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101. Leukotriene and prostaglandin production after infusion of tumour necrosis factor in man.

Author

Moore KP, Sheron N, Ward P, Taylor GW, Alexander GJ, and Williams R

Subjects
Adult, Epoprostenol urine, Hepatitis B drug therapy, Humans, Kinetics, Leukotriene E4, Male, Middle Aged, SRS-A urine, Thromboxane A2 urine, Epoprostenol metabolism, Hepatitis B metabolism, SRS-A analogs & derivatives, Thromboxane A2 metabolism, Tumor Necrosis Factor-alpha therapeutic use
Abstract

Tumor necrosis factor-alpha is believed to be an important mediator of endotoxaemia and septic shock, the effects of which are thought to be mediated through the generation of cysteinyl-leukotrienes, thromboxane A2 and other prostanoids. We have investigated the production of these eicosanoids and also that of prostacyclin in vivo after infusion of tumor necrosis factor-alpha into 4 subjects with a chronic hepatitis B virus infection. This resulted in plasma TNF levels considerably greater than those observed in septic shock. Urinary excretion rate of leukotriene E4 increased by 2 to 3-fold in all subjects by 8 h following TNF infusion. Urinary excretion of thromboxane B2 and 6-oxo-prostaglandin F1 alpha, however, increased in the first 4 h in 3/4 subjects by 2 to 40-fold and returned towards baseline by 8 h. Excretion of the hepatic metabolite, 2,3-dinor 6-oxo-prostaglandin F1 alpha, increased in all subjects (2 to 4-fold at 4h). We conclude that there is increased production of cysteinyl leukotrienes, thromboxane A2 and prostacyclin after infusion of tumour necrosis factor into man.

Published
1991

102. Metabolism of cysteinyl leukotrienes in monkey and man.

Author

Huber M, Müller J, Leier I, Jedlitschky G, Ball HA, Moore KP, Taylor GW, Williams R, and Keppler D

Subjects
Acetylation, Animals, Bile metabolism, Cells, Cultured, Chromatography, High Pressure Liquid, Humans, In Vitro Techniques, Leukotriene E4, Liver metabolism, SRS-A urine, Macaca fascicularis metabolism, SRS-A analogs & derivatives, SRS-A metabolism
Abstract

The proinflammatory cysteinyl leukotrienes are inactivated in primates by (a) intravascular degradation, (b) hepatic and renal uptake from the blood circulation, (c) intracellular metabolism of leukotriene E4 (LTE4), and (d) biliary and renal excretion of LTC4 degradation products. We have analyzed cysteinyl leukotriene metabolites excreted into bile and urine of the monkey Macaca fascicularis and of man. In both species, hepatobiliary leukotriene elimination predominated over renal excretion. In a representative healthy human subject at least 25% of the administered radioactivity were recovered from bile and 20% from urine within 24 h. In monkey and man intravenous administration of 14,15-3H2-labeled LTC4 resulted in the biliary and urinary excretion of labeled LTE4, omega-hydroxy-LTE4, omega-carboxy-LTE4, omega-carboxy-dinor-LTE4, and omega-carboxy-tetranor-dihydro-LTE4. Small amounts of N-acetyl-LTE4 were detected in human urine only. Oxidative metabolism of LTE4 proceeded more rapidly in the monkey resulting in the formation of higher relative amounts of omega-oxidized leukotrienes in this species as compared to man. [3H]H2O amounted to less than 2% of the administered dose in monkey and human bile and urine samples. Incubation of isolated human hepatocytes with [3H2]LTC4, [3H2]LTD4, and [3H2]LTE4 showed that only [3H2]LTE4 underwent intracellular oxidative metabolism resulting in the formation of omega- and beta-oxidation products. N-Acetylated LTE4 derivatives were not detected as products formed by human hepatocytes. By a combination of reversed-phase high-performance liquid chromatography and radioimmunoassay, endogenous LTE4 and N-acetyl-LTE4 were detected in human urine in concentrations of 220 +/- 40 and 24 +/- 3 pM, corresponding to 12 +/- 1 and 1.5 +/- 0.2 nmol/mol creatinine, respectively (mean +/- SEM; n = 10). Endogenous LTD4 and LTE4 were detected in human bile (n = 3) in concentrations between 0.2-0.9 nM. Our results demonstrate that LTD4 and LTE4 are major LTC4 metabolites in human bile and/or urine and may serve as index metabolites for the measurement of endogenously generated cysteinyl leukotrienes. Moreover, omega-oxidation and subsequent beta-oxidation from the omega-end contribute to the metabolic degradation of LTE4 not only in monkey but also in man.

Published
1990
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103. Increased production of cysteinyl leukotrienes in hepatorenal syndrome.

