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51. Apolipoprotein M mediates sphingosine-1-phosphate efflux from erythrocytes

Author

Christensen, Pernille M., Bosteen, Markus H., Hajny, Stefan, Nielsen, Lars B., Christoffersen, Christina, Christensen, Pernille M., Bosteen, Markus H., Hajny, Stefan, Nielsen, Lars B., and Christoffersen, Christina

Abstract

Sphingosine-1-phosphate (S1P) is a bioactive lipid implicated in e.g. angiogenesis, lymphocyte trafficking, and endothelial barrier function. Erythrocytes are a main source of plasma S1P together with platelets and endothelial cells. Apolipoprotein M (apoM) in HDL carries 70% of plasma S1P, whereas 30% is carried by albumin. The current aim was to investigate the role of apoM in export of S1P from human erythrocytes. Erythrocytes exported S1P more efficiently to HDL than to albumin, particularly when apoM was present in HDL. In contrast, export of sphingosine to HDL was unaffected by the presence of apoM. The specific ability of apoM to promote export of S1P was independent of apoM being bound in HDL particles. Treatment with MK-571, an inhibitor of the ABCC1 transporter, effectively reduced export of S1P from human erythrocytes to apoM, whereas the export was unaffected by inhibitors of ABCB1 or ATPase. Thus, ABCC1 could be involved in export of S1P from erythrocytes to apoM.

Published
2017

53. Uremia does not affect neointima formation in mice

Author

Aarup, Annemarie, primary, Nielsen, Carsten H., additional, Bisgaard, Line S., additional, Bot, Ilze, additional, El-Ali, Henrik H., additional, Kjaer, Andreas, additional, Nielsen, Lars B., additional, and Pedersen, Tanja X., additional

Published
2017
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55. Sphingosine-1-Phosphate reduces ischemia/reperfusion injury by phosphorylating the gap junction protein Connexin43

Author

Morel, Sandrine, Christoffersen, Christina, Axelsen, Lene N, Montecucco, Fabrizio, Rochemont, Viviane, Frias, Miguel A, Mach, Francois, James, Richard W, Naus, Christian C, Chanson, Marc, Lampe, Paul D, Nielsen, Morten S, Nielsen, Lars B, Kwak, Brenda R, Morel, Sandrine, Christoffersen, Christina, Axelsen, Lene N, Montecucco, Fabrizio, Rochemont, Viviane, Frias, Miguel A, Mach, Francois, James, Richard W, Naus, Christian C, Chanson, Marc, Lampe, Paul D, Nielsen, Morten S, Nielsen, Lars B, and Kwak, Brenda R

Abstract

AIM: Increasing evidence points to lipoprotein composition rather than reverse cholesterol transport in the cardioprotective properties of high-density lipoproteins (HDL). HDL binding to receptors at the surface of cardiomyocytes activates signalling pathways promoting survival, but downstream targets are largely unknown. Here, we investigate the pathways by which the Sphingosine-1-Phosphate (S1P) constituent of HDL limits cell death induced by cardiac ischemia/reperfusion (I/R).METHODS AND RESULTS: Apolipoprotein M (ApoM) transgenic (Apom-Tg) mice, in which plasma S1P is increased by 296%, and wild-type (WT) mice were subjected to in vivo I/R. Infarct size, neutrophil infiltration into the infarcted area and serum Troponin I were less pronounced in Apom-Tg mice. In vitro experiments suggest that this cardioprotection depends on direct effects of S1P on cardiomyocytes, whereas leukocyte recruitment seems only indirectly affected. Importantly, short-term S1P treatment at the onset of reperfusion was sufficient to reduce ischemia/reperfusion injury in isolated perfused hearts. Mechanistic in vitro and ex vivo studies revealed that 5 min of S1P treatment induced phosphorylation of the gap junction protein Connexin43 (Cx43) on Serine368, which was mediated by S1P2 and S1P3, but not by S1P1, receptors in cardiomyocytes. Finally, S1P-induced reduction of infarct size after ex vivo I/R was lost in hearts of mice with a truncated C-terminus of Cx43 (Cx43(K258/KO)) or in which the Serine368 is mutated to a non-phosphorylatable Alanine (Cx43(S368A/S368A)).CONCLUSION: Our study reveals an important molecular pathway by which modulating the apoM/S1P axis has a therapeutic potential in the fight against ischemia/reperfusion injury in the heart.

Published
2016

58. Altered Metabolism of LDL in the Arterial Wall Precedes Atherosclerosis Regression

Author

Bartels, Emil D., Christoffersen, Christina, Lindholm, Marie W., Nielsen, Lars B, Bartels, Emil D., Christoffersen, Christina, Lindholm, Marie W., and Nielsen, Lars B

Abstract

Rationale: Plasma cholesterol lowering is beneficial in patients with atherosclerosis. However, it is unknown how it affects entry and degradation of low-density lipoprotein (LDL) particles in the lesioned arterial wall. Objective: We studied the effect of lipid-lowering therapy on LDL permeability and degradation of LDL particles in atherosclerotic aortas of mice by measuring the accumulation of iodinated LDL particles in the arterial wall. Methods and Results: Cholesterol-fed, LDL receptor–deficient mice were treated with either an anti-Apob antisense oligonucleotide or a mismatch control antisense oligonucleotide once a week for 1 or 4 weeks before injection with preparations of iodinated LDL particles. The anti-Apob antisense oligonucleotide reduced plasma cholesterol by ≈90%. The aortic LDL permeability and degradation rates of newly entered LDL particles were reduced by ≈50% and ≈85% already after 1 week of treatment despite an unchanged pool size of aortic iodinated LDL particles. In contrast, the size, foam cell content, and aortic pool size of iodinated LDL particles of aortic atherosclerotic plaques were not reduced until after 4 weeks of treatment with the anti-Apob antisense oligonucleotide. Conclusions: Improved endothelial barrier function toward the entry of plasma LDL particles and diminished aortic degradation of the newly entered LDL particles precede plaque regression.

