Regulation of Vascular Smooth Muscle Proliferation by Heparin

Fasciano, Stephen; Patel, Rekha C.; Handy, Indhira; Patel, Chandrashekhar V.

doi:10.1074/jbc.m411458200

Cited by 31 publications

(6 citation statements)

References 94 publications

(93 reference statements)

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“…Heparin binds to PKR at a site that is nonoverlapping with PKR's dsRBD and leads to PKR activation ( 41 , 42 ). Activation of PKR by heparin in vascular smooth muscle cells leads to an arrest in cell cycle progression by causing elevation in p27 kip1 protein levels, inhibition of Cdk2 activity and Rb phosphorylation ( 43 ). PACT interacts with PKR by binding to its dsRBD in a dsRNA-independent manner and activates PKR in response to cellular stress ( 14 ).…”

Section: Introductionmentioning

confidence: 99%

Interaction of human tRNA-dihydrouridine synthase-2 with interferon-induced protein kinase PKR

Mittelstadt

Frump

Khuu

et al. 2007

Nucleic Acids Research

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PKR is an interferon (IFN)-induced protein kinase, which is involved in regulation of antiviral innate immunity, stress signaling, cell proliferation and programmed cell death. Although a low amount of PKR is expressed ubiquitously in all cell types in the absence of IFNs, PKR expression is induced at transcriptional level by IFN. PKR's enzymatic activity is activated by its binding to one of its activators. Double-stranded (ds) RNA, protein activator PACT and heparin are the three known activators of PKR. Activation of PKR in cells leads to a general block in protein synthesis due to phosphorylation of eIF2α on serine 51 by PKR. PKR activation is regulated very tightly in mammalian cells and a prolonged activation of PKR leads to apoptosis. Thus, positive and negative regulation of PKR activation is important for cell viability and function. The studies presented here describe human dihydrouridine synthase-2 (hDUS2) as a novel regulator of PKR. We originally identified hDUS2 as a protein interacting with PACT in a yeast two-hybrid screen. Further characterization revealed that hDUS2 also interacts with PKR through its dsRNA binding/dimerization domain and inhibits its kinase activity. Our results suggest that hDUS2 may act as a novel inhibitor of PKR in cells.

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Section: Introductionmentioning

confidence: 99%

Interaction of human tRNA-dihydrouridine synthase-2 with interferon-induced protein kinase PKR

Mittelstadt

Frump

Khuu

et al. 2007

Nucleic Acids Research

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show abstract

“…In this case, it is obvious that the role of heparin in the function of smooth muscle cells of both circular and longitudinal layers of the choledochus sphincter muscle is quite different. Having in mind the well‐known role of heparin in the inhibition of motility and proliferation of the vascular and myometrial smooth muscle cells (Lake and Castellot, ; Masson et al., ; Fasciano et al., ), it could be presumed a similar role predominates also in the circular smooth layer of the musculus sphincter ductus choledochus . That opinion could also be supported by recently reported data regarding the role of canine and porcine heparin‐positive MCs in the motility of smooth and skeletal muscle cells (Stefanov et al., ; Vodenicharov, ).…”

Section: Discussionmentioning

confidence: 99%

Histochemical Study of Heparin‐positive Mast Cells in the Terminal Part of Porcine Ductus Choledochus and Papilla Duodeni Major

Stefanov

Vodenicharov

Tsandev

et al. 2015

Anat Histol Embryol

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The study presented in detail the localization and density of mast cells (MCs) in the intramural part of the common bile duct (CBD) and in the major duodenal papilla (MDP) of domestic swine. MCs' density (number/mm(2) ) in different layers of both of the duct and papilla was evaluated after toluidine blue staining. Their number was higher in the lamina propria mucosae than in the tunica muscularis of the studied structures. The localization of berberine-positive, (heparin containing) MCs and the ratio between them and toluidine blue-positive MCs with γ-ma metachromasia was also established. Ratios of heparin-containing MCs in comparison with all toluidine blue-positive MCs were found as follows: ductus choledochus - 32% in the subglandular connective tissue of lamina propria mucosae in the intramural part of the duct; m. sphincter ductus choledochus - 31% in the circular and 0.06% in the longitudinal muscle layer; subserosa - 59%; papilla duodeni major - 0.03% in the subepithelial connective tissue and 34% in the subglandular connective tissue of lamina propria mucosae, respectively. The established large difference in heparin-positive MCs in both the subepithelial and subglandular connective tissues of CBD and MDP, respectively, is an evidence for the existence of mucosal and connective tissue MCs.

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“…The cell cycle mechanisms underlying the inhibition of proliferation of VSMCs and VECs after DES implantation remain unclear. However, the G1/S transition point has been shown to play an important role in VSMCs under conditions of mechanical or inflammatory injury [ 23 ]. P27 kip1 regulates the G1/S transition by inhibiting the activity of cyclin E/CDK2, which is considered to be an endogenous regulator in VSMCs.…”

Section: Discussionmentioning

confidence: 99%

Targeted Inhibitory Effect of Lenti-SM22alpha-p27-EGFP Recombinant Lentiviral Vectors on Proliferation of Vascular Smooth Muscle Cells without Compromising Re-Endothelialization in a Rat Carotid Artery Balloon Injury Model

et al. 2015

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AimsIn-stent restenosis remains a serious problem after the implantation of drug-eluting stents, which is attributable to neointima formation and re-endothelialization. Here, we tried to find a new method which aims at selectively inhibiting proliferation of vascular smooth muscle cells (VSMC) proliferation without inhibition of re-endothelialization.Methods and ResultsWe used the smooth muscle-specific SM22alpha promoter in a recombinant lentiviral vector to drive overexpression of cell-cycle inhibitor, p27, in VSMCs. p27 effectively inhibited VSMC proliferation mediated by cell cycle arrest at the G0/G1 checkpoint. The SM22alpha-p27 lentiviral vector inhibited VSMC proliferation more effectively than paclitaxel. Rats infected with Lenti-SM22alpha-p27 had a significantly lower intima/media (I/M) ratio and also showed inhibition of restenosis on day 28 after balloon injury. Moreover, the repair of injured endothelium, and re-endothelialization of the carotid artery wall, was not affected by the smooth muscle cell-specific expression of p27.ConclusionA recombinant lentiviral vector carrying the SM22alpha promoter was used to effectively infect and selectively overexpress p27 protein in VSMCs, leading to inhibition of intimal hyperplasia without compromising endothelial repair.

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Regulation of Vascular Smooth Muscle Proliferation by Heparin

Cited by 31 publications

References 94 publications

Interaction of human tRNA-dihydrouridine synthase-2 with interferon-induced protein kinase PKR

Interaction of human tRNA-dihydrouridine synthase-2 with interferon-induced protein kinase PKR

Histochemical Study of Heparin‐positive Mast Cells in the Terminal Part of Porcine Ductus Choledochus and Papilla Duodeni Major

Targeted Inhibitory Effect of Lenti-SM22alpha-p27-EGFP Recombinant Lentiviral Vectors on Proliferation of Vascular Smooth Muscle Cells without Compromising Re-Endothelialization in a Rat Carotid Artery Balloon Injury Model

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