Hepatic Lipase Deficiency Delays Atherosclerosis, Myocardial Infarction, and Cardiac Dysfunction and Extends Lifespan in SR-BI/Apolipoprotein E Double Knockout Mice

Karackattu, Sharon L.; Trigatti, Bernardo L.; Krieger, Monty

doi:10.1161/01.atv.0000202662.63876.02

Cited by 31 publications

(31 citation statements)

References 56 publications

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“…However, the double apo E/SR-BI KO mice have increased cholesterol (serum cholesterol levels 800 to 1000 mg/dl) and accelerated atherosclerosis ( 4 weeks of age) [119]. Yu et al [120] found that macrophage apo E promotes reductions in serum cholesterol levels, improves HDL subpopulations, provides extensive protection from atherosclerotic lesion development, and prevents premature death in double apo E/SR-BI KO mice [120,121]. Furthermore, treatment of SR-BI/apo E KO mice with probucol (a lipid lowering drug) extended their lives (from 6 to 36 weeks) and essentially reversed all early-onset CHD-associated anatomical, functional, cellular and biochemical pathology [118].…”

Section: Scavenger Receptor Class B Type I (Sr-bi)mentioning

confidence: 99%

Apolipoprotein E Knockout Models

Kolovou¹,

Anagnostopoulou²,

Mikhailidis³

et al. 2008

CPD

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Atherosclerosis is a multifactorial and long-lasting process in humans. Therefore, animal models where more rapid changes occur can be useful for the study of this process. Among such models are the apolipoprotein (apo) E knock out mice. Apo E deficient mice show impaired clearing of plasma lipoproteins and they develop atherosclerosis in a short time. The current review considers lipid metabolism and inflammation as well as nutritional and pharmacological agents affecting atherosclerosis, using the apo E knock out mouse model.

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Section: Scavenger Receptor Class B Type I (Sr-bi)mentioning

confidence: 99%

Apolipoprotein E Knockout Models

Kolovou¹,

Anagnostopoulou²,

Mikhailidis³

et al. 2008

CPD

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“…Studies show that (a) HL is a liver-secreted enzyme that hydrolyzes triglycerides and phospholipids and is involved in processing large lipid-rich HDL into smaller HDL particles (18), and (b) the ligand-binding activity of HL may mediate interactions of lipoproteins with SR-BI or the plasma membrane, thus facilitating selective HDL-CE uptake (19)(20)(21)(22)(23)(24). As such, mice lacking expression of either SR-BI or HL have elevated levels of HDL-C and impaired HDL-C clearance by hepatocytes (14,(25)(26)(27)(28).…”

Section: Introductionmentioning

confidence: 99%

FoxO transcription factors are required for hepatic HDL cholesterol clearance

Lee¹,

Heine²,

Schlein³

et al. 2018

Journal of Clinical Investigation

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“…The influence of SR-BI on murine atherosclerosis has been examined in both the LDL receptor and apoE knockout models. Hepatic overexpression of SR-BI suppresses and loss of SR-BI expression enhances atherosclerosis in these models (45)(46)(47)(48)(49)(50)(51)(52)(53)(54)(55). The atheroprotective activity of SR-BI, even though its expression decreases plasma HDLcholesterol levels, suggests that SR-BI's role in reverse cholesterol transport (the movement of cholesterol from peripheral tissues to the liver and then excretion in the bile) may contribute to its protective activity in mice.…”

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confidence: 99%

Influence of HDL-cholesterol-elevating drugs on the in vitro activity of the HDL receptor SR-BI

Nieland

Shaw

Jaipuri

et al. 2007

Journal of Lipid Research

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Treatment of atherosclerotic disease often focuses on reducing plasma LDL-cholesterol or increasing plasma HDL-cholesterol. We examined in vitro the effects on HDL receptor [scavenger receptor class B type I (SR-BI)] activity of three classes of clinical and experimental plasma HDL-cholesterol-elevating compounds: niacin, fibrates, and HDL376. Fenofibrate (FF) and HDL376 were potent (IC 50 ? 1 mM), direct inhibitors of SR-BI-mediated lipid transport in cells and in liposomes reconstituted with purified SR-BI. FF, a prodrug, was a more potent inhibitor of SR-BI than an activator of peroxisome proliferator-activated receptor a, a target of its active fenofibric acid (FFA) derivative. Nevertheless, FFA, four other fibrates (clofibrate, gemfibrozil, ciprofibrate, and bezafibrate), and niacin had little, if any, effect on SR-BI, suggesting that they do not directly target SR-BI in vivo. However, similarities of HDL376 treatment and SR-BI gene knockout on HDL metabolism in vivo (increased HDL-cholesterol and HDL particle sizes) and structure-activity relationship analysis suggest that SR-BI may be a target of HDL376 in vivo. HDL376 and other inhibitors may help elucidate SR-BI function in diverse mammalian models and determine the therapeutic potential of SR-BI-directed pharmaceuticals.-Nieland, T.

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Hepatic Lipase Deficiency Delays Atherosclerosis, Myocardial Infarction, and Cardiac Dysfunction and Extends Lifespan in SR-BI/Apolipoprotein E Double Knockout Mice

Cited by 31 publications

References 56 publications

Apolipoprotein E Knockout Models

Apolipoprotein E Knockout Models

FoxO transcription factors are required for hepatic HDL cholesterol clearance

Influence of HDL-cholesterol-elevating drugs on the in vitro activity of the HDL receptor SR-BI

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