Published
2015

63. Reply

Author

Larsen, Steen, Stride, Nis, Hey-Mogensen, Martin, Hansen, Christina N, Bang, Lia E, Bundgaard, Henning, Nielsen, Lars B, Helge, Jørn Wulff, Dela, Flemming, Larsen, Steen, Stride, Nis, Hey-Mogensen, Martin, Hansen, Christina N, Bang, Lia E, Bundgaard, Henning, Nielsen, Lars B, Helge, Jørn Wulff, and Dela, Flemming

Published
2013

64. The apolipoprotein m-sphingosine-1-phosphate axis:biological relevance in lipoprotein metabolism, lipid disorders and atherosclerosis

Author

Arkensteijn, Bas W C, Berbée, Jimmy F P, Rensen, Patrick C N, Nielsen, Lars B, Christoffersen, Christina, Arkensteijn, Bas W C, Berbée, Jimmy F P, Rensen, Patrick C N, Nielsen, Lars B, and Christoffersen, Christina

Abstract

Apolipoprotein M (apoM) is a plasma apolipoprotein that mainly associates with high-density lipoproteins. Hence, most studies on apoM so far have investigated its effect on and association with lipid metabolism and atherosclerosis. The insight into apoM biology recently took a major turn. ApoM was identified as a carrier of the bioactive lipid sphingosine-1-phosphate (S1P). S1P activates five different G-protein-coupled receptors, known as the S1P-receptors 1-5 and, hence, affects a wide range of biological processes, such as lymphocyte trafficking, angiogenesis, wound repair and even virus suppression and cancer. The ability of apoM to bind S1P is due to a lipophilic binding pocket within the lipocalin structure of the apoM molecule. Mice overexpressing apoM have increased plasma S1P concentrations, whereas apoM-deficient mice have decreased S1P levels. ApoM-S1P is able to activate the S1P-receptor-1, affecting the function of endothelial cells, and apoM-deficient mice display impaired endothelial permeability in the lung. This review will focus on the putative biological roles of the new apoM-S1P axis in relation to lipoprotein metabolism, lipid disorders and atherosclerosis.

Published
2013

65. Simvastatin effects on skeletal muscle:relation to decreased mitochondrial function and glucose intolerance

Author

Larsen, Steen, Stride, Nis, Hey-Mogensen, Martin, Hansen, Christina N, Bang, Lia E, Bundgaard, Henning, Nielsen, Lars B, Helge, Jørn W, Dela, Flemming, Larsen, Steen, Stride, Nis, Hey-Mogensen, Martin, Hansen, Christina N, Bang, Lia E, Bundgaard, Henning, Nielsen, Lars B, Helge, Jørn W, and Dela, Flemming

Abstract

Glucose tolerance and skeletal muscle coenzyme Q(10) (Q(10)) content, mitochondrial density, and mitochondrial oxidative phosphorylation (OXPHOS) capacity were measured in simvastatin-treated patients (n = 10) and in well-matched control subjects (n = 9).

Published
2013

66. The plasma concentration of HDL-associated apoM is influenced by LDL receptor-mediated clearance of apoB-containing particles

Author

Christoffersen, Christina, Benn, Marianne, Christensen, Pernille Møller, Gordts, Philip L S M, Roebroek, Anton J M, Frikke-Schmidt, Ruth, Tybjaerg-Hansen, Anne, Dahlbäck, Björn, Nielsen, Lars B, Christoffersen, Christina, Benn, Marianne, Christensen, Pernille Møller, Gordts, Philip L S M, Roebroek, Anton J M, Frikke-Schmidt, Ruth, Tybjaerg-Hansen, Anne, Dahlbäck, Björn, and Nielsen, Lars B

Abstract

ApoM is mainly associated with HDL. Nevertheless, we have consistently observed positive correlations of apoM with plasma LDL cholesterol in humans. Moreover, LDL receptor deficiency is associated with increased plasma apoM in mice. Here, we tested the idea that plasma apoM concentrations are affected by the rate of LDL receptor-mediated clearance of apoB-containing particles. We measured apoM in humans each carrying one of three different LDL receptor mutations (n = 9) or the apoB3500 mutation (n = 12). These carriers had increased plasma apoM (1.34 ± 0.13 µM, P = 0.003, and 1.23 ± 0.10 µM, P = 0.02, respectively) as compared with noncarriers (0.93 ± 0.04 µM). When we injected human apoM-containing HDL into Wt (n = 6) or LDL receptor-deficient mice (n = 6), the removal of HDL-associated human apoM was delayed in the LDL receptor-deficient mice. After 2 h, 54 ± 5% versus 90 ± 8% (P <0.005) of the initial amounts of human apoM remained in the plasma of Wt and LDL receptor-deficient mice, respectively. Finally, we compared the turnover of radio-iodinated LDL and plasma apoM concentrations in 45 normocholesterolemic humans. There was a negative correlation between plasma apoM and the fractional catabolic rate of LDL (r = -0.38, P = 0.009). These data suggest that the plasma clearance of apoM, despite apoM primarily being associated with HDL, is influenced by LDL receptor-mediated clearance of apoB-containing particles.

