Effects of the CCKB antagonist L-365, 260 on benzodiazepine withdrawal-induced hypophagia in rats

The effect of the selective CCK_B antagonist L-365, 260 on chlordiazepoxide (CDP) withdrawal-induced hypophagia was assessed in two related studies in rats pretreated for 21 days with CDP at doses escalated from 10 to 30 mg/kg per day (b.i.d.). L-365, 260 was studied at doses from 0.001 to 10 mg/kg (b.i.d.). There was no evidence that L-365, 260 at any dose alleviated CDP withdrawal-induced hypophagia. These data contrast with reports that CCK_B antagonists alleviate behavioural benzodiazepine (BZ) withdrawal symptoms considered to be indicative of anxiogenesis. Presumably, such positive effects of CCK_B antagonists are due to functional antagonism, with enhanced anxiety during BZ withdrawal being attenuated by anxiolytic actions of CCK_B antagonists. Collectively, studies with CCK_B antagonists and other agents involving a number of different BZ withdrawal signs suggest that BZ withdrawal is a heterogeneous syndrome, with various different underlying mechanisms. CCK_B antagonists appear to alleviate only a subset of possible BZ withdrawal signs.     

Chronic administration of the 5-HT3 receptor antagonist BRL 43694; effects on reflex epilepsy and social behaviour of the Mongolian gerbil

The 5-HT₃ receptor antagonist BRL 43694 was administered in drinking fluid to Mongolian gerbils, previously selected for their propensity to exhibit seizures on mild stimulation, for 11 days at doses of 1.5 µg/kg, 150 µg/kg and 1 mg/kg daily, while controls received tap water. Effects upon behaviour during encounters under white light with an untreated resident gerbil were assessed using ethological procedures. Effects upon seizure susceptibility and severity were also examined. All doses of BRL 43694 significantly increased the time spent by gerbils in the social activity attend, and acts of social investigation involving physical contact between animals were significantly increased only by the highest dose of 1 mg/kg, as was occurrence of the specific element, groom. The duration of flight was increased in gerbils receiving the drugs at 1.5 µg/kg. The treatment had no effect upon seizure susceptibility or severity. It is suggested that BRL 43694 increases the sensitivity of gerbils to their social environment. At the lower dose this was seen as an increase in flight, at all doses it was associated with increase of the social activity attend and at the high dose it was manifested as an increase in active social interaction. Further investigations are required to assess the relevance of these findings to the purported anxiolytic activity of 5-HT₃ receptor antagonists.     

A comparison of the effects of TMB-8 and nifedipine on pressor responses to α1- and α2-adrenoceptor agonists in pithed rats

TMB-8 has been characterized as an inhibitor of the release of Ca⁺ from intracellular pools. We have studied the modification of the pressor responses to selective _l-adrenoceptor agonists (methoxamine and phenylephrine), and to selective ₂-adrenoceptor agonists (B-HT 920 and B-HT 933) in pithed rats, produced by TMB-8. We have compared this modification with that produced by the calcium antagonist nifedipine. Nifedipine (100 g/kg, 300 g/kg, and 1000 g/kg) inhibited in a dose-dependent manner the pressor responses to the ₁- and ₂-adrenoceptor agonists, the dose-response curves to the ₂-adrenoceptor agonists being shifted further to the right. TMB-8 at a dose of 3000 g/kg did not modify the pressor effects of the _l-adrenoceptor agonists, and neither did it reinforce the inhibition of such responses produced by nifedipine. By contrast, TMB-8 pretreatment (0.03 g/kg, 0.3 g/kg, 3 g/kg, 30 g/kg, 300 g/kg and 3000 g/kg) inhibited the responses to both ₂-adrenoceptor agonists, the inhibition being more pronounced with B-HT 920. A similar effect was obtained with 0.03 g/kg TMB-8 and 0.3 g/kg TMB-8, particularly in the case of B-HT 920. It was stronger with higher doses, but similar for all doses over 3 g/kg. The inhibition of the pressor responses mediated by the stimulation of ₂-adrenoceptors by TMB-8 was less in rats treated with the Ca²⁺ entry promoter BAY K 8644 (300 g/kg), and could also be reduced by the continuous infusion of CaCl₂ (0.25 g/min). These results suggest that in pithed rats TMB-8 may also behave as an inhibitor of the Ca⁺ influx into vascular smooth muscle.     

