Your search keyword '"Beglinger, Christoph"' showing total 76 results

1. Erythritol and xylitol differentially impact brain networks involved in appetite regulation in healthy volunteers

Author

Meyer-Gerspach, Anne Christin, Wingrove, Jed O., Beglinger, Christoph, Rehfeld, Jens F., Le Roux, Carel W., Peterli, Ralph, Dupont, Patrick, O’Daly, Owen, Van Oudenhove, Lukas, and Wölnerhanssen, Bettina K.

Abstract

ABSTRACTBackgroundThere is a growing consensus that sugar consumption should be reduced and the naturally occurring, low-calorie sweeteners xylitol and erythritol are gaining popularity as substitutes, but their effect on brain circuitry regulating appetite is unknown.AimThe study’s objective was to examine the effects of the two sweeteners on cerebral blood flow (rCBF) and resting functional connectivity in brain networks involved in appetite regulation, and test whether these effects are related to gut hormone release.MethodsThe study was performed as a randomized, double-blind, placebo-controlled, cross-over trial. Twenty volunteers received intragastric (ig) loads of 50g xylitol, 75g erythritol, 75g glucose dissolved in 300mL tap water or 300mL tap water. Resting perfusion and blood oxygenation level-dependent data were acquired to assess rCBF and functional connectivity. Blood samples were collected for determination of CCK, PYY, insulin and glucose.ResultsWe found: (i) xylitol, but not erythritol, increased rCBF in the hypothalamus, whereas glucose had the opposite effect; (ii) graph analysis of resting functional connectivity revealed a complex pattern of similarities and differences in brain network properties following xylitol, erythritol, and glucose; (iii) erythritol and xylitol induced a rise in CCK and PYY, (iv) erythritol had no and xylitol only minimal effects on glucose and insulin.ConclusionXylitol and erythritol have a unique combination of properties: no calories, virtually no effect on glucose and insulin while promoting the release of gut hormones, and impacting appetite-regulating neurocircuitry consisting of both similarities and differences with glucose.

Published

2022

2. Oral administration of glucagon-like peptide 1 or peptide YY 3-36 affects food intake in healthy male subjects

Author

Steinert, Robert E., Poller, Birk, Castelli, M.Cristina, Drewe, Juergen, and Beglinger, Christoph

Subjects

Peptides -- Physiological aspects, Peptides -- Health aspects, Peptides -- Dosage and administration, Peptides -- Research, Food/cooking/nutrition, Health

Abstract

Background: Peripheral infusion of glucagon-like peptide 1 (GLP-1) or peptide YY 3-36 (PYY3-36) reduces food intake in healthy, obese, and diabetic subjects. In vivo, both peptides are cosecreted from intestinal L cells; GLP-1 is subject to rapid breakdown by dipeptidyl peptidase IV, and together with PYY3-36 it is likely to be degraded in the liver before entering the systemic circulation. The largest concentrations are observed in the splanchnic blood rather than in the systemic circulation. Objective: In contrast with peripheral infusion, oral delivery of sodium N-[8-(2-hydroxybenzoyl) amino] caprylate (SNAC) mimics endogenous secretion. We aimed to investigate how this affects food intake. Design: Twelve healthy male subjects were studied in a randomized, double-blind, placebo-controlled, 4-way crossover trial. Each subject received in random order 2.0 mg GLP-1, 1.0 mg PYY3-36, or 2.0 mg GLP-1 plus 1.0 mg PYY3-36; the peptides were mixed with SNAC. The placebo treatment was the delivery agent alone. Food intake during an ad libitum test meal was measured. Results: Both peptides were rapidly absorbed from the gut, leading to plasma concentrations several times higher than those in response to a normal meal. GLP-1 alone, but not PYY3-36, reduced total energy intake significantly, with marked effects on glucose homeostasis. Coadministration of both peptides reduced total energy intake by 21.5% and fullness at meal onset (P < 0.05) but not total 24-h energy intake. Conclusion: The results show a marked effect of orally administered GLP- 1 and PYY3-36 on appetite by showing enhanced fullness at meal onset and reduced energy intake. This trial was registered at clinicaltrials.gov as NCT00822705. Am J Clin Nutr 2010;92: 810-7. doi: 10.3945/ajcn.2010.29663.

Published

2010

3. The ileocecal reservoir for rectal replacement in complicated radiation proctitis

Author

Flue, Markus O. von, Degen, Lukas P., Beglinger, Christoph, and Harder, Felix H.

Subjects

Proctitis, Rectum, Radiation injuries, Health

Abstract

BACKGROUND/AIMS: Total rectal resection is the radical treatment method for radiation proctitis complications. Park's straight colo-anal reconstruction to replace the rectum often impairs anal continence, increases stool frequency, and causes imperative urgency. We developed and assessed a colo-anal reconstruction (ileocecal reservoir) after resection of radiation-damaged rectum. METHODS: An ileocecal segment was isolated on its lymphovascular pedicel, rotated counterclockwise, and reanastomosed at the dentate line. This provided a neorectal segment with intact intrinsic and extrinsic nerve and lymphovascular supply. We evaluated the safety, defecation quality, and anorectal function of this neorectum in two radiation-injured patients when compared with 15 patients after total mesorectal excision without radiation damage. RESULTS: No perioperative morbidity related to this technique was observed. Neorectal patients showed good defecation quality with maximal tolerable volumes, compliances, and anal manometry comparable with patients without radiation injury. CONCLUSIONS: This rectal replacement technique permits good defecation quality and excellent anorectal function.

Published

1996

4. European Registry on Helicobacter pylorimanagement (Hp-EuReg): patterns and trends in first-line empirical eradication prescription and outcomes of 5 years and 21 533 patients

Author

Nyssen, Olga P, Bordin, Dmitry, Tepes, Bojan, Pérez-Aisa, Ángeles, Vaira, Dino, Caldas, Maria, Bujanda, Luis, Castro-Fernandez, Manuel, Lerang, Frode, Leja, Marcis, Rodrigo, Luís, Rokkas, Theodore, Kupcinskas, Limas, Pérez-Lasala, Jorge, Jonaitis, Laimas, Shvets, Oleg, Gasbarrini, Antonio, Simsek, Halis, Axon, Anthony T R, Buzás, Gyo¨rgy, Machado, Jose Carlos, Niv, Yaron, Boyanova, Lyudmila, Goldis, Adrian, Lamy, Vincent, Tonkic, Ante, Przytulski, Krzysztof, Beglinger, Christoph, Venerito, Marino, Bytzer, Peter, Capelle, Lisette, Milosavljević, Tomica, Milivojevic, Vladimir, Veijola, Lea, Molina-Infante, Javier, Vologzhanina, Liudmila, Fadeenko, Galina, Ariño, Ines, Fiorini, Giulia, Garre, Ana, Garrido, Jesús, F Pérez, Cristina, Puig, Ignasi, Heluwaert, Frederic, Megraud, Francis, O'Morain, Colm, and Gisbert, Javier P

Abstract

ObjectiveThe best approach for Helicobacter pylorimanagement remains unclear. An audit process is essential to ensure clinical practice is aligned with best standards of care.DesignInternational multicentre prospective non-interventional registry starting in 2013 aimed to evaluate the decisions and outcomes in H. pylorimanagement by European gastroenterologists. Patients were registered in an e-CRF by AEG-REDCap. Variables included demographics, previous eradication attempts, prescribed treatment, adverse events and outcomes. Data monitoring was performed to ensure data quality. Time-trend and geographical analyses were performed.Results30 394 patients from 27 European countries were evaluated and 21 533 (78%) first-line empirical H. pyloritreatments were included for analysis. Pretreatment resistance rates were 23% to clarithromycin, 32% to metronidazole and 13% to both. Triple therapy with amoxicillin and clarithromycin was most commonly prescribed (39%), achieving 81.5% modified intention-to-treat eradication rate. Over 90% eradication was obtained only with 10-day bismuth quadruple or 14-day concomitant treatments. Longer treatment duration, higher acid inhibition and compliance were associated with higher eradication rates. Time-trend analysis showed a region-dependent shift in prescriptions including abandoning triple therapies, using higher acid-inhibition and longer treatments, which was associated with an overall effectiveness increase (84%–90%).ConclusionManagement of H. pyloriinfection by European gastroenterologists is heterogeneous, suboptimal and discrepant with current recommendations. Only quadruple therapies lasting at least 10 days are able to achieve over 90% eradication rates. European recommendations are being slowly and heterogeneously incorporated into routine clinical practice, which was associated with a corresponding increase in effectiveness.

Published

2021

5. Risk among gastroenterologists of acquiring Helicobacter pylori infection' case-control study

Author

Hildebrand, Pius, Meyer-Wyss, Beat M., Mossi, Sandro, and Beglinger, Christoph

Subjects

Helicobacter infections -- Health aspects, Gastroenterologists -- Health aspects, Disease transmission -- Health aspects, Health, Health aspects

Abstract

It has been suggested that endoscopists are at increased risk of Helicobacter pylori infection, but the results of the different studies have been contradictory.[1 2] Part of the explanation for [...]

