.145 (four MS criteria, p=0.007). LogCRP significantly correlated with fibrinogen, PAI-1, and IMT. In a multiple regression (MR) model with age and gender as covariates, MS load predicted sVCAM and sTM; CRP predicted PAI-1 and fibrinogen; MS load and CRP simultaneously predicted tPA and IMT. For each MS criterion present, IMT significantly increased by 0.04 mm. An increase in CRP from 1 to 3 mg/L resulted in a significant increase of 0.04 mm. Patients with four MS criteria and inflammation (CRP >or=3 mg/L) are predicted to have a 0.21 mm thicker IMT than those without. A second stepwise MR analysis based on gender, traditional risk factors, diabetes-related parameters, renal function, individual MS criteria, and LogCRP as explanatory variables showed a significant effect of systolic and diastolic blood pressure, HDL, and LogCRP on IMT(r(2)=0.36, p<0.001)., Conclusion: MS and low-grade chronic inflammation have an independent impact on vascular phenotype including IMT in DM2.

Published

2008

94. Atorvastatin increases HDL cholesterol by reducing CETP expression in cholesterol-fed APOE*3-Leiden.CETP mice.

Author

de Haan W, van der Hoogt CC, Westerterp M, Hoekstra M, Dallinga-Thie GM, Princen HM, Romijn JA, Jukema JW, Havekes LM, and Rensen PC

Subjects

Animals, Apolipoprotein E3 genetics, Atorvastatin, Cholesterol Ester Transfer Proteins blood, Cholesterol, Dietary pharmacology, Cholesterol, VLDL metabolism, Dose-Response Relationship, Drug, Female, Gene Expression drug effects, Humans, Hypercholesterolemia metabolism, Liver drug effects, Liver metabolism, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, RNA, Messenger metabolism, Cholesterol Ester Transfer Proteins genetics, Cholesterol, HDL metabolism, Heptanoic Acids pharmacology, Hydroxymethylglutaryl-CoA Reductase Inhibitors pharmacology, Hypercholesterolemia drug therapy, Pyrroles pharmacology

Abstract

Objective: In addition to lowering low-density lipoprotein (LDL)-cholesterol, statins modestly increase high-density lipoprotein (HDL)-cholesterol in humans and decrease cholesteryl ester transfer protein (CETP) mass and activity. Our aim was to determine whether the increase in HDL depends on CETP expression., Methods and Results: APOE*3-Leiden (E3L) mice, with a human-like lipoprotein profile and a human-like responsiveness to statin treatment, were crossbred with mice expressing human CETP under control of its natural flanking regions resulting in E3L.CETP mice. E3L and E3L.CETP mice were fed a Western-type diet with or without atorvastatin. Atorvastatin (0.01% in the diet) reduced plasma cholesterol in both E3L and E3L.CETP mice (-26 and -33%, P<0.05), mainly in VLDL, but increased HDL-cholesterol only in E3L.CETP mice (+52%). Hepatic mRNA expression levels of genes involved in HDL metabolism, such as phospholipid transfer protein (Pltp), ATP-binding cassette transporter A1 (Abca1), scavenger receptor class B type I (Sr-b1), and apolipoprotein AI (Apoa1), were not differently affected by atorvastatin in E3L.CETP mice as compared to E3L mice. However, in E3L.CETP mice, atorvastatin down-regulated the hepatic CETP mRNA expression (-57%; P<0.01) as well as the total CETP level (-29%) and cholesteryl esters (CE) transfer activity (-36%; P<0.05) in plasma., Conclusions: Atorvastatin increases HDL-cholesterol in E3L.CETP mice by reducing the CETP-dependent transfer of cholesterol from HDL to (V)LDL, as related to lower hepatic CETP expression and a reduced plasma (V)LDL pool.

Published

2008

95. Olmesartan and pravastatin additively reduce development of atherosclerosis in APOE*3Leiden transgenic mice.

Author

van der Hoorn JW, Kleemann R, Havekes LM, Kooistra T, Princen HM, and Jukema JW

Subjects

Animals, Atherosclerosis blood, Atherosclerosis genetics, Atherosclerosis pathology, Blood Pressure drug effects, Collagen metabolism, Diet, Atherogenic, Drug Synergism, Female, Humans, Inflammation prevention & control, Lipids blood, Macrophages pathology, Mice, Mice, Transgenic, Monocytes pathology, Muscle, Smooth, Vascular pathology, Recombinant Proteins genetics, Serum Amyloid A Protein metabolism, T-Lymphocytes pathology, Angiotensin II Type 1 Receptor Blockers administration & dosage, Apolipoprotein E3 genetics, Atherosclerosis prevention & control, Hydroxymethylglutaryl-CoA Reductase Inhibitors administration & dosage, Imidazoles administration & dosage, Pravastatin administration & dosage, Tetrazoles administration & dosage