Published
2012

67. The pro-inflammatory effect of uraemia overrules the anti-atherogenic potential of immunization with oxidized LDL in apoE-/- mice

Author

Pedersen, Tanja X, Binder, Christoph J, Fredrikson, Gunilla N, Nilsson, Jan, Bro, Susanne, Nielsen, Lars B, Pedersen, Tanja X, Binder, Christoph J, Fredrikson, Gunilla N, Nilsson, Jan, Bro, Susanne, and Nielsen, Lars B

Abstract

BACKGROUND: Uraemia increases oxidative stress, plasma titres of antibodies recognizing oxidized low-density lipoprotein (oxLDL) and development of atherosclerosis. Immunization with oxLDL prevents classical, non-uraemic atherosclerosis. We have investigated whether immunization with oxLDL might also prevent uraemia-induced atherosclerosis in apolipoprotein E knockout (apoE-/-) mice. METHODS: ApoE-/- mice were immunized with either native LDL (n = 25), Cu(2+)-oxidized LDL (n = 25), PBS (n = 25), the apolipoprotein B-derived peptide P45 (apoB-peptide P45) conjugated to bovine serum albumin (BSA) (n = 25) or BSA (n = 25) prior to induction of uraemia by 5/6 nephrectomy (NX). RESULTS: Immunization with oxLDL increased plasma titres of immunoglobulin G (IgG) recognizing Cu(2+)-oxLDL and malondialdehyde-modified LDL (MDA-LDL). However, 5/6 NX induced a marked increase in plasma concentrations of anti-oxLDL antibodies as well as pro-atherogenic cytokines [interleukin (IL)-2 (IL-2), IL-4, IL-6 and IL-12)] in native mouse LDL (nLDL)-, oxLDL- and PBS-immunized mice. Even though nLDL- and oxLDL-immunized mice displayed higher anti-MDA-LDL IgG titres than the PBS group, aortic atherosclerosis lesion size was not affected by immunization. Immunization with the apoB-peptide P45, which consistently reduces classical atherosclerosis in non-uraemic mice, also did not reduce lesion size in uraemic apoE-/- mice. CONCLUSION: The results suggest that the pro-inflammatory and pro-atherogenic effect of uraemia overrules the anti-atherogenic potential of oxLDL immunization in apoE-/- mice.

Published
2010

68. Lipoprotein(a) accelerates atherosclerosis in uremic mice

Author

Pedersen, Tanja X, McCormick, Sally P, Tsimikas, Sotirios, Bro, Susanne, Nielsen, Lars B, Pedersen, Tanja X, McCormick, Sally P, Tsimikas, Sotirios, Bro, Susanne, and Nielsen, Lars B

Abstract

Uremic patients have increased plasma lipoprotein(a) [Lp(a)] levels and elevated risk of cardiovascular disease. Lp(a) is a subfraction of LDL, where apolipoprotein(a) [apo(a)] is disulfide bound to apolipoprotein B-100 (apoB). Lp(a) binds oxidized phospholipids (OxPL), and uremia increases lipoprotein-associated OxPL. Thus, Lp(a) may be particularly atherogenic in a uremic setting. We therefore investigated whether transgenic (Tg) expression of human Lp(a) increases atherosclerosis in uremic mice. Moderate uremia was induced by 5/6 nephrectomy (NX) in Tg mice with expression of human apo(a) (n = 19), human apoB-100 (n = 20), or human apo(a) + human apoB [Lp(a)] (n = 15), and in wild-type (WT) controls (n = 21). The uremic mice received a high-fat diet, and aortic atherosclerosis was examined 35 weeks later. LDL-cholesterol was increased in apoB-Tg and Lp(a)-Tg mice, but it was normal in apo(a)-Tg and WT mice. Uremia did not result in increased plasma apo(a) or Lp(a). Mean atherosclerotic plaque area in the aortic root was increased 1.8-fold in apo(a)-Tg (P = 0.025) and 3.3-fold (P = 0.0001) in Lp(a)-Tg mice compared with WT mice. Plasma OxPL, as detected with the E06 antibody, was associated with both apo(a) and Lp(a). In conclusion, expression of apo(a) or Lp(a) increased uremia-induced atherosclerosis. Binding of OxPL on apo(a) and Lp(a) may contribute to the atherogenicity of Lp(a) in uremia.

Published
2010

69. Association of apolipoprotein M with high-density lipoprotein kinetics in overweight-obese men

Author

Ooi, Esther M M, Watts, Gerald F, Chan, Dick C, Nielsen, Lars B, Plomgaard, Peter, Dahlbäck, Bjorn, Barrett, P Hugh R, Ooi, Esther M M, Watts, Gerald F, Chan, Dick C, Nielsen, Lars B, Plomgaard, Peter, Dahlbäck, Bjorn, and Barrett, P Hugh R