Effects of LSD on open field performance in rats

Summary LSD has been reported to have variable actions on locomotor and exploratory activity in rats. In the present study LSD in doses ranging from 2 to 500 g/kg induced varying effects on different components of Open Field behaviour. The ambulation score showed a linear increase with increasing log doses while the highest dose caused a steep rise. The rearing and preening scores exhibited an inverted U type dose-response relationship, the inversion of the curve occuring with doses higher than 8 g/kg. It is suggested that LSD in normal doses increases all stereotyped activity whereas with higher doses only simple stereotyped activity is increased. Simple horizontal stereotyped activity therefore increases at the cost of vertical stereotype. Thus LSD increases stereotyped activity with increasing dose but while normal doses increase both the horizontal and the vertical type of activity, the higher doses increase only the horizontal type.     

Effects of guanabenz and guanfacine on postsynaptic α2-adrenoceptors in the rat submaxillary and parotid glands

Summary The effects of two ₂-agonists (guanfacine and guanabenz) on both the submaxillary and parotid gland of the rat were studied. Whereas guanfacine in doses ranging between 1,000 and 30,000 g/kg i.v. produced an immediate and persistent secretion of saliva from the submaxillary gland, guanabenz in doses as high as 40,000 g/kg did not induce measurable secretion either from the parotid or the submaxillary gland. Secretion clicited by guanfacine was not modified by yohimbine (300 g/kg) but was abolished by prazosin (100 g/kg).In both glands, low doses of either guanabenz (10 g/kg) or guanfacine (100 g/kg) markedly inhibited the secretory responses induced by noradrenaline, methacholine and substance P, but not that induced by isoprenaline. The inhibition caused by the ₂-agonists was greater for noradrenaline than for either methacholine or substance P. Blockade of ₂-adrenoceptors with yohimbine (300 g/kg) did not modify the response to noradrenaline, methacholine or substance P in either gland. However, the same dose of yohimbine injected 5 min before the ₂-agonists prevented the inhibitory effects of guanfacine and guanabenz on the response induced by either one of the three sialagogic agents. Guanabenz (10 g/kg) did not modify the increase in mean blood pressure observed after the different doses of noradrenaline employed to induce salivary secretion. Guanabenz (10 g/kg) and guanfacine (100 g/kg) did not change the time course of the secretion elicited by either noradrenaline, methacholine or substance P, since the degree of inhibition was of similar magnitude at all the periods of time analyzed.The results obtained give further support to the hypothesis that activation of ₂-adrenoceptors in the submaxillary as well as parotid gland of the rat inhibits secretory responses which are mediated by either muscarine, substance P and ₁-receptors and not those elicited by -adrenoceptors.Partially supported by grants no. 3111 k/83 CONICET and Res 40-5/4/84 SUBCYT     

Cardiovascular effects of the novel histamine H2 receptor agonist amthamine: interaction with the adrenergic system