Abstract

Aim: This study was designed to investigate the effect of the angiotensin II receptor blocker olmesartan alone, or in combination with standard treatment with a statin, pravastatin, on atherosclerosis development in APOE*3Leiden transgenic mice., Methods and Results: Four groups of 15 mice received an atherogenic diet alone (plasma cholesterol 17.4 +/- 2.7 mmol/l) or supplemented with either 0.008% (w/w) olmesartan (9.3 mg/kg per day) (plasma cholesterol 16.4 +/- 3.9 mmol/l), 0.03% (w/w) pravastatin (35 mg/kg per day) (plasma cholesterol 14.6 +/- 2.6 mmol/l), or the combination of both (plasma cholesterol 14.5 +/- 2.9 mmol/l) for 6 months. Treatment with olmesartan or pravastatin reduced the development of atherosclerosis as compared to the control group (-46 and -39%, respectively). Pravastatin also reduced the severity of the lesions. As compared to control the combination of both treatments almost fully prevented atherosclerosis (-91%, P < 0.001) and strongly reduced lesion number (-69%), lesion severity (-79%), number of macrophages (-89%) and T lymphocytes (-86%) per cross-section. Treatment with olmesartan alone and in combination with pravastatin inhibited the adhesion of monocytes to the vessel wall (-22%; P < 0.05 and -25%; P < 0.01, respectively), and reduced the relative quantity of macrophages in the lesions (-38%; P < 0.05 and -26%; NS, respectively) as compared to control., Conclusion: Olmesartan reduced atherosclerosis development mainly by decreasing monocyte adhesion and the relative amount of macrophages, whereas pravastatin inhibited the progression of atherosclerosis to more advanced lesions, reflecting different anti-atherosclerotic modes of action of the two drugs. Combination therapy with olmesartan and pravastatin additively reduced atherosclerosis development, resulting in less and less severe lesions.

Published

2007

96. Cholesterol 7alpha-hydroxylase deficiency in mice on an APOE*3-Leiden background increases hepatic ABCA1 mRNA expression and HDL-cholesterol.

Author

Post SM, Groenendijk M, van der Hoogt CC, Fievet C, Luc G, Hoekstra M, Princen HM, Staels B, and Rensen PC

Subjects

ATP Binding Cassette Transporter 1, ATP-Binding Cassette Transporters genetics, Animals, Apolipoprotein E3 genetics, Bile Acids and Salts metabolism, Cholesterol 7-alpha-Hydroxylase genetics, Cholesterol, HDL genetics, Female, Gene Expression Regulation physiology, Gene Expression Regulation, Enzymologic physiology, Humans, Liver metabolism, Mice, Mice, Knockout, Mice, Transgenic, Phosphatidylcholine-Sterol O-Acyltransferase genetics, Phosphatidylcholine-Sterol O-Acyltransferase metabolism, Phospholipid Transfer Proteins genetics, Phospholipid Transfer Proteins metabolism, RNA, Messenger genetics, ATP-Binding Cassette Transporters metabolism, Apolipoprotein E3 metabolism, Cholesterol 7-alpha-Hydroxylase metabolism, Cholesterol, HDL metabolism, RNA, Messenger metabolism

Abstract

Objective: High-density lipoprotein (HDL) plays a key role in protection against development of atherosclerosis by reducing inflammation, protecting against LDL oxidation, and promoting reverse cholesterol transport from peripheral tissues to the liver for secretion into bile. Cholesterol 7alpha-hydroxylase (Cyp7a1) catalyzes the rate-limiting step in the intrahepatic conversion of cholesterol to bile acids that may have a role in HDL metabolism. We investigated the effect of Cyp7a1 deficiency on HDL metabolism in APOE*3-Leiden transgenic mice., Methods and Results: Reduced bile acid biosynthesis in Cyp7a1-/-.APOE*3-Leiden mice versus APOE*3-Leiden mice did not affect total plasma cholesterol levels, but the distribution of cholesterol over various lipoproteins was different. Cholesterol was decreased in apoB-containing lipoproteins (ie, VLDL and IDL/LDL), whereas cholesterol was increased in HDL. The activity of PLTP and LCAT, which play a role in HDL catabolism, were not changed, and neither was HDL clearance. However, the hepatic cholesterol content was 2-fold increased, which was accompanied by a 2-fold elevated expression of hepatic ABCA1 and increased rate of cholesterol efflux from the liver to HDL., Conclusions: Strongly reduced bile acid synthesis in Cyp7a1-/-.APOE*3-Leiden mice leads to increased plasma HDL-cholesterol levels, as related to an increased hepatic expression of ABCA1.

