Atherogenic, enlarged, and dysfunctional HDL in human PLTP/apoA-I double transgenic mice

Moerland, Matthijs; Samyn, Hannelore; Gent, Teus van; Jauhiainen, Matti; Metso, Jari; Haperen, Rien van; Grosveld, Frank; Tol, Arie van; Crom, Rini de

doi:10.1194/jlr.m700020-jlr200

Cited by 23 publications

(15 citation statements)

References 56 publications

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“…Higher activity of CETP would facilitate transfer of HDLcholesterol to ApoB-containing lipoproteins, reducing the amount of cholesterol in HDL, reducing HDL particle size and increasing their capacity to accept new cholesterol from cells even when ApoB-containing lipoproteins are removed. This is consistent with several reports that smaller particles are more active in cholesterol efflux [40,41], and our recent finding of a correlation between the ability of plasma to support cholesterol efflux and CETP concentration [12]. It is, however, inconsistent with findings that functionality of HDL particles formed as a result of inhibition of CETP was not impaired [42,43].…”

Section: Discussioncontrasting

confidence: 53%

Advanced glycation end-products (AGEs) and functionality of reverse cholesterol transport in patients with type 2 diabetes and in mouse models

et al. 2012

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Aims/hypothesis We investigated the contribution of AGEs to the impairment of reverse cholesterol transport (RCT) variables in diabetic individuals and in two animal models of diabetic obesity and of renal impairment. Methods The capacity of plasma and HDL from 26 individuals with moderately controlled type 2 diabetes to support cholesterol efflux was compared with 26 age-and sexmatched individuals without diabetes. We also compared the rates of RCT in vivo in two animal models: db/db mice and mice with chronic renal failure. Results Diabetic individuals had characteristic dyslipidaemia and higher levels of plasma AGEs. The capacity of whole plasma, ApoB-depleted plasma and isolated HDL to support cholesterol efflux was greater for diabetic patients compared with controls despite their lower HDL-cholesterol levels. The capacity of plasma to support cholesterol efflux correlated with plasma levels of cholesteryl ester transfer protein and levels of ApoB, but not with levels of AGE. RCT was severely impaired in db/db mice despite elevated HDL-cholesterol levels and no change in AGE concentration, whereas RCT in uraemic mice was unaffected despite elevated AGE levels. Conclusions/interpretation AGEs are unlikely to contribute significantly to the impairment of RCT in type 2 diabetes.

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Section: Discussioncontrasting

confidence: 53%

Advanced glycation end-products (AGEs) and functionality of reverse cholesterol transport in patients with type 2 diabetes and in mouse models

et al. 2012

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“…In the mutPLTP tg mice, the extent of atherosclerosis was comparable to that in the control littermates. In PLTP tg mice, however, increased atherosclerotic lesion sizes were found, consistent with earlier findings in mice overexpressing human PLTP (10,16). The presence of cholate in the diet has been shown to regulate PLTP gene expression in vivo by the nuclear farnesoid X receptor (FXR), because the PLTP promoter contains an FXR response element (35).…”

Section: Discussionsupporting

confidence: 79%

“…Furthermore, plasma PLTP has been identified as an HDL conversion factor. It remodels HDL to generate large particles and small lipid-poor preb-HDL (8)(9)(10). In vitro, HDL conversion depends on phospholipid transfer activity of PLTP (11).…”

mentioning

confidence: 99%

Plasma phospholipid transfer activity is essential for increased atherogenesis in PLTP transgenic mice: a mutation-inactivation study