Published

2000

6. Comparison of stool immunoassay with standard methods for detecting Helicobacter pylori infection

Author

Lehmann, Frank, Drewe, Jurgen, Terracciano, Luigi, Stuber, Robert, Frei, Reno, and Beglinger, Christoph

Subjects

Helicobacter infections -- Diagnosis, Feces -- Analysis, Immunoassay

Abstract

Helicobacter pylori is the cause of type B gastritis and associated with peptic ulcer disease. Various methods are available for detecting H pylori, but all have limitations) H pylori infection […]

Published

1999

7. Low Discontinuation Rate of Infliximab Treatment in Steroid-Dependent/Refractory Crohn’s Disease Patients

Author

Kaymak, Tanay, Moriconi, Federico, Niess, Jan H., Beglinger, Christoph, and Hruz, Petr

Abstract

Background:Many patients with moderate to severe Crohn’s disease (CD) are treated with infliximab (IFX). As most of these patients experience a long-lasting therapy, the outcome and withdrawal of IFX treatment are important clinical questions. Methods:In this retrospective study, we analyzed the treatment outcome in moderate to severe CD patients with a steroid-dependent/refractory disease course started on IFX. Withdrawal of IFX was evaluated in patients with deep remission defined as clinical (Harvey-Bradshaw Index ≤4), biochemical (fecal calprotectin [FC] ≤150 μg/g stool) over a period of 2 years, and endoscopic and histological remission before discontinuation of IFX. Results:After induction with IFX, clinical remission was observed in 45/109 patients (41.3%) and clinical response in 61/109 patients (56.0%). Only 8/109 patients (7.3%) achieved deep remission and therefore could be discontinued from IFX therapy. In 4 of these patients (50%), relapse was observed after discontinuation of IFX treatment. FC decreased in these 8 patients in deep remission from 652 ± 168 μg/g stool (mean ± SE) at baseline to 24.9 ± 8.1 μg/g stool at 14 weeks. When compared to patients in deep remission, FC had decreased significantly less at 14 weeks in patients in clinical remission after induction with IFX (n= 31; 154 ± 55 μg/g stool; p= 0.01), in patients with clinical response after induction achieving clinical remission during the maintenance phase (n= 11; 352 ± 67 μg/g stool; p= 0.004), or in patients with chronic active disease course on maintenance therapy (n= 50; 645 ± 93 μg/g stool; p< 0.001). Conclusion:A low discontinuation rate was observed for steroid-dependent/refractory moderate to severe CD patients with IFX treatment. As FC showed a more or less pronounced decrease depending on the response to the IFX treatment, monitoring of FC may become a noninvasive tool for tailoring biological therapy in CD patients.

Published

2018

8. Laparoscopic Sleeve Gastrectomy Versus Roux-Y-Gastric Bypass for Morbid Obesity—3-Year Outcomes of the Prospective Randomized Swiss Multicenter Bypass Or Sleeve Study (SM-BOSS)

Author

Peterli, Ralph, Wölnerhanssen, Bettina Karin, Vetter, Diana, Nett, Philipp, Gass, Markus, Borbély, Yves, Peters, Thomas, Schiesser, Marc, Schultes, Bernd, Beglinger, Christoph, Drewe, Juergen, and Bueter, Marco

Published

2017

9. Multiple once-daily subcutaneous doses of pasireotide were well tolerated in healthy male volunteers: a randomized, double-blind, placebo-controlled, cross-over, Phase I study

Author

Beglinger, Christoph, Hu, Ke, Wang, Ying, Bouillaud, Emmanuel, Darstein, Christelle, Wang, Yanfeng, and Mohideen, Pharis

Abstract

Abstract: A randomized, double-blind, placebo-controlled, cross-over, dose-escalating, single-center study was conducted to evaluate the safety, tolerability, and pharmacokinetic (PK) profile of multiple once-daily (qd) subcutaneous (sc) doses of pasireotide in healthy male subjects. Subjects received pasireotide 50, 200, or 600 μg sc qd for 14 days and placebo in separate sequences. Thirty-three subjects were randomized. The most frequently reported drug-related adverse events were injection–site reactions (n = 18), diarrhea (n = 14) and nausea (n = 10), which were mostly mild or moderate in intensity. Pasireotide 600 μg sc was associated with pre- and post-prandial elevations in glucose levels relative to placebo; however, this effect was less pronounced on day 14 compared with day 1. PK steady state appeared to be achieved after 3 days of dosing and PK exposures had a moderate accumulation of 20–40 % across doses. Pasireotide demonstrated fast absorption (T max,ss: 0.25–0.5 h), low clearance (CL/F ss: 8.10–9.03 L/h), long effective half-life (T ½,eff: ~12 h, on average between 9.7 and 13.1 h for 50, 200, and 600 μg sc qd), and large volume of distribution (V z/F ss: 251–1,091 L) at steady state. Dose proportionality was confirmed for C max,ss; other PK parameters (C max, AUC0–24 h and AUCtau) were approximately dose proportional. Growth hormone inhibition was observed with pasireotide 200 and 600 μg sc qd. Gallbladder volume increased post-prandially with pasireotide 200 and 600 μg sc qd, which appeared to correlate with reduced levels of cholecystokinin at these doses. Pasireotide was generally well tolerated up to the tested dose of 600 μg qd, with a linear and time-independent PK profile after sc qd dosing in healthy subjects.

Published

2012

10. Changes in mRNA Expression Levels of Solute Carrier Transporters in Inflammatory Bowel Disease Patients

Author

Wojtal, Kacper A., Eloranta, Jyrki J., Hruz, Petr, Gutmann, Heike, Drewe, Jürgen, Staumann, Alex, Beglinger, Christoph, Fried, Michael, Kullak-Ublick, Gerd A., and Vavricka, Stephan R.

Abstract

Inflammatory bowel disease (IBD) is an inflammatory condition that affects the gastrointestinal tract. The solute carrier (SLC) superfamily of transporters comprise proteins involved in the uptake of drugs, hormones, and other biologically active compounds. The purpose of this study was to determine the mRNA expression levels of 15 solute carrier transporters in two regions of the intestine in IBD patients. Endoscopic biopsy specimens were taken from two locations (terminal ileum and colon) for histological examination and RNA extraction. We quantitatively measured the mRNA expression of 15 SLC transporters in 107 IBD patients (53 with Crohn's disease and 54 with ulcerative colitis) and 23 control subjects. mRNA expression was evaluated using the quantitative reverse transcription-polymerase chain reaction technique. We observed that in the ileum of IBD patients, mRNA levels for serotonin transporter, equilibrative nucleoside transporter (ENT) 1, ENT2, and organic anion-transporting polypeptide (OATP) 2B1 were significantly elevated, whereas levels for apical sodium-dependent bile acid transporter (ASBT) and organic zwitterion/cation transporter (OCTN) 2 were significantly lower. In colon, mRNA levels for ENT1, ENT2, concentrative nucleoside transporter (CNT) 2, OATP2B1, and OATP4A1 were significantly higher, whereas mRNA levels for OCTN2 were significantly decreased. In inflamed colon of IBD patients the mRNA expression levels of ENT1, ENT2, CNT2, OATP2B1, OATP4A1, and peptide transporter 1 were significantly higher. We conclude that intestinal SLC mRNA levels are dysregulated in IBD patients, which may be linked to the inflammation of the tissue and provides an indication about the role of inflammatory signaling in regulation of SLC expression.

Published

2009

11. Effect of Intravenous Esomeprazole 40 mg and Pantoprazole 40 mg on Intragastric pH in Healthy Subjects

Author

Piccoli, Franziska, Ory, Gaëlle, Hadengue, Antoine, Beglinger, Christoph, and Degen, Lukas

Published

2007

12. Single-Ascending-Dose Pharmacokinetics and Safety of the Novel Broad-Spectrum Antifungal Triazole BAL4815 after Intravenous Infusions (50, 100, and 200 Milligrams) and Oral Administrations (100, 200, and 400 Milligrams) of Its Prodrug, BAL8557, in Healthy Volunteers

Author

Schmitt-Hoffmann, Anne, Roos, Brigitte, Heep, Markus, Schleimer, Michael, Weidekamm, Erhard, Brown, Tom, Roehrle, Michael, and Beglinger, Christoph

Abstract

ABSTRACTBAL8557 is the water-soluble prodrug of a novel antifungal triazole, BAL4815. BAL4815 is active against a broad spectrum of major opportunistic and pathogenic fungi, including strains that are resistant to other azoles. Cohorts of healthy male subjects received single-ascending oral (p.o.) doses of BAL8557 that were equivalent to 100, 200, or 400 mg of BAL4815 or single-ascending, 1-h constant-rate intravenous (i.v.) infusions of BAL8557 which were equivalent to 50, 100, or 200 mg of BAL4815. In each cohort, six subjects were randomly assigned to receive active drug and two subjects were assigned to receive the placebo. All doses were well tolerated, and no severe or serious adverse events occurred. Maximum plasma concentrations of BAL4815 were observed 1.5 to 3 h after p.o. drug intake or at the end of the 1-h infusion. After both routes of administration, values for maximum drug concentration observed in plasma and area under the concentration-time curve increased slightly more than proportionally to the administered dose. Mean elimination half-lives were particularly long (56 to 77 h after p.o. administration and 76 to 104 h after i.v. administration). The volume of distribution was large (155 to 292 liters after p.o. administration and 304 to 494 liters after i.v. administration) and systemic clearance was low (1.9 to 2.8 liter/h after p.o. administration and 2.8 to 5.0 liter/h after i.v. administration). Urinary recovery of BAL4815 was less than 0.4% of the infused dose. Based on the exposure data, oral bioavailability of BAL4815 is assumed to be very high. The pharmacokinetics of BAL4815 are well suited to maintaining concentrations of BAL4815 for a long period of time in the body and to enabling an effective treatment of systemic mycoses.