Published

2006

97. Absence of an atheroprotective effect of the garlic powder printanor in APOE*3-Leiden transgenic mice.

Author

Espirito Santo SM, van Vlijmen BJ, van Duyvenvoorde W, Offerman EH, Havekes LM, Arnault I, Auger J, and Princen HM

Subjects

Animals, Apolipoprotein E3, Disease Models, Animal, Female, Intercellular Adhesion Molecule-1 blood, Lipids blood, Mice, Mice, Transgenic, Serum Amyloid A Protein analysis, Tumor Necrosis Factor-alpha analysis, von Willebrand Factor analysis, Apolipoproteins E genetics, Arteriosclerosis prevention & control, Garlic

Abstract

Numerous animal studies have reported that garlic can protect against atherosclerosis. However, a comparable number of studies do not support this observation. This contradiction may result from differences in study design, use of different animal models, and use of different garlic formulations and preparations. Here, we investigated the effect of the chemically well-characterized and production-controlled garlic powder printanor on atherosclerosis in the APOE*3-Leiden transgenic mouse, a mouse model well suited for evaluating anti-atherosclerotic properties of drugs and food components under human-like conditions. APOE*3-Leiden mice were fed a Western diet supplemented with either 5 or 50 g kg(-1) printanor. As a reference, the commercially available fermented garlic kyolic was included (1.6 g kg(-1) diet). Treatment with printanor demonstrated reduced body weight, coinciding with increased feces production and fecal fatty acids excretion. Printanor and kyolic treatment did not affect plasma lipids, markers of inflammation (serum amyloid A, serum-soluble intercellular adhesion molecule-1, and blood-leukocytes tumor necrosis factor-alpha (TNFalpha) production) and vascular activation (plasma von Willebrand factor (vWF)). As analyzed after 28 weeks of treatment, printanor and kyolic did not affect atherosclerotic lesion type, area or composition. Under conditions relevant to the human situation, the well-characterized and production-controlled garlic powder printanor does not display hypolipidemic, anti-inflammatory or anti-atherosclerotic properties.

Published

2004

98. alpha-Tocopherol levels in plasma in new-onset, insulin-dependent diabetes mellitus.

Author

Muis MJ, Stolk RP, Princen HM, Van Dam PS, Dikkeschei LD, Grobbee DE, and Bilo HJ

Abstract

BACKGROUND: Diabetic complications have been related to increased oxidative stress. Plasma antioxidant levels may be affected by hyperglycemia-induced oxidative stress as well as by insulin therapy. We evaluated the immediate effect of insulin treatment and improved metabolic control on the important antioxidant alpha-tocopherol plasma (vitamin E) levels in new-onset, insulin-dependent diabetes mellitus. METHODS: The study was performed in 15 consecutive patients, aged 20-67 years, with new-onset diabetes mellitus requiring acute insulin treatment. Plasma alpha-tocopherol levels were measured before the start of intensive insulin treatment and monthly for 6 months thereafter. Simultaneously, we studied plasma malondialdehyde (MDA) as a reflection of lipid peroxidation. In addition, comparisons were made to a nondiabetic reference group. RESULTS: Baseline alpha-tocopherol levels did not differ from those in nondiabetic subjects. alpha-Tocopherol decreased significantly, from 33.5+/-12.1 mumol/l before treatment to 28.11+/-6.85 mumol/l (-16%) after 1 month of insulin therapy (p<0.04) to 26.6+/-7.03 mumol/l (-20%) after 3 months of insulin therapy (p<0.02). This trend did not change after adjusting for variations in cholesterol levels. After 6 months, alpha-tocopherol was no longer decreased compared to baseline levels (29.6+/-7.4 mumol/l). MDA concentrations at baseline were significantly higher in the diabetic patients (3.79+/-2.91 mumol/l) than in the nondiabetic subjects (1.57+/-0.21 mumol/l, p=0.006). MDA concentrations decreased significantly following the start of insulin treatment. CONCLUSIONS: Patients with new-onset, insulin-dependent diabetes mellitus have alpha-tocopherol levels that are similar to those in normal subjects. Insulin treatment and/or improved metabolic control cause a significant decrease in alpha-tocopherol levels during the first months.

Published

2004

99. Rosuvastatin reduces atherosclerosis development beyond and independent of its plasma cholesterol-lowering effect in APOE*3-Leiden transgenic mice: evidence for antiinflammatory effects of rosuvastatin.

