Functional coordination of motor activity in colonic smooth muscles in rat experimental model.

Spontaneous and electrically-elicited motor activity was recorded by triple organ bath in rat segment-model preparation as display of excitation of local nerve networks and ascending or descending reflex pathways underlying contractile potency and functional coordination of colonic longitudinal and circular muscles. Spontaneous high-amplitude contractions, but not relaxations, appeared synchronously in both muscles. Electrical field stimulation applied to proximal or distal part of segments elicited both tetrodotoxin (0.1 microM)-sensitive local motor responses of the stimulated part and ascending or descending motor responses of the contralateral, nonstimulated part of the preparations. Contractions characterized the local response of longitudinal muscle. The circular muscle responded with relaxation followed by contraction. Synchronous ascending contractions and descending contraction of the longitudinal muscle and relaxation followed by contraction of the circular muscle were observed when the middle part of segments was stimulated, thus indicating that locally-induced nerve excitation propagated via intrinsic ascending or descending nerve pathways that could be synchronously coactivated by one and the same stimulus. The ascending motor responses were more pronounced and the motor responses of longitudinal muscle were expressed more than those of circular muscle suggesting an essential role of ascending reflex pathways and longitudinal muscle in the coordinated motor activity of colon.

Functional coordination of motor activity in colonic and recto-anal smooth muscles in rat experimental model.

Spontaneous or electrically elicited contraction and/or relaxation of the longitudinal and circular muscles of the colon and rectum and the anal canal in rat segment preparations were recorded simultaneously to display contractile potency and functional coordination of muscles in the large intestine. Spontaneous high-amplitude contractions, but not relaxations, appeared synchronously in the longitudinal and circular muscles of the colon and rectum. The anal canal showed contractions following the activity of rectal muscles. The colonic and rectal longitudinal muscle responded to electrical stimulation with frequency-dependent contraction. The response of the circular muscle of the colon initially consisted of frequency-independent relaxation followed by frequency-dependent contraction, which was more pronounced in the distal colon, while the rectal circular muscle responded with contraction. The responses appeared synchronously, demonstrating the coactivation of the nervous pathways that supply both muscles. The contractions of longitudinal muscles were more pronounced suggesting a dominant role of this layer in the coordinated motor activity. The local response of the internal anal sphincter was biphasic, comprising short contractions followed by relaxation, while the response of the anal canal was contraction. The contractile local responses increased from the colon to the rectum, while differences in the relaxations were not observed, indicating rather higher contractile potency than the relaxation ability of muscles in the distal part of the gut.

Excitatory ascending and descending motor responses in the guinea pig small intestine: a comparative study of longitudinal and circular muscles by a triple bath method.

A triple organ bath was developed to study the ascending and descending reflexes in a guinea pig small intestine model, allowing synchronous recording the motor activity of the longitudinal and circular muscle layers belonging to the oral and anal part of segment preparations. Field electrical stimulation (0.8 msec, 40 V, 5 Hz, 10 sec) applied either to the anal or oral part of the segments elicited both tetrodotoxin (1 microM)-sensitive contractile local motor responses of muscle layers belonging to the stimulated part and ascending and descending contractions of both muscle layers at a distance of 10 mm were observed when the electrical stimulation was applied to the middle part of the segments. Local responses of the circular muscle layer were considerably higher. The ascending motor responses of both muscle layer were expressed more than those of the circular one. It is concluded that locally induced nerve stimulation propagated via intrinsic ascending or descending neural pathways could be synchronously coactivated by one and the same stimulus. Prominent ascending motor responses and contractility of the longitudinal muscle layer in orally directed reflexes.

Apamin-sensitive nitric oxide- and ATP-mediated motor effects on the guinea pig small intestine.

