Ras proteins increase Ca<sup>2+</sup>‐responsiveness of smooth muscle contraction

Satoh, Shoji; Rensland, Hans; Pfitzer, Gabriele

doi:10.1016/0014-5793(93)81395-g

Cited by 54 publications

(28 citation statements)

References 34 publications

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“…(Figure 4) A) RAS. The first demonstration of a role of Ras in the regulation of smooth muscle contraction was provided by the observation that active H-Ras induces tension of permeabilized arteries by increasing the Ca 2ϩ responsiveness in a concentration-dependent manner (416). Downstream of Ras, ERK1/2 activation triggers MLCK phosphorylation, leading to an increase in its sensitivity to calmodulin and, consequently, its ability to phosphorylate MLC (227).…”

Section: Role Of Ras Protein Superfamily Members In Arterial Smooth Mmentioning

confidence: 99%

Small G Proteins in the Cardiovascular System: Physiological and Pathological Aspects

Loirand

Sauzeau

Pacaud

2013

Physiological Reviews

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Small G proteins exist in eukaryotes from yeast to human and constitute the Ras superfamily comprising more than 100 members. This superfamily is structurally classified into five families: the Ras, Rho, Rab, Arf, and Ran families that control a wide variety of cell and biological functions through highly coordinated regulation processes. Increasing evidence has accumulated to identify small G proteins and their regulators as key players of the cardiovascular physiology that control a large panel of cardiac (heart rhythm, contraction, hypertrophy) and vascular functions (angiogenesis, vascular permeability, vasoconstriction). Indeed, basal Ras protein activity is required for homeostatic functions in physiological conditions, but sustained overactivation of Ras proteins or spatiotemporal dysregulation of Ras signaling pathways has pathological consequences in the cardiovascular system. The primary object of this review is to provide a comprehensive overview of the current progress in our understanding of the role of small G proteins and their regulators in cardiovascular physiology and pathologies.

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Section: Role Of Ras Protein Superfamily Members In Arterial Smooth Mmentioning

confidence: 99%

Small G Proteins in the Cardiovascular System: Physiological and Pathological Aspects

Loirand

Sauzeau

Pacaud

2013

Physiological Reviews

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“…We used a mutated vall4p2lrhoA that, because of its very low GTPase activity, is constitutively active in its GTP-bound form (36), eliminating effects due to release of free GTP[y-S] from wild-type p2lrhoA. Constitutively active vall4p2lrhoA caused contraction at constant [Ca2+] and, although such an effect can also be produced by H-ras p21 (12), by detergents (0.3% Na cholate) (M.C.G., S.K., A.V.S., and A.P.S., unpublished observations), and even by some batches of bovine serum albumin (M.C.G., S.K., A.V.S., and A.P.S., unpublished observations), the inhibition of the Ca2+-sensitizing effect of vall4p2lrho by ADP-ribosylation in vitro supports its specificity of action, as do the inhibitory effects of ADP-ribosylation of endogenous p2lrhoA on Ca2+ sensitization by GTP, carbachol, and endothelin (Fig. 3).…”

Section: Discussionmentioning

confidence: 99%

“…This process of Ca2+ sensitization can be inhibited by guanosine 5'-[,B-thioldiphosphate (GDP[/3-S]) (5)(6)(7)(8), but the G protein(s) involved and the transduction pathways between plasma membrane-bound receptors and the myosin filamentbound protein phosphatase (9)(10)(11) have not been definitively identified. Both a constitutively active ras (12) and p2lrhoA activated with guanosine 5'-[y-thio]triphosphate (GTP[-y-S]) (13,11) have been reported to Ca2+-sensitize smooth muscle,…”

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confidence: 99%

Role of guanine nucleotide-binding proteins--ras-family or trimeric proteins or both--in Ca2+ sensitization of smooth muscle.

Gong

Iizuka²,

Nixon³

et al. 1996

Proc. Natl. Acad. Sci. U.S.A.

