The vasorelaxant effects of 1-nitro-2-phenylethane involve stimulation of the soluble guanylate cyclase-cGMP pathway

Brito, Teresinha Silva de; Lima, Francisco Kleber A.; Aragão, Karoline S.; Siqueira, Rodrigo José Bezerra de; Sousa, Pergentino José C.; Maia, José Guilherme S.; Filho, Jairo Diniz; Lahlou, Saad; Magalhães, Pedro J.C.

doi:10.1016/j.bcp.2012.12.012

Cited by 35 publications

(34 citation statements)

References 42 publications

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“…This pharmacological potency was lower than that evoked by other structurally related nitro compounds in the same preparations. The relaxant effects of its analogues on the contractions induced by phenylephrine yielded EC 50 varying between ~30 to 230 μ m . In common, these studies dealt with compounds possessing the NO 2 group in the α‐ or β‐carbon of the aliphatic chain ( Figure , panels c to f).…”

Section: Discussionmentioning

confidence: 99%

“…Substitutions in the aliphatic chain have been demonstrated to impact directly in their effects. 1‐Nitro‐2‐phenylethane ( Figure c), for instance, relaxes rat aorta preparations , but its analogue β‐phenylethylamine ( Figure a) causes aortic constriction in vitro, probably by acting on specific trace‐amine associated receptors . The nitro compound 2‐nitro‐1‐phenyl‐1‐propanol ( Figure d) relaxes rat aorta and mesenteric arteries , whereas its analogue phenylpropanolamine ( Figure b), a sympathomimetic active principle of over‐the‐counter nasal decongestants, reveals vasoconstrictor properties .…”

Section: Introductionmentioning

confidence: 99%

“…In the rat aorta, the vasodilator effects of 1‐nitro‐2‐phenylethane and 2‐nitro‐1‐phenyl‐1‐propanol involved stimulation of the soluble guanylyl cyclase (sGC) and the consequent production of cyclic guanosine monophosphate (cGMP) . In silico analysis predicted that the presence of the NO 2 allowed the putative interaction of the 1‐nitro‐2‐phenylethane with a binding site in the sGC regulatory subunit . Curiously, substitution at β‐carbon of 1‐nitro‐2‐phenylethane by a ketone, such as in the 2‐nitro‐1‐phenylethanone ( Figure e), abolished its vasorelaxant effect through the sGC pathway .…”

Section: Introductionmentioning

confidence: 99%

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Endothelium‐dependent and endothelium‐independent effects of 1‐nitro‐2‐propylbenzene on rat aorta

Vasconcelos

Ribeiro-Filho

Carvalho

et al. 2019

Fundamemntal Clinical Pharma

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A group of nitro compounds contains a benzene ring in a short aliphatic chain with the NO2 group, property that supposedly favors its vasodilator profile. In this study, we evaluated in isolated rat aorta the effects of 1‐nitro‐2‐propylbenzene (NPB), a nitro compound containing the NO2 in the aromatic ring. In aorta precontracted with KCl, NPB (1‐3000 μm) induced full endothelium‐independent relaxation. In endothelium‐intact preparations, phenylephrine‐induced contractions were fully relaxed by NPB, effect unaltered by N(ω)‐nitro‐L‐arginine methyl ester (L‐NAME) or 1H‐[1,2,4]oxadiazolo[4,3‐a]quinoxalin‐1‐one (ODQ). In the concentration range of 30–300 μm, NPB slightly but significantly potentiated the phenylephrine‐induced contraction. Such potentiation was unaltered by the thromboxane‐prostanoid receptor antagonist seratrodast, but was abolished by endothelium removal or by preincubation of endothelium‐intact preparations with L‐NAME, ODQ or by ruthenium red and HC‐030031, blockers of subtype 1 of ankyrin transient receptor potential (TRPA1) channels. Verapamil exacerbated the potentiating effect of NPB. The potentiating effect was undetectable in preparations precontracted by 9,11‐dideoxy‐11α,9α‐epoxymethanoprostaglandin F2α (U‐46619). Relaxation was reduced by ruthenium red while it was enhanced by HC‐030031. In conclusion, NPB has vasodilator properties but with a mechanism of action distinct from its analogues. Contrary to other nitro compounds, its relaxing effects did not involve recruitment of the guanylyl cyclase pathway. NPB has also endothelium‐dependent potentiating properties on phenylephrine‐induced contractions, a phenomenon that putatively required a role of endothelial TRPA1 channels. The present findings reinforce the notion that the functional group NO2 in the aliphatic chain of these nitro compounds determines favorably their vasodilator properties.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Endothelium‐dependent and endothelium‐independent effects of 1‐nitro‐2‐propylbenzene on rat aorta