The involvement of nitric oxide and ATP in both spontaneous and electrically-induced nonadrenergic noncholinergic (NANC) motor activity with special interest in the apamin-sensitive mechanisms was studied in a guinea pig ileum model. Depending on the concentration (0.1 or 1 micromol/l), apamin, a blocker of the calcium-activated potassium channels and antagonist of ATP action, induced either TTX (0.1 micromol/l)-resistant increase in tone or contractions. SNP, a nitric oxide donor, applied cumulatively (0.1-100 micromol/l) evoked a concentration-dependent relaxation, the EC50 value being 0.39 +/- 0.12 micromol/l. At concentrations of 0.1 or 1 micromol/l, apamin decreased the SNP effects and shifted the concentration-response curves for SNP to the right. The EC50 value for SNP in the presence of apamin at a concentration of 0.1 micromol/l increased to 59.34 +/- 36.53 micromol/l. ATP (1 or 50 micromol/l) induced TTX-resistant contractions. The effects of ATP were reduced by apamin (1 micromol/l). The contractile effect of ATP occurred in the presence of SNP. SNP provoked relaxation on the background of ATP. The NANC responses to electrical stimulation (0.8 ms, 40 V, 2 or 20 Hz, 20 s) consisted of an initial relaxation phase followed by a phase of contractions, twitch-like and tonic. L-NNA (0.5 mmol/l), an inhibitor of nitric oxide syntheses, abolished the relaxation phase. L-arginine (0.5 mmol/l) restored it. Apamin (0.1 or 1 micromol/l) completely eliminated the relaxation phase and concentration-dependently inhibited the tonic contraction of the phase of contractions. The present findings indicate that the apamin-sensitive nitric oxide-evoked relaxation could be realized by calcium-activated potassium channels and that the apamin-sensitive ATP-induced contraction is mediated via contraction-producing P2 purinoceptors.

Functional antagonism between nitric oxide and ATP in the motor responses of guinea-pig ileum.

1. The interaction of nitric oxide and ATP in the non-adrenergic, non-cholinergic (NANC) motor responses and the presence of NADPH-diaphorase and quinacrine-positive myenteric neurones were studied on guinea-pig ileum using mechanographic, histochemical and quinacrine-fluorescence techniques. In the presence of phentolamine, propranolol and atropine, the non-precontracted longitudinally oriented organ bath preparations responded to sodium nitroprusside (1-100 microM) or ATP (5-50 microM) with tetrodotoxin (0.1 microM)-resistant relaxation or contraction, respectively. The effects of ATP were suramin (50 microM)- and apamin (5 microM)-sensitive. 2. The NANC motor responses elicited by electrical stimulation (0.8 ms, 1-20 Hz, 20 s) consisted of tetrodotoxin-sensitive relaxation phase followed by a phase of twitch-like and tonic contractions. 3. NG-nitro-L-arginine (L-NNA, 0.1-0.5 mM) inhibited or abolished the relaxation phase. L-arginine (0.5 mM), but not D-arginine (0.5 mM), restored the relaxation phase in L-NNA-pretreated preparations. The relaxation phase increased after ATP-induced desensitization of purinoceptors and in the presence of suramin (50 mciroM) but was abolished by apamin (5 microM). 4. The phase of contractions was enhanced by L-NNA (0.1-0.5 mM) and restored by L-arginine (0.5 mM). The twitch-like and tonic contractions were decreased during ATP-induced purinoceptor desensitization and in the presence of suramin (50 microLM). Apamin (5 microM) inhibited the tonic contractions. 5. The desensitization of purinoceptors by ATP did not change the L-NNA-induced inhibition of the relaxation phase but decreased the L-NNA-increased phase of contractions. L-NNA reduced the relaxation phase and increased the phase of contractions during purinoceptor desensitization. 6. We conclude that in the longitudinal muscle layer of the guinea-pig ileum, nitric oxide mediates the relaxation phase while ATP contributes via smooth muscle P2 purinoceptors to the phase of contractions suggesting a postjunctional functional antagonism between nitric oxide and ATP. The presence of NADPH-diaphorase- and quinacrine-positive neuronal cells and processes running to the muscle cells confirms a physiological role of nitric oxide and ATP in the ileal neurotransmission.

Contribution of nitric oxide and substance P to nonadrenergic, noncholinergic transmission in the guinea pig ileum.