Published

2006

13. Mapping of multidrug resistance gene 1 and multidrug resistance-associated protein isoform 1 to 5 mRNA expression along the human intestinal tract.

Author

Zimmermann, Christian, Gutmann, Heike, Hruz, Petr, Gutzwiller, Jean-Pierre, Beglinger, Christoph, and Drewe, Juergen

Abstract

Efflux transporters such as P-glycoprotein and multidrug resistance-associated proteins (MRPs) in the intestinal wall restrict intestinal drug transport. To overcome this limitation for enteral drug absorption, galenical targeting approaches have been proposed for site-specific luminal drug release in segments of the gut, where expression of the respective absorption-limiting transporter is minimal. Therefore, expression of multidrug resistance gene 1 (MDR1) and MRP1-5 was systematically investigated in 10 healthy subjects. Biopsies were taken from different segments of the gastrointestinal tract (from duodenum and terminal ileum, as well as ascending, transverse, descending, and sigmoid colon). Gene expression was investigated by quantitative real-time PCR (TaqMan). MRP3 appeared to be the most abundantly expressed transporter in investigated parts of the human intestine, except for the terminal ileum, where MDR1 showed the highest expression. The ranking of transporter gene expression in the duodenum was MRP3 >> MDR1 > MRP2 > MRP5 > MRP4 > MRP1. In the terminal ileum, the ranking order was as follows: MDR1 > MRP3 >> MRP1 approximately MRP5 approximately MRP4 > MRP2. In all segments of the colon (ascending, transverse, descending, and sigmoid colon), the transporter gene expression showed the following order: MRP3 >> MDR1 > MRP4 approximately MRP5 > MRP1 >> MRP2. We have shown, for the first time, systematic site-specific expression of MDR1 and MRP mRNA along the gastrointestinal tract in humans. All transporters showed alterations in their expression levels from the duodenum to sigmoid colon. The most pronounced changes were observed for MRP2, with high levels in the small intestine and hardly any expression in colonic segments. This knowledge may be useful to develop new targeting strategies for enteral drug delivery.

Published

2005

14. Role of pantoprazole in the treatment of gastro-oesophageal reflux disease

Author

Lehmann, Frank Serge and Beglinger, Christoph

Abstract

The diagnosis and treatment of gastro-oesophageal reflux disease (GERD) presents many problems, despite the fact that significant advances have been made in recent years in the understanding of its pathogenesis and symptomatology. GERD affects many people and has a significant negative impact on patient quality of life. Heartburn is the most common symptom of GERD which occurs with and without oesophagitis. The predominant causative factor for symptoms is prolonged contact of oesophageal mucosa with refluxed acid and pepsin. Proton pump inhibitors (PPIs) are the most effective treatment for GERD: overall proportions of patients with healing and complete heartburn relief are markedly higher with PPIs than with alternative treatment strategies. Furthermore, the speed of healing and heartburn relief with PPIs is almost twice as rapid as with any other form of therapy. The present review focuses on the effectiveness and safety of the PPI, pantoprazole. The data show that the compound is highly effective in GERD patients with and without oesophagitis. Pantoprazole has an excellent safety record and shows only minor interaction with other drugs.

Published

2005

15. Lanreotide Effect on Splanchnic Blood Flow in Healthy Subjects: Effect of the Rate of Infusion*

Author

Sieber, Cornel C., Beglinger, Christoph, Bart, Simone, Tschoepl, Martin, Currie, Graeme, Larsen, Finn, and Drewe, Juergen

Abstract

Background: Somatostatin is a naturally occurring peptide advocated for the management of hemodynamic complications of chronic liver diseases. The route of administration (bolus application or constant infusion) has been a question of debate.Aim: Our aim was to explore the effects of the somatostatin analog lanreotide, given as a bolus injection or continuous infusion, on food-stimulated hemodynamics in humans.Methods: Twelve healthy subjects (6 men and 6 women) were studied in a double-blind, double-dummy, randomized, crossover study. After a baseline period of 60 minutes, each subject received either a placebo bolus injection and an intravenous infusion of 100 μg/h lanreotide over a period of 8 hours or a placebo infusion over a period of 8 hours and an 800-μg lanreotide bolus injection. Simultaneously, a liquid test meal (Ensure Plus, 6.3 kJ/mL; Abbott Laboratories, Abbott Park, Ill) was perfused intraduodenally at 3 mL/min over a period of 8 hours. Diastolic blood pressure, heart rate, and superior mesenteric arterial and portal venous volume flows were measured at regular intervals by use of echo-Doppler technology. Plasma lanreotide levels were determined at defined intervals.Results: Lanreotide as a 100-μg/h infusion for 8 hours was bioequivalent with lanreotide as an 800-μg bolus injection (mean area under the plasma concentration–time curve [AUC] extrapolated to infinity [AUC∞], 1844.3 ng · min/L versus 1971.0 ng · min/L; AUC∞ratios, 0.99; confidence interval, 0.95-1.02), and clearance was identical (479.2 mL/min versus 413.4 mL/min, P > .05). As expected, significant differences were observed in maximum plasma concentrations (75.58 ng/mL versus 4.85 ng/mL, P < .001) after infusion and bolus injections, respectively. Lanreotide at 100 μg/h over a period of 8 hours was well tolerated and abolished food-stimulated splanchnic hyperemia in both the superior mesenteric artery and the portal vein (mean AUC above baseline values [AUCab], 37.25 L/min · min and 0.51 L/min · min, respectively). In contrast, the same dose of lanreotide given as a bolus injection only temporarily blunted postprandial hyperemia (mean AUCabfor superior mesenteric artery, 251.4 L/min · min, P < .001; mean AUCabfor portal vein, 194.95 L/min · min, P < .001), and subjects had significantly more side effects.Conclusion: On the basis of tolerability and hemodynamic effects, an intravenous infusion of lanreotide seems superior to a bolus injection of the same dose.Clinical Pharmacology & Therapeutics (2004) 75, 70–79; doi: 10.1016/j.clpt.2003.09.006

Published

2004

16. Risk stratification and safe administration of propofol by registered nurses supervised by the gastroenterologist: A prospective observational study of more than 2000 cases

Author

Heuss, Ludwig T., Schnieper, Patrizia, Drewe, Juergen, Pflimlin, Eric, and Beglinger, Christoph

Abstract

Background:Conscious sedation is standard for GI endoscopy. Propofol increasingly is used as an alternative drug to avoid unwanted effects of the commonly used benzodiazepines. Although propofol in the hands of nonanesthesiologists is still controversial, this study characterized the safety profile of propofol administered by nurses under supervision of the gastroenterologist. Methods:All patients undergoing any endoscopic procedure between September 2000 and December 2001 in the gastroenterology department of an academic tertiary medical center were eligible for inclusion in this prospective observational study. Sedation was voluntary. Demographic data, type of endoscopic procedure, and clinical features were recorded. A structured personal history led to a 5-class risk stratification based on the criteria of the American Society of Anesthesiologists. A total of 3475 procedures were performed in 2574 patients using propofol administered by registered nurses. Results:No major complications occurred because of the use of propofol, but overall decreases in the mean values for oxygen saturation (−2%), arterial pressure (−18%), and pulse rate (−10%) were observed. Severe respiratory depression requiring intervention occurred in less than 0.3% of all patients given propofol. Conclusion:The administration of propofol by registered nurses, with careful monitoring under the supervision of the gastroenterologist, is safe for conscious sedation during GI endoscopic procedures. (Gastrointest Endosc 2003;57:664-71.)

