Enzymatically hydrolyzed low-density lipoprotein modulates inflammatory responses in endothelial cells

Fenske, Dominic; Dersch, Katrin; Lux, Cornelia A.; Zipse, Lisa; Suriyaphol, Prapat; Dragneva, Y.; Han, Shan-Rui; Bhakdi, Sucharit; Husmann, Matthias

doi:10.1160/th08-03-0166

Cited by 6 publications

(5 citation statements)

References 28 publications

(39 reference statements)

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“…Next, although Fenske et al . (36) reported that SB203580 does not block IL‐8 production by endothelial cells in response to eLDL, suggesting that p38 activation and IL‐8 up‐regulation observed in endothelial cells exposed to eLDL are not causally related, Hakala et al . (12) reported that p38 MAPK was crucial for the hydrolase‐modified LDL‐induced IL‐8 secretion from macrophages.…”

Section: Discussionmentioning

confidence: 99%

“…Thus, although eLDL has been shown to induce secretion of IL-8 by endothelial cells (10) but not macrophages (22), hydrolase-modified LDL, an LDL modification resembling eLDL, induced substantial secretion of IL-8 by human monocyte-derived macrophages (12). Next, although Fenske et al (36) reported that SB203580 does not block IL-8 production by endothelial cells in response to eLDL, suggesting that p38 activation and IL-8 upregulation observed in endothelial cells exposed to eLDL are not causally related, Hakala et al (12) reported that p38 MAPK was crucial for the hydrolase-modified LDLinduced IL-8 secretion from macrophages. Of course, these discrepancies may be attributable to the different cell lines used.…”

Section: Discussionmentioning

confidence: 99%

“…Among the wide‐ranging downstream activities of phosphorylated p38 MAPK, cytokine production is a decisive component related to atherosclerosis (35). It has been reported that eLDL modulates inflammatory responses in endothelial cells by selective induction of IL‐8 in endothelial cells (10, 36). In the first instance, we investigated whether eLDL uptake by THP‐1 cells induces cytokines known to be regulated by p38 MAPK.…”

Section: Discussionmentioning

confidence: 99%

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Selective p38α MAP kinase/MAPK14 inhibition in enzymatically modified LDL‐stimulated human monocytes: implications for atherosclerosis

et al. 2016

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The first ATP-competitive p38α MAPK/MAPK14 inhibitor with excellent in vivo efficacy and selectivity, skepinone-L, is now available. We investigated the impact of selective p38α MAPK/MAPK14 inhibition on enzymatically modified LDL (eLDL) stimulated human monocytes with its implications for atherosclerosis. Among the different p38 MAPK isoforms, p38α/MAPK14 was the predominantly expressed and activated isoform in isolated human peripheral blood monocytes. Moreover, eLDL colocalized with macrophages positive for p38α MAPK/MAPK14 in human carotid endarterectomy specimens. Using the human leukemia cell line THP-1 and/or primary monocyte-derived macrophages, skepinone-L inhibited eLDL-induced activation of the p38 MAPK pathway, inhibited eLDL induced expression of both cluster of differentiation 36 (CD36) and ATP-binding cassette, subfamily A, member 1 (ABCA1), without a net effect on foam cell formation, had a cell- and time-dependent effect on eLDL-triggered apoptosis, and inhibited eLDL-stimulated secretion of IL-8 and MIP-1β/CCL4 (macrophage inflammatory protein-1β/chemokine, CC motif, ligand 4). Inhibition of a key signaling molecule of the p38 MAPK pathway, p38α MAPK/MAPK14, by selective inhibitors like skepinone-L, conclusively facilitates elucidation of the impact of the complex network of p38 MAPK signaling on atherogenesis and might provide a promising therapeutic tool to prevent inflammatory cascades in atherosclerosis.-Cheng, F., Twardowski, L., Fehr, S., Aner, C., Schaeffeler, E., Joos, T., Knorpp, T., Dorweiler, B., Laufer, S., Schwab, M., Torzewski, M. Selective p38α MAP kinase/MAPK14 inhibition in enzymatically modified LDL-stimulated human monocytes: implications for atherosclerosis.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Selective p38α MAP kinase/MAPK14 inhibition in enzymatically modified LDL‐stimulated human monocytes: implications for atherosclerosis

et al. 2016

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“…eLDL is thus able to promote the selective adhesion of monocytes and T lymphocytes to the endothelium, stimulate transmigration of these cells, and foster their retention in the vessel wall by increasing their adherence to SMCs (44). Likewise, production of IL-8 (interleukin-8) and simultaneous modulation of NF-kappaB in response to eLDL might also serve to protect the vessel wall and promote silent removal of the insudated lipoprotein (45).…”

Section: Cellular Effects Of Eldlmentioning

confidence: 99%

Enzymatically modified LDL atherosclerosis and beyond paving the way to acceptance

Torzewski¹

2018

Front Biosci

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The eLDL (enzymatically modified LDL) hypothesis proposes that modification of LDL during atherogenesis occurs through the action of ubiquitous hydrolytic enzymes. eLDL is recognized by multiple macrophage receptors. Following cellular uptake, eLDL triggers atherosclerotic lesion initiation with reversion or progression depending on the balance between cholesterol insudation and depletion. The effects of eLDL on cellular constituents of the atherosclerotic lesion comprise both pro- and anti-inflammatory mechanisms. eLDL triggered complement activation is centrally involved in atherosclerosis with the first CRP (C-reactive protein)-dependent activation step to prevail at the early stages of atherogenesis (lesion initiation with reversion), and the second situation to gain dominance as local concentrations of eLDL surpass a critical threshold (lesion initiation with progression). Thus, CRP-mediated lipoprotein removal likely underlies the regression of early lesions, which occurs continuously through life. Perhaps CRP should be considered as an antiatherogenic agent and the question whether it is an innocent bystander or proatherogenic culprit is not really to the point. The observed association between CRP and atherosclerosis might simply be reverse causation: atherosclerotic disease progression induces CRP.

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“…ELDL played multifaceted roles in atherosclerosis. ELDL modulated endothelial inflammatory responses by promoting interleukin 8 production and secretion through activation of transcription factor activator protein-1 [12,32]. Upon binding to C1q, eLDL triggered the classical pathway of complement in a CRP-dependent and -independent fashion [33,34], which contributed to pathological process of atherosclerosis.…”

Section: Discussionmentioning

confidence: 99%

C reactive protein and enzymatically modified LDL cooperatively promote dendritic cell-mediated T cell activation

Ren

Wang

et al. 2017

Cardiovascular Pathology

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Enzymatically hydrolyzed low-density lipoprotein modulates inflammatory responses in endothelial cells

Cited by 6 publications

References 28 publications

Selective p38α MAP kinase/MAPK14 inhibition in enzymatically modified LDL‐stimulated human monocytes: implications for atherosclerosis

Selective p38α MAP kinase/MAPK14 inhibition in enzymatically modified LDL‐stimulated human monocytes: implications for atherosclerosis

Enzymatically modified LDL atherosclerosis and beyond paving the way to acceptance

C reactive protein and enzymatically modified LDL cooperatively promote dendritic cell-mediated T cell activation

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