The cardiovascular effects of the new histamine H₂ receptor agonist amthamine were studied in the anaesthetized rat, with particular reference to a possible interaction with the adrenergic system. Amthamine (0.03–3 mol/kg i.v.) caused vasodepressor responses which were antagonized by famotidine (3 mol/kg i.v.). At higher doses (30–100 mol/kg i.v.), amthamine induced a modest increase in the mean arterial pressure, which was significantly enhanced by the blockade of H₂ receptors and significantly reduced by the ₂ adrenoceptor antagonist yohimbine (1 mol/kg i.v.). The vasopressor response to amthamine was not modified in rats pre-treated with reserpine or 6-hydroxydopamine, and was only minimally modified in adrenalectomized animals, thus suggesting a predominant interaction with postjunctional ₂ adrenoceptors in the vascular muscle. The H₂ receptor agonist dimaprit (0.3–100 mol/kg i.v.) caused a reduction in arterial pressure, which was antagonized by famotidine, no pressor response being unmasked.Dimaprit (0.1–30 mol/kg i.v.) did not modify heart rate but caused a modest bradycardia at 100 mol/kg i.v. Amthamine (1-100 mol/kg i.v.) induced a dose-dependent tachycardia, which was only partially (approximately 20%) reduced by famotidine and was totally blocked by propranolol (0.3 mg/kg i.v.). This effect was significantly reduced in rats pre-treated with reserpine or 6-hydroxydopamine and was further reduced by cocaine, thus suggesting a tyramine-like action of amthamine.In conclusion, these data demonstrate that the H₂ receptor agonist amthamine can also interact with the adrenergic system when used at doses higher than those necessary to activate H2 receptors. Whereas the increase in blood pressure induced by amthamine seems to be mainly mediated by a direct activation of postjunctional ₂ adrenoceptors, the increase in heart rate is predominantly due to neuronal release of catecholamines. These effects should be considered when using amthamine in cardiovascular or other studies when high doses are employed.     

Unlike β-endorphin,dynorphin1–13 does not cause retrograde amnesia for shuttle avoidance or inhibitory avoidance learning in rats

Posttraining administration of the opioid peptides, -endorphin or the enkephalins, is known to cause retrograde amnesia for a variety of tasks in rats. The present paper studies the effect of the posttraining administration of dynorphin_1–13 on retention of a step-down inhibitory avoidance task and of a shuttle avoidance task. For the purpose of comparison, the effect of human -endorphin was also studied. In confirmation of previous results, -endorphin (1.0 or 10.0 g/kg, IP) caused retrograde amnesia for the two tasks. Dynorphin_1–13 had no effect at doses between 0.008–125.0 g/kg IP or 1.25–125.0 ng/rat ICV in the inhibitory avoidance task, or at doses of 5.0, 25.0, or 125.0 g/kg in the shuttle avoidance paradigm. These findings suggest that, in contrast to -endorphin, dynorphin_1–13 may not be involved in memory regulation at the posttraining period in rats.     

Modulation of motor activity by α1 and α2 stimulation in mice

Summary The influence of two -adrenoceptor agonists, clonidine and B-HT 920, on motor activity was tested in mice. Both, clonidine and B-HT 920 (2-amino-6-allyl-5,6,7,8-tetrahydro-4H-thiazolo-[4,5-d]-azepine) in the dose range 30–300 g/kg s.c. equieffectively inhibited exploratory activity. On the other hand only clonidine, which stimulates ₂- and ₂-adrenoceptors increased locomotor activity in mice treated with reserpine (5 mg/kg) and apomorphine (3 mg/kg) in the doses of 0.3 and 1 mg/kg i.p. The highly selective ₂-agonist B-HT 920 was ineffective under these conditions up to 30 mg/kg i.p. It is concluded, that in mice sedative -adrenoceptors are of the ₂- and excitatory of the ₁-type.     

β-methyl-digoxin

Summary The tissue/plasma ratio of -methyl-digoxin for cardiac muscle in cats was about the same 24 h after a single dose of 30 g/kg as after a loading dose of 30 g/kg followed by 3 maintenance doses of 7.5 g/kg at 24 h intervals. The ratio for the brain increased 2-fold during that time.After the i.v. injection of a toxic loading dose of 70 g/kg -methyl-digoxin or digoxin, maintenance doses of as little as 15 g/kg at 48 h intervals sufficed to maintain the minimum plasma glycoside concentrations determined by RIA at about 3 ng/ml. There was no difference in the plasma concentrations or in the severity of intoxication produced by both glycosides.Cats vomited within 3 h after i.v. injection of 100 g/kg -methyl-digoxin, whereas a loading dose of 30 g/kg followed by 3 injections of 7.5 g/kg at 24 h intervals were well tolerated. The concentration of radioactivity in the brain 3 h after 100 g/kg was less than 24 h after the last injection of 7.5 g/kg in the experiments with repeated dosage.Cerebral side-effects such as vomiting, loss of appetite and weight were better correlated with the glycoside concentrations in the plasma than with those in the brain.     

