Transcriptional regulation of the rat type IIA phospholipase A2 gene by cAMP and interleukin-1β in vascular smooth muscle cells: interplay of the CCAAT/enhancer binding protein (C/EBP), nuclear factor-κB and Ets transcription factors

Antonio, Valérie; Brouillet, Arthur; Janvier, Brigitte; Monne, Claire; Béréziat, G.; Andreani, Marise; Raymondjean, Michel

doi:10.1042/bj20020658

Cited by 52 publications

(56 citation statements)

References 37 publications

(53 reference statements)

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“…[Ϫ488;ϩ46] sPLA2-luc and mutant constructs were obtained by site-directed mutagenesis as previously described. 23 …”

Section: Plasmid Constructsmentioning

confidence: 99%

“…We have previously shown that the best characterized activators of gene expression during inflammation, the nuclear factor-B (NF-B), CAAT/enhancer-binding protein (C/EBP), and winged helix-turn-helix transcription factors (Ets-1), are involved in the stimulation of rat sPLA2-IIA gene transcription by IL-1␤ and cAMP. 23 Therefore, we investigated whether these transcription factors were involved in the induction of the sPLA2-IIA transcription by the hsPLA2-IIA supernatant using [-488;ϩ46] luc constructs mutated for the transcription factor binding sites. The luciferase/␤-galactosidase activity ratio stimulation obtained with the hsPLA2-IIA supernatant was abolished with the mutant constructs, whereas forskolin still induced the transcription of the mutant Ets and mutant NF-kB constructs (Figure 4).…”

Section: Amandine Et Almentioning

confidence: 99%

“…23 We first reproduced these inductions by cotransfecting VSMCs with a [Ϫ488;ϩ46] sPLA2-luciferase reporter gene and a pCMV-␤-galactosidase gene (cytomegalovirus promoter/enhancer) (used to normalize transfection efficiency) (Figure 4). The luciferase activity measured 24 hours after induction reflected the efficiency of the sPLA2-IIA transcription.…”

Section: Amandine Et Almentioning

confidence: 99%

“…20 VSMCs transfections and luciferase assays were realized as described previously. 23 Ni and V5 Depletions of the Supernatants 8 g of the V5 antibody (In Vitrogen) were incubated 1 night with 50 L of proteins A/G agarose beads (Santa Cruz). Supernatants were depleted by a 2-hour incubation with these beads or Ni-NTA agarose nickel-charged beads (Quiagen), filtered, and used to induce VSMCs.…”

Section: Rna Extraction and Reverse-transcription Pcrmentioning

confidence: 99%

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Autocrine and Paracrine Transcriptional Regulation of Type IIA Secretory Phospholipase A2 Gene in Vascular Smooth Muscle Cells

Jaulmes

Janvier

Andreani

et al. 2005

ATVB

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Objective-The inflammation that occurs during the development of atherosclerosis is characterized by a massive release of sPLA2-IIA (group IIA secretory phospholipase A2) from vascular smooth muscle cells (VSMCs). We have investigated the autocrine function of sPLA2-IIA in rat aortic and human VSMCs. Methods and Results-We found that the transcription of the endogenous sPLA2-IIA gene increased by adding a cell supernatant containing human sPLA2-IIA proteins. We show that this effect was independent of the sPLA2 activity using sPLA2-IIA proteins lacking enzyme activity. Transient transfections with various sPLA2-IIA rat promoterluciferase constructs demonstrated that the C/EBP, NK-B, and Ets transcription factors are involved in the increase in sPLA2-IIA gene transcription. We also found the M-type sPLA2 receptor mRNA in VSMCs, and we showed that the sPLA2-luciferase reporter gene was induced by the specific agonist of the sPLA2 receptor, aminophenylmannopyranoside (APMP), and that this induction was mediated by the same transcription factor-binding sites. Finally, we used a sPLA2-IIA mutant unable to bind heparan-sulfate proteoglycans to show that the binding of wild-type sPLA2-IIA to proteoglycans is essential for the induction of an autocrine loop. Key Words: atherosclerosis Ⅲ autocrine/paracrine effects Ⅲ type IIA sPLA2 Ⅲ vascular smooth muscle cells P hospholipase A2 (PLA2) enzymes (EC 3.1.1.4) hydrolyze ester bonds at the sn-2 position of glyceroacylphospholipids to produce lysophospholipids and nonesterified fatty acids such as arachidonic acid (C20:4 n-6). The latter is further metabolized, contributing to the proinflammatory actions and later resolution. 1 PLA2 enzymes are present in most tissues and 4 groups are distinguished by subcellular location, molecular weight, and calcium dependence. One of these groups is secretory PLA2s (sPLA2s). The sPLA2s are extracellular low-molecular-mass (13 to 18 kDa) enzymes that have 6 to 8 disulfide bridges and require millimolar concentrations of Ca 2ϩ . 2 The isoform sPLA2-IIA is the most abundant sPLA2 in vascular smooth muscle cells (VSMCs). 3 Its synthesis is stimulated by inflammatory cytokines such as interleukin 1␤ (IL-1␤), IL-6, and tumor necrosis factor-1␣. 4 The plasma of patients with various inflammatory diseases, particularly atherosclerosis, contains high concentrations of sPLA2-IIA. 5,6 Transgenic mice that overproduce human sPLA2-IIA have confirmed its involvement in atherosclerosis. 7 sPLA2-IIA also functions as a messenger, and this latter function can be independent of its enzymatic activity. For example, sPLA2-IIA triggers a signaling cascade in monocytic cells that has features similar to those found in other cell types and seems to be unrelated to its catalytic activity. 8,9 The recent identification of membrane proteins binding sPLA2 has highlighted the biological effects of these enzymes. Several studies have shown that sPLA2-IB and sPLA2-IIA act via specific receptors characterized in several species (M-type receptors) to play roles that are...

