Vascular Response of Ruthenium Tetraamines in Aortic Ring from Normotensive Rats

Conceição-Vertamatti, Ana Gabriela; Ramos, Luiz Alberto Ferreira; Calandreli, Ivy; Chiba, Aline Nunes; Franco, Douglas Wagner; Tfouni, Elia; Grassi-Kassisse, Dora Maria

doi:10.5935/abc.20140189

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Original Articles • Arq. Bras. Cardiol. 104 (3) • June 2015 • https://doi.org/10.5935/abc.20140189 copy

Vascular Response of Ruthenium Tetraamines in Aortic Ring from Normotensive Rats

Authorship SCIMAGO INSTITUTIONS RANKINGS

Background:

Ruthenium (Ru) tetraamines are being increasingly used as nitric oxide (NO) carriers. In this context, pharmacological studies have become highly relevant to better understand the mechanism of action involved.

Objective:

To evaluate the vascular response of the tetraamines trans-[Ru^II(NH₃)₄(Py)(NO)]³⁺, trans-[Ru^II(Cl)(NO) (cyclan)](PF₆)₂, and trans-[Ru^II(NH₃)₄(4-acPy)(NO)]³⁺.

Methods:

Aortic rings were contracted with noradrenaline (10⁻⁶ M). After voltage stabilization, a single concentration (10⁻⁶ M) of the compounds was added to the assay medium. The responses were recorded during 120 min. Vascular integrity was assessed functionally using acetylcholine at 10⁻⁶ M and sodium nitroprusside at 10⁻⁶ M as well as by histological examination.

Results:

Histological analysis confirmed the presence or absence of endothelial cells in those tissues. All tetraamine complexes altered the contractile response induced by norepinephrine, resulting in increased tone followed by relaxation. In rings with endothelium, the inhibition of endothelial NO caused a reduction of the contractile effect caused by pyridine NO. No significant responses were observed in rings with endothelium after treatment with cyclan NO. In contrast, in rings without endothelium, the inhibition of guanylate cyclase significantly reduced the contractile response caused by the pyridine NO and cyclan NO complexes, and both complexes caused a relaxing effect.

Conclusion:

The results indicate that the vascular effect of the evaluated complexes involved a decrease in the vascular tone induced by norepinephrine (10⁻⁶ M) at the end of the incubation period in aortic rings with and without endothelium, indicating the slow release of NO from these complexes and suggesting that the ligands promoted chemical stability to the molecule. Moreover, we demonstrated that the association of Ru with NO is more stable when the ligands pyridine and cyclan are used in the formulation of the compound.

