Cholesterol Depletion Upregulates Involucrin Expression in Epidermal Keratinocytes Through Activation of p38

Jans, Ralph; Atanasova, Ganka; Jadot, Michel; Poumay, Yves

doi:10.1111/j.0022-202x.2004.23221.x

Cited by 69 publications

(89 citation statements)

References 75 publications

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“…5A, row 4), The co-localization of caveolin-1 and CT-B was much less conspicuous than in HK and this image was very similar to the image of SLO-HK. The presence of lipid rafts was reflected in the cell morphology; CD treatment caused shrinkage and rounding of the cells, as previously reported [31]. This shape change, which was reversed when Chol was replaced, may be related to the known disruption of the actin cytoskeleton by CD [32].…”

Section: Lipid Raft Content Of Membranes Is Altered In Slo-hksupporting

confidence: 72%

7-Dehydrocholesterol enhances ultraviolet A-induced oxidative stress in keratinocytes: Roles of NADPH oxidase, mitochondria, and lipid rafts

Valencia

Rajadurai

Carle

et al. 2006

Free Radical Biology and Medicine

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Long wavelength solar UVA radiation stimulates formation of reactive oxygen species (ROS) and prostaglandin E 2 (PGE 2 ), which are involved in skin photosensitivity and tumor promotion. High levels of 7-dehydrocholesterol (7-DHC), the precursor to cholesterol, cause exaggerated photosensitivity to UVA in patients with Smith-Lemli-Opitz syndrome (SLOS). Partially replacing cholesterol with 7-DHC in keratinocytes rapidly (<5 min) increased UVA-induced ROS, intracellular calcium, phospholipase A 2 activity, PGE 2 , and NADPH oxidase activity. UVA-induced ROS and PGE 2 production were inhibited in these cells by depleting the Nox1 subunit of NADPH oxidase using siRNA or using a mitochondrial radical quencher, MitoQ. Partial replacement of cholesterol with 7-DHC also disrupted membrane lipid raft domains, although depletion of cholesterol, which also disrupts lipid rafts, did not affect UVA-induced increases in ROS and PGE 2 . Phospholipid liposomes containing 7-DHC were more rapidly oxidized by a free radical mechanism than those containing cholesterol. These results indicate that 7-DHC enhances rapid UVA-induced ROS and PGE 2 formation by enhancing free radical-mediated membrane lipid oxidation and suggests that this mechanism might underlie the UVA-photosensitivity in SLOS.

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Section: Lipid Raft Content Of Membranes Is Altered In Slo-hksupporting

confidence: 72%

7-Dehydrocholesterol enhances ultraviolet A-induced oxidative stress in keratinocytes: Roles of NADPH oxidase, mitochondria, and lipid rafts

Valencia

Rajadurai

Carle

et al. 2006

Free Radical Biology and Medicine

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“…Epidermal growth factor receptor (11), human ErbB2 (11), ERK (11-13), p38 (11,14), Src (15), and ␤-catenin (16) are activated by M␤CD treatment in various cell types. Like other cell lines, MCF-7 cells showed increased ERK phosphorylation following M␤CD treatment.…”

Section: Discussionmentioning

confidence: 99%

“…Effect of M␤CD on Akt and p70S6K Phosphorylation-Cholesterol depletion by M␤CD has been suggested to cause changes in the phosphorylation of signaling molecules like ERK and Src (11,15). Using a phosphokinase array we screened the phosphorylation profiles of 46 kinases and their substrates to find out if M␤CD affected the signaling pathways important in HAS2 regulation.…”

Section: M␤cd Does Not Change the Size Of Hyaluronan Produced By Mcf-7mentioning

confidence: 99%

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Methyl-β-cyclodextrin Suppresses Hyaluronan Synthesis by Down-regulation of Hyaluronan Synthase 2 through Inhibition of Akt