Abstract

Udgivelsesdato: 2010-May, OBJECTIVE: The aim of this study was to investigate associations between plasma apoM concentration and HDL apoA-I and apoA-II kinetics in 60 overweight-obese, insulin resistant men. METHODS: Plasma apoM concentration was determined using a sandwich ELISA with two monoclonal antibodies (CV<5%). The kinetics of HDL apoA-I and apoA-II were measured using intravenous administration of D(3)-leucine, gas chromatography-mass spectrometry and multi-compartmental modeling. RESULTS: Plasma apoM was inversely associated with body mass index and positively associated with plasma total cholesterol, LDL cholesterol and HDL cholesterol (p<0.05). There were no associations between plasma apoM and plasma triglyceride, NEFA, insulin, glucose, HOMA score or adiponectin concentrations. Plasma apoM was positively associated with both apoA-I and apoA-II concentrations (r=0.406, p<0.01 and r=0.510, p<0.01, respectively) and negatively associated with HDL apoA-I and apoA-II fractional catabolic rate (FCR) (r=-0.291, p=0.03 and r=-0.291, p=0.026, respectively). No significant associations were observed between plasma apoM and HDL apoA-I and apoA-II production rate. In multivariate regression models, both plasma apoM and triglycerides were significant, independent predictors of HDL apoA-I FCR (adjusted R(2)=16%, p<0.01) and HDL apoA-II FCR (adjusted R(2)=14%, p<0.01). CONCLUSION: ApoM may be a significant, independent predictor of HDL apoA-I and apoA-II catabolism in overweight-obese, insulin resistant men.

Published
2009

70. Plasma apolipoprotein M is reduced in metabolic syndrome but does not predict intima media thickness

Author

Dullaart, Robin P F, Plomgaard, Peter, de Vries, Rindert, Dahlbäck, Björn, Nielsen, Lars B, Dullaart, Robin P F, Plomgaard, Peter, de Vries, Rindert, Dahlbäck, Björn, and Nielsen, Lars B

Abstract

Udgivelsesdato: 2009-Aug, BACKGROUND: Apolipoprotein (apo) M may exert anti-atherogenic properties in experimental studies. Its hepatic gene expression may be linked to glucose and lipid metabolism. Plasma apoM is decreased in obese mouse models. We hypothesized that plasma apoM is lower in metabolic syndrome (MetS) subjects, and determined whether intima media thickness (IMT) is associated with apoM. METHODS: In 19 non-diabetic subjects with and 60 non-diabetic subjects without MetS (NCEP, ATP III criteria), the relationships of plasma apoM with obesity, glucose, insulin, lipids and adipokines, as well as with IMT were determined. RESULTS: Plasma apoM was on average 15% lower in subjects with MetS compared to subjects without MetS (p=0.036). ApoM correlated inversely with body mass index and waist circumference (p<0.001), and positively with total cholesterol, LDL cholesterol and apoA-I (p<0.05). ApoM was not significantly correlated with glucose, insulin, leptin, adiponectin or resistin (p>0.20). Age- and sex adjusted IMT was lower in subjects with MetS (p<0.05), but was unrelated to apoM (p=0.68). In a multiple linear regression model that included the presence of both MetS and apoM, IMT was only related to MetS (p=0.05). CONCLUSIONS: Plasma apoM is reduced in MetS. In this study, apoM did not predict subclinical atherosclerosis.

Published
2009

71. ApoM: gene regulation and effects on HDL metabolism

Author

Nielsen, Lars B, Christoffersen, Christina, Ahnström, Josefin, Dahlbäck, Björn, Nielsen, Lars B, Christoffersen, Christina, Ahnström, Josefin, and Dahlbäck, Björn

Abstract

Udgivelsesdato: 2009-Mar, The recently discovered apolipoprotein M (apoM) is a plasma protein of the lipocalin family associated with the lipoproteins (mainly high-density lipoproteins, or HDLs). Expression of the apoM gene in the liver is regulated by transcription factors that control key steps in hepatic lipid and glucose metabolism. Although the concentration of plasma apoM correlates with that of cholesterol, apoM was not identified as a risk factor for cardiovascular disease in two prospective studies. In genetically modified mice, however, changes in plasma apoM concentration caused quantitative and qualitative changes in HDLs, and overexpression of the apoM gene reduced atherosclerosis. In conclusion, it seems that apoM plays a part in lipoprotein metabolism; however, the biological impact of apoM in humans remains to be determined.

Published
2009

72. Cardiac expression of microsomal triglyceride transfer protein is increased in obesity and serves to attenuate cardiac triglyceride accumulation

Author

Bartels, Emil D, Nielsen, Jan M, Hellgren, Lars I, Ploug, Thorkil, Nielsen, Lars B, Bartels, Emil D, Nielsen, Jan M, Hellgren, Lars I, Ploug, Thorkil, and Nielsen, Lars B

Abstract

Udgivelsesdato: 2009-null, Obesity causes lipid accumulation in the heart and may lead to lipotoxic heart disease. Traditionally, the size of the cardiac triglyceride pool is thought to reflect the balance between uptake and beta-oxidation of fatty acids. However, triglycerides can also be exported from cardiomyocytes via secretion of apolipoproteinB-containing (apoB) lipoproteins. Lipoprotein formation depends on expression of microsomal triglyceride transfer protein (MTP); the mouse expresses two isoforms of MTP, A and B. Since many aspects of the link between obesity-induced cardiac disease and cardiac lipid metabolism remain unknown, we investigated how cardiac lipoprotein synthesis affects cardiac expression of triglyceride metabolism-controlling genes, insulin sensitivity, and function in obese mice. Heart-specific ablation of MTP-A in mice using Cre-loxP technology impaired upregulation of MTP expression in response to increased fatty acid availability during fasting and fat feeding. This resulted in cardiac triglyceride accumulation but unaffected cardiac insulin-stimulated glucose uptake. Long-term fat-feeding of male C57Bl/6 mice increased cardiac triglycerides, induced cardiac expression of triglyceride metabolism-controlling genes and attenuated heart function. Abolishing cardiac triglyceride accumulation in fat-fed mice by overexpression of an apoB transgene in the heart prevented the induction of triglyceride metabolism-controlling genes and improved heart function. The results suggest that in obesity, the physiological increase of cardiac MTP expression serves to attenuate cardiac triglyceride accumulation albeit without major effects on cardiac insulin sensitivity. Nevertheless, the data suggest that genetically increased lipoprotein secretion prevents development of obesity-induced lipotoxic heart disease.

