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Proteases and antiproteases related to the coagulation system in plasma and ascites — Influence of dexamethasone (1987)

Schölmerich, J. ; Zimmermann, U. ; Köttgen, E. ; [et al.]

Springer

Journal of molecular medicine 65 (1987), S. 639-642

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ISSN: 1432-1440

Keywords: Ascites ; Liver cirrhosis ; Plasminogen ; Antiproteases ; Fibrinolysis ; Dexamethasone

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Fibrinolysis induced by the infusion of plasminogen activators into the circulation has been shown to cause coagulation disorders in ascites retransfusion. Dexamethasone is known to inhibit the synthesis of plasminogen activators by peritoneal macrophages. We therefore assessed its potential in preventing the occurrence of fibrinolysis by injecting 16 mg dexamethasone intraperitoneally in 10 patients 24 h before ascites retransfusion was performed. In addition, the effect of dexamethasone upon the activity or concentration of several proteases and antiproteases related to coagulation in plasma and ascites was analyzed on 15 occasions. An increase of the activity of plasminogen, α2-antiplasmin, and antithrombin III, and in the concentration of α1-protease inhibitor in ascites was induced by the dexamethasone injection. However, the reaction was not identical in all patients. Those patients having an increase of plasminogen activities of 0.6 CTA U/ml or more did not show signs of fibrinolysis during retransfusion. The results obtained indicate that intraperitoneal injection of dexamethasone decreases the concentration of plasminogen activators in ascites and thereby reduces the risk of coagulation disorders during retransfusion procedures. Since the effect is variable and not sustained, assessment of preoperative plasminogen concentrations is mandatory in order to prevent complications.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01875498

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Proteases and antiproteases related to the coagulation system in plasma and ascites — An approach to differentiate between malignant and cirrhotic ascites (1987)

Schölmerich, J. ; Zimmermann, U. ; Köttgen, E. ; [et al.]

Springer

Journal of molecular medicine 65 (1987), S. 634-638

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ISSN: 1432-1440

Keywords: Plasminogen ; Fibronectin ; Antiproteases ; Ascites ; Liver cirrhosis ; Tumors

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The concentrations of several proteases and antiproteases known to be present in ascites were tested in plasma and ascitic fluid with regard to their ability to separate ascites according to malignant or nonmalignant disease. Seventeen patients with proven malignant ascites and 37 with ascites due to liver cirrhosis were included. Activities of plasminogen,α 2-antiplasmin, antithrombin-III, and factor V, and the concentration ofα 1-protease inhibitor were significantly higher in the plasma of patients with malignant ascites than in cirrhotic patients. Fibronectin, plasminogen,α 2-macroglobulin,α 1-protease inhibitor, antithrombin-III, and albumin revealed higher concentrations or activities in malignant ascites than in cirrhotic ascites. Due to a wide variation of most parameters, only fibronectin, antithrombin III, andα 1-protease inhibitor in ascites had a sensitivity and specificity higher than 90% for malignant ascites. When the specific protein/albumin ratio was used, only the accuracy of fibronectin was increased reaching a sensitivity and specificity of 100%. The plasma/ascites gradients of the proteins assessed differed significantly, that of fibronectin being much higher (22±7) than that of all other proteins. In malignant ascites fibronectin concentration was only correlated withα 1-protease inhibitor concentration but not with the concentration or activity of all other proteins, while in cirrhotic ascites most proteins revealed a positive correlation. The determination of the fibronectin concentration or the fibronectin/albumin ratio in ascites can differentiate malignant and nonmalignant ascites. All other proteases and antiproteases assessed are of lesser value for this purpose, although most are significantly increased in ascites and plasma of patients with malignant disorders.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01875497

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Prediction of diuretic mobilization of cirrhotic ascites by pretreatment fractional sodium excretion (1990)

Knauf, H. ; Wenk, E. ; Schölmerich, J. ; [et al.]

