Patients and methods
Forty postoperative ICU patients with mild to moderate pain entered this randomized prospective, single blinded study. After approval by the Institutional Review Board and obtaining informed written consent from patients or their surrogates they were randomized into two groups. First group received intravenous Paracetamo l1 g in 100 mL normal saline (Uni-Pharma pharmaceutical company, Greece) given in 15 min every 6 h and IV Fentanyl (Hameln Company Germany) 25 μg every three h, both for 48 h. Patients who had breakthrough pain or any need for supplemental analgesics were excluded from the study.
Patients had to have adequate mental status to be evaluated for severity of pain with mild to moderate pain based on a Visual Analogue Scale (VAS 2-5) (Diagram 1). Midazolam was the sedative agent which was used with equal doses as needed, for both groups.
The exclusion criteria were history of allergy to Paracetamol or Fentanyl, contraindications to Paracetamol or opioids use, severe pain (VAS ≥ 5), GCS ≤13, renal disease (Serume Creatinine> 1.5 mg/dL), liver disease (liver enzymes >1.5 normal), chronic lung disease, hemorrhagic conditions, coagulation abnormalities, alcoholic patients, history of addiction to opioids, pregnancy and lactation.
The analgesic effects of the drugs were measured on the basis of VAS and physiologic factors like PR (Pulse rate), RR (Respiratory rate), BP (Blood pressure) and perspiration assessed by clinical examination. Pain was assessed by ICU medical staff under supervision of ICU fellows and using VAS at the time zero i.e. before the analgesic administration and following study drugs administration every 6 h for 48 h. Other neurologic signs such as restlessness, hallucination, insomnia were recorded on hourly basis.
Blood pressure was measured and recorded 5 min before drug injections using non-invasive blood pressure monitors at 15, 30, 45, 60,120, 180 and 240 min after the injections then q4h for 48 h. Other Signs such as heart rate, respiratory rate, oxygen saturation and tympanic temperature were measured and absence or presence of perspiration was recorded.
All patients had to have normal liver, renal and coagulation profiles before entering the study. The laboratory investigations including CBC, BUN, Creatinine, Na, K, PT, PTT,ESR, INR, ALT, AST, FBS, BS, Bilirubin (total and direct) and Albumin were performed before and thereafter on 3rd and 6th day following drug administrations.
Statistical analysis of the collected data was performed on SPSS (version 15) with the T-test method. Fisher exact test was used for comparative testing. The statistical significance with a p < 0.05 was considered valuable and all the results were recorded on the basis of percentage of the patient numbers or mean and standard deviation.