Published
2009

73. Effect of treatment with human apolipoprotein A-I on atherosclerosis in uremic apolipoprotein-E deficient mice

Author

Pedersen, Tanja Xenia, Bro, Susanne, Andersen, Mikkel H, Etzerodt, Michael, Jauhiainen, Matti, Moestrup, Søren, Nielsen, Lars B, Pedersen, Tanja Xenia, Bro, Susanne, Andersen, Mikkel H, Etzerodt, Michael, Jauhiainen, Matti, Moestrup, Søren, and Nielsen, Lars B

Abstract

Udgivelsesdato: 2009-Feb, OBJECTIVE: Uremia markedly increases the risk of atherosclerosis. Thus, effective anti-atherogenic treatments are needed for uremic patients. This study examined effects of non-lipidated recombinant human apoA-I (h-apoA-I) and a recombinant trimeric apoA-I molecule (TripA-I) on lipid metabolism and atherosclerosis in uremic apoE-/- mice. METHODS AND RESULTS: Upon intraperitoneal injection, h-apoA-I and TripA-I rapidly associated with plasma HDL and reduced mouse apoA-I plasma levels without affecting total or HDL cholesterol concentrations. The plasma half-life was approximately 36 h for TripA-I and approximately 16 h for h-apoA-I. Injection of h-apoA-I (100mg/kg) or TripA-I (100mg/kg) twice weekly for 7 weeks did not affect the cross-sectional area of atherosclerotic lesions in the aortic root, or the en face lesion area and cholesterol content in the thoracic aorta in uremic apoE-/- mice. Also, the treatments did not affect expression of selected inflammatory genes in the thoracic aorta or plasma concentrations of soluble ICAM-1 and VCAM-1. However, h-apoA-I-treated mice had larger smooth muscle cell-staining areas in aortic root plaques than PBS-treated mice (4.8+/-0.8% vs. 2.5+/-0.6%, P<0.05). CONCLUSIONS: The data suggest that long-term treatment with non-lipidated h-apoA-I or TripA-I might affect plaque composition but does not reduce atherosclerotic lesion size in uremic apoE-/- mice.

Published
2009

74. Progestins oppose the effects of estradiol on the endothelin-1 receptor type B in coronary arteries from ovariectomized hyperlipidemic rabbits

Author

Pedersen, Susan H, Nielsen, Lars B, Mortensen, Alicja, Nilas, Lisbeth, Ottesen, Bent, Pedersen, Susan H, Nielsen, Lars B, Mortensen, Alicja, Nilas, Lisbeth, and Ottesen, Bent

Abstract

Udgivelsesdato: null-null, OBJECTIVE: Progestins may be associated with the adverse cardiovascular outcomes observed with estrogen plus progestogen therapy, but the mechanism is not resolved. In this study we examined the effect of 17beta-estradiol (E2) alone and in combination with two progestins on the endothelin-1 (ET-1) system in coronary arteries. DESIGN: Watanabe heritable hyperlipidemic rabbits were treated orally with either E2 (4 mg/d), medroxyprogesterone acetate (MPA) (10 mg/d), norethisterone acetate (NETA) (2 mg/d), E2 + MPA, E2 + NETA, or placebo for 16 weeks (n=10 in each group). Coronary arteries were used for mRNA and myograph analyses. RESULTS: E2 alone but not in combination with MPA or NETA increased ETB mRNA expression in coronary arteries. Accordingly, E2 alone but not in combination with MPA or NETA reduced the maximal contraction to ET-1, and the reduction was sustained after ETA but not after ETB blockade. E2 reduced preproendothelin-1 mRNA expression; however, this effect was not blunted by MPA or NETA. ETA and ET-converting enzyme-1 mRNA expression was unaffected by treatment. CONCLUSIONS: The data suggest that long-term E2 treatment selectively attenuates ET-1-induced vasoconstriction, possibly by increasing ETB gene expression in rabbit coronary arteries and that this effect is abolished by the two progestins investigated. This observation may help to explain how progestins oppose the supposed beneficial effects of estrogen on the arterial wall.

Published
2008

75. Increased LDL cholesterol and CRP in infants of mothers with type 1 diabetes

Author

Lindegaard, Marie Louise Skakkebæk, Svarrer, Eva Martha Madsen, Damm, Peter, Mathiesen, E.R., Nielsen, Lars Bo, Mathiesen, Elisabeth R, Nielsen, Lars B, Lindegaard, Marie Louise Skakkebæk, Svarrer, Eva Martha Madsen, Damm, Peter, Mathiesen, E.R., Nielsen, Lars Bo, Mathiesen, Elisabeth R, and Nielsen, Lars B

Abstract

Proatherogenic stimuli during foetal life may predispose to development of atherosclerosis in adulthood. Elevated plasma low-density lipoprotein (LDL) cholesterol and C-reactive protein (CRP) expression is associated with increased risk of atherosclerosis.

