THE EFFECTS OF SENSORY DENERVATION ON THE RESPONSES OF THE RABBIT EYE TO PROSTAGLANDIN E<sub>1</sub>, BRADYKININ AND SUBSTANCE P

Butler, John M.; Hammond, B. R.

doi:10.1111/j.1476-5381.1980.tb07040.x

Cited by 116 publications

(40 citation statements)

References 29 publications

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“…Functional studies suggest these responses are caused by nerve-released tachykinins (Butler & Hammond, 1980;Muramatsu et al, 1987), although the identity of the tachykinins released by each of the sensory nerve stimulants remains unclear. Our previous work with selective tachykinin receptor agonists (Hall et al, 1991) and antagonists (Hall et al, 1992b) indicated that activation of NK, and NK3 postjunctional receptors results in contraction in this preparation; while radioligand binding studies have demonstrated specific binding sites for substance P in iris sphincter muscle membrane preparations (Too et al, 1988;Denis et al, 1991).…”

Section: Methodsmentioning

confidence: 99%

Tachykinin receptors mediating responses to sensory nerve stimulation and exogenous tachykinins and analogues in the rabbit isolated iris sphincter

Hall

Mitchell

Morton

1993

British J Pharmacology

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1 We have used selective tachykinin receptor agonists and antagonists to investigate the nature of the receptors mediating responses to endogenous and exogenous tachykinins in the rabbit iris sphincter preparation in vitro.2 The NKI-selective agonist, substance P methyl ester, induced contraction with a pD2 of 9.16 indicating the presence of NK, receptors. In confirmation, the NKI-selective antagonist, GR82334, competitively antagonized responses to substance P methyl ester with high affinity (pKB 7.46). 3 NK3 receptors also mediate contraction since NK3-selective agonists exhibited high potency, e.g. the pD2 of -neurokinin B was 9.67, and their responses were not inhibited by GR82334 (10 1iM). 4 NK2 receptor activation does not seem to contribute to contraction since the NK2-selective agonist -neurokinin A(4-10) had relatively low potency (pD2 6.43), and the NK2-selective antagonists MEN10207 (1 ,lM) and L-659,877 (10 iM) were inactive or had low affinity, respectively. 5 GR82334 (1 jiM) significantly inhibited responses to electrical field-stimulation of non-adrenergic non-cholinergic sensory nerves (3, 10 and 30 Hz), and caused a rightward shift of the log concentrationresponse curve to bradykinin (lateral shift ca. 1000fold). Higher concentrations of GR82334 (10pM) significantly attenuated responses to capsaicin (Hall et al., 1992b;. ' Author for correspondence.Tissue preparation and recording arrangements Male New Zealand albino rabbits (2.5-3.0 kg) were killed by an overdose of i.v. pentobarbitone sodium (Sagatal). The eyes were enucleated immediately after death and opened by an incision 2-3 mm dorsal to the limbus, followed by excision of the iris from the ciliary margin. The sphincter pupillae muscles were dissected free of dilator muscle and mounted intact, either on stainless-steel tissue-holders or between parallel platinum electrodes, in 2 ml silanised glass organ baths in Krebs solution at 37°C. The preparations were attached to isometric Grass FT03B force-displacement transducers under an initial resting tension of 150 mg. Mechanical activity was recorded on Grass model 7E polygraphs. Electrical field stimulation was applied by Scientific Research Instruments Limited (SRI 6051) stimulators.The composition of the Krebs solution was (mM): Na+ 140, K+ 5.9, Cl-104.8, H2PO4-1.2, HC03-24.9, Ca2+ 2.6, Mg2+ 1.15, S042-1.15, glucose 10. The Krebs solution was maintained at pH 7.4 by constant bubbling with 95% 02: 5% CO2. In all experiments the Krebs solution contained hexamethonium (100 jiM), mepyramine, cimetidine, guanethidine, atropine and ibuprofen (all 1 jiM). Experimental protocolsAn equilibration period of 60 min was allowed before commencing regular dosing, after which time the maximal response to carbachol was established. Concentration-response curves for bradykinin were determined at the start, and for substance P at the end, of experiments and a concentrationresponse curve to carbachol was obtained in each prepara- tion. Cumulative concentration-response curves were established to stimul...

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Section: Methodsmentioning

confidence: 99%

Tachykinin receptors mediating responses to sensory nerve stimulation and exogenous tachykinins and analogues in the rabbit isolated iris sphincter

Hall

Mitchell

Morton

1993

British J Pharmacology

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“…Bradykinin excites nociceptive sensory endings (1)(2)(3)(4)(5), producing a sensation of pain (6,7). Chemical mediators released by bradykinin from sensory endings (8)(9)(10) and from sympathetic nerve terminals (11) contribute to vasodilatation and plasma leakage at the site of inflammation. Further, as part of its inflammatory effect, bradykinin triggers the production of prostaglandin E or other arachidonic acid metabolites in some tissues, and these mediators secondarily cause a sensitization of sensory endings to bradykinin and other stimuli (12,13).…”

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confidence: 99%

Identification of a B2 bradykinin receptor expressed by PC12 pheochromocytoma cells.