Kultti

Kärnä

Rilla

et al. 2010

Journal of Biological Chemistry

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Hyaluronan synthases (HAS1-3) are integral plasma membrane proteins that synthesize hyaluronan, a cell surface and extracellular matrix polysaccharide necessary for many biological processes. It has been shown that HAS is partly localized in cholesterol-rich lipid rafts of MCF-7 cells, and cholesterol depletion with methyl-␤-cyclodextrin (M␤CD) suppresses hyaluronan secretion in smooth muscle cells. However, the mechanism by which cholesterol depletion inhibits hyaluronan production has remained unknown. We found that cholesterol depletion from MCF-7 cells by M␤CD inhibits synthesis but does not decrease the molecular mass of hyaluronan, suggesting no major influence on HAS stability in the membrane. The inhibition of hyaluronan synthesis was not due to the availability of HAS substrates UDP-GlcUA and UDP-GlcNAc. Instead, M␤CD specifically down-regulated the expression of HAS2 but not HAS1 or HAS3. Screening of signaling proteins after M␤CD treatment revealed that phosphorylation of Akt and its downstream target p70S6 kinase, both members of phosphoinositide 3-kinase-Akt pathway, were inhibited. Inhibitors of this pathway suppressed hyaluronan synthesis and HAS2 expression in MCF-7 cells, suggesting that the reduced hyaluronan synthesis by M␤CD is due to down-regulation of HAS2, mediated by the phosphoinositide 3-kinase-Akt-mTOR-p70S6K pathway.Cholesterol is an important membrane constituent of mammalian cells, plasma membrane in particular. It decreases the fluidity of the membrane and is a major component of the detergent-resistant membrane microdomains called lipid rafts (1). Increased serum cholesterol and cholesterol accumulation in atherosclerotic lesions have been long associated to cardiovascular disease (2) and atherosclerosis (3, 4), respectively. Abnormal cholesterol accumulation has been also found in some malignancies, such as prostate tumors (5, 6). Furthermore, recent studies suggest that inhibition of the rate-limiting enzyme in cholesterol synthesis (3-hydroxy-3-methyl-glutarylcoenzyme A reductase) by long-term statin therapy decreases the incidence of certain tumor types (7,8).Cellular cholesterol content can be modulated by the cholesterol depleting agent methyl-␤-cyclodextrin (M␤CD) 2 (9). M␤CD disrupts lipid rafts (10) and activates many signaling proteins, like epidermal growth factor receptor (11), extracellular signal-regulated kinase (ERK) (12, 13), p38 (11,14), Src (15), and ␤-catenin (16). On the other hand, M␤CD decreases the growth of MCF-7 breast cancer and A2780 ovarian cancer cells implanted subcutaneously in nude mice (17). In the MCF-7 model M␤CD was even more effective than doxorubicin (17).Hyaluronan, a large glycosaminoglycan mainly present in the extracellular matrix of vertebrates, is composed of repeating disaccharide units containing glucuronic acid (GlcUA) and N-acetylglucosamine (GlcNAc). It is produced at the plasma membrane by three hyaluronan synthases (HAS1-3). HASs use UDP-GlcUA and UDP-GlcNAc as substrates and extrude the forming hyaluronan chain to the extracellu...

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“…45 Altogether, these data suggest a role for p38δ isoform in activation of differentiation-dependent involucrin gene expression. However, the induction of involucrin expression by treatment with cholesterol-depleting agents involves p38α, 46 and constitutively active MEK6 or MEK7, when overexpressed in keratinocytes, increase involucrin via a mechanism that involves p38α, 42,47 suggesting that the engagement of a specific p38 isoform may be stimulus-dependent. Interestingly, a genomic analysis has shown that MAPK13 (a gene that encodes p38δ protein) and involucrin are among genes commonly upregulated both in psoriasis, a benign inflammatory condition characterized by increased proliferation and differentiation, and in well-differentiated locally invasive cutaneous squamous cell carcinomas (SCC).…”

Section: Introductionmentioning

confidence: 99%

p38δ mitogen-activated protein kinase regulates skin homeostasis and tumorigenesis

Efimova¹

2010

Cell Cycle

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Cholesterol Depletion Upregulates Involucrin Expression in Epidermal Keratinocytes Through Activation of p38

Cited by 69 publications

References 75 publications

7-Dehydrocholesterol enhances ultraviolet A-induced oxidative stress in keratinocytes: Roles of NADPH oxidase, mitochondria, and lipid rafts

7-Dehydrocholesterol enhances ultraviolet A-induced oxidative stress in keratinocytes: Roles of NADPH oxidase, mitochondria, and lipid rafts

Methyl-β-cyclodextrin Suppresses Hyaluronan Synthesis by Down-regulation of Hyaluronan Synthase 2 through Inhibition of Akt

p38δ mitogen-activated protein kinase regulates skin homeostasis and tumorigenesis

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