Tolerance to the behavioral and neurochemical effects of haloperidol and morphine in rats chronically treated with morphine or haloperidol

Summary The acute administration of morphine sulfate (79 moles/kg) or haloperidol (6.65 moles/kg) produced catalepsy and concomitant increase in striatal dopamine turnover in rats. The animals made dependent on morphine by 52 morphine injections (maintenance dose of 1056 moles/kg/day, given in four daily doses) and then tested during 3 days of withdrawal from morphine, showed tolerance to the cataleptic and the neurochemical effects of morphine as well as those of haloperidol. That tolerance was not seen after 14 days of withdrawal from morphine. The animals chronically treated with haloperidol for 12 days (maintenance dose of 53.2 moles/kg/day, given in two daily doses) and then tested 72 h after last haloperidol injection, did not show tolerance to the cataleptic or the neurochemical effect of haloperidol or morphine. These results suggest that dopaminergic systems underlying motor coordination and regulation of the neurotransmitter synthesis are among those susceptible to narcotic action and to the process of tolerance development during aarcotic dependence.     

Regulation of gastric acid secretion by histamine H3 receptors in the dog: an investigation into the site of action

The involvement of histamine H₃ receptors in the regulation of gastric acid secretion was investigated in the conscious dog with gastric fistula, by the use of the selective agonist (R)-methylhistamine and the selective antagonist thioperamide. (R)-methylhistamine (0.3–1.2 mol/kg/h) induced a dose-related inhibition of the acid secretion induced by pentagastrin and by bombesin, maximum inhibition not exceeding 60–65%. The inhibitory effect of the H₃ agonist (0.6 mol/kg/h) was inhibitited by thioperamide (0.1 mol/kg/h), suggesting that the effect was entirely mediated by H₃ receptors. Thioperamide was also able to enhance the acid response to submaximal doses of pentagastrin and bombesin. The acid secretion induced by histamine was not modified by (R)a-methylhistamine (0.3–1.2 mol/kg/h) but it was significantly enhanced by thioperamide (0.1 mol/kg/h). Neither (R)-methylhistamine nor thioperamide significantly modified the increase in plasma gastrin levels induced by bombesin. In conclusion these data demonstrate that histamine H₃ receptors may represent an effective mechanism for the negative control of stimulated gastric acid secretion in the dog; however, since the inhibition was mainly evident against stimuli which involve the release of histamine, a location of H₃ receptors in paracrine cells of the gastric mucosa rather than in gastrin producing cells or parietal cells seems more likely. Correspondence to: G. Bertaccini at the above address     

Single-dose toxicokinetics of aluminum in the rat

The toxicokinetics of aluminum (Al) in male Wistar rats was studied after single intragastric (IG) doses of 1000 and 12000 g Al/kg and intravenous (IV) doses of 10, 100, 1000, and 12000 g Al/kg. Serial blood samples, daily samples of urine and feces as well as brain, liver, kidney, spleen, quadriceps muscle, and femur samples were collected. Al was measured by atomic absorption spectrometry. Al blood profiles after IV doses were adequately described by a two-compartment open model. Al toxicokinetics was dose dependent and appeared to plateau at 12000 g/kg. At IV doses between 10 and 1000 g/kg the terminal half-life of elimination from whole blood (t_1/2) increased from 29.9±7.8 to 209.3±32.6 min, and the total body clearance (CL) decreased from 2.45±0.64 to 0.28±0.03 ml min^–1 kg^–1. Following an IV bolus of 10 and 100 g/kg the administered Al was recovered completely from urine (94.4%±9.9% and 98.5%±3.2%). Twenty-nine days after the IV dose of 1000 g/kg daily renal excretion decreased to baseline values while only 55.1%±8.0% of the dose was excreted. Nineteen days after the single IV dose of 1000 g/kg Al accumulated in liver (28.1±7.7 versus 1.7±0.5 g/g of control rats) and spleen (72.5±21.1 versus <0.4 g/g). After the single 1000 g/kg IG dose no absorption of Al was detectable. The IG dose of 12000 g/kg resulted in a maximum blood Al level of 47.9±12.4 g/l after 50 min. The blood concentration time curve fitted a one-compartment open model with a half-life of absorption of 28.2±3.6 min and a t_1/2 of 81.2±20.2 min. Cumulative renal Al excretion was 0.18%±0.10% of the dose and oral bioavailability was 0.02%. Seventeen days after the 12000 g/kg IG dose the Al content in femur samples was increased (2.7±1.3 versus 0.6±0.4 g/g). In no case was fecal elimination of incorporated Al observed.     