Published
2008

77. Reply

Author

Larsen, Steen, primary, Stride, Nis, additional, Hey-Mogensen, Martin, additional, Hansen, Christina N., additional, Bang, Lia E., additional, Bundgaard, Henning, additional, Nielsen, Lars B., additional, Helge, Jørn W., additional, and Dela, Flemming, additional

Published
2013
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78. Familial Hypercholesterolemia and Atherosclerosis in Cloned Minipigs Created by DNA Transposition of a Human PCSK9 Gain-of-Function Mutant

Author

Al-Mashhadi, Rozh H., primary, Sørensen, Charlotte B., additional, Kragh, Peter M., additional, Christoffersen, Christina, additional, Mortensen, Martin B., additional, Tolbod, Lars P., additional, Thim, Troels, additional, Du, Yutao, additional, Li, Juan, additional, Liu, Ying, additional, Moldt, Brian, additional, Schmidt, Mette, additional, Vajta, Gabor, additional, Larsen, Torben, additional, Purup, Stig, additional, Bolund, Lars, additional, Nielsen, Lars B., additional, Callesen, Henrik, additional, Falk, Erling, additional, Mikkelsen, Jacob Giehm, additional, and Bentzon, Jacob F., additional

Published
2013
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79. Simvastatin Effects on Skeletal Muscle

Author

Larsen, Steen, primary, Stride, Nis, additional, Hey-Mogensen, Martin, additional, Hansen, Christina N., additional, Bang, Lia E., additional, Bundgaard, Henning, additional, Nielsen, Lars B., additional, Helge, Jørn W., additional, and Dela, Flemming, additional

Published
2013
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80. Effect of uremia on HDL composition, vascular inflammation, and atherosclerosis in wild-type mice

Author

Bang, Christian A, Bro, Susanne, Bartels, Emil D, Pedersen, Tanja X, Nielsen, Lars B, Bang, Christian A, Bro, Susanne, Bartels, Emil D, Pedersen, Tanja X, and Nielsen, Lars B

Abstract

Udgivelsesdato: 2007-Oct, Wild-type mice normally do not develop atherosclerosis, unless fed cholic acid. Uremia is proinflammatory and increases atherosclerosis 6- to 10-fold in apolipoprotein E-deficient mice. This study examined the effect of uremia on lipoproteins, vascular inflammation, and atherosclerosis in wild-type C57BL/6J mice. Uremia was induced by nephrectomy (NX) and increased plasma urea and creatinine concentrations 2.5- to 4.5-fold; control mice were sham operated. After NX, mice were fed a Western-type diet or the same diet with 0.5% cholic acid. Cholic acid-fed NX mice did not thrive and were killed. In NX mice fed the Western-type diet (n = 7), the total plasma cholesterol concentration was similar to that in sham mice (n = 11), but on gel filtration the LDL/HDL cholesterol ratio was increased. HDL from NX mice contained more serum amyloid A and triglycerides and less cholesterol than HDL from sham mice. Plasma concentrations of sICAM-1 and sVCAM-1 and aortic mRNA expression of ICAM-1 and VCAM-1 did not differ between NX and sham mice. Twenty-six weeks after NX, the average oil red O-stained area of the aortic root was similar in NX and sham mice fed the Western-type diet, while it was increased in cholic acid-fed sham mice. The results suggest that moderate uremia neither induces aortic inflammation nor atherosclerosis in C57BL/6J mice despite increased LDL/HDL cholesterol ratio and altered HDL composition.

Published
2007

81. Endothelial lipase is highly expressed in macrophages in advanced human atherosclerotic lesions

Author

Bartels, Emil D, Nielsen, John E, Lindegaard, Marie Louise Skakkebæk, Hulten, Lillemor M, Schroeder, Torben V, Nielsen, Lars B, Bartels, Emil D, Nielsen, John E, Lindegaard, Marie Louise Skakkebæk, Hulten, Lillemor M, Schroeder, Torben V, and Nielsen, Lars B

Abstract

Endothelial lipase (EL) is expressed in endothelial cells, and affects plasma lipoprotein metabolism by hydrolyzing phospholipids in HDL. To determine the cellular expression of EL mRNA and protein in human atherosclerotic lesions, we performed in situ hybridization and immunohistochemical studies on sections of carotid endarterectomy specimens from patients with symptomatic cerebrovascular disease. In each of eight patients, EL mRNA and/or protein were seen in areas between the necrotic core and the fibrotic cap where they colocalized with LPL and macrophage-specific CD68. Moreover, there was a positive association between the expression of EL mRNA and CD68 mRNA in plaques from 26 patients. The impact of differentiation from monocytes into macrophages, and subsequently foam cells (by incubation with acetylated LDL) on expression was studied using THP-1 monocytes and primary human monocytes. EL mRNA expression increased markedly when either type of monocytes was differentiated into macrophages. Upon further differentiation into foam cells EL mRNA decreased whereas protein levels remained high compared to monocytes. In conclusion, macrophages in advanced human atherosclerotic lesions display high levels of EL expression, and the level of EL expression varies greatly during transformation of blood monocytes into foam cells.

Published
2007

82. Human Apolipoprotein B Transgenic Mice Generated with 207- and 145-Kilobase Pair Bacterial Artificial Chromosomes. Evidence that a distant 5'-element confers appropriate transgene expression in the intestine

Author

Nielsen, Lars B., McCormick, Sally P. A., Pierotti, Vincenzo, Tam, Carmen, Gunn, Michael D., Shizuya, Hiroaki, and Young, Stephen G.