1. The possible contribution of the nonadrenergic noncholinergic (NANC) transmitters nitric oxide (NO) and substance P (SP) to the contractility of guinea pig isolated ileum was studied by the responses of the longitudinal muscle to electrical field stimulation (0.8 msec, 40 V, 1-20 Hz, 20 sec) of the intrinsic nerves and by the presence and distribution of NADPH-diaphorase- and SP-positive nerve structures in the myenteric plexus. 2. The electrically elicited, tetrodotoxin (0.3 microM)-sensitive responses, in the presence of phentolamine (5 microM), propranol (5 microM), and atropine (3 microM) consisted of relaxation, followed by twitch and tonic contraction on which phasic contractions were superimposed. 3. NG-nitro-L-arginine (L-NNA; 0.1 mM or 0.5 mM), an inhibitor of NO synthesis abolished the relaxation. L-arginine (0.1 mM), a substrate for NO synthesis, but not D-arginine, restored it. L-NNA concentration dependently increased the twitch and tonic contractions. Sodium nitroprusside (1 microM or 10 (M), an exogenous donor of NO, was without effect on the electrically evoked responses. 4. AP 13.2 ACOH (AP; 0.1 microM or 10 microM), a blocker of SP receptors, frequency dependently inhibited or even prevented the twitch and tonic contractions. AP concentration-dependently increased the relaxation or reversed the responses to electrical stimulation into a deep relaxation. 5. The concentration-response curve for SP (1 nM-0.1 microM) was shifted to the right by AP, the EC50 values being 5.2 +/- 0.4 nM and 88.0 +/- 3.0 nM, respectively. The effects of SP were not altered by L-NNA (0.1 mM). 6. These findings, supported by morphological data about distribution of NADPH-diaphorase-positive nerve cell bodies and processes and SP-positive varicose fibers, suggest the contribution of NO and SP to NANC transmission. It appears that NO inhibits prejunctionally the SP transmission whereas SP counteracts the NO effect at the postjunctional level.

Pattern of nonadrenergic, noncholinergic responses during short- or long-lasting electrical stimulation in guinea-pig ileum.

1. The pattern of responses of longitudinally oriented guinea pig ileum organ bath preparations was studied during short- (1-5 sec) or long-lasting (20 sec) electrical field stimulation (EFS, 0.8 msec, 40 V, 1-20 Hz). 2. In the presence of phentolamine (5 microM), propranolol (5 microM), and atropine (3 microM), the EFS elicited nonadrenergic, noncholinergic (NANC), tetrodotoxin (0.3 microM)-sensitive responses. 3. The 1-sec EFS evoked relaxation. The response to 5-sec EFS consisted of relaxation followed by twitch, whereas relaxation, twitch and tonic contraction characterized the NANC response to 20-sec EFS. The maximum relaxation was observed at 10-Hz short- or long-lasting EFS. 4. Both N-G-nitro-L-arginine (L-NNA, 0.1-0.5 mM) and apamin (1-5 microM) concentration dependently inhibited the relaxation of the NANC response to 10-Hz 20-sec EFS. During L-NNA treatment, the twitch and the tonic contractions were increased. The inhibitory effect of L-NNA was reversed by L-arginine (0.1-0.5 mM) but not by D-arginine. Sodium nitroprusside (1-10 microM) was without effect. 5. AP 13.2 ACOH (0.1 microM), a blocker of Substance P receptors, inhibited the twitch and the tonic contractions. The contractions were decreased after desensitization of purinoceptors by ATP and in the presence of the GABA(A) receptor antagonist bicuculline (30 microM). 6. Depending on the EFS duration, a subsequent occurrence of relaxation and contractions characterized the NANC responses. It seems that relaxation is mediated by nitric oxide whereas Substance P and ATP are involved in the maintenance of the twitch and the tonic contractions. Nitric oxide appears to exert an inhibitory effect on the excitatory transmitters, whereas purinergic mechanism(s) could modulate the nitric oxide-dependent relaxation.

Met-enkephalin-dependent nitrergically mediated relaxation in the guinea pig ileum.

Met-enkephalin-induced modulation of tetrodotoxin (0.1 microM)-sensitive nonadrenergic, noncholinergic (NANC) nerve-mediated responses of the longitudinal muscle layer of guinea pig ileum during electrical field stimulation (EFS, 0.8 ms, 40 V, 20 s, 1 Hz or 10 Hz) were studied. The response to EFS of untreated preparations was a twitch followed by a low-amplitude tonic contraction. The NANC nerve-mediated response revealed in the presence of phentolamine (5 microM), propranolol (5 microM) and atropine (3 microM) consisted of relaxation followed by a twitch and a tonic contraction. The relaxation was inhibited by NG-nitro-L-arginine (0.1-0.5 mM), a nitric oxide synthase inhibitor. L-arginine (0.5 mM), a substrate of nitric oxide synthase, restored the relaxation to the initial level indicating its nitrergic origin. After adenosine 5'-triphosphate-induced desensitization of purinoceptors the relaxation was enhanced while the contractions decreased. Met-enkephalin (1 nM-1 microM) abolished (J-Hz EFS) or reduced (10-Hz EFS) the relaxation in a frequency-dependent manner, suggesting an inhibitory prejunctional enkephalinergic mechanism modulating the nitrergically mediated relaxant events in the longitudinal muscle layer.

[Cys(O2NH2)2]enkephalin analogues and dalargin: selectivity for delta-opioid receptors.