Published

2003

17. Gene expression of CYP3A4, ABC-transporters (MDR1 and MRP1-MRP5) and hPXR in three different human colon carcinoma cell lines

Author

Pfrunder, Arabelle, Gutmann, Heike, Beglinger, Christoph, and Drewe, Jürgen

Abstract

Colon carcinoma cell lines are used widely as screening models for intestinal absorption of drugs. However, the expression of important transport systems and of metabolic enzymes is not completely characterized yet. The expression and inducibility of multidrug resistance gene 1 (MDR1) and cytochrome P450 isoform 3A4 (CYP3A4) was investigated in Caco-2 parental, Caco-2 TC-7 (TC-7) and LS180 cell lines. In the same three cell lines, we investigated the expression of isoforms of the multidrug resistance associated protein family (MRP1–MRP5) and the human pregnane × receptor (hPXR), which may be important for MDR1 and CYP3A4 induction. Cells were treated with rifampicin or 1α, 25-dihydroxycholecalciferol (1,25(OH)2D3) for 72 h and the total RNA was extracted. Afterwards reverse transcription real-time polymerase chain reaction (TaqMan) assay was performed to determine the mRNA expression level. We have shown that in LS180 cells, MDR1 and CYP3A4 were inducible with both inducers. In Caco-2 parental and TC-7 cells, CYP3A4 was only inducible with 1,25(OH)2D3. Furthermore, differences were shown in gene expression of several transport proteins (MDR1 and MRP1–MRP5) and CYP3A4 in different human colon carcinoma derived cell lines. hPXR mRNA was expressed in all three cell lines but the amount of mRNA detected was significantly higher in LS180 cells than in Caco-2 and TC-7 cells. We concluded that LS180 cells were a suitable model to study MDR1 and CYP3A4 induction, but for drug transport studies Caco-2 parental and TC-7 cells would be preferred as the more physiological model.

Published

2003

18. Neuroendocrine tumor targeting: Study of novel gallium-labeled somatostatin radiopeptides in a rat pancreatic tumor model

Author

Froidevaux, Sylvie, Eberle, Alex N., Christe, Martine, Sumanovski, Lazar, Heppeler, Axel, Schmitt, Jörg S., Eisenwiener, Klaus, Beglinger, Christoph, and Mäcke, Helmut R.

Abstract

Somatostatin analogs labeled with radionuclides are of considerable interest in the diagnosis and therapy of SSTR-expressing tumors, such as gastroenteropancreatic, small cell lung, breast and frequently nervous system tumors. In view of the favorable physical characteristics of the Ga isotopes ⁶⁷Ga and ⁶⁸Ga, enabling conventional tumor scintigraphy, PET and possibly internal radiotherapy, we focused on the development of a Ga-labeled somatostatin analog suitable for targeting SSTR-expressing tumors. For this purpose, 3 somatostatin analogs, OC, TOC and TATE were conjugated to the metal chelator DOTA and labeled with the radiometals ¹¹¹In, ⁹⁰Y and ⁶⁷Ga. They were then evaluated for their performance in the AR4-2J pancreatic tumor model by testing SSTR2-binding affinity, internalization/externalization in isolated cells and biodistribution in tumor-bearing nude mice. Surprisingly, we found that, compared to ¹¹¹In or ⁹⁰Y, labeling with ⁶⁷Ga considerably improved the biologic performance of the tested somatostatin analogs with respect to SSTR2 affinity and tissue distribution. ⁶⁷Ga-labeled DOTA-somatostatin analogs were rapidly excreted from nontarget tissues, leading to excellent tumor-to-nontarget tissue uptake ratios. Of interest for radiotherapeutic application, [⁶⁷Ga]DOTATOC was strongly internalized by AR4-2J cells. Furthermore, our results suggest a link between the radioligand charge and its kidney retention. The excellent tumor selectivity of Ga-DOTA somatostatin analogs together with the different applications of Ga in nuclear oncology suggests that Ga-DOTA somatostatin analogs will become an important tool in the management of SSTR-positive tumors. © 2002 Wiley-Liss, Inc.

Published

2002

19. Pseudotumor of the Pancreatic Head Associated with Idiopathic Retroperitoneal Fibrosis

Author

Wiesner, Walter, Kocher, Thomas, Beglinger, Christoph, Harder, Felix, and Steinbrich, Wolfgang

Abstract

A 68-year-old male presented with abdominal pain and obstructive jaundice. CT revealed a large mass in the pancreatic head that was initially interpreted as pancreatic carcinoma. Needle biopsy revealed only fibrous tissue with signs of chronic inflammation. Together with typical findings of an idiopathic retroperitoneal fibrosis, the final diagnosis of multifocal idiopathic fibrosclerosis with focal pseudotumorous pancreatic head fibrosis could be made.

Published

2001

20. Blockade of GRP receptors inhibits gastric emptying and gallbladder contraction but accelerates small intestinal transit

Author

Degen, Lukas P., Peng, Fuping, Collet, Annette, Rossi, Livid, Ketterer, Silvia, Serrano, Yolanda, Larsen, Finn, Beglinger, Christoph, and Hildebrand, Pius

Abstract

Background & Aims:This study was designed to characterize [D-F5Phe6D-Ala11]Bn(6-13)OMe (BIM26226) as a gastrin-releasing peptide (GRP)-preferring bombesin receptor antagonist and to determine whether GRP physiologically regulates gastrointestinal motility. Intravenous BIM26226 (5–500 μg · kg−1· h−1) inhibits GRP-induced gallbladder contraction and plasma cholecystokinin (CCK) release in a dose-dependent fashion. Methods:Gastric emptying and small bowel transit of a solid meal were quantified using scintigraphy. Meal-stimulated gallbladder contraction was measured by sonography in a 2-period crossover design. Results:Intravenous BIM26226 potently inhibited gastric lag time (114 ± 7 vs. 41 ± 6 minutes [control]) and gastric emptying rate (0.11 ± 0.02%/min vs. 0.26 ± 0.04%/min [control]), whereas concomitant infusion of BIM26226 accelerated small bowel transit time (153 ± 41 vs. 262 ± 20 minutes [control]). A continuous liquid meal perfusion into the duodenum induced complete gallbladder contraction (t50%, 35 ± 4 minutes), which BIM26226 inhibited significantly (t50%, 64 ± 8 minutes). BIM26226 did not alter plasma CCK response, indicating that circulating CCK did not mediate these effects. Conclusions:These data show that BIM26226 is a potent antagonist of exogenous and endogenous GRP and suggest that GRP is a major physiologic regulator of gastric emptying, small bowel transit, and gallbladder contraction.

Published

2001

21. Postoperative gastrointestinal physiology following operations on the stomach

Author

Degen, Lukas P. and Beglinger, Christoph

Published

2001

22. Locally inducible CD66a (CEACAM1) as an amplifier of the human intestinal T cell response

Author

Donda, Alena, Mori, Lucia, Shamshiev, Abdijapar, Carena, Ilaria, Mottet, Christian, Heim, Markus H., Beglinger, Christoph, Grunert, Fritz, Rochlitz, Christoph, Terracciano, Luigi, Jantscheff, Peter, and Libero, Gennaro De

Abstract

CD66a is an adhesion molecule member of the carcinoembryonic antigen immunoglobulin-like family present on the surface of epithelial cells, granulocytes and IL-2 activated T cells. We studied whether CD66a is expressed in vivo by T lymphocytes and whether it affects TCR-mediated activation. CD66a was detected by histochemistry, flow cytometry analysis, reverse transcription PCR and Western blot on fresh colon biopsies and T cell clones. A fraction of T cells in the lamina propria express CD66a, which is induced by IL-7 and IL-15 cytokines. T cells express four different CD66a splice variants and at least two forms of the protein are glycosylated in a cell type-specific manner. Triggering of CD66a on T cells with physiological ligands or with specific mAb increases TCR-mediated lymphokine release, in an antigen dose-independent manner. This effect requires the presence of the CD66a intracytoplasmic domain, which contains two immunoglobulin receptor family tyrosine-based inhibitory motif-like domains, as shown by stimulation of Jurkat cells transfected with different CD66a isoforms and is associated with increased induction of AP1 and NFκB transcription factors. These data indicate that CD66a amplifies T cell activation and thus could facilitate crosstalk between epithelial cells and T lymphocytes in intestinal immune response.

Published

2000

23. Evidence for Different ABC-Transporters in Caco-2 Cells Modulating Drug Uptake

Author

Gutmann, Heike, Fricker, Gert, Török, Michael, Michael, Susanne, Beglinger, Christoph, and Drewe, Jürgen

Abstract

Purpose. Secretory systems contribute to drug absorption in the gastrointestinal tract. The purpose of this study was the identification of members of the ATP binding cassette superfamily of secretory transport proteins that may potentially modulate drug absorption in Caco-2 cells, which are an important cellular model predicting enteral absorption of drugs. Methods. Kinetic studies as well as PCR- and Western blot studies with confluent epithelial layers of human Caco-2 cells. Results. The study demonstrates functional expression of multidrug resistance related protein (MRP) and P-glycoprotein (P-gp) in Caco-2 cells: 1) Efflux studies with the MRP specific substrate glutathion-methylfluorescein (GS-MF) showed functional activity of MRP in Caco-2 cells preloaded with the metabolic precursor of GS-MF, chloro-methylfluoresceine-diacetate, CMFDA. Excretion of GS-MF was decreased in presence of the MRP-blocker MK-571.2) Transport experiments with cyclosporin A demonstrated the functional activity of P-gp. Cellular accumulation was increased in presence of the P-gp blocking agent SDZ-PSC 833.3) The expression of the 190 kDa protein MRP and the 170 kDa protein P-gp in Caco-2 cells was shown by Western blot analysis with specific monoclonal antibodies. 4) The expression of MRP-mRNA in Caco-2 cells was detected by RT-PCR and compared with the MRP over-expressing cell line H69AR. MRP primers recognize specifically human MRP1 (GenBank accession number L05628), but not all other published sequences of MRP (MRP2-MRP6). P-gp expression on mRNA-level was also confirmed by RT-PCR. Conclusions. The data demonstrate that besides P-gp, multidrug resistance related protein (MRP) is functionally expressed in Caco-2 cells and contributes to the active excretion of substrates in this cell line.