Subjects
lipids (amino acids, peptides, and proteins), Caltech Library Services
Abstract

We reported previously that ~80-kilobase pair (kb) P1 bacteriophage clones spanning either the human or mouse apoB gene (clones p158 and p649, respectively) confer apoB expression in the liver of transgenic mice, but not in the intestine. We hypothesized that the absence of intestinal expression was due to the fact that these clones lacked a distant DNA element controlling intestinal expression. To test this possibility, transgenic mice were generated with 145- and 207-kb bacterial artificial chromosomes (BACs) that contained the human apoB gene and more extensive 5'- and 3'-flanking sequences. RNase protection, in situ hybridization, immunohistochemical, and genetic complementation studies revealed that the BAC transgenic mice manifested appropriate apoB gene expression in both the intestine and the liver, indicating that both BACs contained the distant intestinal element. To determine whether the regulatory element was located 5' or 3' to the apoB gene, transgenic mice were generated by co-microinjecting embryos with p158 and either the 5'- or 3'-sequences from the 145-kb BAC. Analysis of these mice indicated that the apoB gene's intestinal element is located 5' to the structural gene. Cumulatively, the transgenic mouse studies suggest that the intestinal element is located between -33 and -70 kb 5' to the apoB gene.

Published
1997

83. Placental triglyceride accumulation in maternal type 1 diabetes is associated with increased lipase gene expression

Author

Lindegaard, Marie Louise Skakkebæk, Damm, Peter, Mathiesen, Elisabeth R, Nielsen, Lars B, Lindegaard, Marie Louise Skakkebæk, Damm, Peter, Mathiesen, Elisabeth R, and Nielsen, Lars B

Abstract

Maternal diabetes can cause fetal macrosomia and increased risk of obesity, diabetes, and cardiovascular disease in adulthood of the offspring. Although increased transplacental lipid transport could be involved, the impact of maternal type 1 diabetes on molecular mechanisms for lipid transport in placenta is largely unknown. To examine whether maternal type 1 diabetes affects placental lipid metabolism, we measured lipids and mRNA expression of lipase-encoding genes in placentas from women with type 1 diabetes (n = 27) and a control group (n = 21). The placental triglyceride (TG) concentration and mRNA expression of endothelial lipase (EL) and hormone-sensitive lipase (HSL) were increased in placentas from women with diabetes. The differences were more pronounced in women with diabetes and suboptimal metabolic control than in women with diabetes and good metabolic control. Placental mRNA expression of lipoprotein lipase and lysosomal lipase were similar in women with diabetes and the control group. Immunohistochemistry showed EL protein in syncytiotrophoblasts facing the maternal blood and endothelial cells facing the fetal blood in placentas from both normal women and women with diabetes. These results suggest that maternal type 1 diabetes is associated with TG accumulation and increased EL and HSL gene expression in placenta and that optimal metabolic control reduces these effects.

Published
2006

84. Endothelial and lipoprotein lipases in human and mouse placenta.

Author

Lindegaard, Marie L S, Olivecrona, Gunilla, Christoffersen, Christina, Kratky, Dagmar, Hannibal, Jens, Petersen, Bodil L, Zechner, Rudolf, Damm, Peter, Nielsen, Lars B, Lindegaard, Marie L S, Olivecrona, Gunilla, Christoffersen, Christina, Kratky, Dagmar, Hannibal, Jens, Petersen, Bodil L, Zechner, Rudolf, Damm, Peter, and Nielsen, Lars B

Published
2005

85. Endothelial and lipoprotein lipases in human and mouse placenta

Author

Lindegaard, Marie Louise Skakkebæk, Olivecrona, Gunilla, Christoffersen, Christina, Kratky, Dagmar, Hannibal, Jens, Petersen, Bodil L, Zechner, Rudolf, Damm, Peter, Nielsen, Lars B, Lindegaard, Marie Louise Skakkebæk, Olivecrona, Gunilla, Christoffersen, Christina, Kratky, Dagmar, Hannibal, Jens, Petersen, Bodil L, Zechner, Rudolf, Damm, Peter, and Nielsen, Lars B

Abstract

Placenta expresses various lipase activities. However, a detailed characterization of the involved genes and proteins is lacking. In this study, we compared the expression of endothelial lipase (EL) and LPL in human term placenta. When placental protein extracts were separated by heparin-Sepharose affinity chromatography, the EL protein eluted as a single peak without detectable phospholipid or triglyceride (TG) lipase activity. The major portion of LPL protein eluted slightly after EL. This peak also had no lipase activity and most likely contained monomeric LPL. Fractions eluting at a higher NaCl concentration contained small amounts of LPL protein (most likely dimeric LPL) and had substantial TG lipase activity. In situ hybridization studies showed EL mRNA expression in syncytiotrophoblasts and endothelial cells and LPL mRNA in syncytiotrophoblasts. In contrast, immunohistochemistry showed EL and LPL protein associated with both cell types. In mouse placentas, lack of LPL expression resulted in increased EL mRNA expression. These results suggest that the cellular expression of EL and LPL in human placenta is different. Nevertheless, the two lipases might have overlapping functions in the mouse placenta. Our data also suggest that the major portions of both proteins are stored in an inactive form in human term placenta.