Behavioral profile of a potent new psychotoxic compound

The first human administration of a new thebaine derivative is described. The drug elicited visual imagery with eyes closed, synaesthesiae and hallucinatory phenomena. In addition to these psychotomimetic effects dysphoria, estrangement, withdrawal and some confusional trends were noted. Physical effects such as tinnitus, ptosis, slurred speech, ataxia, perspiring, tingling of the skin, increase in deep tendon reflexes and variable effects on blood pressure were noted. These effects were of long duration and were elicited by doses of the drug as low as 1 g/kg. The possible significance of the extraordinary potency of this compound is discussed.     

Pharmacokinetics,anticonvulsant efficacy,and adverse effects of trans-2-en-valproate after acute and chronic administration in amygdala-kindled rats

Summary Effects of adenosine and nucleotides on the release of previously stored [3H]-noradrenaline were studied in rabbit brain cortex slices. The slices were stimulated twice, in most experiments by 6 electrical field pulses delivered at 100 Hz.Adenosine and the nucleotides AMP, ADP, ATP, AMPS, ADPS, ATPyS, ,-imido-ATP and ,-methyl-ene-ATP all reduced the evoked overflow of tritiated compounds. For purines for which concentration-response curves were determined, the order of potency was adenosine > ATP ATPyS ,-imido-ATP ADP > ,-methylene-ATP. AMP 30 Etmol/l and AMPS 30 mol/l were approximately equieffective with 30 mol/l of adenosine and ATPS, and ADPS, 30 mol/l was approximately equieffective with 30 mol/l of ADP. ,-Methylene-ADP, 2-methylthio-ATP, UTP and GTPS did not change the evoked overflow of tritium. ,-Methylene-ATP caused an increase; however, the increase was small and became significant only after 59 min of exposure to ,-methylene-ATP or when the slices were stimulated by 30 pulses, 10 H₂. Neither adenosine deaminase (100 U/l) nor the blocker of 5-nucleotidase, ,-methylene-ADP (10 mol/l), attenuated the inhibition caused by ATP, ATPyS and ,-methylene-ATP, despite the fact that adenosine deaminase abolished the effect of adenosine. 8-Cyclopentyl-1,3-dipropylxanthine (DPCPX, 10 nmol/l) shifted the concentration-response curves of adenosine, ATPyS, ,-imido-ATP and ,-methylene-ATP to the right by very similar degrees. 8(p-Sulphophenyl)-theophylline (30 and 300 mol/l) also markedly antagonized the inhibition produced by ATPS. ,-Methylene-ATP (10 and 30 mol/l) and suramin (100 gmol/l) did not modify the effects of adenosine, ATPS and ,-methylene-ATP.It is concluded that nucleotides themselves can inhibit the release of noradrenaline in the rabbit brain cortex. The nucleotides and adenosine seem to act at the same site, i.e., the A₁ subtype of the P₁-purinoceptor. The results support the notion that metabolically stable, phosphate chain-modified nucleotides such as ATPS, ,-imido-ATP and ,-methylene-ATP can be potent P₁ agonists. No evidence was found for presynaptic P_2X-, P_2Y- or P₃-purinoceptors. Send offprint requests to I. von Kugelgen at the above address     

