ABSTRACT
In the present study, female Wistar albino rats were employed as experimental animals. Acetylcholine [Ach] release was collected with the help of collecting cups placed on the cortex every five minuties. Collection was started 30 minutes prior to i. v. t. administration of test drug and continued for 120 minutes. Ach was bioassayed on leech muscle preparation. It was observed that morphine, beta-endorphin, etorphine and met - enkephalin ub decreased the Ach release. Morphine and beta-endorphin showed most potent effect while met - enkephalin had a minimum effect on Ach release. Etorphine induced inhibition was of a transient nature. Leu - enkephalin did not show any inhibitory effect on Ach release. Naloxone administration, 30 minutes after beta-endorphin, reversed the inhibitory effect on Ach release to pre - drug level
Subject(s)
Morphine , Organization and Administration , Brain Chemistry , Rats , BrainABSTRACT
Clonidine, a potent centrally acting antihypertensive drug was screened for the effect on "free" and "bound" content and acetylcholine [Ach] release in brain of morphine dependent and withdrawal rats. "Free" and "total" Ach content in normal [non- dependent animals as well as animals dependent to morphone was not changed by clonidine. Naloxone produced abstinence syndrome in dependent rats with highly significant increase in "free" and release of Arh. Clonidine pretreatment decreased the rise of "free" content and release of Ach produced by Naloxone
Subject(s)
Acetylcholine/biosynthesis , Brain Chemistry , Rats , BrainABSTRACT
A study of antibiotic prescriptions in [Rabegh Area] Saudi Arabia was undertaken. Prescribing patterns in 200 case were surveyed over a period of six months both in the In- Patient and Out-Patient departments of the hospital. Antibiotics were the drugs most frequently prescribed, suggesting an infectious disease or misuse of these drugs. Other commonly prescribed drugs were also discussed
Subject(s)
Drug Prescriptions , Health Surveys , HospitalsABSTRACT
A method for the chronical administration of morphine by the oral route is discussed. The method recommends the administration of morphine HCl dissolved in a 45% sucrose syrup and given orally for 4 weeks. The initial concentration of morphine in the syrup was 1 mg/ml and was increased weekly upto 4 mg/ml at the end of the experiment. This procedure rendered the animals physically dependent on morphine as observed by drugs withdrawal, when abstinence symptoms were easily identified. It became clear that morphine dependence phenomena [tolerance and the drug induced abstinence syndrome] in both rats and mice developed in association with, and were probably attributable to, change in the activity of cholinergic neurons
Subject(s)
Morphine Dependence , Substance Withdrawal Syndrome , RatsABSTRACT
Cimetidine, a H2 receptor antagonist has been screened for anti-inflammatory activity against carrageenin, 5-hydroxytryptamine [5-HT], formaldehyde, nystatin and croton oil-induced inflammatory models representing acute, subacute and chronic inflammations. Aspirin was used as a standard drug for comparison. The drugs were administered orally. Cimetidine has shown significant anti-inflammatory response in carrageenin - induced and 5-HT - induced oedema models, an insignificant response in formaldehyde - induced oedema while no response in nystatin - induced and croton oil - induced inflammatory models. Cimetidine has prevented ulceration of aspirin when administered concomittantly