Dietary Cosupplementation With Vitamin E and Coenzyme Q
            <sub>10</sub>
            Inhibits Atherosclerosis in Apolipoprotein E Gene Knockout Mice

Thomas, Shane R.; Leichtweis, S.; Pettersson, Knut; Croft, Kevin D.; Mori, Trevor A.; Brown, Andrew; Stocker, Roland

doi:10.1161/01.atv.21.4.585

Cited by 126 publications

(82 citation statements)

References 72 publications

(87 reference statements)

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“…5). Both compounds are orally administered, display an excellent safety profile, even at high doses, and are given in combination to increase antioxidant capacity (20,31). We found that treated Mut −/− ;Tg INS-Alb-Mut mice experienced a significant amelioration in the loss of GFR and a normalization of plasma Lcn2 levels compared with untreated animals fed a HP diet, despite exhibiting the same magnitude of elevation of serum metabolites.…”

Section: Discussionmentioning

confidence: 81%

Targeting proximal tubule mitochondrial dysfunction attenuates the renal disease of methylmalonic acidemia

Manoli

Sysol

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

144

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Isolated methylmalonic acidemia (MMA), caused by deficiency of the mitochondrial enzyme methylmalonyl-CoA mutase (MUT), is often complicated by end stage renal disease that is resistant to conventional therapies, including liver transplantation. To establish a viable model of MMA renal disease, Mut was expressed in the liver of Mut −/− mice as a stable transgene under the control of an albumin (INS-Alb- Mut ) promoter. Mut −/− ;Tg INS-Alb- Mut mice, although completely rescued from neonatal lethality that was displayed by Mut −/− mice, manifested a decreased glomerular filtration rate (GFR), chronic tubulointerstitial nephritis and ultrastructural changes in the proximal tubule mitochondria associated with aberrant tubular function, as demonstrated by single-nephron GFR studies. Microarray analysis of Mut −/− ;Tg INS-Alb- Mut kidneys identified numerous biomarkers, including lipocalin-2, which was then used to monitor the response of the GFR to antioxidant therapy in the mouse model. Renal biopsies and biomarker analysis from a large and diverse patient cohort ( ClinicalTrials.gov identifier: NCT00078078) precisely replicated the findings in the animals, establishing Mut −/− ;Tg INS-Alb- Mut mice as a unique model of MMA renal disease. Our studies suggest proximal tubular mitochondrial dysfunction is a key pathogenic mechanism of MMA-associated kidney disease, identify lipocalin-2 as a biomarker of increased oxidative stress in the renal tubule, and demonstrate that antioxidants can attenuate the renal disease of MMA.

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Section: Discussionmentioning

confidence: 81%

Targeting proximal tubule mitochondrial dysfunction attenuates the renal disease of methylmalonic acidemia

Manoli

Sysol

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

144

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“…There is induction of catalase and eNOS in the aorta by vigorous exercise in hypercholesterolemic mice, and vitamin E supplementation in the exercised group does not appear to affect atherosclerosis (32). In contrast, several studies showed clear beneficial effects of vitamin E on lesion progression in hypercholesterolemic mice (37)(38)(39)(40). Consistently, there is increased atherosclerosis in hypercholesterolemic mice deficient in ␣-tocopherol transfer protein and vitamin E (41).…”

mentioning

confidence: 98%

Long-term combined beneficial effects of physical training and metabolic treatment on atherosclerosis in hypercholesterolemic mice

Napoli

Williams-Ignarro

Nigris

et al. 2004

Proc. Natl. Acad. Sci. U.S.A.

105

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CorrectionsPHARMACOLOGY. For the article ''Beneficial effects of antioxidants and L-arginine on oxidation-sensitive gene expression and endothelial NO synthase activity at sites of disturbed shear stress,'' by Filomena de Nigris, Lilach O. Lerman, Sharon Williams Ignarro, Giacomo Sica, Amir Lerman, Wulf Palinski, Louis J. Ignarro, and Claudio Napoli, which appeared in issue 3, February 4, 2003, of Proc. Natl. Acad. Sci. USA (100, 1420-1425 first published January 13, 2003; 10.1073͞pnas.0237367100), the authors should have noted that Louis J. Ignarro developed and markets Niteworks, a dietary supplement of L-arginine, L-citrulline, vitamin E, and vitamin C. Dr. Ignarro is also a member of the Scientific Advisory Board of Herbalife, the distributor of Niteworks. The pathogenic mechanisms by which physical exercise influences atherosclerotic lesion formation remain poorly understood. Because vigorous physical training increases oxidative stress, this study tested the hypothesis that graduated and moderate physical exercise together with metabolic intervention (L-arginine and antioxidants) may contribute to increased vascular protection. Exercise training in mice was induced by graduated swimming. In hypercholesterolemic male mice on an atherogenic high-cholesterol diet, graduated and moderate exercise lowered plasma cholesterol and decreased atherosclerotic lesions compared with sedentary control mice. Antioxidants (1.0% vitamin E added to the chow and 0.05% vitamin C added to the drinking water) and L-arginine (6% in drinking water) supplementation to exercising hypercholesterolemic mice further and synergistically reduced atherosclerosis compared with untreated exercised mice. Arterial oxidation-specific epitopes and systemic oxidative stress were reduced by metabolic intervention. Graduated chronic exercise elicited an increase in production of nitric oxide through increased endothelial nitric oxide synthase expression and ameliorated scavenger activities. Thus, metabolic intervention with L-arginine and antioxidants together with graduated and moderate exercise training reduce atherosclerotic lesion formation.catalase ͉ nitric oxide synthase ͉ vitamin E ͉ oxidative stress ͉ low-density lipoprotein P hysical exercise is a deterrent of cardiovascular disease and atherogenesis in animal models (1-5). Exercise can also positively influence classical risk factors that are associated with coronary heart disease such as diabetes, hypertension, obesity, dyslipidemias, and endothelial dysfunction (6-8). The higher respiration rate during severe physical exercise leads to the generation of more free radicals than the endogenous antioxidant systems can scavenge (9), whereas moderate intensity aerobic exercise enhances endothelium dependent vasodilation in humans (10), and attenuates exercise-induced peroxidation (11) and cardiovascular mortality (12) in the elderly. Moreover, there is an inverse association between intensity of physical activity and the risk of coronary heart disease events (13). A metaanalysis of 51 con...