Investigation into the positive inotropic effect of clondine in isolated hearts

Summary Clonidine in doses 2.5–40 g injected into the aortic cannula of isolated, perfused hearts of guinea pigs produced an increase in contraction amplitude. This positive inotropic effect was not antagonised by infusions of doberol (10 g/min), phentolamine (10 g/min) or pheniramine (50 g/min), it was antagonised by burimamide (30 g/min), a histamine H₂ receptor blocking agent. Clonidine showed some similarities to histamine such as parallel dose-response curves and during infusions of burimamide the curve of clonidine was shifted in a way which indicated competitive inhibition. It is suggested therefore that the action of clonidine is due to stimulation of histamine H₂ receptors.     

The effect of nicotine on the swimming speed of pre-trained rats through a water alley

Summary In sessions of ten runs each, swimming time of rats through a 4 m long water alley was measured. Four doses of nicotine (0.05; 0.1; 0.2; 0.4 mg/kg given intraperitoneally 30 minutes before testing) were tested in sessions with a braking load on the tails of the animals either in all 10 runs of a session, or in every second run, or in none of the 10 runs. Regardless of the swimming condition, nicotine produced a considerable, and at doses of 0.1 mg/kg and over, significant decrease of performance in the first two runs. From the third to the 10th run, the changes caused by nicotine were smaller and differed depending on the swimming conditions.A dose of 0.1 mg nicotine/kg improved performance in the without-load-sessions and the without-load-runs of the alternating sessions, while both 0.1 and 0.2 mg/kg improved performance of the with-load-runs of the alternating sessions. Performance in the without-load-sessions and the without-load-runs was depressed by 0.4 mg/kg and that in the with-load-sessions by 0.2 and 0.4 mg/kg.     

Stimulation of central serotonin turnover by β-adrenoceptor agonists

Summary The ₂-stimulators salbutamol (0.3–30 mg/kg i.v.) and clenbuterol (0.3 and 1 mg/kg i.v.), and, to a lesser extent, the ₁-stimulators dobutamine (30 mg/kg i.v.) and prenalterol (30 mg/kg i.v.) increased serotonin metabolism in several rat brain areas, as indicated by increased concentrations of 5-hydroxyindoleacetic acid (5-HIAA) or increased tryptophan hydroxylation in vivo. With salbutamol, increases in 5-HIAA in c. striatum and brainstem, but not in cortex, were observed after intraventricular administration of relatively low doses (3–30 g). Direct application of the compound into the dorsal raphe nucleus at doses of 100 ng and 1 g were without effect, and only mininal 5-HIAA increases occurred after the high dose of 10 g. The effects of salbutamol on the concentrations of 5-HIAA were antagonized by both propranolol and WB4101, indicating an involvement not only of -receptors but also of postsynaptic -receptors.The evidence for and against a central site of action of -agonists with respect to their effect on serotonergic systems is discussed.     

Modulation of memory by post-training epinephrine: involvement of cholinergic mechanisms

Extensive evidence indicates that memory storage can be modulated by peripheral epinephrine as well as by drugs affecting the muscarinic cholinergic system. Low doses of epinephrine (Epi) facilitate memory while high doses induce amnesia. Retention is enhanced by post-training administration of cholinergic muscarinic agonists and impaired by antagonists. The present experiments examined the interaction of peripheral Epi and cholinergic drugs in memory modulation. Male CFW mice (60 days old) were trained on an inhibitory avoidance response (IA) or a Y-maze discrimination response (YMD), injected (IP) immediately post-training and tested 24 h later. In the Y-maze task, retention was assessed by discrimination reversal training. Findings obtained in the two tasks were comparable. Epi (IA: 3.0 g/kg; YMD: 30.0 g/kg) potentiated the memory-enhancing effect of low doses of oxotremorine (Otm) (IA: 16; YMD: 5.0 g/kg) and physostigmine (Phy) (6.8 and 22.0 g/kg for both IA and YMD). The memory-facilitating effect of Otm (50.0 g/kg) was not blocked by an amnestic dose of Epi (IAT: 0.3 mg/kg; YMD: 1.0 mg/kg). Retention was not affected when these amnestic doses of Epi were administered together with a memory-facilitating dose of Phy (68.0 g/kg). In contrast, atropine (IA: 10.0 mg/kg; YMD: 3.0 mg/kg) completely blocked the facilitatory effect of Epi (IA: 10.0 g/kg; YMD: 300 g/kg). These findings indicate that, when administered in low doses, Epi interacts with Otm and Phy. However, cholinergic drugs can block both the memory-enhancing and the memory-impairing effects of Epi. The findings suggest that Epi may modulate memory through cholinergic systems.     