Published
2005

86. Increased plasma pro-B-type natriuretic peptide in infants of women with type 1 diabetes

Author

Halse, Karen G, Lindegaard, Marie Louise Skakkebæk, Goetze, Jens P, Damm, Peter, Mathiesen, Elisabeth R, Nielsen, Lars B, Halse, Karen G, Lindegaard, Marie Louise Skakkebæk, Goetze, Jens P, Damm, Peter, Mathiesen, Elisabeth R, and Nielsen, Lars B

Abstract

Up to 40% of newborn infants of women with type 1 diabetes have echocardiographic signs of cardiomyopathy. Increased plasma concentrations of B-type natriuretic peptide (BNP) and its precursor (proBNP) are markers of cardiac failure and hypoxia in adults. In this study, we investigated whether plasma concentrations of proBNP and/or BNP are increased in infants of women with type 1 diabetes.

Published
2005

89. Human placenta secretes apolipoprotein B-100-containing lipoproteins

Author

Munk-Madsen, Eva, Lindegaard, Marie Louise Skakkebæk, Andersen, Claus B, Damm, Peter, Nielsen, Lars B, Munk-Madsen, Eva, Lindegaard, Marie Louise Skakkebæk, Andersen, Claus B, Damm, Peter, and Nielsen, Lars B

Abstract

Supply of lipids from the mother is essential for fetal growth and development. In mice, disruption of yolk sac cell secretion of apolipoprotein (apo) B-containing lipoproteins results in embryonic lethality. In humans, the yolk sac is vestigial. Nutritional functions are instead established very early during pregnancy in the placenta. To examine whether the human placenta produces lipoproteins, we examined apoB and microsomal triglyceride transfer protein (MTP) mRNA expression in placental biopsies. ApoB and MTP are mandatory for assembly and secretion of apoB-containing lipoproteins. Both genes were expressed in placenta and microsomal extracts from human placenta contained triglyceride transfer activity, indicating expression of bioactive MTP. To detect lipoprotein secretion, biopsies from term placentas were placed in medium with [(35)S]methionine and [(35)S]cysteine for 3-24 h. Upon sucrose gradient ultracentrifugation of the labeled medium, fractions were analyzed by apoB-immunoprecipitation. (35)S-labeled apoB-100 was recovered in d approximately 1.02-1.04 g/ml particles (i.e. similar to the density of plasma low density lipoproteins). Electron microscopy of negatively stained lipoproteins secreted from placental tissue showed spherical particles with a diameter of 47 +/- 10 nm. These results demonstrate that human placenta expresses both apoB and MTP and consequently synthesize and secrete apoB-100-containing lipoproteins. Placental lipoprotein formation constitutes a novel pathway of lipid transfer from the mother to the developing fetus.

Published
2004

90. Photonic crystal fiber based evanescent-wave sensor for detection of biomolecules in aqueous solutions

Author

Jensen, Jesper Bo Damm, Pedersen, Lars H., Hoiby, Poul E., Nielsen, Lars B., Hansen, Theis Peter, Folkenberg, Jacob Riis, Riishede, Jesper, Noordegraaf, Danny, Nielsen, Kristian, Carlsen, Anneline, Bjarklev, Anders Overgaard, Jensen, Jesper Bo Damm, Pedersen, Lars H., Hoiby, Poul E., Nielsen, Lars B., Hansen, Theis Peter, Folkenberg, Jacob Riis, Riishede, Jesper, Noordegraaf, Danny, Nielsen, Kristian, Carlsen, Anneline, and Bjarklev, Anders Overgaard

Abstract

We demonstrate highly efficient evanescent-wave detection of fluorophore-labeled biomolecules in aqueous solutions positioned in the air holes of the microstructured part of a photonic crystal fiber. The air-suspended silica structures located between three neighboring air holes in the cladding crystal guide light with a large fraction of the optical field penetrating into the sample even at wavelengths in the visible range. An effective interaction length of several centimeters is obtained when a sample volume of less than 1 µL is used.

Published
2004

94. Chamber-dependent expression of brain natriuretic peptide and its mRNA in normal and diabetic pig heart

Author

Christoffersen, Christina, Goetze, Jens P, Bartels, Emil D, Larsen, Tina Marianne, Ribel, Ulla, Rehfeld, Jens F, Rolin, Bidda, Nielsen, Lars B, Christoffersen, Christina, Goetze, Jens P, Bartels, Emil D, Larsen, Tina Marianne, Ribel, Ulla, Rehfeld, Jens F, Rolin, Bidda, and Nielsen, Lars B

Abstract

Brain natriuretic peptide (BNP) is produced in cardiac myocytes, and increased secretion is closely associated with cardiac dysfunction. However, several fundamental aspects of BNP expression in the myocardium have not yet been resolved. In the present study, we report the presence of a precursor BNP mRNA transcript and a mature BNP mRNA transcript in normal porcine hearts. In normal pigs, the amount of precursor BNP mRNA was similar in atrial and ventricular myocardium, whereas the mature BNP transcript was 10- to 50-fold more abundant in atrial than in ventricular myocardium. Quantitation of proBNP in normal porcine hearts by radioimmunoassay disclosed abundant proBNP in the atria, whereas proBNP was undetectable in the ventricles. Laser confocal microscopy revealed proBNP in secretory granules of atrial but not in the ventricular myocardium of normal pigs. Mild streptozotocin-induced diabetes doubled the expression of BNP mRNA in porcine atrial myocardium (P=0.03), but was without effect on BNP mRNA in the ventricular myocardium. The data suggest that BNP mRNA processing and proBNP storage differ between the atrial and ventricular myocardium. The results also imply that diabetes increases cardiac BNP expression in a chamber-dependent manner.

Published
2002

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