To investigate the structure-activity relationships for potent and selective action of enkephalins at the delta-opioid receptors, two newly synthesized analogues, [Cys(O2NH2)2,Leu5]enkephalin and [Cys(O2NH2)2, Met5] enkephalin and the hexapeptide [D-Ala2,Leu5]enkephalyl-Arg (dalargin) were tested and compared with [Leu5]enkephalin and [Met5]enkephalin, for their effectiveness to inhibit electrically evoked contractions of the mouse vas deferens (predominantly enkephalin-selective delta-opioid receptors) and the guinea pig ileum (mu- and kappa-opioid receptors). The mouse vas deferens assays included evaluation of the effects of opioid agonists on the first, purinergic, and the second, adrenergic, components of electrically evoked biphasic responses (10 Hz and 20 Hz) and on ATP- or noradrenaline-evoked, tetrodotoxin-resistant responses. The opioids tested inhibited in a similar manner: (i) the purinergic and the adrenergic components of the electrically evoked contractions; and (ii) the ATP- and noradrenaline-induced postjunctional responses of the mouse vas deferens. Extremely low IC50 values (of 2-5 orders) were found for [Cys(O2NH2)2,Leu5] enkephalin, whose relative potency was between 239 and 1316 times higher than that of [Leu5]enkephalin. The order of potency for the other peptides in this tissue was: [Cys(O2NH2)2,Met5]enkephalin > [Leu5]enkephalin > dalargin > [Met5]enkephalin. The highest IC50 values in the guinea pig ileum assays, indicating the lowest affinity for mu-/kappa-opioid receptors, were obtained for the cysteine sulfonamide analogues, while dalargin showed a potency four times higher than that of [Met5]enkephalin. The order of potency in this tissue was: dalargin > [Met5]enkephalin > [Leu5]enkephalin > [Cys(O2NH2)2,Met5]enkephalin > [Cys(O2NH2)2,Leu5]enkephalin. The ratio, IC50 in guinea pig ileum: IC50 in mouse vas deferens, indicating selectivity of the respective peptide for delta-opioid receptors, was extremely high for [Cys(O2NH2)2,Leu5]enkephalin and especially for the adrenergic component of the responses. This ratio for [Cys(O2NH2)2,Met5]enkephalin was higher than the ratios for dalargin, [Leu5]enkephalin and [Met5]enkephalin, which were about 3 orders of magnitude lower. The results suggest that incorporation of hydrophilic Cys(O2NH2) in the enkephalin molecule greatly increases the potency and selectivity of the analogues at delta-opioid receptors, while both D-Ala2 substitution and lengthening of the peptide chain by Arg6 in the molecule of [Leu5]enkephalin decrease them.

Dalargin and [Cys-(O2NH2)]2 analogues of enkephalins and their selectivity for mu opioid receptors.

1. Effects of the enkephalins Met-enk (M) and Leu-enk (L), of two newly synthesized analogues--[Cys-(O2NH2)]2-Met-enk (CM) and [Cys-(O2NH2)]2-Leu-enk (CL)--and of a hexapeptide--D-Ala2-Leu5-Arg6 (Dalargin; DL) on the spontaneous and electrically stimulated activity were examined with respect to their selectivity for the mu opioid receptors in the longitudinal layer of guinea pig ileum. 2. M and CM exerted relaxing and contractile effects on the spontaneous contractile activity while L, CL and DL produced only relaxation. The order of potency towards the relaxatory phase was DL > M > CM > L > CL and towards the contractile phase CM > M. 3. The effects of enkephalins on the spontaneous activity were naloxone and TTX sensitive except for the contractile phase of M and CM which persisted in the presence of TTX. NO was not involved in the neurotransmission of the relaxatory responses, while the blockade of alpha and beta adrenoceptors showed the participation of adrenergic mechanisms. Relaxation and contraction induced by enkephalins could not be directly attributed to cholinergic neurotransmission. 4. The naloxone-sensitive and concentration-dependent inhibitory effects of enkephalins and their analogues on the electrically stimulated cholinergic contractions were established. The order of the relative potency of opioids was: DL-3.8; M-1.0; L-0.4; CM-0.01; CL-0.005. 5. These data indicated that the D-Ala2 substitution and lengthening of the peptide chain by Arg6 in the molecule of L increased the potency at the mu opiate receptors, while the substitution in position 2 with Cys-(O2NH2) in the molecule of M and L yielded a less potent and selective mu agonists.