Author

Kleemann R, Princen HM, Emeis JJ, Jukema JW, Fontijn RD, Horrevoets AJ, Kooistra T, and Havekes LM

Subjects

Animals, Aorta drug effects, Aorta metabolism, Aorta pathology, Apolipoprotein E3, Arteriosclerosis blood, Arteriosclerosis immunology, Arteriosclerosis pathology, Cell Adhesion, Cholesterol blood, Cytokines metabolism, Female, Lipids blood, Lipoproteins blood, Macrophages immunology, Mice, Mice, Transgenic, Monocytes immunology, Rosuvastatin Calcium, Anti-Inflammatory Agents therapeutic use, Apolipoproteins E genetics, Arteriosclerosis drug therapy, Fluorobenzenes therapeutic use, Hydroxymethylglutaryl-CoA Reductase Inhibitors therapeutic use, Pyrimidines, Sulfonamides

Abstract

Background: Statins can exert anti-inflammatory antiatherosclerotic effects through an anti-inflammatory action, independent of lowering cholesterol. We addressed the question whether the anti-inflammatory activities of statins can reduce atherosclerosis beyond the reduction achieved by cholesterol lowering per se., Methods and Results: Two groups of 20 female APOE*3-Leiden mice received either a high-cholesterol diet (HC) or a high-cholesterol diet supplemented with 0.005% (wt/wt) rosuvastatin (HC+R). The HC diet alone resulted in a plasma cholesterol concentration of 18.9+/-1.4 mmol/L, and administration of rosuvastatin lowered plasma cholesterol to 14.1+/-0.7 mmol/L. In a separate low-cholesterol (LC) control group, the dietary cholesterol intake was reduced, which resulted in plasma cholesterol levels that were comparable to the HC+R group (13.4+/-0.8 mmol/L). Atherosclerosis in the aortic root area was quantified after 24 weeks. As compared with the HC group, the LC group had a 62% (P<0.001) reduction in cross-sectional lesion area. When compared with the LC group, the HC+R group showed a further decrease in cross-sectional lesion area (80%, P<0.001), size of individual lesions (63%, P<0.05), lesion number (58%, P<0.001), monocyte adherence (24%, P<0.05), and macrophage-containing area (60%, P<0.001). Furthermore, rosuvastatin specifically suppressed the expression of the inflammation parameters MCP-1 and TNF-alpha in the vessel wall and lowered plasma concentrations of serum amyloid A and fibrinogen, independent of its cholesterol-lowering effect., Conclusions: Rosuvastatin reduces atherosclerosis beyond and independent of the reduction achieved by cholesterol lowering alone. This additional beneficial effect of rosuvastatin may be explained, at least partly, by its anti-inflammatory activity.

Published

2003

100. Increased fecal bile acid excretion in transgenic mice with elevated expression of human phospholipid transfer protein.

Author

Post SM, de Crom R, van Haperen R, van Tol A, and Princen HM

Subjects

Animals, Biological Transport, Carrier Proteins blood, Carrier Proteins genetics, Cholesterol, HDL blood, Humans, Lipase analysis, Lipoprotein Lipase analysis, Liver metabolism, Male, Membrane Proteins blood, Membrane Proteins genetics, Mice, Mice, Inbred C57BL, Mice, Transgenic, Sterols analysis, Bile Acids and Salts metabolism, Carrier Proteins physiology, Cholesterol metabolism, Feces chemistry, Membrane Proteins physiology, Phospholipid Transfer Proteins

Abstract

Objective: HDL plays a key role in protection against development of atherosclerosis by promoting reverse cholesterol transport from peripheral tissues to the liver for secretion into bile. Phospholipid transfer protein (PLTP) promotes the transfer of phospholipids between lipoproteins and modulates HDL size and composition, thereby having a crucial role in HDL metabolism. We investigated the effect of increased PLTP activity on removal of cholesterol from the body., Methods and Results: On a chow diet, transgenic mice overexpressing human PLTP have a 15-fold increased plasma PLTP activity compared with wild-type mice (572.4+/-59.2 versus 38.6+/-3.6 micromol/mL per h). Plasma cholesterol, mainly present in HDL, is strongly decreased (-92%), caused by a rapid clearance from the circulation by the liver and leading to a 1.8-fold increase in hepatic cholesteryl esters. This results in a 2-fold increase in biliary bile acid secretion without changing the bile saturation index. Consequently, the transgenic mice show a 1.4-fold increase in the amount of excreted fecal bile acids compared with wild-type mice, whereas fecal neutral sterol excretion is unchanged., Conclusions: Our data show that elevation of PLTP activity results in rapid disposal of cholesterol from the body via increased conversion into bile acids and subsequent excretion.

Published

2003