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Characterization of phospholipase A2 activity in aspirates of human pancreatic pseudocysts after isolation by reversed-phase high performance liquid chromatography (1989)

Göke, B. ; Meyer, T. ; Loth, H. ; [et al.]

Springer

Journal of molecular medicine 67 (1989), S. 131-135

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ISSN: 1432-1440

Keywords: Phospholipase A2 ; Pancreatic pseudocysts ; HPLC

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Phospholipase A (PLA) is able to attack membrane phospholipids and thereby plays a putative role in the pathogenesis of pancreatic pseudocysts. We looked for PLA2-like activity in aspirates from human pancreatic pseudocysts. In material originating from one cyst which occurred shortly after an acute pancreatitis attack, hydrolyzing enzymatic activity measured by a sensitive bioassay system for PLA2 activity was found without prior trypsin activation (67×103 U/min/100 µl). A biochemical characterization of this hydrolyzing enzymatic activity was provided after resolution of the respective proteins contained in the cyst fluid by HPLC. High hydrolyzing activities were found in correspondence to one specific, early eluting peak. The purified enzyme had pH optima at 3.5 and 6. Addition of EDTA (5 mM) to the test system abolished the enzymatic activity which mirrored the requirement for calcium ions. The activity was optimal at calcium concentrations ranging from 1–2 mM. Higher calcium concentrations reduced the enzymatic activity. The enzyme showed high heat stability. SDS-gel analysis of the peak showed one single band with a molecular weight of about 20,000 Daltons. Our findings demonstrate the possibility of activated, PLA-like activity in human pancreatic pseudocyst fluid. We speculate that an inappropriate activation of this enzyme in peri- or intrapancreatic “fluid collections” could account for pseudocyst formation after an acute pancreatitis attack.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01711338

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Somatostatin-gastrin interactions in the rat stomach (1988)

Koop, H. ; Bothe, E. ; Eissele, R. ; [et al.]

Springer

Research in experimental medicine 188 (1988), S. 115-121

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ISSN: 1433-8580

Keywords: Gastrin ; Rat ; Somatostatin ; Stomach

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Low concentrations of somatostatin and gastrin within or slightly above the range of physiologically circulating levels were perfused in the isolated, vascularly perfused rat stomach preparation. Somatostatin at 10 and 50 pg/ml significantly inhibited acetylcholine-stimulated gastrin secretion by 26% and 45%, respectively, whereas perfusion of 50 and 500 pg/ml exogenous gastrin did not modify gastric somatostatin secretion. Perfusion of somatostatin-antiserum significantly increased gastrin release by 235%. It is concluded that (1) somatostatin is a powerful inhibitor of the gastrin cell under in vitro conditions; the data are in accordance with a concept that endogenous somatostatin could act as a true hormone; (2) the secretory activity of the somatostatin cell is not significantly affected by circulating gastrin.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01852267

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Elimination of the low-molecular weight proteinase inhibitor camostate (FOY 305) and its degradation products by the rat liver (1987)

Beckh, K. ; Göke, B. ; Müller, R. ; [et al.]

Springer

Research in experimental medicine 187 (1987), S. 401-406

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ISSN: 1433-8580

Keywords: Camostate (FOY 305) ; Degradation ; Rat liver ; HPLC

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The elimination of the low molecular weight proteinase inhibitor camostate (FOY 305) was studied in rats after oral administration and in the the situ perfused rat liver. After feeding of camostate (400 mg/kg b. w.) only the metabolites (FOY 251, GBA) were detected in blood samples withdrawn from the portal and hepatic vein. This indicated a rapid degradation of FOY 305 after absorption from the gut lumen. The hepatic extraction of the anti-proteolytic active metabolite FOY 251 during a single liver passage was 23%. It remained almost constant over the period of 120 min. In the perfused rat liver, FOY 305 was given in concentrations comparable to the in vivo studies. It was eliminated by 20%. In these experiments, the compound was metabolized to FOY 251 and in minor amounts to guanidino-benzoate (GBA), the latter being an anti-proteolytic ineffective degradation product. In conclusion, a low hepatic extraction of FOY 305 led to pharmacologically effective concentrations of the active metabolite FOY 251 in the circulation after oral ingestion of the proteinase inhibitor.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01852177

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Release of tryptophan and serotonin into the portal vein of the isolated perfused rat small intestine (1989)

Richter, G. ; Herrmann, C. ; Göke, B. ; [et al.]

Springer

Research in experimental medicine 189 (1989), S. 281-287

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ISSN: 1433-8580

Keywords: Serotonin ; Tryptophan ; Small intestine ; Rat ; Pargyline

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary To investigate the release of serotonin from intestinal enterochromaffin cells, we used an in vitro technique which allows studies excluding overlapping influences from outside the gut. The entire small intestine of rats fed a standard or tryptophan-enriched (3% of total) diet was totally isolated by ligatures with the exception of the superior mesentric artery and portal vein that supply and drain the intestine. Simultaneously to the vascular perfusion (Krebs-Ringer bicarbonate buffer, 0,4% human albumin, 5 mM glucose, 0.6 mM glutamine) the gut lumen was infused (buffer or 0.1 N HCL). Acidification of the gut lumen resulted in an increment of venously released tryptophan and serotonin. After feeding tryptophan-enriched food the release of tryptophan was increased. However, the total amount of released serotonin after tryptophan diet did not differ as compared to that after standard diet. Addition of a monoamino-oxidase inhibitor (pargyline) to the arterial perfusate enhanced the released amount of serotonin 3-fold in the portal venous effluent (at a concentration of 1 mM but not 0.1 mM). Recovery studies done by arterial infusions of serotonin (1 µM, 10µM) and evaluation of the amounts venously released revealed a high loss of infused serotonin (40%–70%). Our data suggest gut-born serotonin to more likely play a paracrine role than a role as a classical hormone.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01852260

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