Nardone

Gerald²,

Rimawi³

et al. 1994

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

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We Although a bradykinin receptor cDNA has been isolated from rat uterine smooth muscle (22) and from human fibroblasts (23) METHODSCell Culture. PC12 cells were maintained in L15CO2 medium (30) containing 7% horse serum and 7% fetal bovine serum and supplemented with 16.7 mM glucose, penicillin (100 units/ml), streptomycin sulfate (100 pg/ml), fresh vitamin mix (30), and 2 mM glutamine. COS-1 cells (simian Abbreviations: IP2, inositol bisphosphate; IP3, inositol trisphosphate; Thi, f-(2-thienyl)alanine.

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“…Application of susbtance P can induce miosis and other inflammatory responses (Bill et al, 1979;Butler & Hammond, 1980;Mandahl & Bill, 1981), and it can also be released into the aqueous humor (Bill et al, 1979). Furthermore, substance P antagonists may suppress inflammation in the eye (Holmdahl et al, 1981).…”

Section: Discussionmentioning

confidence: 99%

“…It has been suggested that the non-adrenergic non-cholinergic component is mediated by substance P or a similar substance (Ueda et al, 1981;Tornqvist et al, 1982;Bjorkroth, 1983;Zhang et al, 1984), and also that substance P is the neurogenic factor responsible for the miosis of the nerve-mediated response of 'Author for correspondence. the eye to irritation (Bill et al, 1979;Butler & Hammond, 1980;Soloway et al, 1981;Mandahl & Bill, 1981).…”

Section: Introductionmentioning

confidence: 99%

Adenosine‐modulation of cholinergic and non‐adrenergic non‐cholinergic neurotransmission in the rabbit iris sphincter

Gustafsson

Wiklund

1986

British J Pharmacology

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1 The characteristics of smooth muscle responses to transmural nerve stimulation in the rabbit iris sphincter were examined. 2 Transmural stimulation elicited a composite contractile response that could be divided in two phases. Atropine abolished the phase I contraction and inhibited the phase II contraction. The atropine-resistant component of the phase II contraction which was unaltered by sympathetic denervation, was mimicked by substance P and abolished by capsaicin. 3 Adenosine inhibited the phase I contraction. The adenosine analogue L-N6-phenylisopropyladenosine (L-PIA) was more potent than 5'-N-ethylcarboxamideadenosine (NECA) in mimicking this adenosine effect. 4 By contrast, adenosine enhanced the phase II contraction in non-pretreated preparations, as well as the atropine-resistant capsaicin-sensitive part of this contraction. Here, NECA was more potent than L-PIA.5 Adenosine, NECA, L-PIA and D-PIA also enhanced the atropine-sensitive component of the phase II contraction, as well as the contractile response to exogenous acetylcholine or carbachol, but not to exogenous substance P. In this respect, L-PIA was the most powerful adenosine analogue with at least 10 fold higher potency than D-PIA. 6 The adenosine antagonist 8-p-sulphophenyltheophylline enhanced the phase I contraction and decreased the capsaicin-sensitive non-adrenergic non-cholinergic component of the phase II contraction. 7 We conclude that adenosine inhibited the nerve-induced cholinergic twitch (phase I) responses by action at prejunctional Al-receptors. Furthermore, adenosine enhanced the phase II contractile responses via postjunctional enhancement of the cholinergic transmission by action at A,-receptors, and via enhancement of the non-adrenergic non-cholinergic transmission by action at presumably prejunctional A2 receptors.

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THE EFFECTS OF SENSORY DENERVATION ON THE RESPONSES OF THE RABBIT EYE TO PROSTAGLANDIN E₁, BRADYKININ AND SUBSTANCE P

Cited by 116 publications

References 29 publications

Tachykinin receptors mediating responses to sensory nerve stimulation and exogenous tachykinins and analogues in the rabbit isolated iris sphincter

Tachykinin receptors mediating responses to sensory nerve stimulation and exogenous tachykinins and analogues in the rabbit isolated iris sphincter

Identification of a B2 bradykinin receptor expressed by PC12 pheochromocytoma cells.

Adenosine‐modulation of cholinergic and non‐adrenergic non‐cholinergic neurotransmission in the rabbit iris sphincter

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THE EFFECTS OF SENSORY DENERVATION ON THE RESPONSES OF THE RABBIT EYE TO PROSTAGLANDIN E1, BRADYKININ AND SUBSTANCE P

Cited by 116 publications

References 29 publications

Tachykinin receptors mediating responses to sensory nerve stimulation and exogenous tachykinins and analogues in the rabbit isolated iris sphincter

Tachykinin receptors mediating responses to sensory nerve stimulation and exogenous tachykinins and analogues in the rabbit isolated iris sphincter

Identification of a B2 bradykinin receptor expressed by PC12 pheochromocytoma cells.

Adenosine‐modulation of cholinergic and non‐adrenergic non‐cholinergic neurotransmission in the rabbit iris sphincter

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THE EFFECTS OF SENSORY DENERVATION ON THE RESPONSES OF THE RABBIT EYE TO PROSTAGLANDIN E₁, BRADYKININ AND SUBSTANCE P