Published

1999

24. Dose-dependent gastrointestinal effects of the somatostatin analog lanreotide in healthy volunteers*

Author

Drewe, Jürgen, Sieber, Cornel C., Mottet, Christian, Wullschleger, Christoph, Larsen, Finn, and Beglinger, Christoph

Abstract

Objective: To investigate the gastrointestinal effects of intravenous lanreotide.Methods: Twenty healthy male subjects participated in 2 subsequent placebo-controlled, double-blind crossover studies. The effects of 3 doses of lanreotide (50, 100, and 200 μg/h) were investigated on 24-hour intragastric acidity (study I), food-stimulated gallbladder contraction, and plasma cholecystokinin release (study II).Results: Lanreotide showed linear pharmacokinetics. It raised median intragastric pH significantly and in a dose-dependent manner: from 1.4 ± 0.2 (placebo) to 2.5 ± 0.8 (P < .002) during administration of 50 μg/h lanreotide, to 3.2 ± 0.7 (P < .001) during 100 μg/h lanreotide, and to 4.3 ± 0.7 (P < .001) during 200 μg/h lanreotide. However, no significant inhibition of gastrin secretion could be established. All doses completely inhibited postprandial gallbladder contraction.Conclusion: Intravenous administration of lanreotide at rates applied in this study was able to significantly inhibit intragastric acid secretion and postprandial gallbladder contraction; under these conditions few untoward effects were noted.

Published

1999

25. Clinical outcome and quality of life after gastric and distal esophagus replacement with an ileocolon interposition

Author

Metzger, Jürg, Degen, Lukas, Beglinger, Christoph, von Flüe, Markus, and Harder, Felix

Abstract

Abstract: Mainly because of the loss of reservoir function, loss of sphincter function, and exclusion of the duodenal route, patients who undergo gastrectomy suffer from many adverse effects postoperatively. The ileocecal interpositional graft is an attractive method to use as a gastric substitute after gastrectomy and distal esophagectomy. A pedunculated ileocecal graft is placed between the esophagus and the duodenum. The cecum acts as a reservoir while the ileocecal valve protects against enteroesophageal reflux. The duodenal passage is also preserved. Fourteen patients underwent this operation. The technique-related morbidity was low and the quality of life was good. During a mean follow-up of 6 months, no evidence of severe dumping syndrome or reflux esophagitis was observed. Further prospective randomized studies are warranted to compare this technique with the standard methods of gastric reconstruction.

Published

1999

26. ROLE OF CHOLECYSTOKININ IN REGULATION OF GASTROINTESTINAL MOTOR FUNCTIONS

Author

Meyer, BeatM., Beglinger, Christoph, Jansen, JanB.M.J., Rovati, LucioC., Werth, BaseliA., Hildebrand, Pius, Zach, David, and Stalder, GeorgA.

Abstract

By means of loxiglumide, a potent and highly specific antagonist for cholecystokinin (CCK), the effects of blocking CCK receptors on gastrointestinal motility were investigated in a placebo-controlled study in healthy young men (aged 21-39, mean 24 years). Gallbladder contraction stimulated by ingestion of a liquid test meal was completely abolished by oral administration of loxiglumide 30 min before the test meal. Gastric emptying of radio-opaque markers ingested with the test meal was significantly accelerated by loxiglumide (area under the curve [markers × h] 33·3 [SEM 3·8] vs17·9 [2·7] after placebo). No effect of loxiglumide was found on small-bowel transit time, but 7 days' treatment with oral loxiglumide (800 mg three times daily) significantly shortened colonic transit time (29·4 [4·1] h after placebo, 15·0 [3·4] h after loxiglumide). It is concluded that CCK is an important mediator of meal-induced gallbladder contraction and is involved in the regulation of gastrointestinal motility in man.

Published

1989

27. Interaction of the cholinergic system and cholecystokinin in the regulation of endogenous and exogenous stimulation of pancreatic secretion in humans

Author

Adler, Guido, Beglinger, Christoph, Braun, Ute, Reinshagen, Max, Koop, Irmtraut, Schafmayer, Anton, Rovati, Lucio, and Arnold, Rudolf

Abstract

Pancreatic enzyme secretion is regulated in humans by the cholinergic system and by cholecystokinin (CCK). The interaction between both regulatory systems in response to exogenous and endogenous stimulation was analyzed in the present study using the cholinergic antagonist atropine and the CCK antagonist loxiglumide. A dose-dependent stimulation of pancreatic enzyme output was achieved either by duodenal perfusion of graded caloric loads or by IV infusion of increasing doses of cerulein. Prestimulated pancreatic secretion was inhibited by atropine and loxiglumide. Atropine furthermore almost completely blocked meal-stimulated pancreatic secretion, whereas loxiglumide caused 60% inhibition. The enzyme response to graded doses of exogenous CCK was significantly inhibited by atropine and loxiglumide. Plasma levels of CCK were not altered by atropine but increased with infusion of loxiglumide. This study supports the concept that pancreatic enzyme secretion is predominantly dependent on a cholinergic tone and that CCK modulates the enzyme-secretory response.

Published

1991

28. Role of cholecystokinin in the regulation of gastric emptying and pancreatic enzyme secretion in humans

Author

Fried, Michael, Erlacher, Urs, Schwizer, Werner, Löchner, Christine, Koerfer, Jacques, Beglinger, Christoph, Jansen, Jan B., Lamers, Cornelis B., Harder, Felix, Bischof-Delaloye, Angelika, Stalder, Georg A., and Rovati, Lucio

Abstract

The role of cholecystokinin (CCK) in the regulation of gastric emptying and pancreatic enzyme secretion was evaluated by infusing the CCK-receptor antagonist loxiglumide. Gastric emptying rates and pancreatic secretory outputs were measured in five healthy volunteers by the double-indicator perfusion technique using a multiple-lumen tube in the duodenum. Placebo or loxiglumide (22 μmol · kg−1· h−1) was infused throughout each experiment. Five hundred-milliliter liquid intragastric meals of (a) fat, protein, and glucose (Ensure; Abbott, Chicago, IL); (b) glucose, 20 g/dL; and (c) guar gum, 1.1 g/dL, were given in random order. In addition, the effect of a physiologic CCK-8 dose (20 pmol · kg−1· h−1) after an intragastric 500-mL saline meal (0.154 mol/L) was tested. Intravenous CCK-8 induced a marked retardation of the gastric emptying rate of the saline solution (P< 0.05) while stimulating pancreatic secretory outputs; both effects were completely abolished by the infusion of loxiglumide. Loxiglumide markedly accelerated the gastric emptying rates (by ~ 40%) and simultaneously diminished lipase (by ~ 75%) and trypsin (by ~ 50%) outputs of both the mixed meal (P< 0.01) and the pure glucose meal (P< 0.05). Additional experiments using gamma camera scintigraphy confirmed the accelerating effect of loxiglumide on gastric emptying of the mixed meal (P< 0.01). The gastric emptying rate of the guar meal, which did not release CCK, was not influenced by the infusion of loxiglumide. Loxiglumide distinctly augmented plasma CCK levels after the mixed (2.6 times) and the pure glucose (2.1 times) meals while markedly reducing (~ 76%) pancreatic polypeptide release (P< 0.02). It is concluded that endogenous CCK exerts a major role in the regulation of both gastric liquid emptying and pancreatic secretion in humans.

Published

1991

29. Effect of intravenous human gastrin-releasing peptide on food intake in humans

Author

Gutzwiller, Jean-Pierre, Drewe, Juergen, Hildebrand, Pius, Rossi, Livio, Lauper, Johanna Zwimpfer, and Beglinger, Christoph

Abstract

Background/Aims:Bombesin and gastrin-releasing peptide (GRP) are closely related peptides. Both have been proposed to serve as a satiety signal in animals. Methods:To explore further the role of GRP in humans, its effects on satiety and eating behavior were investigated by infusion of GRP into healthy men at three dosages (10, 40, and 160 pmol/kg per hour) and compared with saline infusions. Results:GRP produced a significant reduction in calorie intake (P< 0.05) but only a 19% (nonsignificant) reduction in food intake. Fluid ingestion was not affected by GRP. No overt side effects were produced by GRP, but subjects experienced less hunger and early fullness in the premeal period during GRP infusion but not when receiving saline (P< 0.05−0.01). Conclusions:This study shows that intravenous infusions of GRP can decrease spontaneous food intake at concentrations that produce physiological effects, such as stimulation of acid or pancreatic secretion or gallbladder contraction. The data imply that GRP-like peptides can act as satiety signals in humans, confirming data previously reported in animals.

