Antagonistic Effects of Oxidized Low Density Lipoprotein and α-Tocopherol on CD36 Scavenger Receptor Expression in Monocytes

Munteanu, Adelina; Taddei, Michele; Tamburini, Ilaria; Bergamini, Ettore; Azzi, Angelo; Zingg, Jean‐Marc

doi:10.1074/jbc.m508799200

Cited by 87 publications

(100 citation statements)

References 100 publications

(88 reference statements)

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Several studies have shown the central role of CD36 in the development of atherosclerotic plaques by increasing the cellular uptake of modified LDL (9,10,19,21). CD36 expression is often increased at the atherosclerotic lesion by triggers such as oxLDL via PKB and PPARg activation (21). Interestingly, oxLDL has also been shown to inhibit the proteasome (63) and increased levels of ubiquitinated proteins and decreased proteasome activity were detected in unstable atherosclerotic plaques (12,64).…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Modulation of Proteasome Activity by Vitamin E in THP‐1 Monocytes

et al. 2007

Self Cite

View full text Add to dashboard Cite

SummaryIn THP-1 monocytes, cellular proteasome inhibition by ritonavir or ALLN is associated with increased production of oxidative stress. Both compounds produced comparable amounts of oxidative stress; however, normalization by a-tocopherol occurred solely after inhibition by ritonavir, and not by ALLN. Similar to that, atocopherol could normalize the reduced formation of 3-nitrotyrosine-modified proteins only after ritonavir treatment. In the absence of any proteasome inhibitor, intrinsic cellular proteasome activity was not modulated by a-, b-, and g-tocopherols; however, dtocopherol, a-tocotrienol, and a-tocopheryl phosphate could significantly inhibit cellular proteasome activity and increased the level of p27Kip1 and p53. Since oxidative stress was reduced by atocopherol only after proteasome inhibition by ritonavir and not by ALLN, it is concluded that, in this experimental system, atocopherol does not act as an antioxidant but interferes with the inhibitory effect of ritonavir. IUBMB Life, 59: 771-780, 2007

show abstract

Section: Discussionmentioning

confidence: 99%

“…Extracts were prepared as previously described (21,22). Briefly, THP-1 cells were harvested by centrifugation, washed two times with PBS, and taken up in 100 ml sterile distilled water containing 1 mM DTT.…”

Section: Cellular Proteasome Activitymentioning

confidence: 99%

Modulation of Proteasome Activity by Vitamin E in THP‐1 Monocytes

et al. 2007

Self Cite

View full text Add to dashboard Cite

show abstract

“…One possibility is that the binding of PKC to PKB may protect Thr308 but not Ser473 from being phosphorylated by PDK1. Accumulated evidence has shown that the regulation of PKB phosphorylation by PKCs, whether negatively or positively, mainly occurs at Ser473 [11,22,[36][37][38]. A putative PDK2 is believed to phosphorylate PKB at Ser473 [39].…”

Section: Discussionmentioning

confidence: 99%

12-O-tetradecanoylphorbol-1, 3-acetate induces the negative regulation of protein kinase B by protein kinase Cα during gastric cancer cell apoptosis

Zhang

Xia

2010

Cellular and Molecular Biology Letters

View full text Add to dashboard Cite

Abstract:The PKB signaling pathway is essential for cell survival and the inhibition of apoptosis, but its functional mechanisms have not been fully explored. Previously, we reported that TPA effectively inhibited PKB activity and caused PKB degradation, which was correlated with the repression of PKB phosphorylation at Ser473. In this study, we focus on how PKB is regulated by TPA in gastric cancer cells. One of the TPA targets, PKCα, was found to mediate the inhibition of PKB phosphorylation and degredation caused by TPA. Furthermore, TPA induced the import of PKCα into the nucleus, where PKCα exerted an inhibitory effect on PKB expression and phosphorylation. As a result, cancer cell proliferation was arrested. Our study characterizes a novel function of PKCα in mediating the negative regulation of PKB by TPA, and suggests a potential application in the clinical treatment of gastric cancer.

show abstract

“…Plus récemment, Chawla et al [37] ont démontré que les agonistes de PPAR ont des effets antiinflammatoires indépendants de ce facteur de transcription. Même si le rôle précis de PPAR dans l'inflammation reste encore à élucider, il est indubitable que ce facteur de transcription a une place centrale dans le métabolisme lipidique et l'activation du macrophage via la régulation du récepteur scavenger CD36, la capture des LDL (low density lipoproteins) oxydées et sa capacité intrinsèque de se lier à des acides gras poly-insaturés ou oxydés [38]. Il est particulièrement intéressant de noter ici que le promoteur du gène p21 WAF1/CIP1 possède justement des sites putatifs de réponse aux PPAR et il a d'ailleurs déjà été clairement montré que le promoteur de p21 WAF1/CIP1 est sensible à l'acide rétinoïque (RXR-RAR) ainsi qu'à la vitamine D3 [6,7] (Figure 3).…”

Section: Métabolisme Des Lipidesunclassified