P. L.M. Jansen
University of Amsterdam
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Featured researches published by P. L.M. Jansen.
Inflammatory Bowel Diseases | 2005
Laurens A van der Waaij; Hermie J. M. Harmsen; M Madjipour; Franciscus Kroese; M Zwiers; H M van Dullemen; N. K. H. de Boer; Gjalt W. Welling; P. L.M. Jansen
Background: The commensal intestinal microflora has important metabolic and perhaps also immune modulatory functions. Evidence has accumulated that the microflora plays a role in the pathogenesis of inflammatory bowel disease. Therefore, there is a growing interest in the intestinal microflora and its interaction with the host. Presumably, this interaction takes place at the mucus layer. In this study, we investigated the microflora that is present at the mucus layer and addressed the following questions. Does a specific mucus‐adherent microflora exist? Is there direct contact between commensal bacteria and epithelial cells? Methods: Snap‐frozen biopsies were taken of 5 colon regions and of the terminal ileum in 9 subjects with a normal colon. Fecal samples were also collected. Bacteria were detected in cryosections with fluorescent in situ hybridization (FISH) with 16S ribosomal (r)RNA‐targeted probes for all bacteria and specific probes for the major representatives of anaerobic microflora (bifidobacteria, Bacteroides, clostridia, atopobia) and aerobic microflora (Enterobacteriaceae, enterococci, streptococci, lactobacilli). Results: With this sensitive technique, bacteria were only observed at the luminal side of the intestinal mucus layer. Very few microcolonies were present at the mucus layer, and the composition of the bacterial microflora present in the feces was similar to that at the mucus layer of the terminal ileum and colon regions. Conclusions: We did not observe direct contact between bacteria and epithelial cells. The equal distribution of bacterial species suggests that intestinal commensal bacteria live in suspension in the lumen and that there is no specific mucus‐adherent microflora.
Alimentary Pharmacology & Therapeutics | 2004
Rinse K. Weersma; Frans Peters; Liekele E. Oostenbrug; A. P. van den Berg; M. van Haastert; Rutger J. Ploeg; Posthumus; J. J. Homan van der Heide; P. L.M. Jansen; H.M. van Dullemen
Background : Azathioprine is widely used in Crohns disease. A major drawback is the occurrence of side‐effects, especially acute pancreatitis. Acute pancreatitis is rarely seen when azathioprine is used for other diseases than Crohns disease.
European Journal of Gastroenterology & Hepatology | 1999
Vincent W. Bloks; H. van Goor; J. Bailer; Rick Havinga; Han Moshage; A. van Tol; Henkjan J. Verkade; P. L.M. Jansen; F Kuipers
Erythropoietic protoporphyria (EPP) is an inherited disorder of heme synthesis caused by deficiency of the mitochondrial enzyme ferrochelatase. EPP in humans is associated with liver disease, hypertriglyceridemia, and a low level of high density lipoprotein (HDL) cholesterol. To explore consequences of ferrochelatase deficiency in lipid metabolism, we have analyzed hepatic lipid content and plasma lipoprotein levels in chow-fed BALB/c mice homozygous ( fch/fch) or heterozygous ( fch/1) for a point mutation in the ferrochelatase gene and in wild-type controls (1/1). Livers of fch/fch mice show bile duct proliferation and biliary fibrosis, but bile formation is not impaired. The free cholesterol content of fch/fch livers is significantly increased when compared with fch/1 and 1/1 livers. Plasma cholesterol in fch/fch mice (9.9 +/- 6.4 mM) is elevated when compared with fch/1 and 1/1 mice (2.9 +/- 0.2 and 2.5 +/- 0.3 mM, respectively), because of an increased cholesterol content in the very low density lipoprotein-sized fractions, whereas HDL cholesterol is reduced. The ratio of cholesteryl ester to free cholesterol is 4.3 +/- 0.6, 3.3 +/- 0.3, and 0.3 +/- 0.1 in the plasma of 1/1, fch/1, and fch/fch mice, respectively. The latter is not due to reduced lecithin:cholesterol acyltransferase activity in plasma of fch/fch mice but to the presence of lipoprotein-X (Lp-X), a particle composed of bile-type lipids usually seen only in cholestatic conditions. Expression of mdr2, essential for biliary phospholipid/cholesterol secretion, is increased in fch/fch livers. In spite of this, biliary phospholipid/cholesterol secretion is reduced relative to that of bile salts. It is postulated that an inability of bile salts to stimulate lipid secretion adequately leads to formation of Lp-X in this noncholestatic condition. Distinct atherosclerotic lesions were found in aged fch/fch mice.Thus, ferrochelatase deficiency in mice leads to liver disease associated with altered hepatic lipid metabolism, a characteristic hyperlipidemia, and development of atherosclerosis.-Bloks, V. W., T. Plösch, H. van Goor, H. Roelofsen, J. Baller, R. Havinga, H. J. Verkade, A. van Tol, P. L. M. Jansen, and F. Kuipers. Hyperlipidemia and atherosclerosis associated with liver disease in ferrochelatase-deficient mice. J. Lipid Res. 2001. 42: 41;-50.
Digestive and Liver Disease | 2006
Le Oostenbrug; Ilja M. Nolte; E Oosterom; G. van der Steege; G.J. te Meerman; H.M. van Dullemen; J.P.H. Drenth; D.J. de Jong; K. van der Linde; P. L.M. Jansen; Jan H. Kleibeuker
Transplantation Proceedings | 2001
A. P. van den Berg; Eb Haagsma; A.S.H. (Annette) Gouw; Maarten J. H. Slooff; P. L.M. Jansen
Journal of Hepatology | 2008
Db De Koning; L. van Keimpema; R. H. M. te Morschel; A. P. van den Berg; P. L.M. Jansen; R.A. de Man; Frederik Nevens; B. van Hoek; J.P.H. Drenth
Proceeding: Dutch Transplant Society | 2001
Gerda Drent; Sabina De Geest; Philip Moons; Eb Haagsma; Em ten Vergert; Ivo Abraham; P. L.M. Jansen
Hepatology | 2001
Mh Shoemaker; M Homan; A Beuving; H. van Goor; Klaas Poelstra; P. L.M. Jansen; Han Moshage
Archive | 2000
Charles M. A. Bijleveld; H. (Harry) van Goor; P. L.M. Jansen; F Kuipers; A.J. (Han) Moshage; Michael Müller; F. Stellaard; Pieter J. J. Sauer; Henkjan J. Verkade
Archive | 2000
Charles M. A. Bijleveld; H. (Harry) van Goor; P. L.M. Jansen; F Kuipers; A.J. (Han) Moshage; Michael Müller; F. Stellaard; Pieter J. J. Sauer; Henkjan J. Verkade