Ruthenium; Nitric Oxide; Norepinephrine; Pyridine; Cyclan; Aorta; Rats

	trans- [Ru^II(Cl)(NO)(Cyclan)](PF₆)₂		trans-[Ru(NH₃)₄(Py)(NO)]³⁺		trans-[Ru(NH₃)₄(4-acPy)(NO)]³⁺
	E⁺	E^–	E⁺	E^–	E⁺	E^–
-	1.110,6 ± 225,6	1.068,7 ± 317,5	2.292,2 ± 520,6	1.069,4 ± 317,2	1.949,0 ± 542,4	1.292,9 ± 312,8
L-NAME (10-30 μM)	439,9 ± 75,0^* The area under the curve of Ru tetraamines (AUC) trans-[RuII(Cl)(NO)(Cyclan)](PF6)2, trans-[RuII(NH3)4(Py)(NO)]3+, trans-[RuII(NH3)4(4-acPy)(NO)]3+, trans-[RuII(Cl)(NO)(Cyclan)](PF6)2, and trans-[RuII(NH3)4(Py)(NO)]3+ are shown in the absence and presence of L-NAME, indomethacin, ODQ, and carboxy-PTIO in E+ aortic rings and E− aortic rings. Área sob a curva das tetra-aminas de rutênio (ASC)) trans-[RuII(Cl)(NO)(Cyclan)](PF6)2, trans-[RuII(NH3)4(Py)(NO)]3+ e trans-[RuII(NH3)4(4-acPy)(NO)]3+; trans-[RuII(Cl)(NO)(Cyclan)](PF6)2 e trans-[RuII(NH3)4(Py)(NO)]3+estão apresentadas na ausência e na presença de L-NAME, indometacina, ODQ e carboxy-PTO em anéis de aorta com (CE) e sem (SE) endotélio.	898,7 ± 250,6	852,4 ± 245,4^* The area under the curve of Ru tetraamines (AUC) trans-[RuII(Cl)(NO)(Cyclan)](PF6)2, trans-[RuII(NH3)4(Py)(NO)]3+, trans-[RuII(NH3)4(4-acPy)(NO)]3+, trans-[RuII(Cl)(NO)(Cyclan)](PF6)2, and trans-[RuII(NH3)4(Py)(NO)]3+ are shown in the absence and presence of L-NAME, indomethacin, ODQ, and carboxy-PTIO in E+ aortic rings and E− aortic rings. Área sob a curva das tetra-aminas de rutênio (ASC)) trans-[RuII(Cl)(NO)(Cyclan)](PF6)2, trans-[RuII(NH3)4(Py)(NO)]3+ e trans-[RuII(NH3)4(4-acPy)(NO)]3+; trans-[RuII(Cl)(NO)(Cyclan)](PF6)2 e trans-[RuII(NH3)4(Py)(NO)]3+estão apresentadas na ausência e na presença de L-NAME, indometacina, ODQ e carboxy-PTO em anéis de aorta com (CE) e sem (SE) endotélio.	898,6 ± 250,3	-	-
Indomethacin (5,6 μM)	496,3 ± 92,4^* The area under the curve of Ru tetraamines (AUC) trans-[RuII(Cl)(NO)(Cyclan)](PF6)2, trans-[RuII(NH3)4(Py)(NO)]3+, trans-[RuII(NH3)4(4-acPy)(NO)]3+, trans-[RuII(Cl)(NO)(Cyclan)](PF6)2, and trans-[RuII(NH3)4(Py)(NO)]3+ are shown in the absence and presence of L-NAME, indomethacin, ODQ, and carboxy-PTIO in E+ aortic rings and E− aortic rings. Área sob a curva das tetra-aminas de rutênio (ASC)) trans-[RuII(Cl)(NO)(Cyclan)](PF6)2, trans-[RuII(NH3)4(Py)(NO)]3+ e trans-[RuII(NH3)4(4-acPy)(NO)]3+; trans-[RuII(Cl)(NO)(Cyclan)](PF6)2 e trans-[RuII(NH3)4(Py)(NO)]3+estão apresentadas na ausência e na presença de L-NAME, indometacina, ODQ e carboxy-PTO em anéis de aorta com (CE) e sem (SE) endotélio.	741,1 ± 161,9	796,07 ± 119,1^* The area under the curve of Ru tetraamines (AUC) trans-[RuII(Cl)(NO)(Cyclan)](PF6)2, trans-[RuII(NH3)4(Py)(NO)]3+, trans-[RuII(NH3)4(4-acPy)(NO)]3+, trans-[RuII(Cl)(NO)(Cyclan)](PF6)2, and trans-[RuII(NH3)4(Py)(NO)]3+ are shown in the absence and presence of L-NAME, indomethacin, ODQ, and carboxy-PTIO in E+ aortic rings and E− aortic rings. Área sob a curva das tetra-aminas de rutênio (ASC)) trans-[RuII(Cl)(NO)(Cyclan)](PF6)2, trans-[RuII(NH3)4(Py)(NO)]3+ e trans-[RuII(NH3)4(4-acPy)(NO)]3+; trans-[RuII(Cl)(NO)(Cyclan)](PF6)2 e trans-[RuII(NH3)4(Py)(NO)]3+estão apresentadas na ausência e na presença de L-NAME, indometacina, ODQ e carboxy-PTO em anéis de aorta com (CE) e sem (SE) endotélio.	740,7 ± 161,9	-	-
ODQ (3-10 μM)	1.424,5 ± 453,1	646,3 ± 149,8	1.109,4 ± 388,4	646,7 ± 149,9	-	-
C-PTIO (10-300 μM)	1.062,7 ± 159,9	646,3 ± 109,6	1.718,9 ± 276,8	1.223,7 ± 327,6	-	-
L-NAME (10-30 μM), indomethacin (5,6μM) and ODQ (3-10μM)	-	-	1.111,850 ± 350,891	1.329,567 ± 510,506	-	-

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