EEG effects of subcutaneous and intracerebroventricular injections of arginine vasopressin in the rat

Several studies have suggested that arginine vasopressin (AVP) may act centrally as a neurohormone or neuromodulator to produce electrophysiological and behavioral effects. However, there are few reports of EEG effects of AVP in unanesthetized, behaving animals. In the present study the EEG effects of behaviorally relevant subcutaneous (SC) doses of AVP (6 g/kg) known to raise blood pressure were compared to behaviorally relevant intracerebroventricular (ICV) doses (0.1–1.0 ng) and multiple toxic ICV doses (1.0 g) of AVP. Central injections of toxic doses of AVP produced behavioral arrest, bodily barrel rolling, and EEG slowing, but did not induce electrographic signs of seizure activity. Comparison of the spectral characteristics of the EEG revealed some similarities in the distribution of power between SC and the 1.0 ng ICV dose; whereas ICV doses of 0.1 and 0.5 ng produced power distributions that were different from those seen following saline or SC doses of AVP. The similarities in EEG activity between SC injections and the 1.0 ng ICV dose suggest a common brain state may be induced by the two routes of administration in those dose ranges.     

Behavioral vigilance in rats: task validation and effects of age,amphetamine, and benzodiazepine receptor ligands

An operant task for the measurement of sustained attention or vigilance in rats was characterized. The task requires the animals to respond to the presentation of visual signals (presented for 25, 50, or 500 ms) by operating one lever (hits) and to the absence of a signal by operating the opposite lever (correct rejection). Incorrect responses (misses and false alarms, respectively) were not rewarded. Performance in this task is a function of signal length, i.e., the shorter the signals the higher the number of misses. An increase in background noise by flashing the chamber houselight (at 0.5 Hz) impaired the animals' ability to discriminate between signal and nonsignal events. Also, flashing the houselight augmented the vigilance decrement observed for shortest signals. An increase in the event-rate also resulted in a vigilance decrement. Finally, the inability of the animals to time signals was examined by testing the effects of an increase in event asynchrony. In a second experiment, the performance of differently aged rats (6- and 20 month-old male BNNia/F344 rats) was studied. Compared to young animals, 20-month-old rats showed a decrease in their ability to discriminate between shortest signals (25 ms) and non-signal events but did not differ in their ability to correctly reject nonsignal trials. Administration of the benzodiazepine receptor (BZR) agonist chlordiazepoxide (CDP; 3, 5, 8 mg/kg) resulted in an impairment of the animals' ability to discriminate between signal and non-signal events and, similar to the effects of age, this effect was exclusively due to an increase in the number of misses. CDP generally produced potent effects while affecting the aged animals to a greater degree. BZR-ligands with weak or selective inverse agonist properties (ZK 93426;-CCtB) did not affect vigilance performance. The BZR partial inverse agonist RU 33965 (0.1, 0.5 mg/kg) dose-dependently impaired vigilance performance. The administration of amphetamine (0.4, 0.8 mg/kg) also impaired performance, but these impairments were possibly based on effects unrelated to attentional mechanisms. The finding that performance in this task revealed the interactions between the effects of age and BZR agonists on attentional abilities further supports the validity of measures of performance generated by this task.