Published

1994

30. Tolerability and Absorption Enhancement of Intranasally Administered Octreotide by Sodium Taurodihydrofusidate in Healthy Subjects

Author

Kissel, Thomas, Drewe, Juergen, Bantle, Siegfried, Rummelt, Andreas, and Beglinger, Christoph

Abstract

Nasal sprays containing different concentrations of the somatostatin analogue octreotide and sodium tauro-24,25-dihydrofusidate (STDHF) as an absorption promoter were evaluated in two consecutive pharmacokinetic studies in healthy volunteers to characterize their bioavailability and local tolerability. The concentrations of STDHF were selected on the basis of a phase diagram generated by a dynamic laser light-scattering technique to ensure that the mixture was above the critical micellar concentrations. Compared to a 50-µg subcutaneous injection, the nasal spray formulation without STDHF had a mean relative bioavailability of 17.9%. For nasal formulations containing 3 and 1.65% (w/v) of STDHF, the bioavailability increased to 29.0 and 25.7%, respectively. The enhancement of nasal absorption was dependent on the STDHF concentrations as shown by decreasing the amounts to 1.2 and 0.8% (w/v) for tolerability reasons; the bioavailability was reduced to 15.3 and 20.5% in these cases, respectively. The local tolerability of all STDHF-containing sprays was poor, leading to stinging sensations and lacrimation. The poor local tolerability of the octreotide nasal spray containing different concentrations of STDHF required for effective nasal absorption enhancement appears to be impractical for further clinical development. These findings clearly stress the necessity to investigate tolerability and safety issues of new drug delivery systems in early developmental phases.

Published

1992

31. Hormonal Control of Pancreatic Secretion by Intrajejunal HCl

Author

Niebel, Wolfgang, Beglinger, Christoph, and Singer, Manfred V.

Abstract

To elucidate the role of hormones in the control of pancreatic secretion, we developed, in seven dogs, a model of total extrinsic denervation of the jejunoileum by autotransplanting this segment of bowel. A Thomas-like cannula was placed into the stomach, the duodenum (to collect pure pancreatic juice), and the proximal part of the jejunum. Thus, intestinal stimulants could only stimulate the pancreas via release of humoral (= hormonal) mediators. Seven control dogs received only the three fistulas. After recovery, dose-response curves of pancreatic bicarbonate and protein response to perfusion of the extrinsically denervated or innervated jejunoileum with HC1 (1.5 to 48 mmol h−1) were performed with and without atropine (14 nmol kg−1h−1i.v.). Plasma levels of secretin were determined by radioimmunoassay. The maximal bicarbonate output occurred in response to 24 mmol h−1of HC1 and was significantly (p < 0.05) higher in intact as compared to denervated animals. Atropine only significantly depressed the bicarbonate response to HC1 in dogs with a denervated jejunoileum. HC1 caused a dose-dependent increase in plasma levels of secretin, which was not altered by denervation and/or atropine. Irrespective of the innervation of the small bowel, pancreatic protein output was only significantly stimulated above basal when high loads (12–48 mmol h−1) of HC1 were given. Atropine significantly reduced these responses. We conclude that (a) intrajejunal HC1 stimulates pancreatic bicarbonate and protein secretion via release of hormones; (b) extrinsic denervation of the jejunoileum lowers the maximal pancreatic bicarbonate response to intrajejunal HC1; (c) cholinergic extrinsic nerves of the jejunoileum are probably not involved in the control of pancreatic bicarbonate response to HC1; (d) release of secretin by HC1 does not depend on the extrinsic and intrinsic cholinergic nerves of the jejunoileum; and (e) high loads of HC1 stimulate pancreatic protein output by an atropine-sensitive mechanism that is independent of the integrity of the extrinsic nerves of the jejunoileum.

Published

1991

32. Pancreatic Secretory Responses to LongTerm Infusions of Secretin and Cerulein in Humans

Author

Adler, Guido, Drewe, Jürgen, Steinmetz, Andrea, Liyanage, Karin, and Beglinger, Christoph

Abstract

We measured pancreatic enzyme and bicarbonate responses to graded doses of intravenous secretin or cerulein alone or together in healthy human subjects. Bicarbonate responses were steady and well maintained during the last 3.5 h of the 4 h of infusions of secretagogues, giving evidence for a constant pancreatic flow rate. Potentiation (more-than-additive response) was observed between secretin and cerulein for bicarbonate secretion, but not for enzyme secretion. Secretin stimulated pancreatic enzyme secretion. The effect was most pronounced with amylase secretion and less prominent with lipase, trypsin, and chymotrypsin secretion. Changes in the proportion of enzymes were seen over time, with trypsin and chymotrypsin output declining towards the end of cerulein infusion. We conclude that in humans the effects of secretin on pancreatic enzyme secretion are complex and include timedependent changes in the enzyme mixture, but potentiation between secretin and cerulein does not occur for enzyme output.

Published

1990

33. Human secretin

Author

Christ, Andreas, Werth, Baseli, Hildebrand, Pius, Gyr, Klaus, Stalder, Georg A., and Beglinger, Christoph

Abstract

The action of synthetic human secretin, which differs in two amino acid residues from porcine secretin, was compared with synthetic porcine secretin in 6 healthy volunteers. Pancreatic secretion was assessed by a marker perfusion technique and plasma secretin concentrations were assessed by a specific radioimmunoassay. Increasing doses of either human or porcine secretin produced increasing bicarbonate output (p < 0.01), whereas trypsin and lipase were not stimulated over basal. The highest doses of secretin induced a significant increase in pancreatic amylase secretion. The two secretin preparations were found to be equipotent with respect to pancreatic secretion and plasma kinetics. Significant increases of plasma secretin were observed after a steak meal in 15 volunteers (p < 0.001). When human secretin was infused at postprandial concentrations, significant increases in pancreatic bicarbonate output were observed (p < 0.05). We conclude (a) that the substitution of two amino acids in human secretin does not affect biologic activity and plasma metabolism of the compound; (b) secretin does not stimulate pancreatic enzyme secretion at physiologic concentrations; and (c) the stimulatory effects of secretin on pancreatic amylase remain to be elucidated. The study suggests that human secretin is a true hormone.

Published

1988

34. Relevance of pH Dependency on in Vitro Release of Bromocriptine from a Modified-Release Formulation

Author

Drewe, Juergen, Keck, Martin, Guitard, P., Pellet, Andre, Johnston, Britton, and Beglinger, Christoph

Abstract

Since pH profiles of the dissolution rate are thought to be predictive for the in vivo performance of oral modified-release formulations with respect to bioavailability and dose dumping with food, these pH profiles were established for a new modified-release (MR) formulation for bromocriptine (Parlodel SRO). The results show a marked decrease of bromocriptine dissolution with increasing pH of the dissolution medium. However, when measured in native human duodenal juice (pH 8.1), dissolution was significantly higher than when measured in buffer of comparable pH. In a human pharmacokinetic study, this MR formulation showed good bioavailability and no food effect on the pharmacokinetic profile. Therefore, pH profiles alone seem to have only a limited predictive power for the in vivo performance of this MR formulation for bromocriptine.

Published

1991

35. Calcitonin gene-related peptides I and II and calcitonin: Distinct effects on gastric acid secretion in humans

Author

Beglinger, Christoph, Born, Walter, Hildebrand, Pius, Ensinck, John W., Burkhardt, Franziska, Fischer, Jan A., and Gyr, Klaus

Abstract

The human calcitonin gene-related peptides I and II (CGRP I and CGRP II) are two neuropeptides that have been recognized throughout the gastrointestinal system including the stomach. The present study was undertaken to compare in healthy volunteers the effects of intravenous infusions of CGRP I and CGRP II (79 pmol/kg · h) on pentagastrinstimulated acid secretion to those of calcitonin (88 pmol/kg · h). Calcitonin gene-related peptide I did not inhibit basal or pentagastrin-stimulated acid secretion. However, CGRP II and calcitonin inhibited pentagastrin-stimulated acid responses by 20% and 28%, respectively (p < 0.05 and p < 0.01), whereas basal acid output was only reduced with calcitonin (p < 0.05). These effects were recognized with low doses of pentagastrin, and absent with high doses suggesting competitive inhibition. Furthermore, step-doses of CGRP I and CGRP II (79–320 pmol/kg · h) were given intravenously on continuous pentagastrin stimulation and compared with calcitonin (88–352 pmol/kg h). Calcitonin gene-related peptide II and calcitonin induced a dose-dependent decrease of acid output, whereas CGRP I was ineffective. The inhibitory effects of CGRP II and calcitonin are not due to increased gastric alkaline secretion or to somatostatin release, as neither peptide stimulated gastric bicarbonate secretion or induced an increase in circulating somatostatin. In conclusion, CGRP II, unlike CGRP I, inhibits gastric acid secretion in humans. Inhibitory effects of CGRP II and of calcitonin were comparable. The results imply that CGRP I and II, at the level of the stomach, have distinct biological properties in humans.