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“…Vitamin E is the antioxidant used in most of the clinical trials to date. In mouse models of atherosclerosis it has been effective alone 32 or in combination with other antioxidants, 33,34 but most of the studies in rabbits have been negative. 35 Moreover, when administered to humans, vitamin E has been shown to have only a modest inhibitory effect on LDL oxidation ex vivo (delaying copper-induced oxidation by 15 to 20 minutes) but nowhere near the almost complete protection afforded by such a potent antioxidant as probucol (which can delay oxidation for as much as 20 hours).…”

Section: Have the Clinical Trials Been Done With The Right Antioxidanmentioning

confidence: 99%

Is the Oxidative Modification Hypothesis Relevant to Human Atherosclerosis?

2002

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S everal large-scale, double-blind, placebo-controlled trials have shown convincingly that neither ␤-carotene 1-3 nor vitamin E, alone [3][4][5] or in combination with other antioxidant vitamins, 6 reduces the risk of fatal or nonfatal infarction (or other hard clinical end points) in an unselected population of people with established coronary heart disease (CHD) or at high risk of CHD. Two end point trials, much smaller trials that used vitamin E, have reported positive results, 7,8 and one trial, which used ultrasound, showed that a combination of vitamins E and C slowed the progression of carotid artery lesions. 9 However, these are far outweighed by the negative results in the other, much larger trials. Certainly there is no basis for recommending vitamin E supplementation to patients with CHD, especially because it may blunt the effectiveness of hypolipidemic therapy with statins and niacin. 6 A surprisingly large fraction of cardiologists (Ϸ40%) have been recommending such regimens 10 despite warnings that this use was premature. 11 At first glance, it might seem that these negative results close the book and that additional clinical trials of any antioxidants would be pointless. Closer examination, we believe, will show that such a conclusion would be premature and inappropriate. 12 The hypothesis that oxidative modification of LDL plays a significant role in atherogenesis in humans is not necessarily disproved by the failure of these particular clinical trials any more than a negative trial of an ineffectual antibiotic in Pneumococcal pneumonia would prove that pneumonia is not a bacterial disease. The oxidative modification hypothesis is not that vitamin E will ameliorate the human disease but that oxidative modification of LDL and/or other oxidative events play a significant role in human atherogenesis as it does in animal models of atherogenesis. A corollary of the hypothesis is that some appropriate antioxidant intervention, at some appropriate dosage, in appropriately selected patients over an appropriate time interval has the potential to improve prognosis. Otherwise, of course, the role of oxidation would remain of academic interest only. In the present report, we put the currently available information into context by briefly reviewing the origins of the LDL modification hypothesis and explaining why the trials to date have not adequately tested the basic hypothesis, as pointed out by a number of authors. 12-21 It would be a mistake to jettison as irrelevant to humans a hypothesis that is so strongly supported by many epidemiological studies and by so many positive results in several animal models, including nonhuman primates, and with the use of several different antioxidant compounds. 12 Instead, perhaps we should be reexamining the science underlying the hypothesis and asking what additional basic information we need to design trials that will appropriately test the hypothesis. Origins of the Oxidative Modification HypothesisThe concept that circulating LDL must undergo some kind of structura...

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Dietary Cosupplementation With Vitamin E and Coenzyme Q ₁₀ Inhibits Atherosclerosis in Apolipoprotein E Gene Knockout Mice

Cited by 126 publications

References 72 publications

Targeting proximal tubule mitochondrial dysfunction attenuates the renal disease of methylmalonic acidemia

Targeting proximal tubule mitochondrial dysfunction attenuates the renal disease of methylmalonic acidemia

Long-term combined beneficial effects of physical training and metabolic treatment on atherosclerosis in hypercholesterolemic mice

Is the Oxidative Modification Hypothesis Relevant to Human Atherosclerosis?

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Dietary Cosupplementation With Vitamin E and Coenzyme Q 10 Inhibits Atherosclerosis in Apolipoprotein E Gene Knockout Mice

Cited by 126 publications

References 72 publications

Targeting proximal tubule mitochondrial dysfunction attenuates the renal disease of methylmalonic acidemia

Targeting proximal tubule mitochondrial dysfunction attenuates the renal disease of methylmalonic acidemia

Long-term combined beneficial effects of physical training and metabolic treatment on atherosclerosis in hypercholesterolemic mice

Is the Oxidative Modification Hypothesis Relevant to Human Atherosclerosis?

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Product

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Dietary Cosupplementation With Vitamin E and Coenzyme Q ₁₀ Inhibits Atherosclerosis in Apolipoprotein E Gene Knockout Mice