Author

Moore KP, Taylor GW, Maltby NH, Siegers D, Fuller RW, Dollery CT, and Williams R

Subjects
Adolescent, Adult, Aged, Aged, 80 and over, Creatine urine, Female, Follow-Up Studies, Glomerular Filtration Rate physiology, Hepatorenal Syndrome epidemiology, Hepatorenal Syndrome etiology, Humans, Infusions, Intra-Arterial, Kidney metabolism, Kidney physiopathology, Leukotriene E4, Liver metabolism, Liver physiopathology, Male, Middle Aged, SRS-A administration & dosage, SRS-A analogs & derivatives, SRS-A metabolism, Tritium, Hepatorenal Syndrome urine, SRS-A urine
Abstract

The cysteinyl leukotrienes C4 and D4 are potent renal vasoconstrictors which may modulate glomerular function in vivo, and may therefore be important in the pathogenesis of hepatorenal syndrome. Urinary leukotriene E4, the major metabolite of leukotrienes C4 and D4, was elevated in patients with hepatorenal syndrome (17.8 ng/h) when compared with normal controls (5.1 ng/h) or subjects with renal failure alone (1.9 ng/h). Urinary leukotriene E4 was also elevated in subjects with decompensated liver disease (cirrhosis with ascites 28.6 ng/h, severe hepatocellular dysfunction 57.5 ng/h), but normal in compensated liver disease (6.7 ng/h). In the early stages of hepatorenal syndrome, leukotriene E4 excretion rate was up to 100-fold higher (560 ng/h) than in normals, and fell in parallel with creatinine clearance, indicative of the glomerular filtration rate-dependent renal excretion. Following correction for creatinine clearance, leukotriene E4, excretion was considerably higher in hepatorenal syndrome (54.1 pg/ml creatinine clearance) compared with normals (1.0 pg/ml creatinine clearance), chronic renal failure (3.2 pg/ml creatinine clearance), decompensated liver disease (ascites 7.7 pg/ml creatinine clearance, and severe hepatocellular dysfunction 11.0 pg/ml creatinine clearance), and compensated liver disease (1.9 pg/ml creatinine clearance). To interpret the significance of these findings, we determined renal clearance and endogenous metabolism of the cysteinyl leukotrienes by infusion of [3H]leukotriene C4 into a single subject with hepato-renal syndrome and two control subjects. Renal clearance of leukotriene E4, was reduced in hepatorenal syndrome (2.4 ml/min) compared with controls (greater than 17 ml/min) which together with the increased excretion rate of leukotriene E4 demonstrates that there is increased cysteinyl leukotriene production in hepatorenal syndrome. This may be one of the factors involved in its pathogenesis.

Published
1990
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104. Respiratory consequences of burn injury.

Author

Breheny FX and Moore KP

Subjects
Adolescent, Burns complications, Humans, Male, Respiration Disorders therapy, Burns, Inhalation complications, Respiratory Insufficiency etiology
Published
1981

110. Frequency of pancreatitis in fulminant hepatic failure using isoenzyme markers.

Author

Ede RJ, Moore KP, Marshall WJ, and Williams R

Subjects
Acute Disease, Adolescent, Adult, Female, Humans, Male, Middle Aged, Pancreas enzymology, Pancreatitis etiology, Amylases blood, Clinical Enzyme Tests, Isoenzymes blood, Lipase blood, Liver Diseases complications, Pancreatitis diagnosis
Abstract

Evidence of acute pancreatitis was sought in 35 patients with fulminant hepatic failure. Total amylase was raised in 22 patients and isoenzyme separation showed a distinct P3 isoenzyme (indicative of pancreatitis) in 14. In four patients with marked hyperamylasaemia (greater than 1000 U/l) the predominant isoenzyme was the salivary fraction. Pancreatic lipase was abnormally raised (greater than 200 U/l) in 34 patients but exceeded 1000 U/l in 12 of the 14 with a distinct P3 isoenzyme. Thus on the basis of a distinct P3 isoenzyme of amylase and an increased pancreatic lipase activity evidence of pancreatitis was found in 34% of patients in this series.

Published
1988
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112. Anaesthesia for congenital hypertrophic pyloric stenosis. A review of 350 patients.

Author

MacDonald NJ, Fitzpatrick GJ, Moore KP, Wren WS, and Keenan M

Subjects
Humans, Hypertrophy, Infant, Infant, Newborn, Postoperative Complications etiology, Pyloric Stenosis surgery, Anesthesia, Inhalation adverse effects, Anesthesia, Intravenous adverse effects, Pyloric Stenosis congenital
Abstract

The anaesthetic management of 350 consecutive patients with congenital hypertrophic pyloric stenosis over an 8-year period is reviewed. The anaesthetic technique is discussed and the complications encountered reviewed. The morbidity rate was 15.9%. The anaesthetic related morbidity rate was 3.7%. One patient in the series died (0.27%) 8 weeks after pyloromyotomy, as a result of an underlying myopathy.

Published
1987
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122. Jaundice after anaesthesia.

Author

Campkin TV, McNeil WT, and Moore KP

Subjects
Adult, Chemical and Drug Induced Liver Injury, Drug Hypersensitivity, Female, Humans, Postoperative Complications, Vision Disorders complications, Anesthesia, General, Halothane adverse effects, Jaundice chemically induced
Published
1969
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