1995
DOI: 10.1111/j.1476-5381.1995.tb15129.x
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Inhibition of relaxations to nitrergic stimulation of the mouse anococcygeus by duroquinone

Abstract: (1 gM) and S-nitroso-glutathione (30 uM), but potentiated those to 8-Br-cyclic GMP (100 Mm).4 Neither hydroquinone (HQ; 100 MM) nor l,4-benzoquinone (BQ; 100 MM), both of which reduced responses to exogenous NO, inhibited relaxations induced by field stimulation in DETCA-treated tissues. Indeed, when added during DQ-induced inhibition of nitrergic relaxations, both HQ and BQ produced partial reversal of the block. 5 DQ had no effect on the detection of superoxide anions estimated via the xanthine: xanthine oxi… Show more

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Cited by 37 publications
(41 citation statements)
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“…Therefore, it is hypothesized that there are endogenous antioxidant defense mechanisms, enzymatic and nonenzymatic, for the neurotransmission process to be mediated by free NO. Similar conclusions were also obtained from studies using an irreversible inhibitor of superoxide dismutase (Martin et al, 1994;Lilley and Gibson, 1995;Paisley and Martin, 1996;Okamura et al, 1998a;Tanaka et al, 1999). Goyal and He (1998) noted that nitrergic slow IJP and hyperpolarization evoked by the NO ⅐ redox donor, diethylenetriamine/NO adduct, were suppressed by guanylyl cyclase inhibitors but not by apamin in the guinea pig ileal circular muscle, whereas hyperpolarization caused by sodium nitroprusside and solubilized NO gas was antagonized by apamin but not by guanylyl cyclase inhibitors.…”
Section: Is the Nitrergic Neurotransmitter Free Radical Nitric Oxisupporting
confidence: 67%
“…Therefore, it is hypothesized that there are endogenous antioxidant defense mechanisms, enzymatic and nonenzymatic, for the neurotransmission process to be mediated by free NO. Similar conclusions were also obtained from studies using an irreversible inhibitor of superoxide dismutase (Martin et al, 1994;Lilley and Gibson, 1995;Paisley and Martin, 1996;Okamura et al, 1998a;Tanaka et al, 1999). Goyal and He (1998) noted that nitrergic slow IJP and hyperpolarization evoked by the NO ⅐ redox donor, diethylenetriamine/NO adduct, were suppressed by guanylyl cyclase inhibitors but not by apamin in the guinea pig ileal circular muscle, whereas hyperpolarization caused by sodium nitroprusside and solubilized NO gas was antagonized by apamin but not by guanylyl cyclase inhibitors.…”
Section: Is the Nitrergic Neurotransmitter Free Radical Nitric Oxisupporting
confidence: 67%
“…These results might suggest that antioxidant enzymes may have an important protective role on the NO-mediated neurotransmission. This was recently illustrated by the finding that an inhibitor of Cu/Zn SOD made the nitrergic neurotransmitter sensitive to superoxides in the bovine retractor penis muscle and in the mouse anococcygeus muscle Lilley & Gibson, 1995;Paisley et al, 1996). In addition, in bioassay experiments, we previously demonstrated that responses to the nitrergic neurotransmitter of the canine ileocolonic junction were inhibited by superoxide anion generators to an comparable extent as the responses to authentic NO, whereas those to nitrosothiols were not affected (Boeckxstaens et al, 1994;De Man et al, 1995b).…”
Section: Introductionmentioning
confidence: 90%
“…In a second series of experiments, the rat gastric fundus was treated for 2 h with the inhibitors of Cu/Zn superoxide dismutase (Cu/Zn SOD), diethyldithiocarbamate (1 mM, Martin et al, 1994;Lilley & Gibson, 1995) and triethylenetetramine (0.1 mM, Abdalla & Will, 1995). After wash-out, the effect of this treatment in the presence and absence of pyrogallol or duroquinone was investigated on the frequency-response curve to electrical stimulation (1-8 Hz, 1 ms), on the concentrationresponse curve to NO (0.03-3 pM) and on the relaxation to ATP (10 gM).…”
Section: Experimental Protocolsmentioning
confidence: 99%
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“…However, they did not examine the property of nitrergic nerve in vasculature. On the other hand, it was noted that treatment with diethyldithiocarbamate, a membrane-permeable inhibitor of Cu/Zn SOD, allowed pyrogallol, hydroquinone, and duroquinone to inhibit the NO-mediated neurogenic response in the bovine retractor penis muscle and mouse anococcygeus muscle Lilley and Gibson, 1995). The inhibition was reversed by FIG.…”
Section: Pharmacology Of Neurogenic No In Blood Vesselmentioning
confidence: 99%