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“…[Ϫ488;ϩ46] sPLA2-luc and mutant constructs were obtained by site-directed mutagenesis as previously described. 23 …”

Section: Plasmid Constructsmentioning

confidence: 99%

Section: Amandine Et Almentioning

confidence: 99%

Section: Amandine Et Almentioning

confidence: 99%

Section: Rna Extraction and Reverse-transcription Pcrmentioning

confidence: 99%

See 2 more Smart Citations

Autocrine and Paracrine Transcriptional Regulation of Type IIA Secretory Phospholipase A2 Gene in Vascular Smooth Muscle Cells

Jaulmes

Janvier

Andreani

et al. 2005

ATVB

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“…I). Sp1 is a transcription factor known to regulate the activities of proteins involved in eicosanoid production, such as cPLA 2 [55], sPLA 2 [56], platelet-activating factor acetylhydrolase (PAF-AH) [57], and 12(S)-lipoxygenase [58].…”

Section: A Sp1-binding Stimulatory Element and An Inhibitory Element mentioning

confidence: 99%

Alteration in the activation state of new inflammation-associated targets by phospholipase A2-activating protein (PLAA)

Zhang

Sha

Wood

et al. 2008

Cellular Signalling

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Phospholipase A 2 (PLA 2 )-activating protein (PLAA) is a novel signaling molecule that regulates the production of prostaglandins (PGE 2 ) and tumor necrosis factor (TNF)-α. To characterize the function of native PLAA in situ, we generated HeLa (Tet-off) cells overexpressing plaa (plaa high ) and control (plaa low ) cells, with the plaa gene in opposite orientation in the latter construct. The plaa high cells produced significantly more PGE 2 and interleukin (IL)-6 compared to plaa low cells in response to TNF-α. There was increased activation and/or expression of cytosolic PLA 2 , cyclooxgenase-2, and NF-κB after induction of plaa high cells with TNF-α compared to the respective plaa low cells. Microarray analysis of plaa high cells followed by functional assays revealed increased production of proinflammatory cytokine IL-32 and a decrease in the production of annexin A4 and clusterin compared to plaa low cells. We demonstrated the role of annexin A4 as an inhibitor of PLA 2 and showed that addition of exogeneous clusterin limited the production of PGE 2 from plaa high cells. To understand regulation of plaa gene expression, we used a luciferase reporter system in HeLa cells and identified one stimulatory element, with Sp1 binding sites, and one inhibitory element, in exon 1 of the plaa gene. By using decoy DNA oligonucleotides to Sp1 and competitive binding assays, we showed that Sp1 maintains basal expression of the plaa gene and binds to the above-mentioned stimulatory element. We demonstrated for the first time that the induction of native PLAA by TNF-α can perpetuate inflammation by enhancing activation of PLA 2 and NF-κB.

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Secretory phospholipase A2‐IIa is a target gene of the HER/HER2‐elicited pathway and a potential plasma biomarker for poor prognosis of prostate cancer

et al. 2011

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BACKGROUND Our previous study showed that prostate cancer cells overexpress and secrete secretory phospholipases A2 group IIa (sPLA2-IIa) and plasma sPLA2-IIa was elevated in prostate cancer patients. The current study further explored the underlying mechanism of sPLA2-IIa overexpression and the potential role of sPLA2-IIa as a prostate cancer biomarker. METHODS Plasma and tissue specimens from prostate cancer patients were analyzed for sPLA2-IIa levels. Regulation of sPLA2-IIa expression by Heregulin-α was determined by western blot and reporter assay. RESULTS We found that Heregulin-α enhanced expression of the sPLA2-IIa gene via the HER2/HER3-elicited pathway. The EGFR/HER2 dual inhibitor Lapatinib and the NF-kB inhibitor Bortezomib inhibited sPLA2-IIa expression induced by Heregulin-α. Heregulin-α upregulated expression of the sPLA2-IIa gene at the transcriptional level. We further confirmed that plasma sPLA2-IIa secreted by mouse bearing human prostate cancer xenografts reached detectable plasma concentrations. A Receiver Operating Characteristic (ROC) analysis of patient plasma specimens revealed that high levels of plasma sPLA2-IIa, with the optimum cutoff value of 2.0 ng/ml, were significantly associated with high Gleason score (8~10) relative to intermediate Gleason score (6~7) prostate cancers and advanced relative to indolent cancers. The area under the ROC curve (AUC) was 0.73 and 0.74, respectively. CONCLUSION We found that Heregulin-α, in addition to EGF, contributes to sPLA2-IIa overexpression in prostate cancer cells. Our findings support the notion that high levels of plasma sPLA2-IIa may serve as a poor prognostic biomarker capable of distinguishing aggressive from indolent prostate cancers, which may improve decision making and optimize patient management.

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Transcriptional regulation of the rat type IIA phospholipase A2 gene by cAMP and interleukin-1β in vascular smooth muscle cells: interplay of the CCAAT/enhancer binding protein (C/EBP), nuclear factor-κB and Ets transcription factors

Cited by 52 publications

References 37 publications

Autocrine and Paracrine Transcriptional Regulation of Type IIA Secretory Phospholipase A2 Gene in Vascular Smooth Muscle Cells

Autocrine and Paracrine Transcriptional Regulation of Type IIA Secretory Phospholipase A2 Gene in Vascular Smooth Muscle Cells

Alteration in the activation state of new inflammation-associated targets by phospholipase A2-activating protein (PLAA)

Secretory phospholipase A2‐IIa is a target gene of the HER/HER2‐elicited pathway and a potential plasma biomarker for poor prognosis of prostate cancer

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