Vasconcelos

Ribeiro-Filho

Carvalho

et al. 2019

Fundamemntal Clinical Pharma

Self Cite

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“…For an endothelium-independent vasodilator, possible mechanisms that may be involve in its inhibition of any of the downstream steps in the contractile apparatus (Allen and Walsh, 1994;Brito et al, 2013;Park et al, 2009).…”

Section: Serum Calcium Channel Blocking Effect Of Nbf-asmementioning

confidence: 99%

Mechanisms underlying the antihypertensive effect of Alstonia scholaris

Bello

Usman

Mahmud

et al. 2015

Journal of Ethnopharmacology

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“…For example, resolving the crystal structure of the binding of the sGC activator BAY 60–2770 to an NO-sensitive heme domain homologous to sGC demonstrated that BAY 60–2770 shows a slightly more efficient conformational shift of the heme-binding domain than its parent compound cinaciguat, explaining its marginally more potent stimulation of sGC activity [48*]. And finally, the vasodilatory molecule 1-nitro-2-phenylethane was recently characterized as a novel heme-dependent sGC stimulator, distinct from the previously discovered riociguat-related compounds [49]. All these compounds hold great therapeutic potential in a variety of cardiovascular and other defects related to sGC dysfunction.…”

Section: Development and Characterization Of New Sgc Stimulating And mentioning

confidence: 99%

New insights into the role of soluble guanylate cyclase in blood pressure regulation

Buys

Sips

2014

Current Opinion in Nephrology and Hypertension

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Purpose of review Nitric oxide (NO) – soluble guanylate cyclase (sGC)-dependent signaling mechanisms have a profound effect on the regulation of blood pressure. In this review, we will discuss recent findings in the field which support the importance of sGC in the development of hypertension. Recent findings The importance of sGC in blood pressure regulation was highlighted by studies using genetically modified animal models, chemical stimulators/activators and inhibitors of the NO/sGC signaling pathway, and genetic association studies in humans. Many studies further support the role of NO/sGC in vasodilation and vascular dysfunction, which is underscored by the early clinical success of synthetic sGC stimulators for the treatment of pulmonary hypertension. Recent work has uncovered more details about the structural basis of sGC activation, enabling the development of more potent and efficient modulators of sGC activity. Finally, the mechanisms involved in the modulation of sGC by signaling gases other than NO as well as the influence of redox signaling on sGC have been the subject of several interesting studies. Summary sGC is fast becoming an interesting therapeutic target for the treatment of vascular dysfunction and hypertension, with novel sGC stimulating/activating compounds as promising treatment options in the clinic.

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The vasorelaxant effects of 1-nitro-2-phenylethane involve stimulation of the soluble guanylate cyclase-cGMP pathway

Cited by 35 publications

References 42 publications

Endothelium‐dependent and endothelium‐independent effects of 1‐nitro‐2‐propylbenzene on rat aorta

Endothelium‐dependent and endothelium‐independent effects of 1‐nitro‐2‐propylbenzene on rat aorta

Mechanisms underlying the antihypertensive effect of Alstonia scholaris

New insights into the role of soluble guanylate cyclase in blood pressure regulation

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