271

219

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The purpose of this study was to identify guanine nucleotide-binding proteins (G proteins) MgCl2/1 mM dithiothreitol/1 mM phenylmethylsulfonyl fluoride/20 ,tM GTP (buffer A), disrupted in a glass homogenizer, and centrifuged at 640 x g for 15 min, and the supernatant was decanted. The residue was twice resuspended in 70 ml of buffer A and recentrifuged. The combined supernatants containing the cell membrane fragments were centrifuged at 186,000 x g for 90 min, and the pellet was resuspended in 50 ml of buffer A containing 2% octyl glucoside, homogenized, and gently shaken for 45 min. The solution was centrifuged at 142,000 x g for 90 min, and the supematant was filtered through a 0.45-,tm Minisart cellulose acetate filter (Sartorius). The solution (-0.4 mg of protein per ml) was loaded into a 10-ml MonoS column equili-

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“…[7][8][9] Until recently, the relationships between Ras and the regulation of blood pressure have scarcely been studied. Previous reports suggested a role for Ras in the cellular response to angiotensin II, 10,11 but no definite relationship between this protein and blood pressure was established. However, genetic manipulation of the different isoforms of the Ras gene has underscored the relevance of this protein as a hemodynamic regulator.…”

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confidence: 95%

Targeted Genomic Disruption of H-Ras Induces Hypotension Through a NO-cGMP-PKG Pathway–Dependent Mechanism

et al. 2010

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Abstract-The aim of the present experiments was to evaluate the differences in arterial pressure between H-Ras lacking mice and control mice and to analyze the mechanisms involved in the genesis of the differences. H-Ras lacking mice and mouse embryonic fibroblasts from these animals were used. Blood pressure was measured using 3 different methods: direct intraarterial measurement in anesthetized animals, tail-cuff sphygmomanometer, and radiotelemetry. H-Ras lacking mice showed lower blood pressure than control animals. Moreover, the aorta protein content of endothelial nitric oxide synthase, soluble guanylyl cyclase, and cyclic guanosine monophosphate-dependent protein kinase was higher in H-Ras knockout mice than in control animals. The activity of these enzymes was increased, because urinary nitrite excretion, sodium nitroprusside-stimulated vascular cyclic guanosine monophosphate synthesis, and phosphorylated vasoactive-stimulated phosphoprotein in aortic tissue increased in these animals. Furthermore, mouse embryonic fibroblasts from H-Ras lacking mice showed higher cyclic guanosine monophosphate-dependent protein kinase promoter activity than control cells. These results strongly support the upregulation of the nitric oxide-cyclic guanosine monophosphate pathway in H-Ras-deficient mice. Moreover, they suggest that H-Ras pathway could be considered as a therapeutic target for hypertension treatment. (Hypertension. 2010;56:484-489.)

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Ras proteins increase Ca²⁺‐responsiveness of smooth muscle contraction

Cited by 54 publications

References 34 publications

Small G Proteins in the Cardiovascular System: Physiological and Pathological Aspects

Small G Proteins in the Cardiovascular System: Physiological and Pathological Aspects

Role of guanine nucleotide-binding proteins--ras-family or trimeric proteins or both--in Ca2+ sensitization of smooth muscle.

Targeted Genomic Disruption of H-Ras Induces Hypotension Through a NO-cGMP-PKG Pathway–Dependent Mechanism

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Ras proteins increase Ca2+‐responsiveness of smooth muscle contraction

Cited by 54 publications

References 34 publications

Small G Proteins in the Cardiovascular System: Physiological and Pathological Aspects

Small G Proteins in the Cardiovascular System: Physiological and Pathological Aspects

Role of guanine nucleotide-binding proteins--ras-family or trimeric proteins or both--in Ca2+ sensitization of smooth muscle.

Targeted Genomic Disruption of H-Ras Induces Hypotension Through a NO-cGMP-PKG Pathway–Dependent Mechanism

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Ras proteins increase Ca²⁺‐responsiveness of smooth muscle contraction