Published

1988

36. Neurohormonal Control of Human Pancreatic Exocrine Secretion

Author

Adler, Guido, Nelson, Daniel K., Katschinski, Martin, and Beglinger, Christoph

Published

1995

37. Mechanisms of TerbutalineInduced Inhibition of Exocrine Pancreatic Secretion in Humans

Author

Meyer, Beat, Hildebrand, Pius, Meyer, Monald, Stalder, Georg A., and Beglinger, Christoph

Abstract

Terbutaline, a selective P,-adrenoreceptor agonist, has recently been advocated as a potential agent for treating patients with pancreatic fistulae. In the present study, we attempted to quantify the presumed effects of terbutaline on exocrine pancreatic secretion in humans and to characterize possible mechanisms of action. In six healthy volunteers, the pancreas was stimulated by infusion of graded doses of secretin (15.5-250 ng/kg/h) or by infusion of secretin (15.5 ng/kg/h) plus graded doses of caerulein (3.3-30 ng/ kgh). The experiments were repeated in each subject without and with administration of terbutaline. Pancreatic secretion was assessed by a marker perfusion technique and plasma somatostatin and pancreatic polypeptide (PP) levels by radioimmunoassay. Terbutaline had no significant effect on secretinstimulated pancreatic secretion, but significantly inhibited caerulein-stimulated pancreatic fluid secretion and trypsin output. Plasma somatostatin and PP levels were not affected by terbutaline. The inhibitory effect required the administration of pharmacologically large doses of terbutaline. We conclude that the weak inhibitory effect of terbutaline on exocrine pancreatic secretion is not mediated via somatostatin nor PP and that our data do not support a major role for P-adrenergic mechanism as regulator of pancreatic secretion.

Published

1988

38. Effect of Circulating Somatostatin on Exocrine Pancreatic Secretion in Conscious Dogs

Author

Köhler, Erich, Beglinger, Christoph, Ribes, Gérard, Grötzinger, Ulrich, Loubatiéres-Mariani, Marie-Madeleine, and Gyr, Klaus

Abstract

We determined the effects of exogenous somatostatin-14 (100 and 200 ng/kg/h; mimicking postprandial somatostatin concentrations) on pancreatic responses to a background infusion of secretion in combination with graded doses of CCK-8 in conscious dogs with chronic gastric and duodenal fistulas. The lower dose of somatostatin-14 (S-14), which produced S-14 plasma levels lower than measured after a meal, did not change basal or stimulated pancreatic secretion. The upper dose of S-14, which produced plasma S-14 concentrations slightly above the postprandial range, caused inhibition of pancreatic fluid and protein secretion to low doses of CCK-8 (p <0.05). The inhibition was surmountable with higher doses of CCK-8. We interpret these data as indicating that circulating S-14 is not an important hormonal regulator of exocrine pancreatic secretion.

Published

1986

39. Effect of a New Somatostatin Analogue on Pancreatic Function in Healthy Volunteers

Author

Kohler, Erich, Beglinger, Christoph, Dettwiler, Sabine, Whitehouse, Ian, and Gyr, Klaus

Abstract

We studied the effect of four graded doses of SMS 201-995, a synthetic octapeptide somatostatin analogue (27, 80, 240, and 720 ng/kg/h) on the basal and secretin-plus-cerulein-stimulated exocrine pancreatic function and pancreatic polypeptide (PP) release in five healthy volunteers. Duodenal fluid secretion and bicarbonate output under basal and stimulated conditions were not significantly affected by any dose of SMS. The basal and stimulated enzyme secretion were decreased in a non-dose-dependent manner by all SMS doses used in the study and showed a 75 inhibition of the secretin-plus-cerulein-stimulated trypsin and amylase output. The cerulein-stimulated PP release was significantly suppressed by all four SMS doses. SMS appears to be a strong inhibitor of pancreatic enzyme secretion, at the same time affecting the PP release.

Published

1986

40. Frontiers in Pancreatic Physiology

Author

Beglinger, Christoph and Gyr, Klaus

Published

1987

41. Performance of panel-based criteria to evaluate the appropriateness of colonoscopy: a prospective study

Author

Froehlich, Florian, Pache, Isabelle, Burnand, Bernard, Vader, John-Paul, Fried, Michael, Beglinger, Christoph, Stalder, Georg, Gyr, Klaus, Thorens, Joël, Schneider, Catherine, Kosecoff, Jacqueline, Kolodny, Marvin, DuBois, Robert W., Gonvers, Jean-Jacques, and Brook, Robert H.

Abstract

Background:Prospective data describing the appropriateness of use of colonoscopy based on detailed panel-based clinical criteria are not available. Methods:In a cohort of 553 consecutive patients referred for colonoscopy to two university-based Swiss outpatient clinics, the percentage of patients who underwent colonoscopy for appropriate, equivocal, and inappropriate indications and the relationship between appropriateness of use and the presence of relevant endoscopic lesions was prospectively assessed. This assessment was based on criteria of the American Society for Gastrointestinal Endoscopy and explicit American and Swiss criteria developed in 1994 by a formal panel process using the RAND/UCLA appropriateness method. Results:The procedures were rated appropriate or equivocal in 72.2% by criteria of the American Society for Gastrointestinal Endoscopy, in 68.5% by explicit American criteria, and in 74.4% by explicit Swiss criteria (not statistically significant, NS). Inappropriate use (overuse) of colonoscopy was found in 27.8%, 31.5%, and 25.6%, respectively (NS). The proportion of appropriate procedures was higher with increasing age. Almost all reasons for using colonoscopy could be assessed by the two explicit criteria sets, whereas 28.4% of reasons for using colonoscopy could not be evaluated by the criteria of the American Society for Gastrointestinal Endoscopy (p< 0.0001). The probability of finding a relevant endoscopic lesion was distinctly higher in the procedures rated appropriate or equivocal than in procedures judged inappropriate. Conclusions:The rate of inappropriate use of colonoscopy is substantial in Switzerland. Explicit criteria allow assessment of almost all indications encountered in clinical practice. In this study, all sets of appropriateness criteria significantly enhanced the probability of finding a relevant endoscopic lesion during colonoscopy. (Gastrointest Endosc 1998;48:128-36.)

Published

1998

42. To extract or not to extract in secretin radioimmunoassay?

Author

Fried, Michael, Schulthess, Cornelia, Beglinger, Christoph, Müller, Brigitte, and Gyr, Klaus

Abstract

Summary: The importance of an ethanol extraction procedure in the radioimmunoassay of plasma secretin was investigated. The extraction step led to a higher assay sensitivity of 0.35 fmol/ml, compared to 5.93 fmol/ml using unextracted samples. The rise of plasma secretin after infusion of a low dose of secretin (1 pmol·kg−1·h−1) in 10 healthy humans was only detected after sample extraction. Higher doses (3 and 9 pmol·kg−1·h−1) resulted in increments of plasma IRS (immunoreactive secretin), which could be recorded both with and without sample extraction. After a steak meal 7 of 10 subjects showed a significant increase of plasma secretin assaying extracted plasma samples. The secretin release occurred in spikes. The mean increase of plasma IRS in this group was 0.6 fmol/ml, the mean maximal secretin release above basal was 2.3 fmol/ml. Without sample extraction, plasma secretin was not significantly changed. We conclude that plasma samples should be extracted in order to detect physiological postprandial secretin release.

Published

1988

43. Dissociation of cholecystokinin and pancreaticobiliary response to intraduodenal bile acids and cholestyramine in humans

Author

Koop, Irmtraut, Dorn, Stefanie, Koop, Herbert, Witzleb, Stefan, Beglinger, Christoph, Schafmayer, Anton, and Arnold, Rudolf

Abstract

The role of intraduodenal bile acids in the regulation of cholecystokinin (CCK), pancreatic polypeptide (PP), and secretin as well as exocrine pancreatic and biliary secretion was investigated by means of a duodenal marker perfusion technique in volunteers. The following solutions were perfused: (1) liquid test meal, (2) test meal with 6 g cholestyramine, (3) test meal with 2 g chenodeoxycholic acid (CDC), (4) test meal with 6 g cholestyramine and 2 g CDC, (5) 6 g cholestyramine alone, and (6) 2 g CDC alone. The test meal caused an immediate increase in CCK and PP plasma levels, whereas secretin was not significantly altered. CCK release was further enhanced by addition of cholestyramine, whereas CDC inhibited release. The stimulatory effect of cholestyramine was abolished by CDC. CDC alone and in combination with the test meal stimulated secretin release. The response of PP to the test meal was not altered by addition of either compound. Cholestyramine and CDC alone caused only a very small increase in CCK levels, whereas PP was stimulated to nearly postprandial values. Meal-stimulated pancreatic and biliary secretion was significantly enhanced by cholestyramine, CDC, and the combination of both. CDC and cholestyramine alone each stimulated enzyme and bile secretion to a greater extent than the test meal. We conclude that intraduodenal bile salts are a modulator of postprandial CCK release. Changes in exocrine pancreatic and biliary and PP secretion do not necessarily parallel CCK concentrations, suggesting that different mediators are involved in the observed bile acid-induced changes in humans.

Published

1991

44. Pancreatic bicarbonate response to intraduodenal tryptophan in dogs

Author

Niebergall-Roth, Elke, Teyssen, Stephan, Hartel, Mark, Beglinger, Christoph, Riepl, Rudolf L., and Singer, Manfred V.

