Effects of postoperative sedation with propofol and midazolam on pancreatic function assessed by pancreatitis-associated protein

This prospective randomised controlled study evaluated the effects of postoperative sedation with propofol and midazolam on pancreatic function. We studied 42 intensive care unit patients undergoing elective major surgery who were expected to be sedated postoperatively. Patients were randomly assign...

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Published in	Anaesthesia Vol. 56; no. 9; pp. 836 - 840
Main Authors	PIPER, S. N, KUMLE, B, MALECK, W. H, SUTTNER, S. W, FENT, M. T, BOLDT, J
Format	Journal Article
Language	English
Published	Oxford Blackwell 01.09.2001
Subjects	Acute-Phase Proteins - metabolism Adult Aged Antigens, Neoplasm Biological and medical sciences Biomarkers - blood Biomarkers, Tumor Cholesterol - blood Conscious Sedation - methods Critical Care - methods Drug toxicity and drugs side effects treatment Female Hemodynamics - drug effects Humans Hypnotics and Sedatives - pharmacology Lectins, C-Type Male Medical sciences Midazolam - pharmacology Middle Aged Pancreas - drug effects Pancreas - physiopathology Pancreatitis-Associated Proteins Pharmacology. Drug treatments Postoperative Care - methods Propofol - pharmacology Prospective Studies Toxicity: digestive system Triglycerides - blood Human Postoperative Intensive care Amylase Enzyme Cholesterolemia Toxicity Triacylglycerol lipase Esterases Sedation Carboxylic ester hydrolases Surgery Digestive diseases Hydrolases Benzodiazepine derivatives Midazolam Propofol Sedative Pancreas Comparative study Pancreatic disease Triglyceridemia
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Abstract	This prospective randomised controlled study evaluated the effects of postoperative sedation with propofol and midazolam on pancreatic function. We studied 42 intensive care unit patients undergoing elective major surgery who were expected to be sedated postoperatively. Patients were randomly assigned to a propofol group (n = 21) or a midazolam group (n = 21). To assess pancreatic function, the following parameters were measured: pancreatitis-associated protein, amylase, lipase, cholesterol and triglyceride prior to start of sedation on the intensive care unit, 4 h after the sedation was started and at the first postoperative day. Patients in the propofol group received on average (SD) 1292 (430) mg propofol and were sedated for 9.03 (4.26) h. The midazolam group received 92 (36) mg midazolam and were sedated for 8.81 (4.68) h. Plasma cholesterol concentrations did not differ significantly between groups. Triglyceride plasma levels 4 h after the start of infusion were significantly higher in the propofol group (140 (54) mg.dl(-1)) than the midazolam-treated patients (81 (29) mg.dl(-1)), but were within normal limits. There were no significant differences between the two groups regarding amylase, lipase and pancreatitis-associated protein plasma concentrations at any time. No markers of pancreatic dysfunction were outside the normal range. We conclude that postoperative sedation with propofol induced a significant increase of serum triglyceride levels but that pancreatic function is unchanged with standard doses of propofol.
AbstractList	This prospective randomised controlled study evaluated the effects of postoperative sedation with propofol and midazolam on pancreatic function. We studied 42 intensive care unit patients undergoing elective major surgery who were expected to be sedated postoperatively. Patients were randomly assigned to a propofol group (n=21) or a midazolam group (n=21). To assess pancreatic function, the following parameters were measured: pancreatitis-associated protein, amylase, lipase, cholesterol and triglyceride prior to start of sedation on the intensive care unit, 4h after the sedation was started and at the first postoperative day. Patients in the propofol group received on average (SD) 1292(430)mg propofol and were sedated for 9.03(4.26)h. The midazolam group received 92(36)mg midazolam and were sedated for 8.81(4.68)h. Plasma cholesterol concentrations did not differ significantly between groups. Triglyceride plasma levels 4h after the start of infusion were significantly higher in the propofol group (140(54)mg.dl super(-1)) than the midazolam-treated patients (81(29)mg.dl super(-1)), but were within normal limits. There were no significant differences between the two groups regarding amylase, lipase and pancreatitis-associated protein plasma concentrations at any time. No markers of pancreatic dysfunction were outside the normal range. We conclude that postoperative sedation with propofol induced a significant increase of serum triglyceride levels but that pancreatic function is unchanged with standard doses of propofol. This prospective randomised controlled study evaluated the effects of postoperative sedation with propofol and midazolam on pancreatic function. We studied 42 intensive care unit patients undergoing elective major surgery who were expected to be sedated postoperatively. Patients were randomly assigned to a propofol group (n = 21) or a midazolam group (n = 21). To assess pancreatic function, the following parameters were measured: pancreatitis-associated protein, amylase, lipase, cholesterol and triglyceride prior to start of sedation on the intensive care unit, 4 h after the sedation was started and at the first postoperative day. Patients in the propofol group received on average (SD) 1292 (430) mg propofol and were sedated for 9.03 (4.26) h. The midazolam group received 92 (36) mg midazolam and were sedated for 8.81 (4.68) h. Plasma cholesterol concentrations did not differ significantly between groups. Triglyceride plasma levels 4 h after the start of infusion were significantly higher in the propofol group (140 (54) mg.dl(-1)) than the midazolam-treated patients (81 (29) mg.dl(-1)), but were within normal limits. There were no significant differences between the two groups regarding amylase, lipase and pancreatitis-associated protein plasma concentrations at any time. No markers of pancreatic dysfunction were outside the normal range. We conclude that postoperative sedation with propofol induced a significant increase of serum triglyceride levels but that pancreatic function is unchanged with standard doses of propofol.
Author	BOLDT, J MALECK, W. H PIPER, S. N SUTTNER, S. W FENT, M. T KUMLE, B
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Keywords	Human Postoperative Intensive care Amylase Enzyme Cholesterolemia Toxicity Triacylglycerol lipase Esterases Sedation Carboxylic ester hydrolases Surgery Digestive diseases Hydrolases Benzodiazepine derivatives Midazolam Propofol Sedative Pancreas Comparative study Pancreatic disease Triglyceridemia
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SubjectTerms	Acute-Phase Proteins - metabolism Adult Aged Antigens, Neoplasm Biological and medical sciences Biomarkers - blood Biomarkers, Tumor Cholesterol - blood Conscious Sedation - methods Critical Care - methods Drug toxicity and drugs side effects treatment Female Hemodynamics - drug effects Humans Hypnotics and Sedatives - pharmacology Lectins, C-Type Male Medical sciences Midazolam - pharmacology Middle Aged Pancreas - drug effects Pancreas - physiopathology Pancreatitis-Associated Proteins Pharmacology. Drug treatments Postoperative Care - methods Propofol - pharmacology Prospective Studies Toxicity: digestive system Triglycerides - blood
Title	Effects of postoperative sedation with propofol and midazolam on pancreatic function assessed by pancreatitis-associated protein
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