Low‐dose oral sirolimus reduces atherogenesis, vascular inflammation and modulates plaque composition in mice lacking the LDL receptor

Zhao, Liang; Ding, Tao; Cyrus, Tillmann; Cheng, Yong; Tian, Huikai; Ma, Minghong; Falotico, Robert; Praticò, Domenico

doi:10.1111/j.1476-5381.2008.00080.x

Cited by 48 publications

(45 citation statements)

References 34 publications

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“…No studies have addressed this notion directly. However, sirolimus and everolimus, both inhibitors of the autophagy-suppressing kinase mTOR and thus classic stimulators of autophagy, are anti-atherogenic in mice (Castro et al, 2004; Mueller et al, 2008; Pakala et al, 2005; Zhao et al, 2009). Calorie-restricted mice, another stimulus for autophagy induction (Wohlgemuth et al, 2007), also have reduced atherosclerosis (Guo et al, 2002).…”

Section: Discussionmentioning

confidence: 99%

Autophagy Links Inflammasomes to Atherosclerotic Progression

et al. 2012

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SUMMARY We investigated the role of autophagy in atherosclerosis. During plaque formation in mice, autophagic markers co-localized predominantly with macrophages (mϕ). Atherosclerotic aortas had elevated levels of p62, suggesting that dysfunctional autophagy is characteristic of plaques. To determine if autophagy directly influences atherogenesis, we characterized Beclin-1 heterozygous-null and mϕ-specific ATG5-null (ATG5-mϕKO) mice, commonly used models of autophagy haploinsufficiency and deficiency, respectively. Haploinsufficent Beclin-1 mice had no atherosclerotic phenotype, but ATG5-mϕKO mice had increased plaques suggesting an essential role for basal levels of autophagy in atheroprotection. Defective autophagy is associated with pro-atherogenic inflammasome activation. Classic inflammasome markers were robustly induced in ATG5-null mϕ, especially when co-incubated with cholesterol crystals. Moreover, cholesterol crystals appear to be increased in ATG5-mϕKO plaques, suggesting a potentially vicious cycle of crystal formation and inflammasome activation in autophagy-deficient plaques. These results show that autophagy becomes dysfunctional in atherosclerosis and its deficiency promotes atherosclerosis in part through inflammasome hyperactivation.

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Section: Discussionmentioning

confidence: 99%

Autophagy Links Inflammasomes to Atherosclerotic Progression

et al. 2012

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“…by guest on May 9, 2018 http://circres.ahajournals.org/ Downloaded from to decreased LDLR expression. Rapamycin/rapalogs downregulate hepatic LDLR expression in mice via mTORC1, leading to elevated LDL-cholesterol levels.…”

Section: Systemic Administration Of Rapamycin and Rapalogsmentioning

confidence: 99%

“…Administration of rapalogs in mouse or rabbit models of atherosclerosis, either orally or subcutaneously, results in a marked reduction of both plaque size and plaque complexity despite severe hypercholesterolemia. [96][97][98][99][100][101][102][103][104][105] Indeed, rapalogs can prevent accumulation of macrophages and lipids and reduce cell proliferation and intraplaque angiogenesis via mTOR inhibition. 48 However, it is currently not known whether autophagy is involved in these plaque-stabilizing effects.…”

Section: Systemic Administration Of Rapamycin and Rapalogsmentioning

confidence: 99%

Autophagy in Vascular Disease

Meyer

Grootaert

Michiels

et al. 2015

Circulation Research

243

179

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A utophagy is a complex intracellular process that delivers cytoplasmic constituents for degradation into lysosomes.1,2 Three main types of autophagy have been described: (1) microautophagy, comprising direct engulfment of cytoplasmic material by lysosomes via inward invaginations of the lysosomal membrane, (2) macroautophagy, characterized by formation of double-membrane sequestering compartments termed autophagosomes that fuse with lysosomes for delivery of cytoplasmic cargo, and (3) chaperone-mediated autophagy, mediated by a chaperone complex and lysosomal-associated membrane protein type 2A to degrade cytosolic proteins with a specific targeting motif. The term autophagy usually refers to macroautophagy, which is the most prevalent and beststudied form of autophagy. Also in this review, we will focus exclusively on macroautophagy, further cited as autophagy.Autophagy occurs at basal levels in most tissues to allow constitutive turnover of cytosolic components but is stimulated by environmental stress-related signals (eg, nutrient deprivation and oxidative injury) to recycle nutrients and to generate energy for maintenance of cell viability in unfavorable conditions.1 In addition to cellular stress, basal autophagy can be intensified by specific drugs, 3 indicating that the autophagic machinery is a potential therapeutic target for diverse diseases. Indeed, given that autophagy is involved in the prevention

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“…In some studies, CSF isoprostane levels, considered to be a biomarker of oxidative stress (30), which is characteristic of inflammation (31), have been associated with CSF levels of amyloid beta 42 (32). Both oxidative stress and inflammatory mechanisms have also been implicated in depression, and higher plasma isoprostane levels have been observed in elderly depressed patients relative to healthy comparison subjects (33).…”

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confidence: 99%

Lower CSF Amyloid Beta Peptides and Higher F2-Isoprostanes in Cognitively Intact Elderly Individuals With Major Depressive Disorder

Pomara

Bruno²,

Sarreal³

et al. 2012

AJP

121

101

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Objective Major depressive disorder is common in the elderly, and symptoms are often not responsive to conventional antidepressant treatment, especially in the long term. Soluble oligomeric and aggregated forms of amyloid beta peptides, especially amyloid beta 42, impair neuronal and synaptic function. Amyloid beta 42 is the main component of plaques and is implicated in Alzheimer's disease. Amyloid beta peptides also induce a depressive state in rodents and disrupt major neurotransmitter systems linked to depression. The authors assessed whether major depression was associated with CSF levels of amyloid beta, tau protein, and F2-isoprostanes in elderly individuals with major depressive disorder and age-matched nondepressed comparison subjects. Method CSF was obtained from 47 cognitively intact volunteers (major depression group, N=28; comparison group, N=19) and analyzed for levels of soluble amyloid beta, total and phosphorylated tau proteins, and isoprostanes. Results Amyloid beta 42 levels were significantly lower in the major depression group relative to the comparison group, and amyloid beta 40 levels were lower but only approaching statistical significance. In contrast, isoprostane levels were higher in the major depression group. No differences were observed in total and phosphorylated tau proteins across conditions. Antidepressant use was not associated with differences in amyloid beta 42 levels. Conclusions Reduction in CSF levels of amyloid beta 42 may be related to increased brain amyloid beta plaques or decreased soluble amyloid beta production in elderly individuals with major depression relative to nondepressed comparison subjects. These results may have implications for our understanding of the patho-physiology of major depression and for the development of treatment strategies.

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Low‐dose oral sirolimus reduces atherogenesis, vascular inflammation and modulates plaque composition in mice lacking the LDL receptor

Cited by 48 publications

References 34 publications

Autophagy Links Inflammasomes to Atherosclerotic Progression

Autophagy Links Inflammasomes to Atherosclerotic Progression

Autophagy in Vascular Disease

Lower CSF Amyloid Beta Peptides and Higher F2-Isoprostanes in Cognitively Intact Elderly Individuals With Major Depressive Disorder

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