Springer

Journal of molecular medicine 68 (1990), S. 545-551

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ISSN: 1432-1440

Keywords: Ascites ; Liver cirrhosis ; Xipamide ; Spironolactone ; Furosemide ; Resistance to diuretics ; Fractional sodium excretion ; Side effects

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary In a randomized prospective study the efficacy and side effects of xipamide versus the combination spironolactone/furosemide in the treatment of cirrhotic ascites were studied. Out of 27 patients four responded to a basic treatment consisting of salt and water restriction and one had to be excluded because of deterioration of kidney function. The remaining 22 patients were randomized to additional treatment with either 20 mg xipamide/day (group I) or 200 mg spironolactone/ day combined with 40 mg of furosemide every other day (group II). A response to treatment during the first 4 days was seen in 7 of 11 patients of group I versus only 3 of 11 patients in group II. In the latter group 7 of 11 patients finally responded after 8 days of treatment. Responsiveness to either diuretic treatment strongly depended on pretreatment fractional Na excretion, FENa. The resistance to diuretic treatment can be predicted by a FENa〈0.2%, and could be overcome by additional strategies known to reduce avid proximal Na reabsorption. Xipamide frequently induced hypokalemia, whereas hyperkalemia was seen following treatment with spironolactone/furosemide. Kidney function remained stable during either diuretic treatment.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01667146

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Granulocyte elastase in assessment of severity of acute pancreatitis (1990)

Gross, V. ; Schölmerich, J. ; Leser, H. -G. ; [et al.]

Springer

Digestive diseases and sciences 35 (1990), S. 97-105

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ISSN: 1573-2568

Keywords: acute pancreatitis ; granulocyte elastase ; C-reactive protein ; α1-antitrypsin, α2-macroglobulin

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Complexes of granulocyte elastase and α1-antitrypsin are markers for granulocyte activation. In 75 patients with acute pancreatitis these complexes were immunologically determined daily in plasma during the first week of hospitalization. Patients were classified into three groups: mild pancreatitis (I, ≤1 complication, N=34), severe pancreatitis (II, ≥2 complications, N= 29), lethal outcome (III, N=12). Initially, granulocyte elastase (mean±sem) was lower in group I (348±39 μg/liter) as compared to groups II (897±183 μg/l) and III (799±244 μg/liter), P〈0.001 for I vs II + III. Initial elastase concentrations 〉400 μg/liter were consistent with a severe or fatal course of the disease but did not distinguish between severe and lethal pancreatitis. In patients with mild or severe disease, mean elastase concentrations decreased continuously during the following days (197±15 μg/liter in mild cases, 325±30 μg/liter in severe cases at day 7). In patients with lethal disease, however, mean elastase concentrations even increased at day 2 and remained higher than 700 μg/liter during the observation period. At days 1 and 2 the predictive value for severe or lethal disease of raised (〉400 μg/liter) elastase concentrations [positive predictive value (PPV) 82%, negative predictive value (NPV) 81%] was better than that of elevated (〉100 mg/liter) C-reactive protein (PPV 73%, NPV 73%), elevated (〉4.0 g/liter) α1-antitrypsin (PPV 59%, NPV 50%), or decreased (〈1.5 g/liter) α2-macroglobulin (PPV 82%, NPV 67%). When the time course of the concentrations of the acute-phase proteins was studied, it was found that rises of granulocyte elastase were followed by elevated C-reactive protein levels after one day, by elevated α1-antitrypsin levels after two days and by decreased α2-macroglobulin levels after three to four days. We conclude that granulocyte elastase is a good early marker for the severity of acute pancreatitis. Compared with elevated levels of C-reactive protein and α1-antitrypsin release of granulocyte elastase reflects an event that precedes acute-phase protein induction.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01537230

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Scintigraphic assessment of leukocyte infiltration in acute pancreatitis using technetium-99m-hexamethyl propylene amine oxine as leukocyte label (1991)

Schölmerich, J. ; Schümichen, C. ; Lausen, M. ; [et al.]

