Heparin Inhibits the Progression Phase of Subcultured Endothelial Cell Proliferation in Rat Aorta

Kimura, Ikuko; Nagaura, Takeshi; Naitoh, Takeshi; Kobayashi, Shogo; Kimura, Masayasu

doi:10.1254/jjp.60.369

Cited by 10 publications

(7 citation statements)

References 32 publications

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“…Heparin and heparan sulfate are complex glycosaminoglycans that exert antiproliferative effects in different cell types [32,33,14–16]. Consonant with growth inhibition, heparin inhibits the expression of the early proto‐oncogenes c‐fos and c‐myc by acting selectively on a PKC‐dependent pathway [18–20].…”

Section: Discussionmentioning

confidence: 99%

“…The crucial role of PKC in transducing growth regulatory signals is also highlighted by the finding that the down‐regulation of PKC‐dependent pathways elicits growth inhibitory responses. In particular, glycosaminoglycan‐mediated inhibition of cell proliferation [14–16] and angiogenesis [17] has been associated, at least in part, to the ability of heparin and heparan sulfate to counteract PKC‐mediated events [18–20]. In this regard, we have recently shown that heparin markedly reduced both the serum‐ and phorbol ester‐stimulated DNA synthesis in HEC by eliciting the down‐regulation of the PKC‐mediated ornithine decarboxylase gene expression (ODC) [21].…”

Section: Introductionmentioning

confidence: 99%

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Heparin down‐regulates the phorbol ester‐induced protein kinase C gene expression in human endothelial cells: enzyme‐mediated autoregulation of protein kinase C‐α and ‐δ genes¹

et al. 1999

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Overexpression of protein kinase C-K K and protein kinase C-N N has been shown to modulate a number of biological effects, including the cell growth and differentiation. We hypothesized that heparin, a potent antimitogenic drug, could affect the cell proliferation by inhibiting the expression of specific protein kinase C genes. Heparin, markedly but not completely, inhibited the serum-stimulated protein kinase C-K K and -N N mRNA expression. Protein kinase C inhibition or downregulation significantly decreased the serum-induced protein kinase C isoenzyme gene expression. Heparin failed to inhibit the residual effect of serum that was resistant to the abovementioned treatments. Phorbol 12-myristate 13-acetate elicited an increase of protein kinase C isoenzyme gene expression that was completely prevented by protein kinase C inhibition or downregulation. Heparin dose-dependently counteracted and ultimately abolished the increase in the protein kinase C isoenzyme gene expression elicited by phorbol 12-myristate 13-acetate. These results suggest that the inhibition of an autoregulatory role wielded by protein kinase C on the protein kinase C-K K and -N N gene expression might represent a possible mechanism by which glycosaminoglycans modulate the cell growth.z 1999 Federation of European Biochemical Societies.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Heparin down‐regulates the phorbol ester‐induced protein kinase C gene expression in human endothelial cells: enzyme‐mediated autoregulation of protein kinase C‐α and ‐δ genes¹

et al. 1999

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“…We have previously analyzed PDGF and FBS-stimulated competence of DNA synthesis by a convenient method (7,12). Heparin does not inhibit the PDGF-induced compe tence phase, suggesting that it inhibits the progression phase in the SMC (7).…”

Section: Discussionmentioning

confidence: 99%

“…Analysis of indices of competence and progression inhibi tions We analyzed the inhibitory effects of cnidium rhizome derived phthalides on competence and progression phases of SMC proliferation by using the convenient assay reported previously (7,12). Proliferation lines of the SMC number from 3 x 104 to 6 x 104 cells/well as a func tion of culturing time were fitted to the individual data of SMC number by the least-squares method.…”

Section: Assay Of Smc Proliferationmentioning

confidence: 99%

“…Proliferation lines of the SMC number from 3 x 104 to 6 x 104 cells/well as a func tion of culturing time were fitted to the individual data of SMC number by the least-squares method. These indices of the competence and progression inhibitions were esti mated as relative difference of the starting time between with and without drug, ((Ct Cc)/Cc), and relative differ ence of the doubling time from the starting time, which was calculated by the slope of the proliferation line, be tween with and without drug, ((Pt Pc)/Pc), respectively (7,12).…”