Abstract

Conclusions: In dogsActivation of cholecystokinin-receptors is needed for an adequate pancreatic bicarbonate response to secretin;Cholinergic nerve fibers ending on M1-receptors are probably of little or no importance for the bicarbonate response to secretin in the given dose;The bicarbonate response to tryptophan, given with a secretin background, is controlled by cholinergic M1-fibers and by cholecystokinin;M1-fibers mainly mediate the bicarbonate response to low loads of tryptophan, whereas cholecystokinin controls the response to low and high loads of tryptophan; andBoth mediators interact in a synergistic manner. Methods: In six conscious dogs with chronic gastric and duodenal fistulas, we compared the action of the M1-receptor antagonisttelenzepine (20.25–81.0 nmol/kg/h), the cholecystokinin-receptor antagonist L-364,718 (0.025–0.1 mg/kg/h), and combinations of both on the pancreatic bicarbonate response to graded loads of intraduodenal tryptophan (0.37–10.0 mmol/h), given against a background of secretin (20.5 pmol/kg/h). Results: Secretin significantly (p&lt;0.05) stimulated the pancreatic bicarbonate output above basal levels. All doses of L-374,718, but not telenzepine, significantly decreased the bicarbonate response to secretin by up to 64%. Additional administration of telenzepine together with L-364,718 had no further inhibitory effect on the secretinstimulated bicarbonate output as compared to L-364,718 given alone. All loads of tryptophan significantly increased the bicarbonate output over that seen with secretin alone (= incremental bicarbonate response to tryptophan). Telenzepine significantly decreased the incremental bicarbonate response to the two lower loads (0.37–1.1 mmol/h) of tryptophan (by 82–124%); L-364,718 decreased the incremental bicarbonate response to all loads of tryptophan (by 50–118%). The incremental bicarbonate output, as well as the 180-min integrated bicarbonate response to all loads of tryptophan, were abolished by all combinations of both antagonists.

Published

1998

45. Effect of loxiglumide, a cholecystokinin antagonist, on pancreatic polypeptide release in humans

Author

Meier, Rémy, Hildebrand, Pius, Thumshirn, Myriam, Albrecht, Cornelia, Studer, Bernhard, Gyr, Klaus, and Beglinger, Christoph

Abstract

The purpose of this study was to determine the role of cholecystokinin in the regulation of postprandial pancreatic polypeptide secretion in humans. The pancreatic polypeptide responses to modified sham feeding and gastric instillation of a test meal were first compared with the response to oral ingestion of the same meal. The experiments were repeated under cholinergic (atropine) and cholecystokinin (loxiglumide) blockade. Atropine completely abolished the pancreatic polypeptide response to sham feeding and caused significant reductions after gastric and oral food intake. Loxiglumide, on the other hand, significantly reduced pancreatic polypeptide release to oral food (51% inhibition) without affecting the response to sham feeding. In separate experiments using a duodenal perfusion system, the effects of atropine and loxiglumide on intestinal phase-stimulated pancreatic polypeptide release were examined, and both cholinergic and cholecystokinin blockade induced complete suppression. It was concluded (a) that cholecystokinin is involved in postprandial pancreatic polypeptide response, especially during the intestinal phase stimulation, and (b) that the cholinergic system is crucial and superimposed on cholecystokinin in stimulating pancreatic polypeptide release.

Published

1990

46. Role of circulating cholecystokinin in control of fat-induced inhibition of food intake in humans

Author

Drewe, Jürgen, Gadient, Andreas, Rovati, Lucio C., and Beglinger, Christoph

Abstract

Cholecystokinin (CCK) has been proposed to serve as a satiety signal in animals and humans. To further explore the role of CCK in humans, the effect on satiety and eating behavior of a specific CCK-receptor antagonist, loxiglumide, that preferentially inhibits peripheral (CCK-A) receptors was investigated. In a randomized, blind, four-period latin square design, 10 subjects received intravenous saline (placebo) or loxiglumide (10 mg/kg per hour) with concomitant intrajejunal perfusions of isotonic saline or fat (containing 50% corn oil and 3% albumin). Food intake and plasma CCK concentrations were assessed, and subjects scored their feelings of hunger and fullness in paired experiments. In placebo-treated subjects, the duration of the meal was shorter during fat perfusion (30 ± 2 minutes vs. 35 ± 2 minutes; P< 0.01; mean ± SEM). The amount of food intake was reduced (361 ± 31 g vs, 454 ± 35 g; P< 0.05), and fluid ingestion was inhibited (490 ± 31 mL vs. 625 ± 38 mL; P< 0.01). Loxiglumide did not affect any parameter and did not change the pattern of responses. In loxiglumide-treated subjects there was a 4–5-fold elevation in plasma CCK levels. These results confirm that jejunal infusion of lipid reduces the size of the meal and stimulates early satiety. The data imply that these effects are not mediated through peripheral endogenous CCK under these conditions.

Published

1992

47. A physiological role for cholecystokinin as a regulator of gastrin secretion

Author

Beglinger, Christoph, Hildebrand, Pius, Meier, Rémy, Bauerfeind, Peter, Hasslocher, Heike, Urscheler, Niklaus, Delco, Fabiola, Eberle, Alex, and Gyr, Klaus

Abstract

To explore the role of cholecystokinin (CCK) in regulating gastrin secretion in humans, the effect of a CCK antagonist (loxiglumide) on meal-stimulated hormone responses was investigated. Subjects received 500 mL of a liquid test meal in the presence and absence of loxiglumide (22 μmol · kg−1· h−1). In the control experiments, both plasma gastrin and CCK levels increased postprandially. In loxiglumide-treated subjects there was a marked elevation in gastrin (area under the curve, 11,042 ± 1493/120 min vs. 2156 ± 281 pg/120 min) and CCK levels compared with the control experiment. These observations were confirmed in experiments with modified sham feeding and gastrin-releasing peptide stimulation in which loxiglumide pretreatment also caused a significant increase in gastrin release compared with saline (P< 0.05). Further studies with intravenous infusion of gastrin, CCK-8, and CCK-33 with and without loxiglumide showed that the increases in CCK and gastrin during loxiglumide application cannot be explained by alterations in clearance rates. The findings of this study show that postprandial gastrin secretion is influenced by CCK and support the concept of a negative feedback control of gastrin secretion by CCK.

Published

1992

48. Cephalic stimulation of gastrointestinal secretory and motor responses in humans

Author

Katschinski, Martin, Dahmen, Gudrun, Reinshagen, Max, Beglinger, Christoph, Koop, Herbert, Nustede, Rainer, and Adler, Guido

Abstract

The present study was designed (a) to investigate the cephalic phase of gastropancreatic secretion, antroduodenal motility, and regulatory peptide release in six healthy young men and (b) to assess its regulation by the cholinergic system and endogenous cholecystokinin. Sham feeding performed for 15 minutes induced a concurrent stimulation of gastropancreatic secretion, antroduodenal motility, and pancreatic polypeptide release that lasted for 30 minutes. Reappearance of interdigestive phases III was retarded in the post-sham-fed state. Atropine abolished secretory, motor, and pancreatic polypeptide responses to sham feeding and enhanced gastrin release. The cholecystokinin receptor antagonist loxiglumide did not attenuate pancreatic enzyme response but diminished antral motor response by 72% (P< 0.05) and release of pancreatic polypeptide by 91% (P< 0.05); it enhanced gastrin release and abolished retardation of reappearance of phase III with sham feeding. It is concluded that (a) there is a distinct cephalic phase of gastropancreatic secretion, antroduodenal motility, and pancreatic polypeptide release in humans that is primarily under cholinergic control and that (b) endogenous cholecystokinin is involved in antral motor, gastrin, and pancreatic polypeptide responses to sham feeding.

Published

1992

49. Evidence for hormonal inhibition of exocrine pancreatic function by somatostatin 28 in humans

Author

Hildebrand, Pius, Ensinck, John W., Gyr, Klaus, Mossi, Sandro, Leuppi, Jörg, Eggenberger, Christoph, and Beglinger, Christoph

Abstract

Somatostatin 28 (S-28), originating in gastrointestinal cells, is secreted into the circulation and increases in humans after ingestion of a mixed meal. To evaluate the possibility that the increased levels of S-28 post cibum might modulate the release of enzymes and bicarbonate from the exocrine pancreas, S-28 was infused intravenously into healthy volunteers to levels seen after food intake. During S-28 infusion, the output of lipase, trypsin, amylase, and bicarbonate stimulated by either exogenous cholecystokinin octapeptide or endogenous signals from intraduodenal administration of tryptophan or a mixture of amino acids was significantly reduced. It is concluded that S-28 released from the gut during food intake modulates pancreatic exocrine function in humans.

Published

1992

50. Diagnostic procedures in esophageal disease

Author

Degen, L. and Beglinger, Christoph

Abstract

Auch für Erkrankungen des Ösophagus gilt, dass das klinische Bild mit seinen Leitsymptomen das diagnostische Vorgehen bestimmt. Im vorliegenden Artikel werden die wichtigsten diagnostischen Verfahren vorgestellt und gewertet. Dabei steht die flexible Endoskopie im Vordergrund, während bildgebende radiologische Verfahren gezielt eingesetzt werden. Schließlich werden die wichtigsten funktionellen Verfahren vorgestellt und gewichtet.

Published

2001