Springer

Digestive diseases and sciences 36 (1991), S. 65-70

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ISSN: 1573-2568

Keywords: leukocyte scintigraphy ; technetium-99m-hexamethyl propylene amine oxine ; acute pancreatitis

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract The infiltration of leukocytes has been linked to the pathophysiology of complicated or severe pancreatitis. We have tested the ability of leukocyte scintigraphy using technetium-99m-hexamethyl propylene amine oxine (HM-PAO) as label to demonstrate the localization of leukocytes in the pancreas during acute pancreatitis. Twenty-eight patients with acute pancreatitis (eight with biliary, 13 with alcoholic, and seven with unknown origin) were studied with leukocyte scintigraphy using planar imaging and single photon emission computed tomography (SPECT). Fourteen patients had a mild (group I), 11 a severe (group II), and three a lethal outcome (group III) of pancreatitis. All patients of group III, six of group II, and two of group I had a positive leukocyte scan. Thus, the sensitivity of leukocyte scintigraphy for the detection of a lethal course, of acute pancreatitis was 100%, of a severe course 54%, and of a severe or lethal course 64%. The specificity of a negative scan for a mild pancreatitis was 86%. Comparison of the results of leukocyte scintigraphy with those of contrast enhanced CT showed that six of eight patients with pancreatic necrosis in CT had a positive leukocyte scan, but only five of 20 patients without detectable pancreatic necrosis in CT. In summary, leukocyte infiltration into the pancreas during pancreatitis can be demonstrated by noninvasive leukocyte scintigraphy using technetium-99m-HM-PAO as label. A correlation between the severity of the disease and leukocyte infiltration exists.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01300089

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Zytokine bei akuter Pankreatitis – Pathophysiologische Bedeutung sowie diagnostische und therapeutische Implikation (1998)

Messmann, H. ; Reng, M. ; Schölmerich, J.

Springer

Intensivmedizin und Notfallmedizin 35 (1998), S. 574-581

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ISSN: 1435-1420

Keywords: Key words Pancreatitis ; cytokines ; anti-cytokines ; Schlüsselwörter Pankreatitis ; Zytokine ; Antizytokine

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Description / Table of Contents: Zusammenfassung Zytokine und ihre endogenen Antagonisten werden von Entzündungszellen während der akuten Pankreatitis freigesetzt. Die Rolle der Zytokine in der Initiation der akuten Pankreatitis läßt sich eindrucksvoll am Tiermodell, aber auch an der ERP induzierten Pankreatitis beim Menschen untersuchen. Dabei zeigt sich, daß die Zytokinfreisetzung mit einer gegenregulatorischen Erhöhung der Antizytokine einhergeht. Die Zytokinfreisetzung korreliert gut mit dem Schweregrad der Pankreatitis und erlaubt mithin die Prognose des Krankheitsverlaufes vorauszusagen, wenngleich dies durch die klinische Beurteilung oder mit der Bestimmung der Leukozytenelastase ebenfalls möglich ist. Antientzündliche Zytokine, wie IL-10 oder lösliche Antagonisten/ Rezeptoren von Zytokinen, wie IL-1β und TNF-α sind möglicherweise vielversprechende Stoffe in der Therapie der akuten Pankreatitis, wie dies an Tiermodellen gezeigt wurde und in klinischen Studien jetzt bestätigt werden sollte.

Notes: Summary Cytokines and their endogenous antagonists are released from inflammatory cells during acute pancreatitis. The role of cytokines in the initiation of acute pancreatitis has been examined in animal models but also in patients using the post-ERP pancreatitis model. Cytokine release was followed by an anti-cytokine release. Serum levels of cytokines correlate well with the severity of the pancreatitis and may be useful as prognostic parameters. However, clinical scores as well as PMN elastase are established in determining prognosis. Anti-inflammatory cytokines, like IL-10 or soluble antagonists/receptors of IL-1β und TNF-α may be promising mediators in the treatment of acute pancreatitis as demonstrated in animal experiments. However, clinical trials are necessary to confirm these promising anticytocine therapeutic strategies.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/s003900050181

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