Section: Assay Of Smc Proliferationmentioning

confidence: 99%

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Chemical Structure-Activity of Cnidium Rhizome-Derived Phthalides for the Competence Inhibition of Proliferation in Primary Cultures of Mouse Aorta Smooth Muscle Cells

Kobayashi

Mimura

Naitoh

et al. 1993

Japanese Journal of Pharmacology

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ABSTRACT-Inhibitory effects of cnidium rhizome-derived phthalides on competence and progression phases of fetal bovine serum (10%)-induced proliferation were compared in primary cultures of mouse aorta smooth muscle cells (SMC). Their potencies for the competence inhibition were in the order of senkyunolide L ((Z)-6-hydroxy-7-chloro-6,7-dihydroligustilide)> senkyunolide H ((Z)-6,7-dihydroxy-6,7 dihydroligustilide) > senkyunolide J ((3S)-(E)-6,7-dihydroxy-3,6,7,8-tetrahydroligustilide) > senkyunolide I ((E)-6,7-dihydroxy-6,7-dihydroligustilide) > ligustilide = senkyunolide A ((3S)-3,8-dihydroligustilide) > butylidenephthalide. The order of their potencies for the progression inhibition was parallel with that for the competence inhibition. Senkyunolide L is considered to have been formed during the extraction of cnidium. These results demonstrate that the (Z)-6,7-dihydroxy isomer of the dihydroligustilide derivatives is essential for the anti-competent effect on proliferation of the SMC in primary culture. Senkyunolide H in cnidium rhizome may be a prototype for a new anti-atherosclerotic drug.

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Interferon-γ-activated macrophages enhance angiogenesis from endothelial cells of rat aorta

et al. 1994

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Heparin Inhibits the Progression Phase of Subcultured Endothelial Cell Proliferation in Rat Aorta

Cited by 10 publications

References 32 publications

Heparin down‐regulates the phorbol ester‐induced protein kinase C gene expression in human endothelial cells: enzyme‐mediated autoregulation of protein kinase C‐α and ‐δ genes¹

Heparin down‐regulates the phorbol ester‐induced protein kinase C gene expression in human endothelial cells: enzyme‐mediated autoregulation of protein kinase C‐α and ‐δ genes¹

Chemical Structure-Activity of Cnidium Rhizome-Derived Phthalides for the Competence Inhibition of Proliferation in Primary Cultures of Mouse Aorta Smooth Muscle Cells

Interferon-γ-activated macrophages enhance angiogenesis from endothelial cells of rat aorta

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Heparin Inhibits the Progression Phase of Subcultured Endothelial Cell Proliferation in Rat Aorta

Cited by 10 publications

References 32 publications

Heparin down‐regulates the phorbol ester‐induced protein kinase C gene expression in human endothelial cells: enzyme‐mediated autoregulation of protein kinase C‐α and ‐δ genes1

Heparin down‐regulates the phorbol ester‐induced protein kinase C gene expression in human endothelial cells: enzyme‐mediated autoregulation of protein kinase C‐α and ‐δ genes1

Chemical Structure-Activity of Cnidium Rhizome-Derived Phthalides for the Competence Inhibition of Proliferation in Primary Cultures of Mouse Aorta Smooth Muscle Cells

Interferon-γ-activated macrophages enhance angiogenesis from endothelial cells of rat aorta

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Heparin down‐regulates the phorbol ester‐induced protein kinase C gene expression in human endothelial cells: enzyme‐mediated autoregulation of protein kinase C‐α and ‐δ genes¹

Heparin down‐regulates the phorbol ester‐induced protein kinase C gene expression in human endothelial cells: enzyme‐mediated autoregulation of protein kinase C‐α and ‐δ genes¹