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Matches in Nanopublications for { ?s ?p ?o <http://www.tkuhn.ch/bel2nanopub/RAHTTaBVO2O8KTus9Wi4LOX4FfpL4o1Zp3dvzIL133BIA#provenance>. }

• _6 label "Selventa" provenance.
• large_corpus.bel rights "Copyright (c) 2011-2012, Selventa. All rights reserved." provenance.
• _5 value "3-hydroxy-3methylglutaryl coenzyme A (HMG-CoA) reductase inhibitors have shown beneficial effects in the treatment of cardiovascular diseases as lipid lowering drugs. Recent work points to cholesterol-independent actions such as inhibition of isoprenylation and activation of G proteins. Angiotensin II (AngII) participates in the development of fibrosis during vascular damage. Connective tissue growth factor (CTGF) has been described as a novel fibrotic mediator. Our aim was to investigate whether HMG-CoA reductase inhibitors could modulate AngII responses, investigating in vascular smooth muscle cells the effect on CTGF expression. Results: In growth-arrested VSMC, AngII, via AT1 receptor, induced CTGF mRNA expression (Northern) and protein production (5-fold vs control; 10-7 mol/L AngII at 24 h; Western). A CTGF antisense oligonucleotide decreased AngII-induced fibronectin synthesis, suggesting that CTGF could be a mediator of fibrogenic effects of AngII. Pretreatment of VSMC with simvastatin (10-7 mol/L to 10-10mol/L) time and dose-dependently inhibited AngII-induced CTGF production (maximal 10-7mol/L: 80% inhibition vs AngII; Western). The inhibition of CTGF expression was prevented when cells were incubated with mevalonate, geranylgeranylpyrophosphate and, in a lesser extend, with farnesylpyrophospate. Different receptors coupled to G proteins, including AT1, activate p21ras and Rho kinase. Overexpression of dominant negative mutant of RhoA suppressed CTFG induction by AngII. The inhibitor of Rho kinase Y-27632, dose-dependently decreased AngII-induced CTGF production, implicating RhoA as a signaling module downstream of AngII and showing that the Rho-kinase pathway may be a novel target to inhibit AngII signaling. Conclusions: Our data suggest that HMG-CoA reductase inhibitors, via Rho proteins, regulate AngII-induced CTGF, a protein related to the development of fibrosis, suggesting that some of the beneficial effects of these drugs could be due to modulation of AngII-mediated vascular damage, explaining cholesterol independent protective effects." provenance.
• _5 wasQuotedFrom _4 provenance.
• assertion hadPrimarySource _4 provenance.
• large_corpus.bel title "BEL Framework Large Corpus Document" provenance.
• _4 title "AHA Abstracts 621" provenance.
• large_corpus.bel description "Approximately 61,000 statements." provenance.
• assertion wasDerivedFrom large_corpus.bel provenance.
• assertion wasDerivedFrom _5 provenance.
• large_corpus.bel authoredBy _6 provenance.
• large_corpus.bel version "20131211" provenance.
• _4 identifier "AHA Abstracts 621" provenance.
• _4 type "Other" provenance.