Samyn

Moerland

Gent

et al. 2008

Journal of Lipid Research

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Plasma phospholipid transfer protein (PLTP) interacts with HDL particles and facilitates the transfer of phospholipids from triglyceride (TG)-rich lipoproteins to HDL. Overexpressing human PLTP in mice increases the susceptibility to atherosclerosis. In human plasma, highactive and low-active forms of PLTP exist. To elucidate the contribution of phospholipid transfer activity to changes in lipoprotein metabolism and atherogenesis, we developed mice expressing mutant PLTP, still able to associate with HDL but lacking phospholipid transfer activity. In mice heterozygous for the LDL receptor, effects of the mutant and normal human PLTP transgene (mutPLTP tg and PLTP tg, respectively) were compared. In PLTP tg mice, plasma PLTP activity was increased 2.9-fold, resulting in markedly reduced HDL lipid levels. In contrast, in mutPLTP tg mice, lipid levels were not different from controls. Furthermore, hepatic VLDL-TG secretion was stimulated in PLTP tg mice, but not in mutPLTP tg mice. When mice were fed a cholesterol-enriched diet, atherosclerotic lesion size in PLTP tg mice was increased more than 2-fold compared with control mice, whereas in mutPLTP tg mice, there was no change. Our findings demonstrate that PLTP transfer activity is essential for the development of atherosclerosis in PLTP transgenic mice, identifying PLTP activity as a possible target to prevent atherogenesis, independent of plasma PLTP concentration.-Samyn, H., M. Moerland, T. van Gent, R. van Haperen, J. Metso, F. Grosveld, M. Jauhiainen, A. van Tol, and R. de Crom. Plasma phospholipid transfer activity is essential for increased atherogenesis in PLTP transgenic mice: a mutation-inactivation study. Phospholipid transfer protein (PLTP) is a multifunctional protein secreted by various cell types into the plasma, where it associates with HDL particles. Plasma PLTP has a central role in cholesterol and lipoprotein metabolism. It mediates the transfer of phospholipids between lipoprotein particles (1, 2). In addition, PLTP in vitro is able to transfer other lipophilic substances such as diacylglycerol (3), cholesterol (4), lipopolysaccharide (5, 6), and a-tocopherol (7), an important anti-oxidant. Furthermore, plasma PLTP has been identified as an HDL conversion factor. It remodels HDL to generate large particles and small lipid-poor preb-HDL (8-10). In vitro, HDL conversion depends on phospholipid transfer activity of PLTP (11).Studies using genetically modified mouse models have provided more insight into the (patho-) physiological role of PLTP in lipoprotein metabolism and the development of atherosclerosis. PLTP-deficient mice have markedly reduced HDL levels (12). These mice are more resistant to atherosclerosis development; this is partly attributable to diminished secretion and lower levels of apolipoprotein B (apoB)-containing lipoproteins and to the increase in bioavailability of vitamin E in these particles (13,14). When overexpressing human PLTP in mice, elevation of plasma PLTP activity levels results in a dose-dependent decrease ...

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“…30 It has also been shown that RCT is less efficient in transgenic mice overexpressing PLTP, which may indicate that elevated levels of PLTP may promote atherogenesis by the accumulation of cholesterol in the blood vessel wall. 31 PLTP activity can be monitored by phospholipid carrying capacity from VLDL and LDL to HDL. PLTP activity is strongly correlated with the concentration of triglycerides in plasma and triglyceride content in HDL particles; this is probably due to the increased ability of phospholipid binding by HDL particles rich in triglycerides.…”

Section: The Role Of Pltp and Cetp In Lipoprotein Metabolismmentioning

confidence: 99%

Plasma lipid transfer proteins: The role of PLTP and CETP in atherogenesis

Chowaniec

Skoczyńska

2018

Adv Clin Exp Med

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Cardiovascular diseases are still the main cause of death in Poland and throughout the world. Independent risk factors of cardiovascular disease, in addition to elevated LDL cholesterol, are both low HDL levels and high levels of non-HDL cholesterol. Plasma phospholipid-transfer protein (PLTP) and cholesteryl ester transfer protein (CETP) both play a major role in the metabolism of those lipoproteins. A lack of these proteins increases HDL and lowers LDL levels. In the light of current knowledge, it seems reasonable to search for compounds that may decrease the activity of CETP, and thus reduce the incidence of cardiovascular disease. Whereas on the one hand there are reports about the adverse effect of torcetrapib and the lack of therapeutic effects of dalcetrapib, on the other hand the question arises whether the CETP inhibitors that are currently in clinical trials will rise to the challenges before them. Currently, it is known that the activity of PLTP, while affecting the metabolism of lipoproteins, especially HDL, plays a major role in atherogenesis. Still, there are some contradictions and controversies about the effect of PLTP on reverse cholesterol transport (RCT). There are a number of studies about the role that PLTP plays in the pathogenesis of various diseases. Further studies are needed to clearly determine the impact of PLTP activity on the formation and development of pathological processes in the cardiovascular system.

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Atherogenic, enlarged, and dysfunctional HDL in human PLTP/apoA-I double transgenic mice

Cited by 23 publications

References 56 publications

Advanced glycation end-products (AGEs) and functionality of reverse cholesterol transport in patients with type 2 diabetes and in mouse models

Advanced glycation end-products (AGEs) and functionality of reverse cholesterol transport in patients with type 2 diabetes and in mouse models

Plasma phospholipid transfer activity is essential for increased atherogenesis in PLTP transgenic mice: a mutation-inactivation study

Plasma lipid transfer proteins: The role of PLTP and CETP in atherogenesis

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