Generation of a Recombinant Apolipoprotein E Variant with Improved Biological Functions

Kypreos, Kyriakos E.; Dijk, Ko Willems van; Havekes, Louis M.; Zannis, Vassilis I.

doi:10.1074/jbc.m413458200

Cited by 34 publications

(20 citation statements)

References 24 publications

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“…In humans and experimental animals plasma apoE levels correlate with plasma triglyceride levels (57,58). On the basis of this information we hypothesized that expression of dn-c-Jun in apoE Ϫ/Ϫ mice would not affect the plasma lipid levels.…”

Section: Discussionmentioning

confidence: 99%

A Dominant Negative Form of the Transcription Factor c-Jun Affects Genes That Have Opposing Effects on Lipid Homeostasis in Mice

Drosatos

Sanoudou

Kypreos

et al. 2007

Journal of Biological Chemistry

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c-Jun is a transcription factor activated by phosphorylation by the stress-activated protein kinase/c-Jun N-terminal kinase pathway in response to extracellular signals and cytokines. We show that adenovirus-mediated gene transfer of the dominant negative form of c-Jun (dn-c-Jun) in C57BL/6 mice increased greatly apoE hepatic mRNA and plasma levels, increased plasma cholesterol, triglyceride, and very low density lipoprotein levels, and resulted in the accumulation of discoidal high density lipoprotein particles. A similar but more severe phenotype was generated by overexpression of the mouse apoE in C57BL/6 mice, suggesting that dyslipidemia induced by dn-c-Jun was the result of apoE overexpression. Unexpectedly, infection of apoE ؊/؊ mice with adenovirus expressing dn-c-Jun reduced plasma cholesterol by 70%, suggesting that dn-c-Jun affected other genes that control plasma cholesterol levels. To identify these genes, we performed whole genome expression analysis (34,000 genes) of isolated livers from two groups of five apoE ؊/؊ mice, infected with adenoviruses expressing either the dn-c-Jun or the green fluorescence protein. Bioinformatic analysis and Northern blotting validation revealed that dn-c-Jun increased 40-fold the apoE mRNA and reduced by 70% the Scd-1 (stearoylCoA-desaturase 1) mRNA. The involvement of Scd-1 in lowering plasma cholesterol was confirmed by restoration of high cholesterol levels of apoE ؊/؊ mice following coinfection with adenoviruses expressing dn-c-Jun and Scd-1. In conclusion, dnc-Jun appears to trigger two opposing events in mice that affect plasma cholesterol and triglyceride levels as follows: one results in apoE overexpression and triggers dyslipidemia and the other results in inhibition of Scd-1 and offsets dyslipidemia.

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Section: Discussionmentioning

confidence: 99%

A Dominant Negative Form of the Transcription Factor c-Jun Affects Genes That Have Opposing Effects on Lipid Homeostasis in Mice

Drosatos

Sanoudou

Kypreos

et al. 2007

Journal of Biological Chemistry

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“…High expression levels of hepatic apoE result in a notable increase in VLDL triglyceride secretion (11,12). The C-terminal domain is required for the promotion of VLDL triglyceride secretion, particularly the hydrophobic amino acids between residues 260 and 270 (13). The multiple roles of apoE in VLDL homeostasis are concentration dependent with low levels of apoE sufficient to promote receptor-mediated lipoprotein clearance and higher concentrations required to induce hypertriglyceridemia.…”

Section: Apoe and Triglyceride-rich Lipoprotein Productionmentioning

confidence: 99%

Apoprotein E as a lipid transport and signaling protein in the blood, liver, and artery wall

Getz

Reardon

2009

Journal of Lipid Research

225

143

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Apoprotein E (apoE) is synthesized by a number of tissues including the liver, brain, adipose tissue, and artery wall. The majority of apoE is found in the plasma associated with specific lipoprotein subclasses and is derived primarily from the liver. However the fact that apoE expression is sustained in nonhepatic tissues suggests that the local production must have some unique functional attribute. ApoE is involved in many steps in lipid and lipoprotein homeostasis, for the triglyceride-rich lipoproteins and for HDL. ApoE is also important for lipid homeostasis in the brain, artery wall, and adipose tissue through its synthesis by glial cells, adipocytes, and macrophages. In addition, nonlipid related functions have also been attributed to apoE, including effects on immune response and inflammation, oxidation, and smooth muscle proliferation and migration. Some of these effects have been shown to be dependent upon different domains of the protein, different concentrations, and lipidation state. Thus, this multifunctional protein impacts normal and pathophysiology at multiple levels.-Getz, G. S., and C. A. Reardon. Apoprotein E as a lipid transport and signaling protein in the blood, liver, and ar tery wall.

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“…Cholesterol input from these lipoproteins induces a downregulation of LDLR and thus a higher concentration of circulating cholesterol (141). It has also been suggested that apoE4-associated hyperlipidemia may be a consequence of deficient lipoprotein lipase activity and/or reduced affinity/visibility of lipoprotein-bound apoE4 (142). The apoE2 and apoE4 phenotypes are associated with increased levels of plasma TGs relative to apoE3.…”

Section: In Peripheral and Brain Lipid Homeostasismentioning

confidence: 99%

Lipid homeostasis and apolipoprotein E in the development and progression of Alzheimer's disease

Lane

Farlow

2005

Journal of Lipid Research

156

127

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Generation of a Recombinant Apolipoprotein E Variant with Improved Biological Functions

Cited by 34 publications

References 24 publications

A Dominant Negative Form of the Transcription Factor c-Jun Affects Genes That Have Opposing Effects on Lipid Homeostasis in Mice

A Dominant Negative Form of the Transcription Factor c-Jun Affects Genes That Have Opposing Effects on Lipid Homeostasis in Mice

Apoprotein E as a lipid transport and signaling protein in the blood, liver, and artery wall

Lipid homeostasis and apolipoprotein E in the development and progression of Alzheimer's disease

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